Most Favored Nation (MFN) Model, 76180-76259 [2020-26037]
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Federal Register / Vol. 85, No. 229 / Friday, November 27, 2020 / Rules and Regulations
DEPARTMENT OF HEALTH AND
HUMAN SERVICES
Centers for Medicare & Medicaid
Services
42 CFR Part 513
[CMS–5528–IFC]
RIN 0938–AT91
Most Favored Nation (MFN) Model
Centers for Medicare &
Medicaid Services (CMS), HHS.
ACTION: Interim final rule with comment
period.
AGENCY:
This interim final rule with
comment period (IFC) implements the
Most Favored Nation (MFN) Model, a
new Medicare payment model under
section 1115A of the Social Security Act
(the Act). The MFN Model will test
whether more closely aligning payment
for Medicare Part B drugs and
biologicals (hereafter, referred to as
‘‘drugs’’) with international prices and
removing incentives to use higher-cost
drugs can control unsustainable growth
in Medicare Part B spending without
adversely affecting quality of care for
beneficiaries.
SUMMARY:
Effective date: These regulations
are effective on November 27, 2020.
Comment date: To be assured
consideration, comments must be
received at one of the addresses
provided below, no later than 5 p.m. on
January 26, 2021.
ADDRESSES: In commenting, please refer
to file code CMS–5528–IFC. Because of
staff and resource limitations, we cannot
accept comments by facsimile (FAX)
transmission.
Comments, including mass comment
submissions, must be submitted in one
of the following three ways (please
choose only one of the ways listed):
1. Electronically. You may submit
electronic comments on this regulation
to https://www.regulations.gov. Follow
the ‘‘Submit a comment’’ instructions.
2. By regular mail. You may mail
written comments to the following
address ONLY: Centers for Medicare &
Medicaid Services, Department of
Health and Human Services, Attention:
CMS–5528–IFC, P.O. Box 8013,
Baltimore, MD 21244–8013.
Please allow sufficient time for mailed
comments to be received before the
close of the comment period.
3. By express or overnight mail. You
may send written comments to the
following address ONLY: Centers for
Medicare & Medicaid Services,
Department of Health and Human
Services, Attention: CMS–5528–IFC,
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DATES:
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Boulevard, Baltimore, MD 21244–1850.
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SUPPLEMENTARY INFORMATION section.
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SUPPLEMENTARY INFORMATION:
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instructions on that website to view
public comments.
I. Executive Summary
A. Purpose
High drug prices are impacting the
wallets of Medicare beneficiaries,
especially during the Coronavirus
disease 2019 Public Health Emergency
(PHE). Increases in drug prices are
accelerating at a rate that significantly
outpaces the growth in spending on
other Medicare Part B services, and
prices in the United States (U.S.) for
most Medicare Part B drugs with the
highest Medicare spending far exceed
prices in other countries. Specifically,
drugs have consistently been a major
contributor to the overall Medicare Part
B spending trend. Medicare Part B FeeFor-Service (FFS) spending for
separately payable physicianadministered drugs and drugs furnished
in a hospital outpatient department
represented about 11 percent of
Medicare Part B FFS benefit spending in
2015, but accounted for about 37
percent of the change in Medicare Part
B FFS benefit spending from 2015 to
2020, and spending on these Medicare
Part B FFS drugs increased to represent
roughly 14 percent of Medicare Part B
FFS benefit spending in 2019.1 In
addition to the continued growth in
spending, the U.S. already pays almost
twice as much on average as other
developed countries pay. In one
analysis of 27 drugs, acquisition costs in
the U.S. were 1.8 times higher than in
comparator countries.2 A more recent
1 2020 Annual Report of the Boards of Trustees
of the Federal Hospital Insurance and Federal
Supplementary Medical Insurance Trust Funds.
Accessed via: https://www.cms.gov/files/document/
2020-medicare-trustees-report.pdf.
2 ‘‘Comparison of U.S. and International Prices for
Top Medicare Part B Drugs by Total Expenditures’’
accessed via https://aspe.hhs.gov/pdf-report/
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analysis using the prescription drugs
and countries in the MFN Model
suggests Medicare Part B paid at least
2.05 times as much as other higherincome countries in 2018.3 The Centers
for Medicare & Medicaid Services’
(CMS) Center for Medicare and
Medicaid Innovation (Innovation
Center) is taking action on President
Trump’s goal to lower drug costs and
seeking to realign financial incentives
by implementing the Most Favored
Nation (MFN) Model as described in
this IFC.
Medicare pays substantially more
than other countries for many of the
highest-cost Medicare Part B drugs that
beneficiaries receive in an outpatient
setting for which Medicare Part B allows
separate payment.4 In many instances,
Medicare pays more than twice as much
for certain drugs as other countries
do.5, 6 This is because Medicare
generally establishes the payment for
separately payable Medicare Part B
drugs using the methodology in section
1847A of the Act. In most cases, this
means payment is based on the Average
Sales Price (ASP) plus a statutorily
mandated 6 percent add-on. Under this
methodology, the Medicare program
does not get the benefit of the
substantial discounts provided in other
comparison-us-and-international-prices-topmedicare-part-b-drugs-total-expenditures.
3El-Kilani Z, Finegold K, Mulcahy A, and
Bosworth A. Medicare FFS Part B and International
Drug Prices: A Comparison of the Top 50 Drugs.
Washington, DC: Office of the Assistant Secretary
for Planning and Evaluation, U.S. Department of
Health and Human Services. November 20, 2020
(https://aspe.hhs.gov/pdf-report/medicare-ffs-partb-and-international-drug-prices).
4 ‘‘Comparison of U.S. and International Prices for
Top Medicare Part B Drugs by Total Expenditures’’
accessed via https://aspe.hhs.gov/pdf-report/
comparison-us-and-international-prices-topmedicare-part-b-drugs-total-expenditures; El-Kilani
Z, Finegold K, Mulcahy A, and Bosworth A.
Medicare FFS Part B and International Drug Prices:
A Comparison of the Top 50 Drugs. Washington,
DC: Office of the Assistant Secretary for Planning
and Evaluation, U.S. Department of Health and
Human Services. November 20, 2020 (https://
aspe.hhs.gov/pdf-report/medicare-ffs-part-b-andinternational-drug-prices).
5 ‘‘Comparison of U.S. and International Prices for
Top Medicare Part B Drugs by Total Expenditures’’
accessed via https://aspe.hhs.gov/pdf-report/
comparison-us-and-international-prices-topmedicare-part-b-drugs-total-expenditures; El-Kilani
Z, Finegold K, Mulcahy A, Bosworth A. Medicare
FFS Part B and International Drug Prices: A
Comparison of the Top 50 Drugs. Washington, DC:
Office of the Assistant Secretary for Planning and
Evaluation, U.S. Department of Health and Human
Services. November 20, 2020 (https://aspe.hhs.gov/
pdf-report/medicare-ffs-part-b-and-internationaldrug-prices).
6 Individual countries differ in the regulatory
processes and standards governing approval of
drugs and biologicals. Use of international drug
prices in the MFN Model should not be interpreted
to connote FDA approval or to otherwise describe
any scientific or regulatory relationship between
U.S.-approved and non-U.S.-approved products.
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countries, because ASP is calculated
using only the prices that manufacturers
charge to certain U.S.-based purchasers.
ASP-based payments may encourage the
use of more expensive drugs because the
dollar amount of the 6 percent add-on
portion is larger for drugs with higher
ASPs.7 As MedPAC noted in its June
2017 Report, ‘‘Although, in some cases,
drugs with patent protection may face
competition from other brand drugs in
the same therapeutic class, price
competition between such products may
be limited because the [Medicare] Part
B drug payment system is not structured
to facilitate competition among brand
products with similar health effects.’’ 8
Thus, the ASP-based payment approach
currently used in Medicare Part B may
not promote price competition or
provide sufficient incentive to minimize
avoidable costs.
The MFN Model aims to take a global
approach to calculating Medicare Part B
drug payment amounts, by testing a new
payment methodology that takes into
account the discounts that other
countries enjoy, and pays providers and
suppliers with a fixed add-on amount
that does not reward the use of highercost drugs. We expect that this model
will reduce Medicare program
expenditures while preserving or
enhancing quality of care furnished to
Medicare beneficiaries, and will lower
beneficiary cost-sharing through lower
drug payment amounts. The MFN
Model will be tested in all states and
U.S. territories by the CMS Innovation
Center for 7 performance years, from
January 1, 2021 to December 30, 2027.
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B. Summary of the Major Provisions
The MFN Model will focus on a select
cohort of separately payable Medicare
Part B drugs. This cohort will initially
include 50 single source drugs and
biologicals (including biosimilar
biological products) that encompass a
high percentage of Medicare Part B drug
spending. The MFN Model will require
mandatory participation. Participants in
the MFN Model will include all
providers and suppliers that participate
in the Medicare program and submit a
separately payable claim for an MFN
Model drug with limited exceptions,
such as providers and suppliers that are
paid for separately payable Medicare
Part B drugs based on reasonable costs.
The vast majority of providers and
7 MedPAC, June 2017, ‘‘Medicare Part B Drug
Payment Policy Issues,’’ accessed via https://
medpac.gov/docs/default-source/reports/jun17_
ch2.pdf.
8 MedPAC, June 2017, ‘‘Medicare Part B Drug
Payment Policy Issues,’’ accessed via: https://
medpac.gov/docs/default-source/reports/jun17_
ch2.pdf.
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suppliers that furnish separately
payable Medicare Part B drugs are
physicians and non-physician
practitioners, supplier groups (such as a
group of physicians or other
practitioners), hospital outpatient
departments (HOPDs), including on- or
off-campus provider-based departments
(PBDs), whether paid under the
outpatient prospective payment system
(OPPS) or the physician fee schedule
(PFS), and ambulatory surgical centers
(ASCs) paid under the ASC Payment
System. Claims from these providers
and suppliers will encompass
approximately 88 percent of the annual
Medicare Part B spending on the drugs
we selected for inclusion in the MFN
Model beginning in performance year 1.
Other types of providers and suppliers
that furnish separately payable selected
drugs will also be required to participate
in the MFN Model, but they may not
often furnish the selected drugs or may
not typically receive separate payment
for Medicare Part B drugs.
The MFN Model will—
• Calculate the payment amount for
MFN Model drugs based on a price that
reflects the lowest per capita Gross
Domestic Product-adjusted (GDPadjusted) price of any non-U.S. member
country of the Organisation for
Economic Co-operation and
Development (OECD) with a GDP per
capita 9 that is at least sixty percent of
the U.S. GDP per capita, based on
available data;
• Make an alternative add-on
payment for MFN Model drugs that will
remove or reduce the financial incentive
to prescribe higher-cost drugs more
frequently; and
• Reduce beneficiary cost sharing on
MFN Model drugs.
C. Summary of Costs and Benefits
We believe the MFN Model will
substantially lower drug payment
amounts for the most costly Medicare
Part B drugs, thereby lowering program
expenditures and out-of-pocket costs for
beneficiaries. As discussed in more
detail in section VI. of this IFC, we
estimate that the MFN Model will result
in substantial overall Medicare savings
during the 7-year model performance
period (that is, 28 calendar quarters). In
the CMS Office of the Actuary (OACT)
estimate, OACT estimates savings of
roughly $64.4 billion in Medicare FFS
benefits, $49.6 billion in Medicare
Advantage (MA) payments, and $9.9
9 For the purposes of this IFC, GDP means GDP
based on purchasing power parity (PPP), rather than
nominal GDP. A nation’s GDP at purchasing power
parity (PPP) exchange rate is the sum value of all
goods and services produced in the country valued
at prices prevailing in the U. S.
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76181
billion in Medicaid 10 spending ($5.7
billion in federal payments and $4.3
billion in state payments). Overall,
OACT estimates that the MFN Model
will result in savings of $85.5 billion,
net of the associated change in the Part
B premium, in Medicare Part B
spending. In addition, OACT estimates
that all beneficiaries will save a total of
$28.5 billion from a reduction in the
Medicare Part B premium as a result of
the MFN Model, and will also see their
coinsurance reduced. In the HHS Office
of the Assistant Secretary for Planning
and Evaluation (ASPE) estimate, ASPE
estimates roughly a net reduction of
$87.8 billion in spending on MFN
Model drugs by the federal government,
state governments, and beneficiaries
over the 7 years of the model. We note
that there is much uncertainty around
the assumptions for both the OACT and
ASPE estimates and refer readers to
section VI. of this IFC for a more
complete discussion of potential
impacts of the MFN Model.
II. Background on Need for Regulatory
Action
On May 11, 2018, President Trump
released his Blueprint to Lower Drug
Prices and Reduce Out-of-Pocket
Costs,11 which outlined the steps his
administration is taking to combat high
drug prices, end foreign freeloading, and
spur biomedical innovation.12
On October 25, 2018, CMS released an
advance notice of proposed rulemaking
(ANPRM) (83 FR 54546) 13 (hereafter
called the October 2018 ANPRM)
describing a potential model, referred to
in the October 2018 ANPRM as the
International Pricing Index Model (IPI),
that would test whether changing the
payment amount for selected Medicare
Part B drugs would reduce Medicare
expenditures and preserve or enhance
quality of care. In the October 2018
ANPRM, we sought comment on a
model test that would—
• Calculate the Medicare payment
amount for selected Medicare Part B
10 Medicaid savings estimates do not include
impacts of changes in Average Manufacturer Price
(AMP) and Best Price on manufacturer rebates
under the Medicaid Drug Rebate Program.
11 American Patients First: The Trump
Administration Blueprint to Lower Drug Prices and
Reduce Out-of-Pocket Costs, Available at: https://
www.hhs.gov/sites/default/files/
AmericanPatientsFirst.pdf?language=es.
12 ‘‘President Donald J. Trump’s Blueprint To
Lower Drug Prices,’’ accessed via: https://
www.whitehouse.gov/briefings-statements/
president-donald-j-trumps-blueprint-lower-drugprices/.
13 International Pricing Index Model for Medicare
Part B Drugs; Medicare Program, 83 Fed. Reg (210)
54246 (Oct 30, 2018) available at: https://
www.govinfo.gov/content/pkg/FR-2018-10-30/pdf/
2018-23688.pdf.
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drugs to be phased down to more
closely align with international prices;
• Allow private-sector vendors to
negotiate prices for drugs, take title to
drugs, and compete for physician and
hospital business;
• Increase the drug add-on payment
to reflect 6 percent of historical drug
costs; and
• Pay physicians and hospitals the
add-on based on a set payment amount
structure.
We considered the comments that we
received in response to the October
2018 ANPRM in developing the MFN
Model described in this IFC. In addition
to considering these comments, we
considered feedback and suggestions
from a broad set of stakeholders
gathered through comments on the
President’s Blueprint and through
numerous meetings with stakeholders.
President Trump discussed an
Executive Order (E.O.) regarding an
MFN payment model for Medicare Part
B drugs on July 24, 2020, and
subsequently published a superseding
Executive Order on Lowering Drug
Prices by Putting America First on
September 13, 2020.14 In response to the
September 13, 2020 Executive Order, we
will implement the MFN Model
described in this IFC.
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A. Medicare Part B Drug Benefit and
ASP Payment Methodology
Medicare Part B includes a limited
drug benefit for drugs and biologicals
described in section 1861(t) of the Act.
The majority of drugs paid under
Medicare Part B generally fall into three
categories: Drugs furnished incident to a
physician’s service in the physician
office, HOPD, or other outpatient
setting; drugs administered via a
covered item of durable medical
equipment (DME); and other categories
of drugs specified by statute (generally
in section 1861(s)(2) of the Act).
Many drugs covered under Medicare
Part B are administered via injection or
infusion in a physician’s office, an
HOPD, and certain other outpatient
settings, such as ASCs, and, when
Medicare allows separate payment for
these drugs, the payment limit is
typically based on the methodology
described in section 1847A of the Act.
The payment amount for these drugs
does not include payment for
administering the drug to a beneficiary;
payment for drug administration
services is made in accordance with the
applicable payment policy for the
setting in which the drug was furnished,
14 Executive Order 13948, https://
www.govinfo.gov/content/pkg/FR-2020-09-23/pdf/
2020-21129.pdf.
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such as the Physician Fee Schedule
(PFS) (https://www.cms.gov/Medicare/
Medicare-Fee-for-Service-Payment/
PhysicianFeeSched/), the
Hospital Outpatient Prospective
Payment System (OPPS) (https://
www.cms.gov/Medicare/Medicare-Feefor-Service-Payment/
HospitalOutpatientPPS/), or
the Ambulatory Surgical Center
Payment System (https://www.cms.gov/
Medicare/Medicare-Fee-for-ServicePayment/ASCPayment/).
Medicare Part B also allows separate
payment for drugs in less common
situations such as osteoporosis drugs
furnished by a home health agency, and
when a beneficiary does not have
benefits available under the Part A
program.
The payment methodology for drugs
described in section 1847A of the Act is
generally based on the volume-weighted
ASP for all National Drug Codes (NDCs)
that are assigned to a Healthcare
Common Procedure Coding System
(HCPCS) code for the drug plus a 6
percent add-on. The volume-weighted
ASP for a HCPCS code is calculated
quarterly using manufacturer-submitted
data 15 on sales to all purchasers (with
limited exceptions as articulated in
section 1847A(c)(2) of the Act, such as
sales at nominal charge and sales
exempt from Medicaid best price 16)
with manufacturers’ rebates, discounts,
and price concessions included in the
ASP calculation (that is, the sales price
is net of these rebates, discounts, and
price concessions). The ASP+6 percent
payment amount that Medicare pays for
an individual Medicare Part B drug
claim generally does not vary based on
the exact price an individual provider or
supplier pays to acquire the drug. In the
case of multiple source drugs, the price
of a brand name drug and its generic
equivalent(s) included in the same
billing code are averaged together to
determine the payment allowance.17 As
noted earlier, this payment methodology
may create an incentive for the use of
more expensive drugs, but, as noted in
the MedPAC report (and by sources
cited in the report; pages 68 and 79), an
add-on may be needed to account for
handling and overhead costs and
additional mark-up in distribution
15 OMB
16 Best
Control Number 0938–0921.
price is defined in section 1927(c)(1)(C) of
the Act.
17 Under section 3139 of the Affordable Care Act
(Pub. L. 111–148) the add-on amount for a
biosimilar is based on the ASP of the reference
product. Biosimilars are not grouped together with
one another or the reference product for payment
purposes.
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channels that are not captured in the
manufacturer-reported ASP.
Currently, under Medicare Part B,
beneficiaries’ cost-sharing 18 is generally
20 percent of the Medicare-allowed
amount. The term ‘‘Medicare-allowed
amount’’ means the maximum amount
that a provider or supplier will be paid
for a covered health care service or drug.
However, for items and services paid
under the OPPS, beneficiaries are only
financially responsible for a copayment
amount up to the amount of the
inpatient hospital deductible.19
Medicare pays for the remaining portion
of the Medicare-allowed amount.20
B. Medicare and Beneficiary Spending
Medicare Part B spending for
separately payable physicianadministered drugs and drugs furnished
in hospital outpatient departments
represented about 11 percent of
Medicare Part B FFS spending in 2015
but increased to represent roughly 14
percent of Medicare Part B FFS
spending in 2019; spending on these
Medicare Part B separately payable
drugs accounted for about 37 percent of
the change in Medicare Part B FFS
spending from 2015 to 2019.
Furthermore, Medicare Part B FFS
spending per capita for separately
payable drugs has increased at an
average annual rate of 11.5 percent over
this same period while Medicare Part B
FFS spending per capita has increased
by 3.8 percent. From 2015 to 2019,
Medicare Part B spending for separately
payable drugs increased from $19.4
billion to $29.8 billion (a nearly 55percent increase) with per capita
spending increasing from $583 to $900.
This increase in Medicare Part B FFS
spending for separately payable drugs
during this period reflects increases in
the prices of drugs, introduction of new
drugs, changes in utilization of these
drugs, changes in Medicare Part B FFS
enrollment, and changes in the mix of
drugs for those beneficiaries who
received them.21 Since beneficiaries
18 Not
including the annual deductible.
1833(t)(8)(C)(i) of the Act limits the
amount of beneficiary copayment that may be
collected for a procedure performed in a year to the
amount of the inpatient hospital deductible for that
year. This limit is $1,408 in 2020.
20 2020 Medicare Parts A & B Premiums and
Deductibles: Fact Sheet, available at: https://
www.cms.gov/newsroom/fact-sheets/2020medicare-parts-b-premiums-and-deductibles.
21 The average annual growth in number of
Medicare Part B FFS beneficiaries was less than 0
percent from 2015 to 2019, so the change in
Medicare Part B beneficiaries does not fully account
for the average annual growth (11.4 percent) in
Medicare Part B spending for physicianadministeredpayable drugs. Instead, the increase
during this period is more fully explained by
increases in the prices of drugs, introduction of new
19 Section
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without supplemental insurance
typically pay 20 percent of the
Medicare-allowed amount, as described
in section II.A. of this IFC, they have
faced similar increases in spending on
Medicare Part B drugs as has
Medicare.22
A new Issue Brief from the Office of
the Assistant Secretary for Planning and
Evaluation (ASPE) provides additional
evidence of the need for the rule.
Between 2006 and 2017, Medicare Part
B FFS drug spending per enrollee grew
at 8.1 percent, more than twice as high
as per capita spending on Medicare Part
D (3.4 percent) and nearly three times as
high as overall retail prescription per
capita drug spending (2.9 percent).
Spending and enrollment projections by
OACT for the 2021 President’s Budget
suggest that per capita spending on
Medicare Part B physician-administered
drugs and separately payable hospital
outpatient drugs will grow at a very
similar annual rate of 8 percent between
2020 and 2027, before consideration of
any COVID–19 pandemic impacts.23
Because biologics account for about 77
percent of Medicare Part B FFS
prescription drug spending, there has
been little opportunity to reduce
Medicare Part B spending growth
through generic substitution, as has
occurred in Medicare Part D and in
retail pharmacy overall.24
C. Relative High Price of Medicare Part
B Drugs
Drug acquisition costs in the U.S.
exceed those in Europe, Canada, and
Japan, according to an October 2018
ASPE analysis 25 of Medicare Part B
physician-administered drugs. This
finding was generally consistent with
the existing evidence base as described
in the HHS analysis’s background
section, which found peer-reviewed
literature on this topic to be relatively
limited and dated, but with similar
findings of higher drug prices in the
U.S. compared to other countries.26 The
HHS analysis compared U.S. drug
acquisition costs for a set of Medicare
Part B physician-administered drugs to
acquisition costs in 16 other developed
economies—Austria, Belgium, Canada,
Czechia, Finland, France, Germany,
Greece, Ireland, Italy, Japan, Portugal,
Slovakia, Spain, Sweden, and the
United Kingdom (UK).27 The main
analysis in the HHS report focused on
27 drugs accounting for 64 percent of
total Medicare Part B drug spending in
2016.28 Among the 27 drugs included in
the analysis, acquisition costs in the
U.S. were 1.8 times higher than in
comparator countries. Acquisition cost
ratios ranged from U.S. prices being on
par with international prices for one of
the 27 drugs, to U.S. prices being up to
7 times higher than the international
prices for others. There was variability
across the 16 countries in the study as
well, with no one country consistently
acquiring drugs at the lowest prices. The
U.S. had the highest drug prices for 19
of the 27 products.29
A new ASPE Issue Brief updates the
earlier analysis for the set of Medicare
Part B drugs and the set of countries in
the MFN Model. In 2018, based on
available data, ASP rates were at least
2.05 times the value-weighted average
price for these drugs in OECD countries
with per capita GDP at least 60 percent
of that in the U.S.30
drugs, changes in drug utilization, and changes in
the mix of drugs than by increases in Medicare
enrollment.
22 In 2016, 8 in 10 beneficiaries in traditional
Medicare (81 percent) had some type of
supplemental insurance (which typically covers
some or all of Medicare Part A and Medicare Part
B cost-sharing), including employer-sponsored
insurance (30 percent), Medigap (29 percent), and
Medicaid (22 percent). Nearly 1 in 5 beneficiaries
in traditional Medicare (19 percent)—6.1 million
beneficiaries overall—had no source of
supplemental coverage in 2016. https://
www.kff.org/medicare/issue-brief/sources-ofsupplemental-coverage-among-medicarebeneficiaries-in-2016/.
23 ASPE analysis of OACT spending and
enrollment projections.
24 Nguyen X. Nguyen and Steve Sheingold.
Medicare Part B Drugs: Trends in Spending and
Utilization, 2006–2017. Washington, DC: Office of
the Assistant Secretary for Planning and Evaluation,
U.S. Department of Health and Human Services.
November 20, 2020 (https://aspe.hhs.gov/pdfreport/medicare-part-b-drugs-spending-andutilization).
25 Comparison of U.S. and International Prices for
Top Medicare Part B Drugs by Total Expenditures’’
accessed via https://aspe.hhs.gov/pdf-report/
comparison-us-and-international-prices-topmedicare-part-b-drugs-total-expenditures.
26 ‘‘Comparison of U.S. and International Prices
for Top Medicare Part B Drugs by Total
Expenditures’’ accessed via https://aspe.hhs.gov/
pdf-report/comparison-us-and-international-pricestop-medicare-part-b-drugs-total-expenditures.
27 Please refer to the HHS report (‘‘Comparison of
U.S. and International Prices for Top Medicare Part
B Drugs by Total Expenditures’’ accessed via
https://aspe.hhs.gov/pdf-report/comparison-us-andinternational-prices-top-medicare-part-b-drugstotal-expenditures) for more information on the
countries selected for analysis.
28 ‘‘Comparison of U.S. and International Prices
for Top Medicare Part B Drugs by Total
Expenditures’’ accessed via https://aspe.hhs.gov/
pdf-report/comparison-us-and-international-pricestop-medicare-part-b-drugs-total-expenditures.
29 The ASPE report utilized ex-manufacturer
prices (sometimes called the ex-factory price) stated
in U.S. currency on the transaction date. The report
defines ex-manufacturer prices as the price received
by manufacturers of a product, including discounts
applied at the point of sale.
30 El-Kilani Z, Finegold K, Mulcahy A, and
Bosworth A. Medicare FFS Part B and International
Drug Prices: A Comparison of the Top 50 Drugs.
Washington, DC: Office of the Assistant Secretary
for Planning and Evaluation, U.S. Department of
Health and Human Services. November 20, 2020
(https://aspe.hhs.gov/pdf-report/medicare-ffs-partb-and-international-drug-prices).
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The results of these reports
demonstrate that, save for a few outlier
cases, the U.S. prices used to calculate
ASP rates are significantly higher than
the prices in international comparator
countries.31 Based on this significant
difference, which aligns with the
analysis we present in this IFC, we will
test the impact of more closely aligning
payment for Medicare Part B drugs and
biologicals with international prices in
the MFN Model.
III. Provisions of the Interim Final Rule
With Comment Period
A. Model Performance Period
In part 513, we codify the MFN Model
that will be tested for 7 performance
years. We define ‘‘model performance
period’’ to mean January 1, 2021, the
date the model will begin, through
December 31, 2027. We are testing a 7year performance period because it will
allow a smooth transition to the MFN
Price (described in section III.E.5. of this
IFC) by performance year 4 and
adequate duration to understand the
impact of the MFN Model. As discussed
in section III.N. of this IFC, we will
assess for potential impacts of the MFN
Model across quarterly time periods
throughout the performance period.
Further, we will assess initial impacts of
the MFN Model on quality of care,
including access to drugs, prior to
beginning performance year 5.
B. Defined Population
Our goal is to include all beneficiaries
who are furnished an MFN Model drug
by an MFN participant and who, on the
date of service, are enrolled in Medicare
Part B, have Medicare as the primary
payer, and are not covered under
Medicare Advantage or any other group
health plan, including a United Mine
Workers of America health plan,
hereafter called MFN beneficiaries.
Thus, the defined population for the
MFN Model will be Medicare FFS
beneficiaries who receive an MFN
Model drug from an MFN participant
where payment for such drug is allowed
under the MFN Model. We define the
term ‘‘MFN beneficiary’’ in § 513.2.
Testing the model in the population
of beneficiaries who receive drugs with
high annual Medicare Part B spending
allows the MFN Model payment to
apply to a broad set of conditions,
drugs, medical specialties, clinical
settings, and localities rather than
having MFN Model payment focused on
a particular clinical presentation, course
of treatment or single type of care
setting. Defining the population in this
31 ASP is defined in statute, and based on sales
in the U.S.
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manner allows CMS to observe the
implications of a global approach to
calculating Medicare Part B drug
payment amounts and an alternative
add-on approach across a broad set of
providers and suppliers and
beneficiaries, as well as a large set of
manufacturers. Learnings from the MFN
Model will inform CMS and other
stakeholders about the effect of applying
the innovative payment model to a
broad set of drugs on a diverse set of
beneficiaries and to the Medicare
program.
C. MFN Participants
1. Eligible Providers and Suppliers
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A majority of Medicare spending on
separately payable Medicare Part B
drugs is for drugs that are furnished
incident to a physician’s service (see
section 1861(s)(2)(A) of the Act), in a
HOPD (see section 1861(s)(2)(B) of the
Act), including in an on- or off-campus
PBD (regardless of whether those PBDs
are excepted or nonexcepted),32 or in an
ASC (see section 1832(a)(2)(F)(i) of the
Act). Depending upon the
circumstances, Medicare Part B allows
separate payment for drugs to other
providers and suppliers, such as
pharmacies, home health agencies,
hospices, radiation therapy centers,
independent diagnostic testing facilities,
ambulance suppliers, durable medical
equipment (DME) suppliers, mass
immunization suppliers, inpatient
hospitals (when Part A payment is not
permitted), and other types of providers
and suppliers. Our goal is to broadly
include providers and suppliers that
receive separate payment for MFN
Model drugs as MFN participants, with
limited exceptions. MFN participants
will consist of Medicare participating
providers and suppliers that submit a
claim for a separately payable drug that
is an MFN Model drug furnished to an
MFN beneficiary, unless otherwise
excluded.33 Because separately payable
Medicare Part B drugs (that is, potential
MFN Model drugs) are most often
furnished by physicians, non-physician
practitioners, supplier groups (such as
group practices), hospitals that are paid
under the OPPS as defined in 42 CFR
419.20 (including off-campus PBDs paid
32 That is, regardless of whether those PBDs are
excepted or nonexcepted under section
1833(t)(21)(B)(ii) of the Act, as added by section 603
of the Bipartisan Budget Act of 2015 (Pub. L. 114–
74).
33 These providers and suppliers will be included
as participants in the MFN Model only if they
participate in Medicare; this means that
nonparticipating physicians and non-physician
practitioners will not be MFN participants and will
continue to be paid in accordance with current
program policies.
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under the PFS), and ASCs, these
providers and suppliers will represent
the vast majority of MFN participants.
Other types of providers and suppliers
(that are not excluded) also will be MFN
participants to the extent that they
submit a claim for an MFN Model drug
furnished to an MFN beneficiary. For
example, a home health agency that
receives separate payment for an
osteoporosis drug (defined in section
1861(kk) of the Act) will be an MFN
participant if such drug is an MFN
Model drug and the home health agency
furnishes such drug to an included
beneficiary and a claim is submitted.
We will exclude certain types of
providers and suppliers that are
ultimately not paid for drugs based on
ASP as well as those who are subject to
the hold harmless provision in section
1833(t)(7)(D)(ii) of the Act. Thus, in
§ 513.100(c), we exclude from the MFN
Model the following providers and
suppliers: Children’s hospitals (defined
under section 1886(d)(1)(B)(iii) of the
Act); PPS-exempt cancer hospitals
(defined under section 1886(d)(1)(B)(v)
of the Act); critical access hospitals
(CAHs) (defined under section 1820 of
the Act); Indian Health Service (IHS)
facilities (described in section 1880 of
the Act), except when MFN Model
drugs are furnished and such service is
described in section 1880(e)(2)(B) of the
Act; Rural Health Clinics (RHCs)
(defined under section 1861(aa)(2) of the
Act); Federally Qualified Health Centers
(FQHCs) (defined under section
1861(aa)(4) of the Act); hospitals that are
not subsection (d) hospitals (as defined
in section 1886(d)(1)(B) of the Act) and
are paid on the basis of reasonable costs
subject to a ceiling under section
1886(b) of the Act; and extended
neoplastic disease care hospitals
(defined in section 1886(d)(1)(B)(vi) of
the Act). In addition, for the first quarter
and second quarter of performance year
1, we will exclude acute care hospitals
that participate in a CMS Innovation
Center model under which they are paid
for outpatient hospital services
furnished to Medicare FFS beneficiaries,
including MFN Model drugs, on a fully
capitated or global budget basis in
accordance with a waiver under such
model of section 1833(t) of the Act. This
exclusion, codified at § 513.100(c)(9),
will apply during the first quarter and
second quarter of performance year 1,
and only if the hospital participates in
a CMS Innovation Center model under
which it is paid on a fully capitated or
global budget basis. As codified at
§ 513.100(c)(10), for the third quarter of
performance year 1 (that is, beginning
July 1, 2021) and beyond, acute care
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hospitals that participate in a CMS
Innovation Center model under which
they are paid for outpatient hospital
services furnished to Medicare FFS
beneficiaries, including MFN Model
drugs, on a fully capitated or global
budget basis in accordance with a
waiver under such model of section
1833(t) of the Act will be excluded from
the MFN Model if the parameters of the
other CMS Innovation Center model
adjust for the difference in payment for
MFN Model drugs between the MFN
Model and non-MFN Model drug
payments such that savings under the
MFN Model are incorporated into the
other CMS Innovation Center model’s
parameters (for example, the annual
global budget) for the duration of the
MFN Model. Thus, acute care hospitals
that are participating in the Maryland
Total Cost of Care Model will not be
MFN participants during the first two
calendar quarters of 2021 while they are
paid on a fully capitated or global
budget basis. Further, if the parameters
of the Maryland Total Cost of Care
Model have been updated to adjust for
the difference in payment for MFN
Model drugs between the MFN Model
and non-MFN Model drug payments
such that savings under the MFN Model
are incorporated into the parameters for
the Maryland Total Cost of Care Model
(for example, the annual global budget)
for the duration of the MFN Model, then
these acute care hospitals will remain
excluded from the MFN Model
beginning with the third quarter of
performance year 1 and beyond.
However, if the parameters of the
Maryland Total Cost of Care Model
change such that the participating acute
care hospitals are no longer paid on a
fully capitated or global budget basis or
if a participating acute care hospital
leaves the Maryland Total Cost of Care
Model such that they are paid under
section 1833(t) of the Act, then such
hospitals would no longer fall under
this exclusion. This exclusion also
applies on the same terms to acute care
hospitals participating in the
Pennsylvania Rural Health Model that
otherwise meet the definition of MFN
participant, unless the parameters of the
Pennsylvania Rural Health Model
change such that the participating acute
care hospitals are no longer paid on a
fully capitated or global budget basis or
if a participating acute care hospital
leaves the Pennsylvania Rural Health
Model such that they are paid under
section 1833(t) of the Act. We expect
that the CMS Innovation Center will
adjust the parameters of the Maryland
Total Cost of Care Model and the
Pennsylvania Rural Health Model such
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that the participants in these CMS
Innovation Center models will remain
excluded from the MFN Model for the
duration of the MFN Model. Further, as
discussed in section III.J.1. of this IFC,
the CMS Innovation Center intends to
address model overlaps with other CMS
Innovation Center models whether or
not the participants in other models are
MFN participants, for example we will
account for changes in Medicare Part B
drug payments that impact other
models’ financial calculations.
We note that community mental
health centers, comprehensive
outpatient rehabilitation facilities
(CORF), outpatient rehabilitation
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facilities (ORF), and certain other
providers and suppliers do not submit
claims for Medicare Part B drugs or are
not paid separately for Medicare Part B
drugs; thus, an express exclusion for
these providers and suppliers is not
necessary. We also note that including
these providers and suppliers in the
MFN Model would complicate the
model design and make it challenging to
test the impact of the MFN Model on
these types of providers and suppliers
because of the varied payment
structures among these providers and
suppliers.
Table 1 shows the distribution of 2019
Medicare Part B allowed charges for
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separately payable Medicare Part B
drugs by provider and supplier type
using available final action claims
where Medicare was the primary payer,
with limited exclusions as noted. This
table shows the distribution of Part B
drug claims among provider and
supplier types. To assign claims to a
provider or supplier type, we
considered the type of Medicare
Administrative Contractor (MAC) that
processed the claim, type of bill,
provider number, revenue center, line
place of service code, and specialty of
the health care practitioner associated
with the drug claim line.
BILLING CODE 4120–01–P
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To minimize the complexity of the
MFN Model, we are not including in the
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MFN Model Medicare Part B drugs that
are furnished in the inpatient setting,
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administered through covered DME,
orally administered, or paid under the
End-Stage Renal Disease Prospective
Payment System (ESRD PPS). Therefore,
in § 513.100(d), we provide an
exception for claims submitted by acute
care hospitals for separately payable
Medicare Part B drugs that were
administered during an inpatient stay or
included on an inpatient claim, such as
when a beneficiary has exhausted their
Part A benefit days, claims administered
by the Durable Medical Equipment
Medicare Administrative Contractors
(DME MACs) as described in 42 CFR
421.404(c)(2), and claims paid under the
ESRD PPS, including claims for drugs
that are paid using the transitional drug
add-on payment adjustment.
Under the approach set forth in
§ 513.100(b), all Medicare participating
providers and suppliers that submit a
claim for an MFN Model drug
(excluding claims specified in
§ 513.100(d)) furnished to an MFN
beneficiary will be included as MFN
participants unless otherwise excluded
(as specified in § 513.100(c)), regardless
of the volume of MFN Model drugs for
which they submit claims. As Table 1
shows, a significant proportion of
suppliers bill for a relatively lower
volume of MFN Model drugs, such as
less than $2,000 in total annual allowed
charges, and will likely have limited
claims paid under the MFN Model. We
considered whether to make specific
payment adjustments under the MFN
Model for MFN participants that bill for
a low volume of MFN Model drugs
during a historical period or whether
low-volume providers and suppliers
could have the option to opt into or out
of the MFN Model. However, we believe
that requiring participation in the model
only of providers and suppliers that bill
for a higher volume of MFN Model
drugs would not allow us to observe the
impact of the MFN Model on a full
range of providers and suppliers and
would create opportunities for shifting
sites of care and gaming. As such, we
are including a broad set of providers
and suppliers as MFN participants,
regardless of their volume of billing for
MFN Model drugs. As described in
section III.I.2. of this IFC, the MFN
Model includes a financial hardship
exemption in the form of a potential
reconciliation amount for MFN
participants that are significantly
affected by their participation in the
MFN Model.
We note that MFN Model drugs could
be furnished to a beneficiary in an
HOPD who is subsequently admitted to
an inpatient hospital stay. When a
beneficiary receives outpatient hospital
services, including MFN Model drugs,
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during the 3 days immediately
preceding admission to a hospital
defined under section 1886(d) of the
Act, the outpatient hospital services are
treated as inpatient services if the
beneficiary has Medicare Part A
coverage and such services are not
separately payable under Medicare Part
B. We will apply this policy
consistently under the MFN Model such
that if a beneficiary receives an MFN
Model drug in an HOPD that is an MFN
participant and is admitted to this
hospital within 3 days, then those
services, including drugs, will be treated
as inpatient services (in accordance
with Medicare inpatient payment
policies) and will not be separately
payable under the MFN Model. We note
that when a beneficiary receives
outpatient hospital services during the
day immediately preceding a hospital
admission to a hospital not paid under
the Inpatient Prospective Payment
System (IPPS), such as psychiatric
hospitals and units, inpatient
rehabilitation hospitals and units, longterm care hospitals, children’s hospitals,
and cancer hospitals, the statutory
payment window is one day preceding
the date of the patient’s admission; but
because these categories of hospitals
will be excluded from the MFN Model,
as discussed previously, the payment
window policy will not be applicable
for this model.
We are codifying these provisions in
§§ 513.100(a) through (d).
We note that we include a limitation
on the MFN Drug Payment Amount in
§ 513.210(d)(5) that will apply to certain
claims submitted by 340B covered
entities as described in section III.E.10.
of this IFC to ensure that beneficiaries
who are furnished MFN Model drugs by
a 340B covered entity do not face
increased cost-sharing under the MFN
Model than would otherwise apply.
2. Mandatory Participation and
Requirements
Model participation will be
mandatory for Medicare participating
providers and suppliers that satisfy the
MFN participant definition. There will
be no specific enrollment activities for
MFN participants; rather, their
participation will be effectuated by the
submission of a claim for an MFN
Model drug furnished to an MFN
beneficiary, and we will apply the MFN
Model payment to such a claim.
As we have described in previous
rules implementing models with
required provider or supplier
participation, such as the
Comprehensive Care for Joint
Replacement (CJR) Model, mandatory
participation can enhance the
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generalizability of model results, as
mandatory model participants may be
more broadly representative of all entity
types that could be affected by a model.
Requiring participation in the MFN
Model will allow us to observe the
experiences of providers and suppliers
with diverse characteristics, such as
geographies, patient populations, and
specialty mixes. Mandatory
participation (with specified exceptions)
by providers and suppliers submitting
claims for MFN Model drugs in a
nationwide model, as further discussed
in section III.C.3. of this IFC, will
minimize administrative complexity
and risk to the integrity of the MFN
Model.
In § 513.100(e) and § 513.100(f), we
are codifying MFN participant
requirements during and after the MFN
Model. During the MFN Model
performance period described in
§ 513.1(c), MFN participants must—
• Adhere to the beneficiary
protections requirements in § 513.410 to
ensure beneficiaries’ access to care is
not adversely impacted;
• Adhere to the MFN Model-specific
billing instructions established by CMS
and the MAC responsible for processing
the MFN participant’s claims, including
without limitation those described in
§ 513.200, to ensure appropriate and
accurate Medicare payments; and
• Participate in MFN Model
monitoring and evaluation activities in
accordance with 42 CFR 403.1110(b),
including collecting and reporting of
information as the Secretary of Health
and Human Services (the Secretary)
determines is necessary to monitor and
evaluate the MFN Model, including
without limitation ‘‘protected health
information’’ as that term is defined at
45 CFR 160.103.
For 2 years after termination of the
MFN Model, MFN participants must
participate in MFN monitoring activities
as described in § 513.420.
MFN participants will continue to bill
Medicare for separately payable MFN
Model drugs furnished to MFN
beneficiaries and be responsible for
collecting beneficiary cost sharing
amounts for MFN Drug Payment
Amounts. As such, we anticipate MFN
participants will have the same
administrative requirements for
collection of beneficiary cost-sharing
amounts under the MFN Model as apply
to collection of beneficiary cost-sharing
outside the MFN Model.
As discussed in section III.L. of this
IFC, manufacturers will exclude from
their calculation of ASP all units of
MFN Model drugs that are furnished to
MFN beneficiaries and for which
payment under § 513.210 is allowed.
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Manufacturers will need to determine
the number of units to exclude and may
adjust purchasing arrangements with
MFN participants in order to obtain
information about such units. While
MFN participants are not required to
provide data to manufacturers related to
the number of units of MFN Model
drugs that were furnished to MFN
beneficiaries and for which payment
under § 513.210 was allowed, we
anticipate that manufacturers may
establish mechanisms to obtain such
information, which also may create
administrative burden for MFN
participants related to the MFN Model.
For example, manufacturers could
require use of separate purchasing
accounts, or reporting of information
about units of MFN Model drugs that
were furnished to MFN beneficiaries
and for which payment under § 513.210
was allowed in order to receive a more
favorable purchase price.
3. Model Geographic Area
In the October 2018 ANPRM, CMS
anticipated the geographic area
included in a potential IPI Model would
encompass 50 percent of Medicare Part
B drug spending. Several commenters
expressed concern that having model
participants subjected to multiple
payment methodologies for included
drugs based on having some but not all
of their locations within the model’s
geographic area would be
administratively burdensome.
Additionally, some commenters
expressed concern at the idea of
requiring participation in some
geographic areas but not others, noting
that this approach would
disproportionately affect some providers
and suppliers and not others. Multiple
commenters noted that reduced costsharing for patients in the model
compared to those outside of the model
would create potential differences in
access for beneficiaries. One commenter
noted that there would be a risk of
patient steering if the model created a
financial incentive for providers and
suppliers to provide care at sites outside
of the model geographic area rather than
at sites in the model geographic area.
Due to the administrative complexity
and risk to model integrity associated
with a limited scope, CMS believes that
the MFN Model cannot realize its full
potential in spending reductions for
Medicare and its beneficiaries and
improvement in quality of care without
broad participation of Medicare
participating providers and suppliers
through a nationwide scope. Section
1115A(b) of the Act gives the Secretary
discretion in the design of models,
including the scope of models. Section
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1115A(a)(5) of the Act states that the
Secretary may elect to limit testing of a
model to certain geographic areas. It
follows that the Secretary could
similarly elect not to limit testing to
certain geographic areas, and instead
test a nationwide model.
The MFN Model requires mandatory,
nationwide participation of Medicare
participating providers and suppliers
(with limited exclusions) to be able to
successfully test the model for the
reasons described later in this section.
First, a nationwide scope avoids
additional administrative burden on
MFN participants with some service
locations inside the MFN Model
geographic area and others outside of
the MFN Model geographic area, which
could lead to such MFN participants
needing to track and follow separate
requirements for how drugs are
acquired, furnished, and billed,
depending on the service location.
Second, a nationwide model geographic
area eliminates the potential for MFN
participants with service locations both
inside and outside the MFN Model’s
geographic area to seek to influence
beneficiaries’ choice of treatment
location in response to the differences
between non-model payments and the
MFN Model payments. This potential
issue is of particular concern for the
MFN Model given the broad use of MFN
Model drugs and the ambulatory
settings in which these drugs may be
furnished, which can be geographically
distributed over wide areas. Third, CMS
also believes that a nationwide model
geographic area maintains continuity
with current treatment patterns by
limiting disruption to beneficiary and
health care provider treatment plans
that may arise due to potential changes
in the site of care. Fourth, a nationwide
model geographic area allows all
eligible beneficiaries who receive an
MFN Model drug from an MFN
participant where separate payment is
allowed to benefit from the cost-sharing
reductions under the MFN Model.
Finally, CMS believes that a nationwide
model geographic area along with
mandatory participation creates the
necessary market participation to
increase the likelihood of MFN
participants being able to acquire MFN
Model drugs at lower prices as
discussed in section VI. of this IFC.
CMS notes that several of these points
were commented on by several
respondents to the October 2018
ANPRM. These points highlight the
challenges that accompany a limited
scope (non-nationwide) model
geographic area. CMS therefore believes
a nationwide scope is the most
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appropriate for the MFN Model. Thus,
we are codifying in § 513.120 that the
MFN Model geographic area includes all
states and U.S. territories.
As described in section VI. of this IFC,
we anticipate that there could be
potential challenges associated with a
mandatory, nationwide model, namely
greater impacts on manufacturers, a
greater number of MFN participants that
potentially receive lower payments for
drugs under the model, and fewer nonparticipants who potentially increase
their patient volume should
beneficiaries need to locate alternative
sites of care. We have designed the
model to mitigate these potential
challenges where possible.
D. MFN Model Drugs
We will begin the MFN Model with
50 Medicare Part B drugs, identified by
Healthcare Common Procedure Coding
System (HCPCS) codes with high annual
spending during 2019 (based on dates of
service and after applying certain
exclusions), that will be included on the
MFN Model Drug HCPCS Codes List
(described later in this section), and
maintain approximately 50 Medicare
Part B drugs on the MFN Model Drug
HCPCS Codes List during the 7-year
model performance period. We will
focus the model on the separately
payable, physician-administered
Medicare Part B drugs with the highest
annual spending which make up a
portion of the roughly 550 HCPCS codes
listed on the quarterly ASP pricing files,
but encompass approximately threequarters of annual Medicare Part B drug
spending, 34 and are furnished by the
types of providers and suppliers that
frequently bill under Medicare Part B.
The MFN Model payments will apply
only to MFN Model drugs when these
drugs are administered by MFN
participants to MFN beneficiaries and
Medicare Part B allows separate
payment as the primary payer.
In § 513.130(b), we exclude some
categories of Medicare Part B drugs from
the model, such as certain vaccines,
radiopharmaceuticals, oral drugs,
compounded drugs, and intravenous
immune globulin products. We also
exclude drugs that are billed with
HCPCS codes to which any generic
drugs are assigned, including in
applicable instances where single
34 CMS publishes a Medicare Part B Drug
Dashboard which can be used to view annual
spending on drugs by HCPCS code. The
downloadable file can be used to examine the
proportion of annual spending for the included
drugs. See: https://www.cms.gov/ResearchStatistics-Data-and-Systems/Statistics-Trends-andReports/Information-on-Prescription-Drugs/
MedicarePartB.
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source drugs or biologicals were within
the same billing and payment code as of
October 1, 2003. For purposes of the
MFN Model, we consider a drug to be
a generic drug if it is approved under an
abbreviated new drug application
(ANDA) under section 505(j) of the
Federal Food, Drug, and Cosmetic Act.
In accordance with President Trump’s
Blueprint to Lower Drug Prices, we are
excluding such drugs because these
drugs are already subject to competitive
market forces and because the Medicare
Part B payment allowances for these
drugs already reflect price competition
from generic products. In addition, we
are excluding drugs for which there is
an Emergency Use Authorization (EUA)
or approval by the Food and Drug
Administration (FDA) to treat patients
with suspected or confirmed
coronavirus disease 2019 (COVID–19).
Since there may likely be urgent, high
demand for such drugs and available
supply may be targeted to certain
populations, this exclusion allows
maximum flexibility for potential
changes in drug distribution for such
drugs.
To encourage introduction and use of
biosimilars, the Trump Administration
has taken several actions, including
establishing separate HCPCS codes for
Medicare Part B biosimilar biological
products. We are not excluding
biosimilar biological products from the
MFN Model, however, given the relative
lower annual Medicare Part B spending
for HCPCS codes for separately payable
biosimilar biological products through
2019, only one biosimilar biological
product is included among the
performance year 1 MFN Model Drug
HCPCS Codes List in Table 2.
We further discuss the drugs that will
be included in or excluded from the
MFN Model in the following four
subsections.
1. MFN Model Drug HCPCS Codes List
We will use an approach for including
drugs in the MFN Model that is similar
to what we described in the October
2018 ANPRM. However, rather than
beginning with approximately 27 drugs,
as discussed in the October 2018
ANPRM, and adding drugs annually, we
will include approximately 50 Medicare
Part B drugs in the MFN Model for each
performance year. We will identify the
top 50 Medicare Part B separately
payable drugs with the highest
aggregated Medicare Part B total
allowed charges in the baseline period,
after excluding certain claims, to result
in an initial set of drugs that will be
included in the model beginning in
performance year 1. Thereafter, annual
additions will follow a similar process
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using claims data for the subsequent
year.
Compared to beginning with a smaller
number of drugs and phasing in
additional drugs in each subsequent
performance year, beginning with 50
Medicare Part B drugs simplifies the
model design and reduces complexity
for MFN participants. Based on
spending patterns over time for high
spend Medicare Part B drugs,35 we
expect the set of included Medicare Part
B drugs to remain relatively stable over
the model’s 7-year performance period,
and we believe that a generally stable
set of MFN Model drugs will help MFN
participants plan their drug acquisition
strategies. We believe the benefits of this
stability outweigh the incremental
challenge of beginning the MFN Model
with a longer drug list than envisioned
in the October 2018 ANPRM, and allows
Medicare and its beneficiaries to benefit
from the model payment methodology
sooner for more of the highest spend
Medicare Part B drugs, if anticipated
savings are realized.
By focusing the MFN Model on
separately payable Medicare Part B
drugs, payments for products that are
bundled or otherwise included in
payment for a procedure or other
services will not be affected by the MFN
Model and payments for such bundled
services will not have to be separated or
adjusted. This approach does not
exclude drugs that are packaged under
a Medicare payment system in certain
settings and separately payable in other
settings. However, the MFN Model
payment only applies to such drugs in
settings where separate payment is
allowed.
In § 513.130, we describe the creation
and periodic updates of an MFN Model
Drug HCPCS Codes List, which
designates the MFN Model drugs that
are subject to the MFN Model payments
specified in § 513 subpart C.
Specifically, to select the list of drugs
included in the MFN Model for the
beginning of performance year 1 (that is,
beginning January 1, 2021), the
regulation text at § 513.130(a)(1) codifies
that, after making the exclusions
specified in § 513.130(b)(1) and (b)(2),
CMS identifies the top 50 drugs by
HCPCS code with the highest aggregate
2019 Medicare Part B total allowed
charges, and adds those HCPCS codes to
the MFN Model Drug HCPCS Codes
List, after updating such HCPCS codes
35 CMS publishes a Medicare Part B Drug
Dashboard, which can be used to view annual
spending on drugs by HCPCS code. See: https://
www.cms.gov/Research-Statistics-Data-andSystems/Statistics-Trends-and-Reports/
Information-on-Prescription-Drugs/
MedicarePartB.html.
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for any applicable changes. We will use
HCPCS codes to identify drugs because
they are an established way to identify,
bill, and pay for separately payable
Medicare Part B drugs in the Medicare
claims processing system, and they are
commonly used in other Medicare Part
B drug payment resources like the ASP
drug pricing files. For this process, we
will use final action Medicare Part B
claims for separately paid drugs with
dates of service within calendar year
2019 and allowed charges greater than
$0 where Medicare was the primary
payer from all Medicare providers and
suppliers as the baseline period. This
period is the most recent full calendar
year of claims data that was sufficiently
available prior to the model
performance period start on January 1,
2021. Accordingly, we arrayed drugs,
using HCPCS codes, in descending
order based on the aggregate Medicare
Part B total allowed charges in the 2019
baseline period, after making the
exclusions specified in § 513.130(b)(1)
and (b)(2), and identified the 50
Medicare Part B drugs (identified by
HCPCS codes) with the highest total
Medicare Part B allowed charges. These
HCPCS codes are included on the MFN
Model Drug HCPCS Codes List for the
beginning of performance year 1 as
shown in Table 2 of this IFC.
The MFN Model uses an annual
calendar year baseline period for
purposes of identifying the drugs that
will be added to the MFN Model Drug
HCPCS Codes List for performance year
1 (and annually thereafter, using the
next subsequent calendar year as the
baseline) because: The vast majority of
HCPCS Code updates occur annually in
the January HCPCS update; the model
will use an annual baseline period to
calculate the alternative add-on
payment amount described in section
III.F. of this IFC; and these baseline
periods will be aligned for consistency
in the model design.
This approach for identifying the
drugs that are included in the MFN
Model at the beginning of performance
year 1 captures most of the drugs listed
in the October 2018 ASPE report,36
which used the Medicare Part B
National Summary Drug file from 2016
to identify approximately 27 HCPCS
codes associated with high amounts of
spending, and nearly all the drugs listed
in the November 20, 2020 ASPE report,
which applied the criteria in the MFN
Model to Medicare Part B claims data
36 ‘‘Comparison of U.S. and International Prices
for Top Medicare Part B Drugs by Total
Expenditures’’ https://aspe.hhs.gov/pdf-report/
comparison-us-and-international-prices-topmedicare-part-b-drugs-total-expenditures.
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for 2018.37 This approach also results in
the inclusion of a variety of drugs and
biologicals (including biosimilar
biological products) that are used to
treat common conditions in the
Medicare Part B beneficiary population.
These drugs and biologicals with high
annual Medicare allowed charges are
frequently prescribed and administered
by various physician specialties to
beneficiaries with various medical
conditions. Examples of uses of the
drugs included in the MFN Model are:
Drugs and biologicals used to treat
cancer and related conditions,
biologicals used for the treatment of
rheumatoid arthritis and other immune
mediated conditions, and biologicals
used to treat macular degeneration.
Beneficiaries who receive such drugs,
often on a recurring basis, face
substantial cost-sharing liability directly
or through their supplemental
insurance, and such costs may be partly
avoidable (that is, reduced) if Medicare
payment for these drugs were not based
on the current ASP methodology.
Beginning with 50 of the highest
spend HCPCS codes based on annual
Medicare Part B allowed charges during
2019, after taking into account certain
exclusions, focuses the MFN Model on
a wide variety of frequently utilized
Medicare Part B drugs and specialties
that administer such drugs to Medicare
FFS beneficiaries, and allows CMS to
test the MFN Model payment on a broad
set of drugs and biologicals that are
furnished to many beneficiaries. We
believe that including single source
drugs and biologicals (including
biosimilar biological products) that
move into the top 50 HCPCS codes on
an annual basis will capture potential
shifts in utilization to drugs that had not
yet been included in the MFN Model, if
such shifting were to occur, and will
mitigate the potential for medically
unnecessary shifts in utilization.
In developing this approach, we also
considered comments we received in
response to the October 2018 ANPRM
on using drug classes to help inform
which drugs to include in the MFN
Model, as well as requests to consider
how access to Medicare Part B drugs (as
a whole and for specific subsets of
drugs) might be affected by inclusion in
the model. We considered these
suggestions and believe that using
annual Medicare Part B allowed charges
37 El-Kilani Z, Finegold K, Mulcahy A, and
Bosworth A. Medicare FFS Part B and International
Drug Prices: A Comparison of the Top 50 Drugs.
Washington, DC: Office of the Assistant Secretary
for Planning and Evaluation, U.S. Department of
Health and Human Services. November 20, 2020
(https://aspe.hhs.gov/pdf-report/medicare-ffs-partb-and-international-drug-prices).
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as a primary factor is a more
transparent, consistent, and clear
approach because attempting to identify
drugs for inclusion in the MFN Model
based on groups or classes of drugs
could become complicated and
confusing for MFN participants. There
are numerous drug classification
approaches available; for example, drug
classification can be based on a
chemical class, site of action,
mechanism of action, as well as other
factors. These approaches can become
difficult to apply consistently when
drugs from different chemical classes
are used to treat the same condition,
when a drug has more than one
mechanism of action, or when
conditions are treated with drugs having
more than one mechanism of action. For
example, the Medicare Part B biological
products commonly used to treat
rheumatoid arthritis include a variety of
monoclonal antibodies. Using broad
terms such as monoclonal antibodies to
identify a ‘‘group’’ of MFN Model drugs
would include a variety of biologicals
that are commonly also used in treating
other conditions, such as Crohn’s
disease, ulcerative colitis, cancer, and
multiple sclerosis. Attempting to select
MFN Model drugs using more narrow
terms, for example by specifying agents
that exert effects on more specific
inflammatory pathways, such as tumor
necrosis factor and interleukins, would
miss biologicals that affect other
pathways, like T cell stimulation. These
approaches may also miss products that
are primarily used to treat other
diseases, but may be used less
frequently in rheumatoid arthritis, and
these approaches may not be readily
adaptable for novel products that may
be introduced over the 7-year
performance period of the model.
In § 513.130(a)(2), we are codifying
the process for annual updates of the
MFN Model Drug HCPCS Codes List to
update the list of drugs that will be
included in the MFN Model for the
subsequent performance year, as further
described in section III.D.3. of this IFC.
2. Exclusion of Certain HCPCS Codes
and Claims
In the October 2018 ANPRM, we
discussed the potential exclusion of
several groups of drugs from the
potential IPI Model (83 FR 54555).
Commenters generally agreed that these
drugs should be excluded. As codified
in § 513.130(b)(1), the MFN Model
excludes the following types of drugs,
by excluding claims at the HCPCS code
level, before identifying the top 50 drugs
with the highest aggregate annual
Medicare Part B total allowed charges:
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• Medicare Part B vaccines specified
in section 1861(s)(10) of the Act (that is,
influenza, pneumococcal pneumonia,
and Hepatitis B vaccines, and any future
vaccine for COVID–19). These
preventive products are paid under
section 1842(o)(1)(A)(iv) based on
average wholesale price (AWP), a price
that does not include discounts or
rebates. Including such drugs in the
MFN Model also would not comport
with our test of an alternative add-on
payment amount (described in section
III.F. of this IFC) because the statutory
add-on percentage under section 1847A
of the Act does not apply to these drugs.
• Radiopharmaceuticals. Many
radiopharmaceuticals are typically
acquired outside of the traditional drug
supply chain. Nuclear pharmacies are
frequently involved in the preparation
of patient-ready doses of these drugs,
and Medicare Part B payment is
frequently based on contractor pricing.
We are excluding radiopharmaceuticals
from the MFN Model because it is
unlikely that we will be able to obtain
reliable international drug pricing
information for radiopharmaceuticals.
• Oral Medicare Part B drugs,
including oral anticancer drugs
described in section 1861(s)(2)(Q) of the
Act, oral antiemetic drugs described in
section 1861(s)(2)(T) of the Act and
immunosuppressive drugs described in
section 1861(s)(2)(J) of the Act. Oral
anticancer, antiemetic, and many
immunosuppressive drugs are often
used outside of the provider and
supplier settings (for example, these
drugs are often used at home); therefore,
we are excluding these oral drugs from
the MFN Model.
• Compounded drugs including
products prepared by outsourcing
facilities.38 Although subject to certain
FDA requirements, these products are
not approved by FDA per se, and with
one exception under the OPPS 39 are not
billed under drug-specific HCPCS
codes; they are typically billed using
under ‘‘not otherwise classified’’ (NOC)
codes. Also, compounded drugs are
typically acquired outside of the
traditional drug supply chain, and
Medicare Part B payment for
compounded drugs is generally based
on contractor pricing, such as invoice
pricing. We are excluding these drugs
because it is unlikely that we will be
able to obtain reliable international drug
pricing information for compounded
drugs.
38 See section 503B of the Federal Food, Drug,
and Cosmetic Act (21 U.S.C. 353b) with respect to
the definition of outsourcing facilities and their
regulation by FDA.
39 C9257 Injection, bevacizumab, 0.25 mg.
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• Intravenous immune globulin
products. In response to the October
2018 ANPRM, a commenter suggested
that CMS exclude plasma-derived
products and stated such products have
potential unique sourcing and
distribution, and past supply shortages.
We note that FDA has identified a
current shortage related to one of the
HCPCS codes that is among the top
drugs with high aggregate 2019
Medicare Part B total allowed charges
(J1569, Gammagard liquid infusion).
Three other immune globulin products
are also among the top drugs in 2019,
J1459 (Inj ivig privigen 500 mg), J1561
(Gamunex-c/gammaked), and J1568
(Octagam injection). After considering
this concern, we are excluding
intravenous immune globulin products
from the MFN Model because these
products are at higher risk of shortage
based on their complex sourcing and
production, and we are aware of the
ongoing exploration of the potential
benefit of plasma in the treatment of
patients with COVID–19.
• Drugs that are subject to an EUA or
receive FDA approval to treat patients
with suspected or confirmed COVID–19.
The exclusion of these drugs will
minimize any potential for the MFN
Model to impact rapid, widespread
availability of such drugs in the U.S. to
treat patients with suspected or
confirmed COVID–19.
• Drugs without drug-specific HCPCS
codes, that is, those billed under ‘‘not
otherwise classified’’ (NOC) codes, such
as J3490. NOC codes are used to bill for
drugs not assigned to a particular
HCPCS code. NOC codes typically
include a variety of unrelated drugs that
cannot be easily separated for the
purpose of ranking allowed charges of
the individual drugs. Also, significantly
greater claims processing complexity for
Medicare and MFN participants would
result if we had to identify whether an
MFN Model drug was billed under a
NOC code during MFN Model
operations. By excluding HCPCS codes
for these types of drugs, these drugs will
be fully excluded from the MFN Model.
While we intend that the MFN Model
drugs will encompass a wide variety of
frequently utilized Medicare Part B
drugs, we also intend that drugs will not
be included on the basis of substantial
use at home. Thus, in § 513.130(b)(2),
we codify the exclusion of claims that
were processed and paid by the DME
MACs as described in 42 CFR
421.404(c)(2), and professional claims
with a place of service code that
indicates the drug was used in a home,
including home-like settings, prior to
identifying the top 50 drugs (by HCPCS
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code).40 The place of service exclusion
applies only to professional claims
because place of service codes are not
used on institutional claims to identify
home use. Specifically, professional
claims with place of service codes 04—
homeless shelter, 12—home, 13—
assisted living facility, 14—group home,
16—temporary lodging, and 33—
custodial care facility will be excluded
prior to identifying the top 50 drugs (by
HCPCS code).
For future years of model
implementation, we seek comment on
whether all blood related, plasma
derived, and human tissue products
should be included in or excluded from
the MFN Model. We also seek comment
on how CMS should define such
products and what would be the
supporting rationale for such an
exclusion and how to address such
considerations in the future. We note
that we are also considering as a
potential addition to the model design
whether certain drugs, such as certain
gene and cell therapies (for example,
chimeric antigen receptor T-cell (CAR–
T) products) and drugs approved by
FDA after the start of the MFN Model
that are indicated for and used to treat
rare diseases or conditions, should be
excluded from the MFN Model for all
performance years, or for several years
after the drug is first sold in the U.S. We
note that under the MFN Model, annual
Medicare Part B allowed charges would
have to exceed tens of millions of
dollars for such drugs to reach the top
50 and be added to the MFN Model. We
also note that many of the top 50 drugs
in 2019 are used to treat conditions with
limited populations and were first
approved within the last 5 years. In
addition, we note that while drugs may
initially be approved for one or a few
very narrow indications, subsequently
approved indications can quickly
expand the use of the drug to a much
larger patient population. We are
considering whether we should exclude
certain gene and cell therapies based on
supply chain criteria, similar to our
policy to exclude vaccines and
compounded drugs. For future years, we
seek comment on whether we should
exclude certain gene and cell therapies
or new drugs for the treatment of rare
diseases and conditions from the MFN
Model, and how CMS would identify
such drugs for exclusion, particularly
how we would define such drugs,
identify rare diseases and conditions for
40 The DME MACs process Medicare Durable
Medical Equipment, Orthotics, and Prosthetics
(DMEPOS) claims for a defined geographic area or
‘‘jurisdiction,’’ servicing suppliers of DMEPOS.
Professional claims must comply with the ASC X12
837 Professional guide (005010X222A1).
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76191
purposes of the MFN Model, and
determine the appropriate length of
such exclusion (for example, all
performance years or several years after
the drug is first sold in the U.S.).
Some commenters have suggested that
drugs in short supply (based on
inclusion on the FDA drug shortages
list) should be excluded from drug
payment models. As discussed
previously, we are excluding
intravenous immune globulin products
from inclusion on the MFN Model Drug
HCPCS Codes List, because these
products are at higher risk of shortage
based on their complex sourcing and
production. Otherwise, based on our
experience with ASP pricing, shortages
of high cost single source drugs and
biologicals are uncommon, of short
duration, and generally apply to some
but not all package sizes of a drug. As
described in section III.E.12. of this IFC
and codified in § 513.210(d)(2), we
include a quarterly payment exception
for MFN drugs that are in short supply
(based on inclusion on the FDA drug
shortages list). We believe it will be less
disruptive to the MFN Model to include
a quarterly payment exception for MFN
Model drugs during the time they are in
short supply than to exclude such drugs
from the MFN Model altogether because
a quarterly payment exception approach
will avoid changing the inclusion status
of drugs should a shortage occur and
again when the shortage is resolved,
eliminate the need to consider
developing a process to add and remove
replacement drugs to maintain the
number of MFN Model drugs, and avoid
manufacturers having to change
processes for capturing sales of such
drugs in their ASP calculations as
discussed in section III.L. of this IFC
(under this policy, manufacturers will
not include in their calculation of the
manufacturer’s ASP any units of MFN
Model drugs billed by MFN participants
where the MFN Drug Payment Amount
is paid by Medicare as the primary
payer).
Finally, we considered whether an
exception to inclusion on the MFN
Model Drug HCPCS Codes List might be
appropriate for MFN Model drugs in
cases where pharmaceutical
manufacturers that distribute the drug
in the U.S. do not own the rights to the
drug product for distribution outside the
U.S. and therefore do not control exU.S. pricing for the drug product. To
avoid a gaming opportunity whereby
manufacturers’ new or recent business
arrangements create such cases, this
type of exception could be defined such
that only ownership rights that were
transferred prior to the October 2018
ANPRM, when CMS announced a new
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Medicare Part B drug payment model
was being developed, would qualify. To
avoid an exception being too broad, we
are concerned that additional criteria
should be required to qualify for it, such
as whether the increase in the MFN
Model drug’s applicable ASP (a measure
of U.S. prices) based on sales since
October 2018 has been slower than
inflation (that is, the change in the CPI–
U from the end of October 2018 through
the ASP calendar quarter for the first
calendar quarter of the model), and
whether the U.S. manufacturer makes a
legally enforceable commitment to
future U.S. price increases being slower
than inflation moving forward, if such
an exception were to be granted. In
addition, to maintain the exception for
the remainder of the model, the increase
in the MFN Model drug’s applicable
ASP since October 2018 would need to
be assessed quarterly to determine
whether it continues to be slower than
inflation. Given the complex and
numerous relationships that
manufacturers may have across U.S. and
international markets, we are not
including such an exception for the
MFN Model.
We seek comments for future years on
our approach to identifying and
maintaining the MFN Model Drug
HCPCS Codes List and whether there is
a need for an exception relating to
manufacturers’ ownership of drug
products internationally, and if so, how
such an exception might be defined and
operated transparently.
3. Annual Updates to the MFN Model
Drug HCPCS Codes List
As discussed in section III.D.1. of this
IFC, the MFN Model will begin with 50
drugs and biologicals by HCPCS code on
the MFN Model Drug HCPCS Codes List
for performance year 1. We will keep
approximately 50 drugs by HCPCS code
in the MFN Model during the 7-year
performance period so that drugs that
continue to account for a large portion
of Medicare Part B drug spending will
continue to be included in the model.
However, we believe that some
adjustments to the MFN Model Drug
HCPCS Codes List will likely be
required from time to time as drugs
enter and exit the market and as
utilization of Medicare Part B drugs
(measured by annual total allowed
charges) changes. Thus, we will update
the MFN Model Drug HCPCS Codes List
annually. The annual update process
will occur prior to the beginning of each
performance year rather than more
frequently, such as a quarterly process,
because less frequent changes to the
MFN Model Drug HCPCS Codes List
will decrease the burden associated
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with participating in the model. We
believe that making fewer changes to the
MFN Model Drug HCPCS Codes List
will result in MFN participants having
to make fewer changes to acquisition
arrangements, and this in turn will
lessen any potential for disruption in
workflow and care delivery compared to
a quarterly update process.
Additionally, as specified in
§ 513.130(a)(4), some quarterly changes
may be necessary to comport with
HCPCS coding updates that are
applicable to the HCPCS codes on the
MFN Model Drug HCPCS Codes List,
such as when a code is terminated and
a successor code is established.
For each annual update for
performance years 2 through 7, as
described in § 513.130(a)(2), we will
array in descending order all separately
payable Medicare Part B drugs, using
HCPCS codes, based on total allowed
charges after applying the exclusions
codified in § 513.130(b)(1) and (b)(2),
using the most recent full calendar
year’s Medicare Part B claims from all
providers and suppliers. Those drugs (as
identified by HCPCS codes) that have
total allowed charges that fall in the top
50 drugs by spending for that calendar
year that are not already on the MFN
Model Drug HCPCS Codes List will be
added to the MFN Model Drug HCPCS
Codes List to take effect on the first day
of the next performance year and the
MFN Drug Payment Amount that will
apply will be based on the applicable
MFN Price phase-in for that
performance year and will follow the
annual payment updates thereafter. This
process will be used only to add HCPCS
codes that are new to the top 50—to
maintain consistency, we will not
remove any codes from the MFN Model
Drug HCPCS Codes List on the grounds
that the HCPCS code dropped out of the
top 50. We will keep all HCPCS codes
that were included on the MFN Model
Drug HCPCS Codes List for the prior
performance year on the MFN Model
Drug HCPCS Codes List, except in
certain circumstances as noted in
section III.D.4. of this IFC, in order to
have greater stability in the set of drugs
that are included in the MFN Model
across the performance years. As a
result, in performance years 2 through 7,
the number of HCPCS codes on the
MFN Model Drug HCPCS Codes List
may be greater than 50. We believe this
approach has the potential to identify
drugs that are alternative therapies to
MFN Model drugs, such as competitor
products, where MFN participants may
shift utilization to avoid using drugs
subject to the MFN Model payment, and
will provide a mechanism for adding
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such drugs to the MFN Model. In
addition, this approach will serve as a
mechanism to identify newer drugs with
high annual Medicare Part B spending
for inclusion in the MFN Model.
To maintain transparency, when we
add HCPCS codes that are new to the
top 50 or are replacement codes for
HCPCS codes that are listed on the MFN
Model Drug HCPCS Codes List, we will
list the code’s start date for inclusion in
the MFN Model. In addition, we will
revise HCPCS codes on the MFN Model
Drug HCPCS Codes List as necessary to
reflect quarterly HCPCS code updates
that are applicable to the HCPCS codes
on the MFN Model Drug HCPCS Codes
List, for example when a permanent
code replaces a temporary code, a
HCPCS code is terminated and a
replacement code is established, or a
HCPCS code is established for Medicare
use. In such case, we will include an
end date on the MFN Model Drug
HCPCS Codes List for the terminated
code. We will notify MFN participants
of updates to the MFN Model Drug
HCPCS Codes List no less frequently
than quarterly by adding the updated
MFN Model Drug HCPCS Codes List to
the MFN Model website (https://
innovation.cms.gov/initiatives/mostfavored-nation-model).
4. Approach for Removing Drugs From
the MFN Model Drug HCPCS Codes List
We do not anticipate that drugs will
be removed from the MFN Model
frequently. In accordance with
§ 513.130(a)(3), we will remove drugs
from the MFN Model Drug HCPCS
Codes List only under the following
limited circumstances, but no more
frequent than quarterly, to align with
quarterly MFN Model payment updates:
• If they are permanently withdrawn
from the U.S. market;
• If a specific HCPCS code included
on the MFN Model Drug HCPCS Codes
List is terminated with no replacement
code available or planned; or
• The drug is excluded from the MFN
Model pursuant to the exclusions in
§ 513.130(b)(1), for example a HCPCS
code describes a generic drug approved
under an ANDA or a drug with an EUA
or FDA approval to treat patients with
suspected or confirmed COVID–19.
To maintain transparency, we will
remove HCPCS codes by setting an end
date on the MFN Model Drug HCPCS
Codes List at the next quarterly update
after CMS becomes aware, through
environmental scanning activities, that
all of the NDCs assigned to a HCPCS
code have been withdrawn from the
U.S. market and the drug is permanently
withdrawn from the U.S. market, or the
HCPCS code has been terminated with
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no replacement code available or
planned, or the exclusion in
§ 513.130(b) applies. HCPCS codes that
are removed from the MFN Model Drug
HCPCS Codes List will no longer be
subject to the MFN Model payment, but
rather will be subject to current
Medicare payment policies. If the
conditions for removal no longer exist,
the HCPCS code could again qualify for
inclusion on the MFN Model Drug
HCPCS Codes List at the next annual
update.
5. Performance Year 1 MFN Model Drug
HCPCS Codes List
To create the MFN Model Drug
HCPCS Codes List for performance year
1, we arrayed drug HCPCS codes by
aggregate 2019 Medicare Part B total
allowed charges 41 after applying the
exclusions in § 513.130(b)(1) and (b)(2).
We then identified the top 50 drugs by
HCPCS code with the highest aggregate
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41 We used 2019 final action claims data that were
available in the CMS Chronic Conditions Data
Warehouse in September 2020 where Medicare was
the primary payer.
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2019 Medicare Part B total allowed
charges. This process excluded HCPCS
codes for two influenza vaccines (90662
(Iiv no prsv increased ag im) and 90653
(Iiv adjuvant vaccine im)), two
pneumococcal pneumonia vaccines
(90732 (Ppsv23 vacc 2 yrs+ subq/im)
and 90670 (Pcv13 vaccine im)), and a
radiopharmaceutical (A9606 (Radium
ra223 dichloride ther)) from the MFN
Model Drug HCPCS Codes List. The
exclusion of intravenous immune
globulin products excluded four HCPCS
codes: J1459, Inj ivig privigen 500 mg;
J1561, Gamunex-c/gammake; J1568,
Octagam injection; and J1569,
Gammagard liquid injection.
Additionally, one HCPCS code that
describes a generic drug (J9395,
Injection, fulvestrant) was excluded.
Excluding claims that were processed
and paid by the DME MACs resulted in
the following HCPCS codes no longer
falling within the top 50 drugs in 2019:
J7605 (Arformoterol non-comp unit);
J7686 (Treprostinil, non-comp unit); and
J3285 (Treprostinil injection). Excluding
claims based on the place of service
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exclusion resulted in one HCPCS code,
J7192 (Factor viii recombinant nos), no
longer falling within the top 50 drugs in
2019.
Using this approach for selecting
MFN Model drugs, the resulting
performance year 1 MFN Model Drug
HCPCS Codes List includes single
source drugs and biologicals that
accounted for approximately 75 percent
of annual Medicare Part B drug allowed
charges for separately payable drugs
during 2019. Table 2 displays the list of
MFN Model drugs (by HCPCS code) that
are included on the MFN Model Drug
HCPCS Codes List for the beginning of
performance year 1, along with the top
billing specialties.
CMS will publish the MFN Model
Drug HCPCS Codes List quarterly on the
MFN Model website (https://
innovation.cms.gov/initiatives/mostfavored-nation-model), in advance of
the calendar quarter, along with MFN
Model Payment amounts and other
MFN Model information and materials.
BILLING CODE 4120–01–P
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BILLING CODE 4120–01–C
E. Model Payment Methodology for MFN
Model Drugs
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The MFN Model will test an
innovative approach to calculating drug
payment through use of a more
comprehensive set of drug pricing data
to calculate an alternative payment
amount for MFN Model drugs, along
with an alternative add-on payment,
which is described in section III.F. of
this IFC. Payment for drug
administration services, when
applicable, will continue to be
separately billed by model participants
to Medicare; there will be no change in
the payment for drug administration
services under the MFN Model.
Providers and suppliers will continue to
purchase MFN Model drugs, furnish
such drugs to beneficiaries, submit
claims to Medicare, and collect
applicable beneficiary cost-sharing.
Under the MFN Model, payments for
separately payable Medicare Part B
drugs will include the alternative drug
payment amount and the alternative
add-on payment amount, both subject to
sequestration, as applicable.
Similar to the current approach under
section 1847A of the Act, the MFN
Model alternative payment limit for the
‘‘drug portion’’ of payment for MFN
Model drugs (that is, not including the
add-on amount) will be calculated by
CMS quarterly. This amount is called
the MFN Drug Payment Amount. The
calculation of the MFN Drug Payment
Amounts is codified in § 513.210(b).
Beneficiary cost-sharing will apply to
the MFN Drug Payment Amount for
included drugs.
We will calculate an MFN Drug
Payment Amount for each drug on the
MFN Model Drug HCPCS Codes List
based on an MFN Price, which will be
derived from the lowest GDP-adjusted
country-level price, based on non-U.S.
OECD member countries with a GDP per
capita that is at least 60 percent of the
U.S. GDP per capita.42 We will use GDP
per capita information that is based on
purchasing power parity. We are also
establishing limits such that the MFN
Drug Payment Amount will not exceed
non-model payment for the drug
(excluding any non-model add-on
payment amount), will not apply to
drugs that are not separately payable,
42 Individual countries differ in the regulatory
processes and standards governing approval of
drugs and biologicals. Use of international drug
pricing information in the MFN Model should not
be interpreted to connote FDA approval or to
otherwise describe any scientific or regulatory
relationship between U.S.-approved and non-U.S.approved products.
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and certain other limitations discussed
later in this section.
Section III.E.1. of this IFC identifies
the data sources for the MFN Model
drugs’ international drug pricing
information that we will use to calculate
the MFN Price for each drug. Section
III.E.2. of this IFC outlines the
international drug pricing information
we will include in these calculations
and the included countries. Section
III.E.3. of this IFC defines the MFN Drug
Payment Amount. Section III.E.4. of this
IFC outlines our approach to calculating
each drug’s MFN Drug Payment
Amount. Section III.E.5. of this IFC
describes the phase-in of the MFN Price.
Section III.E.6. of this IFC describes the
alternative calculation for the MFN Drug
Payment Amount for situations where
no international drug pricing
information is available for an MFN
Model drug. Section III.E.7. of this IFC
provides illustrative MFN Drug Payment
Amounts for each drug on the
performance year 1 MFN Model Drug
HCPCS Codes List in Table 2 using
historical data. Section III.E.8. of this
IFC describes the timing of data and
MFN Drug Payment Amount updates.
Section III.E.9. of this IFC describes
adjustments to the phase-in formula and
incentives for manufacturers to address
rising U.S. drug prices. Section III.E.10.
of this IFC describes the limitation on
the MFN Drug Payment Amount.
Section III.E.11. of this IFC describes the
method for establishing MFN Drug
Payment Amounts for MFN Model
drugs added to the model for
performance year 2 and subsequent
performance years. Section III.E.12. of
this IFC describes the quarterly payment
exception for MFN Model drugs in short
supply. Section III.E.13. of this IFC
describes continued payment of the
blood clotting factor furnishing fee
under the MFN Model.
1. Data Sources on International Drug
Pricing Information
We will rely on existing data sources
to obtain data that we will use to
calculate and update the MFN Drug
Payment Amounts. We will use existing
data sources that contain international
drug pricing information, including list
prices, sales and/or volume data (for
example, package size and number of
packages sold), as available, in order to
optimize operational efficiency. Sales
may be based on ex-manufacturer prices
(sometimes called the ex-factory price),
that represent actual or calculated prices
paid to the manufacturer by wholesalers
and other distributors, retail prices,
prices for other distribution channels, or
a combination thereof. Confidential
manufacturer rebates will not likely be
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accounted for within these data;
therefore, existing sources for
international drug sales data may
overstate actual prices realized by
manufacturers.
In the October 2018 ANPRM, we
considered establishing a data collection
system for manufacturers to report to
CMS their international drug sales data
for prices and units sold to support the
calculation of the model payment for
each drug. In response to the October
2018 ANPRM, we received comments
stating that CMS should use existing
data sources for international drug
pricing information in order not to place
burden on manufacturers. Some
commenters expressed concerns that
new data reporting would greatly
increase burdens and costs for
manufacturers, further limiting their
ability to invest in research and
development for innovative therapies,
and would be impractical because
defining price reporting for foreign
markets would be too complex and
could not adequately capture fluid
pricing policy changes. We appreciate
these concerns, and as such, we will
rely on existing data sources for
purposes of calculating MFN Drug
Payment Amounts. We believe that
existing data sources are adequate for
purposes of calculating country-level
prices, GDP-adjusted country-level
prices, and the MFN Prices, as described
in this IFC, that will be used to calculate
the MFN Drug Payment Amount.
Commenters also noted that one
potential adverse reaction to the model
described in the October 2018 ANPRM
may be a shift internationally to a high
price and high rebate pricing strategy.
Specifically, commenters expressed
concern that if the international drug
pricing information used to establish
payment under a model relied on the
list prices in the included countries,
then manufacturers would restructure
their pricing arrangements to increase
the list prices of the model’s drugs in
those countries, and offer higher rebates
to offset the increased list price. CMS
appreciates this concern, and we will
prioritize use of available international
drug pricing information that
incorporate discounts and rebates to the
extent possible, rather than just the list
prices.
We have assessed several existing
data sources to determine the
availability and sufficiency of
international drug pricing information.
In § 513.140(c), we are codifying the use
of one or more international drug
pricing data sources. Specifically, we
will use one or more data sources,
available to CMS at least 20 business
days prior to the start of a calendar
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quarter, that utilize a standardized
method for identifying drugs across
countries within that data source, such
as using an internationally recognized
method for identifying scientific and
nonproprietary names (for example,
active ingredient name) and a standard
method for identifying drug forms that
at a minimum distinguishes among
injectable, oral, and other forms of a
drug. For example, the data source
might use the International
Nonproprietary Names (INN), as
applicable.43 This process requires
mapping between the data source’s
standardized method for identifying
scientific and nonproprietary names and
HCPCS codes, as discussed and
illustrated in section III.E.7. of this IFC.
Further, we will use one or more data
sources that contain international drug
pricing information stated in U.S.
currency, such as list prices, exmanufacturer prices (sometimes called
the ex-factory price) that represents
actual or calculated prices paid to the
manufacturer by wholesalers and other
distributors, actual or calculated sales
for retail and other distribution
channels, or volume data (for example,
number of units sold).
If more than one data source is
available for an MFN Model drug, as
noted previously, we will prioritize the
data sources using a hierarchy that we
describe later in this section. Thus, for
each MFN Model drug, we will identify
and use the most comprehensive data
source available, using the hierarchy
codified in § 513.140(c)(3). We will use
only one data source for an MFN Model
drug for a quarter, meaning we will not
combine data from different data
sources or time periods to calculate the
MFN Drug Payment Amount for an
MFN Model drug for a quarter.
Whenever possible, we will use
international drug pricing information
from two calendar quarters prior to the
calendar quarter to which the MFN Drug
Payment Amount will apply since the
ASP payment limits that apply to that
calendar quarter are based on
manufacturers’ U.S. sales from two
calendar quarters prior such that the
U.S. and international drug pricing data
will be based on information from the
same calendar quarter. We use the term
applicable ASP calendar quarter to
mean the period that is two calendar
quarters prior to the calendar quarter to
which the MFN Drug Payment Amount
will apply.
The hierarchy of data sources we will
use is as follows:
43 World Health Organization, International
Nonproprietary Names accessed via https://
www.who.int/medicines/services/inn/en/.
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• A data source with sales and
volume data for the applicable ASP
calendar quarter from at least one
included country, that is, a non-U.S.
OECD member country at the end of the
applicable ASP calendar quarter with a
GDP per capita that is at least 60 percent
of the U.S. GDP per capita.
• A data source that does not have
sales and volume data for the applicable
ASP calendar quarter, but contains sales
and volume data for any prior calendar
quarter beginning on or after October 1,
2019 from at least one included country.
• The extracted data used by CMS to
determine the most recent MFN Price
used to calculate an MFN Drug Payment
Amount posted on the MFN Model
website.
• A data source with ex-manufacturer
price data for the applicable ASP
calendar quarter from at least one
included country.
• A data source with list price data
for the applicable ASP calendar from at
least one included country.
In each of these cases, if there is more
than one data source meeting the
requirements in § 510.140(c), we will
use the data source at the highest level
of the hierarchy that contains
information from the highest number of
included countries, and, if available,
incorporates discounts and rebates into
its drug pricing information. It is
possible that we will use different data
sources for different drugs over different
quarters. We will use the data as
available from the data source, and we
will not make adjustments to account
for differences between the data sources
or for confidential rebates. We note that,
based on the performance year 1 MFN
Model Drug HCPCS Codes List shown in
Table 2, levels 4 and 5 of the hierarchy
will only apply to MFN Model drugs
that are added to the MFN Model Drug
HCPCS Codes List after performance
year 1 and perhaps for Q2043
(Sipuleucel-t auto cd54+) 44 and J2507
(Pegloticase injection), because for other
MFN Model drugs in performance year
1, the first three levels of the hierarchy
will always result in an available data
source as we consider the data used by
CMS to create the illustrative MFN
Prices and MFN Drug Payment Amounts
in Table 6 of this IFC to satisfy level 3
of our hierarchy. To illustrate: Suppose
we identified four data sources meeting
the requirements of § 510.140(c), where
Data Source 1 contains sales and
volume data for MFN Model drug X for
the applicable ASP calendar quarter
44 No data on international pricing or sales of
Sipuleucel-t auto cd54+ were available in the data
source used for Table 6, but international drug
pricing information for this drug could be available
in other sources.
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from 10 included countries, Data Source
2 contains sales and volume data for
MFN Model drug X for the applicable
ASP calendar quarter from 15 included
countries, Data Source 3 contains sales
and volume data from the third calendar
quarter of 2020 for MFN Model drug X
from 16 included countries, and Data
Source 4 contains list price information
for the applicable ASP calendar quarter
from all included countries. In this
scenario, we would use information
solely from Data Source 2 to determine
the MFN Price for MFN Model drug X
by calculating unadjusted country-level
prices for each of the 15 countries for
which Data Source 2 contains
information, and we would not use Data
Sources 1, 3, or 4 to calculate the MFN
Price for MFN Model drug X for that
quarter. For further illustration of how
we will apply the hierarchy in
calculating MFN Drug Payment
Amounts, see section III.E.4.a. of this
IFC.
We will use international sales and
volume information from as early as the
third calendar quarter in 2020 to
minimize the possibility of having no
international sales and volume
information with which to calculate the
MFN Price and to mitigate the potential
effect of manufacturers’ limiting the
reporting of international drug pricing
information during the model
performance period.
In addition, the one or more data
sources we will use will have
mechanisms in place to maintain,
update, and correct, if necessary, the
data source on at least a quarterly basis.
Further, the data sources we will use
will be maintained by organizations that
seek to limit the lag inherent in data to
no more than 180 days from the end of
the calendar quarter for which drug
pricing information is compiled to the
time that the organization makes such
updates available to users of the data
source.
We plan to monitor the
implementation of a World Health
Assembly (WHA) resolution to
‘‘improve the transparency of markets
for medicines, vaccines, and other
health products.’’ This resolution aims
to help Member States make more
informed decisions when purchasing
health products, negotiate more
affordable prices, and ultimately expand
access to health products for their
populations. In particular, the WHA
resolution 45—
• Urges Member States to publicly
share information on net prices paid for
45 World Health Assembly Update, 28 May 2019,
accessed via: https://apps.who.int/gb/ebwha/pdf_
files/WHA72/A72_R8-en.pdf.
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health products, to promote greater
transparency on pharmaceutical patents
and clinical trial results and to improve
suppliers’ reporting of information such
as sales revenues and units sold; and,
• Requests the WHO secretariat to
support the development and
implementation of national policies
relevant to transparency and to monitor
the impact of transparency on
affordability and availability of health
products, including the effect of
differential pricing.
We will monitor developments
related to this WHA resolution and
assess its impact on the availability of
data we will use to calculate and update
MFN Drug Payment Amounts.
As discussed previously, we will use
a hierarchy when selecting from
available data sources and start by using
data sources that incorporate discounts
and rebates to the extent possible in
order to address commenters’ concerns
about a shift internationally to a high
price and high rebate pricing strategy.
We believe that using one or more data
sources will help to ensure that we will
capture sufficient information to
monitor the international drug pricing
landscape and to calculate and update
MFN Drug Payment Amounts. Data
sources that include the information
described previously, as determined by
CMS, will be considered sufficient, and
as such, we will calculate MFN Drug
Payment Amounts for MFN Model
drugs using information extracted from
such data sources. Specifically, as
necessary, for each MFN Model drug,
we will extract and use data that align
with the data sources’ standardized
method for identifying scientific and
nonproprietary names and dosage forms
(for example, injectable forms), and with
the HCPCS code’s long descriptor,
including dosage form, for the HCPCS
codes on the MFN Model Drug HCPCS
Codes List, as applicable. Further, we
will only use the extracted data for
dosage formulations that could be
described by the MFN Model drug’s
HCPCS code descriptor as determined
by CMS when such limitation is not
feasible prior to extracting the data. For
example, for a drug, one HCPCS code
may include drug products that are a
certain type of formulation, such as
short-acting, intravenously administered
drug products, and another HCPCS code
may include drug products with the
same scientific and nonproprietary
name but a different formulation (such
as a long-acting suspension for
intramuscular injection), and the
extracted data contains international
drug pricing information for both
formulations. In such case, we will align
the extracted data in accordance with
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the HCPCS code descriptor for the MFN
Model drug. In order to align with our
existing policies for how we utilize
manufacturer-reported ASP data to
calculate payment limits, we may find
it necessary to make adjustments to the
data that we extract from international
drug pricing information data sources.
For example, in calculating payment
amounts based on ASP we do not adjust
the volume or units of a drug (that is,
the amount of a drug in a package) for
intentional overfill (see 75 FR 73466). If
we find that a data source from which
we obtain international drug pricing
information makes adjustments for
overfill, we will make adjustments to
the data that we extract from such
source so that the extracted data is
comparable to ASP data. There could be
other cases where we will have to
examine the extracted data and make
adjustments to align the data with a
HCPCS code descriptor for an MFN
Model drug. Specifically, we will adjust
the extracted international drug pricing
information for MFN Model drugs when
the data source shows the package size
of a drug product that is inconsistent
with the manufacturer’s information
about that product as determined by
CMS. In such cases where we confirm
a difference, we will make adjustments
to the pricing, sales and volume data as
necessary before calculating the
unadjusted country-level price for the
drug at the HCPCS code level. We
believe that such cases will be rare.
However, we identified the need to
make such adjustment to the
international drug pricing information
we used to illustrate the MFN Drug
Payment Amounts for J9311 (Inj
rituximab, hyaluronidase) shown in
Table 6 to align the package size volume
with manufacturer labeling and the
HCPCS code dosage descriptor. We note
that there could be additional cases if
international drug pricing data sources
that we will select show prices, sales or
volume data that are adjusted for
intentional overfill, include multiple
ingredients for a single drug product, or
are in error (for example, the package
size represents the maximum volume of
a vial instead of the volume of drug in
a package).
We will only use the extracted data
that have complete package size
information. As discussed previously,
we will use a hierarchy to determine
which data source to use for each MFN
Model drug for a quarter, in which we
will select a data source that includes
sales and volume data first. Data
without both sales and volume data will
not be able to be combined with other
data, therefore we will exclude such
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observations. For data sources with
international sales and volume data for
a given MFN Model drug, we will
exclude from the calculation of the
unadjusted country-level price data that
fall below a minimum threshold or are
incomplete, that is, international pricing
data with less than $1,000 in quarterly
sales, with less than 1,000 units in
quarterly volume, or where both sales
and volume data are not present. We
believe that $1,000 in quarterly sales
and 1,000 units in quarterly volume for
a package size is an appropriate
minimum necessary to establish
sufficient sales and volume for data to
be included in the calculation of a
meaningful and reliable unadjusted
country-level price for an MFN Model
drug and will minimize inclusion of
potential outlier data. We will exclude
presentations with low volume or low
sales to prevent outlier presentations
from exerting undue influence.
In developing the illustrative MFN
Prices shown in Table 6, we applied
these exclusions. Minimal sales and
volume across all countries were
excluded because of the low volume or
sales exclusion criteria. We explored the
impact of different volume and
expenditure thresholds, and determined
that $1,000 in quarterly sales and 1,000
units are a reasonable threshold to
reduce risk associated with extremely
low values. We found that data with
potential outlier sales remained
relatively common with lower
thresholds (that is, below $1,000 in
quarterly sales). While using higher
thresholds may further reduce potential
inclusion of outlier sales data, doing so
would result in having less data to
calculate unadjusted country-level
prices.
The exclusion of international pricing
data with less than $1,000 in quarterly
sales or with less than 1,000 units in
quarterly volume from the calculation of
the unadjusted country-level price will
greatly minimize the potential risk for
including possible outlier or errant data.
To better understand this potential
issue, we considered the impact of
including or excluding data with less
than $1,000 in quarterly sales or less
than 1,000 units in quarterly volume in
the calculation of the unadjusted
country-level price. There was little
impact from including these data but, as
a potential safeguard to prevent
inclusion of inappropriately low or high
international drug pricing information
in our calculations for the MFN Model,
we will exclude such data from the
calculation of the unadjusted countrylevel price. Overall, where this
approach had more than a 1 percent
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impact, there tended to be an increase
in the MFN Prices.
We also considered whether pricing
information that is greater than or less
than 95 percent of the mean across all
data for the drug at the equivalent of the
HCPCS code billing unit level should be
considered a possible outlier or error
and whether trimming such data or
removing such data would be
warranted. In our experience with
international drug pricing information
data sources, outlier or potentially
erroneous data appear only in isolated
instances and are often suggestive of
unintended differences in the unit at
which data is shown. For example, the
pricing data for a product with a
standard unit of one gram in one
country could appear to be 1,000 times
lower than the pricing data for that same
product from other countries in the data
source; in such a case, it seems likely
that the data for the one country with a
very low relative price represents the
price per milligram not per gram and
such data would likely be corrected over
time by the data source. We believe
international drug pricing data sources
have mechanisms to correct such
discrepancies based on market research
of currently available international drug
pricing information data sources.
Further, as codified in § 513.140(c), the
international drug pricing information
data sources that we will obtain will
have mechanisms in place to maintain,
update, and correct, if necessary, the
information on international drug
pricing in the database on at least a
quarterly basis. As such, because we
will revise the MFN Drug Payment
Amounts quarterly, we will recalculate
the MFN Drug Payment Amounts for up
to four prior quarters when revised
international drug pricing information is
available in the data source that we used
to calculate the MFN Model drug’s MFN
Price for the relevant quarter or ASP
updates for the relevant quarter are
available.46 In cases where an MFN
Drug Payment Amount for a prior
quarter is recalculated by CMS, CMS
will prospectively apply the
recalculations in the quarterly update
following the availability of revised
international drug pricing information
and ASP updates, and will not
automatically reprocess claims to apply
the recalculation, but reserves the right
to do so. To the extent that MFN Model
claims are reprocessed due to revisions
to the international drug pricing
information, the Medicare payment
46 We will apply the recalculations in the
quarterly update following the availability of
revised international drug pricing information and
ASP updates.
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amount and beneficiary cost sharing
will be recalculated to reflect the
revised prices. If prior to calculating the
unadjusted-country level prices for a
quarter, the data source confirms that
there is an error that they plan to correct
in a future version of the dataset and we
have the corrected information, we will
make the correction to avoid the need to
reprocess claims later. Therefore, we do
not believe it is necessary to take further
steps to trim or remove potential outlier
or erroneous international drug pricing
information before calculating the
unadjusted country-level prices. We
note that CMS does not make outlier
adjustments to ASP data.
In addition, for future years, we seek
comment on whether a threshold should
be applied to determine whether the
MFN Drug Payment Amount should be
recalculated for a prior quarter.
Specifically, we are interested in
comments on whether recalculations
should only occur when the
international drug pricing information
data source used corrects its data and
the impact on the MFN Price is more
than a nominal amount. We seek
comment on the appropriate amount of
such threshold and how a nominal
amount should be defined. Finally, in
the event that the international drug
pricing information data source that we
used to calculate the MFN Drug
Payment Amount for an MFN Model
drug for a quarter identifies an error in
their data and does not correct such
error within 180 days after the
applicable ASP calendar quarter, we
seek comment on whether CMS should
recalculate the MFN Drug Payment
Amount for such MFN Model drug and
quarter using international drug pricing
information in accordance with the
hierarchy in § 513.140(c)(3) after
excluding the data source we initially
used. We also seek comment on whether
CMS should adopt an alternative
approach to remediating such data
errors.
2. International Data Included in the
MFN Model
In the October 2018 ANPRM, for
purposes of a potential IPI Model, we
stated that we were considering using
pricing data from the following
countries: Austria, Belgium, Canada,
Czechia, Denmark, Finland, France,
Germany, Greece, Ireland, Italy, Japan,
Netherlands, and the United Kingdom.
We considered including these
countries’ data as they are either
economies comparable to the U.S. or
they are included in Germany’s market
basket for reference pricing for their
drug prices, and existing data sources
contain pricing information for these
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countries. We received wide-ranging
and helpful feedback in response to the
October 2018 ANPRM regarding which
countries’ data to include in a model. In
addition to comments received to the
October 2018 ANPRM, we also
conducted significant outreach to
stakeholders, such as stakeholder
meetings and conference calls, to gather
targeted feedback. There was also a
substantial number of media and press
reports surrounding which countries’
data to include in the MFN Model.
Generally, we received a significant
number of comments that expressed
opposition to including data from
countries that have health care systems
that are substantially dissimilar to the
U.S.’s health care system. Specifically,
many commenters stated that data from
countries utilizing government-run
health care systems or imposing strict
drug price controls should be excluded.
Alternatively, other commenters noted
that CMS should consider broadening
the scope to include more countries,
because the more countries that are
included in the index, the harder it
would be for pharmaceutical companies
to manipulate or game the pricing
changes. Commenters also
recommended utilizing various criteria
for selecting the countries that would be
included, such as the launching speed
of new drugs, the presence of rigorous
health technology assessment, the
proportions of public and private
markets, the economies of those
countries, and Human Development
Index (HDI).47
Based on the comments received, we
believe the most appropriate criteria for
considering a country for MFN pricing
is membership in the OECD and GDP
per capita relative to the U.S. The
current list of OECD countries includes
all countries included in the October
2018 ANPRM as well as Australia,
Chile, Colombia, Estonia, Hungary,
Iceland, Israel, Latvia, Lithuania,
Luxembourg, New Zealand, Norway,
Poland, Portugal, Republic of Korea,
Slovakia, Slovenia, Spain, Switzerland,
and Turkey. OECD countries comprise a
set of countries that share with the U.S.
democratic principles and commitment
to market-based economies, and these
countries’ GDP per capita (based on
purchasing power parity) range from
47 The Human Development Index is utilized by
the United Nations and is ‘‘is a summary measure
of average achievement in key dimensions of
human development: a long and healthy life, being
knowledgeable and have a decent standard of
living. The HDI is the geometric mean of
normalized indices for each of the three
dimensions.’’ Please see the United Nations
Development Programme’s Human Development
Reports for more information: https://hdr.undp.org/
en/content/human-development-index-hdi.
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approximately 25 percent of the U.S.
GDP per capita to over 175 percent of
the U.S. GDP per capita. Based on this
wide range of GDP per capita data, we
believe it is most appropriate to include
available international drug pricing
information for countries with a GDP
per capita of at least 60 percent of the
U.S. GDP per capita, as codified in
§ 513.140(b). We believe that applying a
minimum of 60 percent of the U.S. GDP
per capita strikes a balance between—
(1) having too low a GDP per capita
threshold and including data from
countries with economies that are
substantially different from the U.S.,
while; (2) also not having such a high
GDP per capita threshold that the list of
countries would be very short, which
commenters suggested we should avoid.
To avoid creating a potential incentive
for countries to discontinue their
membership in the OECD, we will
include available international drug
pricing information for countries that
were OECD members as of October 1,
2020, regardless of whether they remain
OECD members after October 1, 2020,
unless the country’s GDP per capita, as
determined by CMS quarterly, falls
below the threshold of 60 percent of the
U.S. GDP per capita. Based on available
data, this means that we will calculate
the MFN Price for the first quarter of
performance year 1 based on available
international drug pricing information
from Australia, Austria, Belgium,
Canada, Denmark, Finland, France,
Germany, Iceland, Ireland, Israel, Italy,
Japan, Republic of Korea, Luxembourg,
Netherlands, New Zealand, Norway,
Spain, Sweden, Switzerland, and the
United Kingdom.48 These 22 OECD
countries are among the countries with
the highest GDP per capita worldwide.49
We considered alternative approaches
to including data from countries for the
MFN Model. Specifically, we
considered including all non-U.S. OECD
countries or selecting countries based
on factors such as World Health
Organization (WHO) recognition as a
Stringent Regulatory Authority (SRA)
and intellectual property protections.
We also considered including data from
only countries that may represent large
markets for drug manufacturers such as
the European Union, Canada, Japan, and
United Kingdom. Additionally, the
Foundation for Research on Equal
48 The non-U.S. OECD countries that will not be
an included country for purposes of calculating the
MFN Price for MFN Model drugs for the first
quarter of performance year 1 will be Chile,
Colombia, Czechia, Estonia, Greece, Hungary,
Latvia, Lithuania, Mexico, Poland, Portugal,
Slovakia, Slovenia, and Turkey.
49 https://www.cia.gov/library/publications/theworld-factbook/fields/211rank.html.
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Opportunity (FREOPP) recommended
an alternative approach called the
Market-Based International Index (MBII)
as a benchmark for evaluating other
countries’ prescription drug pricing
systems; 50 this approach would include
data from the following countries that
FREOPP identified as having marketbased health care systems: Austria,
Belgium, Czechia, Denmark, France,
Germany, Ireland, Japan, Netherlands,
Portugal, Singapore, Slovakia, and
Switzerland.
Based on analyses examining
potential alternatives, we believe that
none of these alternative approaches
would be as objective and predictable
for purposes of calculating MFN Prices
as our approach. Our approach will
result in a large set of countries that are
economically similar, have reasonably
comparable purchasing power to the
U.S., and generally have existing
international drug pricing information
that is available. We considered an
alternative that would phase-in
countries over time based on a defined
set of characteristics, such GDP per
capita or average drug prices. We
believe that phasing in countries over
time would create instability in the
MFN Price. Thus we are adopting a set
of included countries that meet the
requirements in § 513.140(b), which
allows for the inclusion of data from
countries that were non-U.S. OECD
member countries as of October 1, 2020,
when CMS calculates the MFN Drug
Payment Amounts for a calendar
quarter. That means that at the end of
each applicable ASP calendar quarter,
CMS will assess the non-U.S. OECD
member countries as of October 1, 2020,
that have a GDP per capita that is at
least 60 percent of the U.S. GDP per
capita. Because available GDP data are
updated infrequently, we believe this
approach will result in a highly stable
process for developing the MFN Prices.
We will include available
international drug pricing information
from the included countries when such
data are contained in the data sources
that we have described in § 513.140(c),
as described in section III.E.1. of this
IFC.
There are several existing sources for
GDP data, including the Central
Intelligence Agency (CIA) World
Factbook,51 the World Bank,52 and the
International Monetary Fund.53 Upon
examining these sources, we noted that
the GDP data across these sources are
highly associated with one another. We
will use the CIA World Factbook as our
source for GDP data as it is issued by a
U.S. government agency and includes
estimates for all OECD member
countries. We will use the following
process to determine the countries that
were non-U.S. OECD member countries
as of October 1, 2020, with a GDP per
capita that is at least 60 percent of the
U.S. GDP per capita. For each country,
we will assess the GDP per capita based
on purchasing power parity that is
available in the CIA World Factbook at
the end of the applicable ASP calendar
quarter. The CIA World Factbook
contains the most recent estimate of
GDP per capita based on purchasing
power parity for a country as well as
historical data. We will identify whether
a country has a GDP per capita that is
at least 60 percent of the U.S. GDP per
capita by dividing the most recent
estimate of GDP per capita based on
purchasing power parity for a country
by the U.S. GDP per capita, using data
for the same year, and assessing the
results. We will use the GDP per capita
from the same year as the international
drug pricing information that is used to
calculate the unadjusted country-level
price, if available, or the most recent
prior year.
50 Roy, A. (2018) The Foundation for Research on
Equal Opportunity, ‘‘What Medicare Can Learn
From Other Countries on Drug Pricing,’’ accessed
via https://freopp.org/what-medicare-can-learnfrom-other-countries-on-drug-pricingbf298d390bc5.
51 https://www.cia.gov/library/publications/theworld-factbook/fields/211rank.html.
52 https://data.worldbank.org/indicator/
ny.gdp.mktp.cd.
53 https://www.imf.org/external/pubs/ft/weo/
2019/01/weodata/weoselgr.aspx.
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3. Definition of the MFN Drug Payment
Amount
As described later in this section, we
will calculate the MFN Drug Payment
Amount for a calendar quarter for the
MFN Model drug based on a phased-in
blend of the applicable ASP and the
MFN Price, which we will determine by
selecting the lowest GDP-adjusted
country-level price from the included
countries for the applicable ASP
calendar quarter.
4. Calculation of the MFN Drug Payment
Amounts
We will calculate an MFN Drug
Payment Amount for each MFN Model
drug for which there is international
drug pricing information from at least
one data source that meets our criteria
for at least one included country.
Section III.E.6. of this IFC describes an
alternative approach for calculating the
MFN Drug Payment Amount for
situations where no international drug
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pricing information is available for an
MFN Model drug, for example, because
the MFN Model drug is not approved for
marketing by any included country.
When using international drug pricing
information to calculate the MFN Drug
Payment Amounts, we want to account
for the relative economic resources of
non-U.S. countries to be able to fairly
compare country-level prices. We will
address relative economic resources in
two ways: (1) We will only use available
international drug pricing information
from non-U.S. OECD member countries
with a GDP per capita that is at least 60
percent of the U.S. GDP per capita; and
(2) we will adjust the extracted countrylevel prices using a GDP adjuster that
adjusts for a country’s GDP per capita if
it is lower than that of the U.S.
Specifically, to calculate the MFN
Drug Payment Amounts for a calendar
quarter in a performance year, we will
follow a multi-step process using the
corresponding quarterly ASP pricing
file, as well as the available
international drug pricing information
for included countries for the applicable
ASP calendar quarter, where available.
The key steps to calculate the MFN Drug
Payment Amount for each MFN Model
drug will be—
• Identify the available international
drug pricing information for the MFN
Model drug (by applying the hierarchy
of data sources obtained by CMS and
extracting the relevant data); 54
• Remove incomplete and low sales
and volume data, as applicable;
• Convert extracted volume data to
the HCPCS code unit level and adjust
for volume issues such as intentional
overfill, as applicable;
• Calculate 55 the unadjusted countrylevel price (representing the average
price per unit of drug where the unit of
drug is the same as the HCPCS code
billing unit) for the MFN Model drug for
each included country with available
data in the selected data source for that
drug;
• Calculate the GDP adjuster for each
included country;
54 Applicable subsequent steps depend upon the
level of the hierarchy for the selected data source.
For example, when there are no international sales
and volume data available for the drug for an
applicable ASP calendar quarter or from any quarter
beginning on or after October 1, 2019, in accordance
with level 3 of the hierarchy, we will use the
extracted data used by CMS to determine the most
recent MFN Price used to calculate an MFN Drug
Payment Amount posted on the MFN Model
website, including the data used by CMS to create
the illustrative MFN Prices and MFN Drug Payment
Amounts in Table 6 of this IFC. In such case, it will
not be necessary to redo steps to extract data from
the data source; however, CMS will follow the
remaining steps in the MFN Drug Payment Amount
calculation.
55 The calculation used depends upon whether
volume data is available.
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• Apply the GDP adjuster to the
unadjusted country-level price;
• Select the lowest GDP-adjusted
country-level price for each MFN Model
drug, which, if available, will be the
MFN Price;
• Identify the applicable ASP (which
we define as the payment amount
determined in accordance with 1847A
of the Act, less the applicable add-on
percentage, for the MFN Model drug’s
HCPCS code); 56
• Compare the MFN Price to the
applicable ASP (to apply limit, if
applicable);
• Identify the applicable phase-in
formula and adjustments; and
• Apply the applicable phase-in
formula and adjustments, if applicable,
to calculate the MFN Drug Payment
Amount.
The following paragraphs further
describe how we will calculate the MFN
Model Drug Payment Amounts for each
MFN Model drug for each calendar
quarter during the model:
a. Identify the Available International
Drug Pricing Information for the MFN
Model Drug
Using the data sources that we obtain
and applying the hierarchy described
previously in this IFC, we will extract
the available international drug pricing
information for an MFN Model drug for
the applicable time period (that is, the
applicable ASP calendar quarter) by
aligning the MFN Model drug’s HCPCS
code long description (in terms of name
and dosage form) with the data sources’
standard method for identifying
scientific names or nonproprietary
names (such as the International
Nonproprietary Names). That is, for an
MFN Model drug, we will identify the
data sources’ standardized scientific
name or nonproprietary name for that
drug, and then use that naming to
identify data for all products within that
data source with an applicable
formulation. We will extract the
applicable data (for example, data for all
package sizes for injectable forms of the
drug aligned with the identified
scientific or nonproprietary name and
formulations, for the included
countries) from the data source for the
applicable ASP calendar quarter, and in
accordance with our hierarchy, select
the data source for the MFN Model drug
for that quarter.
56 In general, the ASP Pricing File contains
payment limits based on 106 percent of the volume
weighted average of manufacturers’ ASP for a given
HCPCS code. To identify the applicable ASP, we
will divide the payment limit by 1.06 after
removing the blood clotting factor furnishing fee, if
applicable. For a biosimilar, we will remove the
amount that represents 6 percent of the reference
biological product’s ASP.
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As previously discussed in this IFC,
we will only use extracted data from the
selected data source that appears
complete and represent dosage
formulations that could be described by
the MFN Model drug’s HCPCS code
descriptor, as determined by CMS. For
example, J0178, Aflibercept injection,
represents injectable ophthalmic
formulations whereas a data source may
contain data for aflibercept for both
ophthalmic and systemic formulations;
only data for ophthalmic formulations
will be used to calculate the MFN Price
for such drug. The international drug
pricing data used to calculate the MFN
Price will not be limited to distinguish
between products with different
inactive ingredients (for example,
different excipients) or whether or not
the product is protein bound. However,
we will limit the international drug
pricing data for combination drugs that
contain multiple active ingredients or
biological products to the extent
feasible, as determined by CMS. This
approach is particularly relevant for
four of the MFN Model drugs for
performance year 1, aflibercept injection
(J0178), which represents ophthalmic
formulations compared to systemic
formulations; paclitaxel protein bound
(J9264), which represents protein bound
formulations compared to formulations
of paclitaxel that are not protein bound;
ferric carboxymaltos (J1439), which
represents injected formulations
compared to oral formulations; and
rituximab, hyaluronidase (J9311), which
represents formulations for
subcutaneous administration compared
to formulations of rituximab for
intravenous administration.
In accordance with the hierarchy for
selecting international drug pricing
information data sources, we will
prioritize use of international drug
pricing information that includes sales
and volume data for the applicable ASP
calendar quarter if such information is
available for a drug for one or more
included countries. If more than one
such data source is available, we will
select the data source with international
drug pricing information for the
applicable ASP calendar quarter, even if
another data source includes a higher
number of included countries. For
example, if the applicable ASP calendar
quarter is the third quarter of 2021 and
an available data source has sales and
volume data for a drug for 20 of the
included countries for the second
quarter of 2021 and for 15 included
countries for the third quarter of 2021,
we would extract and then calculate
unadjusted country-level prices for that
drug based on sales and volume data
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from the third quarter of 2021 only for
the 15 included countries for which
data from that quarter are available.
If there are available data from a data
source at the second level of our
hierarchy (that is, no international sales
and volume data for the applicable ASP
calendar quarter, but sales and volume
data from any quarter beginning on or
after October 1, 2019), for a drug, we
will use available international sales
and volume data from that data source
for the most recent prior quarter that
begins on or after October 1, 2019 for
that drug for included countries.
If there are no international sales and
volume data available for the drug, we
will use the extracted data used by CMS
to determine the most recent MFN Price
used to calculate an MFN Drug Payment
Amount posted on the MFN Model
website, in accordance with the third
level of the hierarchy.
If no MFN Drug Payment Amount has
been publicly posted for the drug, we
will use a data source at the fourth level
of our hierarchy if available (the data
source contains ex-manufacturer price
data but does not include volume data
for the applicable ASP calendar
quarter).
If ex-manufacturer price data for the
applicable ASP calendar quarter are not
available, we will use a data source at
the fifth level of our hierarchy (the data
source contains list price data for the
applicable ASP calendar quarter).
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b. Remove Incomplete Low Sales and
Volume Data, as Applicable
If the data source we select has sales
and volume data at the package level for
an included country, we will apply the
exclusions for data with incomplete
data and low sales and volume. That is,
we will exclude data without both sales
and volume data, with less than $1,000
in quarterly sales (expressed as U.S.
currency), or with less than 1,000 units
in quarterly volume.
c. Convert the Extracted Volume Data to
the HCPCS Code Unit Level and Adjust
for Volume Issues, Such as Intentional
Overfill, as Applicable
We will adjust the remaining volume
data to the same level as the HCPCS
billing unit, as applicable. For example,
if the data for a package size shows the
volume is 1,000 units and each unit
represents a 1 MG vial package and for
another package size the volume is 500
units and each unit represents a 10 MG
vial package, and both of these data are
for a drug assigned to the same HCPCS
code with a HCPCS billing unit of 1 MG,
the adjusted volume data for these
packages would be 1,000 units and
5,000 units, respectively, for a total
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adjusted volume of 6,000 units. The
volume for the 1 MG vial package is
unchanged because the amount of drug
in one package (that is, 1 MG) equals the
amount of drug in one HCPCS billing
unit. The volume for the 10 MG vial
package is changed to be 10 times
higher because the amount of drug in
one vial (that is, 10 MG) equals 10 times
the amount of drug in one HCPCS
billing unit.
Before this step is performed, as
applicable, we will adjust the extracted
volume information before converting it
to the HCPCS billing unit level when
the data source shows the package size
of a drug product that is inconsistent
with the manufacturer’s information
about that product based on the
available product information, such as
package labeling, compared to the data
extracted from the data source. In
addition, we will limit the number of
billing units in a package when the
available package labeling specifies use
of a limited amount of drug is to be used
from the package. For example, we will
limit the number of billing units in a
package for an aflibercept vial to one 2
mg dose in accordance with available
package labeling, which specifies that
each vial, regardless of the labeled
volume, has one 2 mg dose. For
injectable formulations for HCPCS codes
with dosage specified as per dose, we
will limit the number of billing units in
a package to no more than one per vial.
This approach was applied to illustrate
the MFN Prices for J7324 (Orthovisc inj
per dose) in Table 6.
d. Calculate the Unadjusted CountryLevel Price for the MFN Model Drug’s
HCPCS Code for Each Included Country
With Available Data in the Selected
Data Source for That Drug
Using the data available after
completing the prior steps, we will
calculate the unadjusted country-level
price for each included country with
available data. The unadjusted countrylevel price represents the average price
per unit of drug where the unit of drug
is the same as the HCPCS code billing
unit.
We will use a calculation that is
applicable to the data available at this
step. If volume data are available, we
will use a calculation that includes
volume-weighting across the different
data (which often represent different
package sizes) of the drug included in
the data source for the country to
calculate the unadjusted country-level
price. If volume data are not available,
we will use a calculation that treats all
packages of the drug included in the
data source for the country equally, after
converting the pricing data to the
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HCPCS code unit level, in calculating
the unadjusted country-level price.
If sales and volume data are available,
we will first sum the adjusted volume
data for all package sizes for the drug.
We will then sum the total sales for all
package sizes for the drug, and divide
that sum by the sum the adjusted
volume data for all package sizes for the
drug, resulting in an average price per
unit of drug where the unit of drug is
the same as the HCPCS code billing
unit. If the data source we select has exmanufacturer or list prices and does not
have volume data, we will calculate the
number of HCPCS billing units in a
package and divide the ex-manufacturer
price or list price for a package by the
number of HCPCS billing units in the
package, resulting in a price per unit of
drug for each package listed in the data
source. We will then sum the price per
unit of drug for each package listed in
the data source for the drug and divide
the sum by the number of packages
listed in the data source for the drug,
resulting in an average price per unit of
drug where the unit of drug is the same
as the HCPCS code billing unit.
We will repeat this process for each
country specified in § 513.140(b), to the
extent international drug pricing
information for the drug for the country
is available from the selected data
source. As explained previously and
specified in § 513.140(c)(3)(i), we will
use the highest tier data source, in
accordance with the hierarchy, which
includes data for the drug in at least one
included country. If the selected data
source for a drug for a calendar quarter
does not include data from a particular
included country, we will still calculate
the MFN Price for that drug using the
data from the selected data source based
on the included countries from which
there are data for the drug. We will not
include any information from countries
that did not have data in the selected
data source for that drug. In cases where
there is no data source that meets our
criteria for using international drug
pricing information (that is, there are no
international sales, volume, or other
pricing data available from any of the
included countries in our international
drug pricing information data sources,
including data used by CMS to
determine the most recent MFN Price
used to calculate an MFN Drug Payment
Amount posted on the MFN Model
website, for an MFN Model drug for any
quarter beginning on or after October 1,
2019 up to and including the model
performance period, we will not
calculate an unadjusted country-level
price (or GDP-adjusted country-level
price) and will instead use the
applicable ASP (which we will define as
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the payment amount determined in
accordance with section 1847A of the
Act minus the applicable add-on
percentage, for the MFN Model drug’s
HCPCS code) as the MFN Model Drug
Payment Amount, as described in
section III.E.6. of this IFC.
e. Calculate the GDP Adjuster for Each
Included Country
As discussed previously, we want the
MFN Price to account for the relative
economic resources and purchasing
power for each included country to be
able to fairly compare country-level
prices. As such, we will calculate a GDP
adjuster, using a country’s GDP per
capita based on purchasing power
parity, that will be used to adjust the
unadjusted country-level price for each
drug (whether based on international
sales and volume data or international
ex-manufacturer or list prices) to reflect
the country’s economic resources
relative to the U.S. We believe that GDP
per capita based on purchasing power
parity represents a broadly used and
reliable measure of a country’s
economic resources to ensure a
meaningful comparison of country-level
prices.
As previously mentioned, there are
several existing sources for GDP data,
including the CIA World Factbook,57
the World Bank,58 and the International
Monetary Fund.59 Our analyses suggest
that the GDP data across these sources
are highly associated with one another.
We will use the CIA World Factbook as
our source for GDP data as it is issued
by a U.S. government agency and
includes estimates for all current OECD
member countries. The GDP adjuster
will be based on the GDP per capita
available from the CIA World Factbook
at the end of the applicable ASP
calendar quarter. We will use the most
recent GDP per capita data available for
each included country and the U.S. GDP
per capita from the same year as the
GDP per capita data that is available
from the included country. For example,
if the most recent GDP per capita from
the comparison OECD country is from
2016 and the most recent U.S. GDP per
capita is 2017, then we will use the GDP
per capita from 2016 for both countries
when comparing. In cases where we use
international drug pricing information
from a quarter other than the applicable
ASP calendar quarter (that is, an earlier
time period) to determine the
unadjusted country-level price, we will
use the GDP per capita data for that time
period, if available, or the most recent
earlier data available. That is, CMS will
use the GDP per capita for the same year
as the data used to calculate the
unadjusted country-level price, if
available, or the most recent earlier year
available.
To create a simple, easily
understandable GDP adjuster, each
country’s GDP adjuster will be a straight
ratio of its GDP per capita based on
purchasing power parity divided by
U.S. GDP per capita, subject to the
limitation described later in this section.
The U.S. GDP per capita for 2017, the
most current data available, was
$59,800. Table 4 presents GDP per
capita for 2017 and the GDP adjusters
for each non-U.S. OECD member
country, based on the U.S. GDP per
capita of $59,800 for 2017, that we will
use to calculate the MFN Drug Payment
Amounts for performance year 1,
quarter 1. In cases when an included
76203
country’s GDP per capita and the U.S.
GDP per capita are not updated in the
CIA World Factbook at the same time,
we will use the most recent GDP per
capita for the included country and the
U.S. GDP per capita from the same year
to ensure that the GDP adjuster for an
included country is calculated using
GDP data from both countries from the
same time period. For example, if at the
end of an applicable calendar quarter a
2018 estimate of a country’s GDP per
capita based on purchasing power parity
becomes available in the CIA World
Factbook but the most recent U.S. GDP
per capita available in the CIA World
Factbook continues to be for 2017, we
will continue to use data from 2017 for
both countries to calculate the GDP
adjuster for that country.
The GDP adjuster will be capped at 1
such that the adjuster will only increase
the unadjusted country-level price for a
drug; it will not decrease it. We will cap
the GDP adjuster at 1 because its
purpose is to adjust for countries’
economic resources when lower than
those of the U.S. Capping the GDP
adjuster at 1 will ensure that we do not
make an adjustment that would result in
an amount that would be lower than the
unadjusted country-level price. For
example, if Country X with a higher
GDP per capita based on purchasing
power parity than the U.S., such as a
GDP per capita ratio of 2, has an
unadjusted country-level price of $100
for an MFN Model drug, we would use
a GDP adjuster of 1.0 and calculate a
GDP-adjusted country-level price of
$100 rather than using a GDP adjuster
of 2.0 and calculating a GDP-adjusted
country-level price of $50.
TABLE 4—NON-U.S. OECD MEMBER COUNTRY GDP PER CAPITA (BASED ON PURCHASING POWER PARITY) AND GDP
ADJUSTERS FOR PERFORMANCE YEAR 1, QUARTER 1
CIA GDP
per capita,
based on
purchasing
power parity
(2017)
OECD countries
GDP adjuster
for performance
year 1,
quarter 1
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The following countries have a GDP per capita of at least 60 percent of U.S. GDP per capita:†
Australia ....................................................................................................................................................
Austria * .....................................................................................................................................................
Belgium * ...................................................................................................................................................
Canada * ...................................................................................................................................................
Denmark * .................................................................................................................................................
Finland * ....................................................................................................................................................
France * .....................................................................................................................................................
Germany * .................................................................................................................................................
Iceland ......................................................................................................................................................
Ireland * .....................................................................................................................................................
Israel .........................................................................................................................................................
57 https://www.cia.gov/library/publications/theworld-factbook/fields/211rank.html.
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58 https://data.worldbank.org/indicator/
ny.gdp.mktp.cd.
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$50,400
50,000
46,600
48,400
50,100
44,500
44,100
50,800
52,200
73,200
36,400
0.843
0.836
0.779
0.809
0.838
0.744
0.737
0.849
0.873
** 1.000
0.609
59 https://www.imf.org/external/pubs/ft/weo/
2019/01/weodata/weoselgr.aspx.
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TABLE 4—NON-U.S. OECD MEMBER COUNTRY GDP PER CAPITA (BASED ON PURCHASING POWER PARITY) AND GDP
ADJUSTERS FOR PERFORMANCE YEAR 1, QUARTER 1—Continued
CIA GDP
per capita,
based on
purchasing
power parity
(2017)
OECD countries
Italy * .........................................................................................................................................................
Japan * ......................................................................................................................................................
Republic of Korea .....................................................................................................................................
Luxembourg ..............................................................................................................................................
Netherlands * ............................................................................................................................................
New Zealand ............................................................................................................................................
Norway ......................................................................................................................................................
Spain .........................................................................................................................................................
Sweden .....................................................................................................................................................
Switzerland ...............................................................................................................................................
United Kingdom * ......................................................................................................................................
GDP adjuster
for performance
year 1,
quarter 1
38,200
42,900
39,500
105,100
53,900
39,000
72,100
38,400
51,200
62,100
44,300
0.639
0.717
0.661
** 1.000
0.901
0.652
** 1.000
0.642
0.856
** 1.000
0.741
24,600
14,400
35,500
31,700
27,800
29,600
27,700
32,400
19,900
29,600
30,500
33,100
34,500
27,000
0.411
0.241
0.594
0.530
0.465
0.495
0.463
0.542
0.333
0.495
0.510
0.554
0.577
0.452
The following countries have a GDP per capita below 60 percent of U.S. GDP per capita:
Chile ..........................................................................................................................................................
Colombia ...................................................................................................................................................
Czechia * ...................................................................................................................................................
Estonia ......................................................................................................................................................
Greece * ....................................................................................................................................................
Hungary ....................................................................................................................................................
Latvia ........................................................................................................................................................
Lithuania ...................................................................................................................................................
Mexico ......................................................................................................................................................
Poland .......................................................................................................................................................
Portugal ....................................................................................................................................................
Slovakia ....................................................................................................................................................
Slovenia ....................................................................................................................................................
Turkey .......................................................................................................................................................
* Indicates countries that were listed as potential included countries in the October 2018 ANPRM (83 FR 54557).
** Indicates that the GDP adjuster is capped at 1.000.
† The 2017 U.S. GDP per capita is $59,800.
f. Apply the Applicable GDP Adjuster
To Calculate the GDP-Adjusted CountryLevel Price for the MFN Model Drug
Next, we will apply the countryspecific GDP adjuster to the unadjusted
country-level price for that country by
dividing the unadjusted country-level
price by the country’s GDP adjuster. The
result will be the GDP-adjusted countrylevel price for the MFN Model drug for
that country. We will repeat this
calculation to produce a GDP-Adjusted
Price for every country for which we
have calculated an unadjusted countrylevel price for the MFN Model drug.
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g. Identify the Lowest GDP-Adjusted
Country-Level Price for the MFN Model
Drug
We will examine the GDP-adjusted
country-level prices for the MFN Model
drug, and identify the lowest GDPadjusted country-level price for the
MFN Model drug. The lowest GDPadjusted country-level price will be the
MFN Price for the MFN Model drug.
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h. Compare the MFN Price to the
Applicable ASP
As a safeguard for beneficiaries, we
will compare the MFN Price to the
applicable ASP in order to ensure that
beneficiaries are always paying the
lowest amount of coinsurance available.
If the applicable ASP is less than the
MFN Price, we will establish the MFN
Price as equal to the applicable ASP.
i. Identify the Applicable Phase-In
Formula and Adjustments
As described in section III.E.5. of this
IFC, we will phase-in the use of the
MFN Price over the course of the MFN
Model. As discussed in section III.E.9.
of this IFC, we will also accelerate the
applicable phase-in formula when the
applicable ASP for an MFN Model drug
rises faster than both a designated
inflation factor and the change in MFN
Price, and lower the MFN Drug Payment
Amount below the MFN Price by a
certain percentage if the applicable ASP
for an MFN Model drug continues to
increase faster than the inflation factor
and the MFN Price after the full phasein of the MFN Price. In this step of the
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process to calculate the MFN Drug
Payment Amount, we will determine
the applicable phase-in formula and
whether any of these adjustments will
apply.
j. Calculate the MFN Drug Payment
Amount
As the last step, we will calculate the
MFN Drug Payment Amount for the
MFN Model drug using the applicable
phase-in formula, which blends the
applicable ASP and the MFN Price as
described in section III.E.5. of this IFC.
This calculation, including any
adjustments that apply, will result in
the MFN Drug Payment Amount for the
MFN Model drug (except as otherwise
specified).
5. Phase-In of the MFN Price
We will use a phase-in approach that
will blend the MFN Price with the
applicable ASP to allow MFN
participants time to adjust to the model
payment amounts and processes. The
phase-in formula will be stable for a
given performance year, whereas the
MFN Price and applicable ASP will vary
quarterly based on fluctuations in drug
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prices in the U.S. and in included
countries. We will phase-in the MFN
Price by 25 percent per year for
performance years 1 to 3 of the model,
reaching 100 percent of the MFN Price
for performance years 4 through 7 of the
model. The phase-in formula uses a
blend of the applicable ASP and MFN
Price for an MFN Model drug as shown
in Table 5. The MFN Drug Payment
Amount will be based on 100 percent of
the MFN Price starting in performance
year 4, unless an adjustment that
accelerates the phase-in applies as
described in section III.E.9. of this IFC.
Thus, the phase-in represents the outer
bound in terms of the amount of time
it will take for the MFN Drug Payment
Amount to transition to 100 percent of
the MFN Price.
We believe that a phase-in approach
during the initial years of the model will
enable MFN participants and the
markets to adjust to the model’s
payment methodology, while enabling
CMS to test the full phase-in of the MFN
76205
Price over a 7-year model performance
period. As noted in section III.E.11. of
this IFC, when MFN Model drugs get
added to the MFN Model Drug HCPCS
Codes List during the model
performance period, their MFN Drug
Payment Amount gets determined as set
forth for the corresponding performance
year, meaning that if an MFN Model
drug were to be added during
performance year 4, the MFN Drug
Payment Amount will equal 100 percent
of the MFN Price.
TABLE 5—PHASE-IN OF MFN PRICES BY PERFORMANCE YEAR
Performance year
Year
Year
Year
Year
Year
Year
Year
1
2
3
4
5
6
7
Blend of the ASP and MFN price for an MFN model drug at the HCPCS code level
.................................................................
.................................................................
.................................................................
.................................................................
.................................................................
.................................................................
.................................................................
We are codifying the phase-in formula
in § 513.210(b)(8).
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6. Alternative Calculation for the MFN
Drug Payment Amount
Over the course of the MFN Model,
we may determine that the international
drug pricing information data sources
that we obtain do not contain any
international drug pricing information
(meaning no sales, volume, exmanufacturer price, or list price data
from any included country from any
quarter beginning in the fourth calendar
quarter of 2018 through the applicable
quarter in the model performance
period) for an MFN Model drug, for
example, because the MFN Model drug
is not approved for marketing in the
included countries. For such cases, we
will establish the MFN Drug Payment
Amount at the applicable ASP for the
applicable calendar quarter, subject to
any adjustment in § 513.210(d) that
applies, until international drug pricing
information is available.
Because international drug pricing
information may become available for a
subsequent calendar quarter, we will
use this method to establish the MFN
Drug Payment Amount instead of
excluding or removing drugs without
any international drug pricing
information from the model until
international drug pricing information
becomes available. We believe having a
stable list of MFN Model drugs will be
more predictable for MFN participants,
lessening MFN participants’ need to
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75 percent applicable ASP and 25 percent MFN Price.
50 percent applicable ASP and 50 percent MFN Price.
25 percent applicable ASP and 75 percent MFN Price.
100 percent MFN Price.
100 percent MFN Price.
100 percent MFN Price.
100 percent MFN Price.
monitor changes to the MFN Model
Drug HCPCS Codes List, and will avoid
creating an opportunity for
manufacturers to get their products out
of the model by stopping the reporting
of international drug pricing
information. Based on our experience
with international drug pricing
information data sources, we expect the
potential of no international drug
pricing information for an MFN Model
drug across all included countries will
be limited. We note that our approach
may increase model payments
compared to non-model payments for
MFN Model drugs with no international
drug pricing information because the
alternative add-on payment, a single flat
add-on amount per dose (see section
III.F. of this IFC), could be greater than
the add-on payment outside of the
model.
7. Illustrative MFN Drug Payment
Amounts
To illustrate how CMS will calculate
the MFN Drug Payment Amounts under
the MFN Model in accordance with
§§ 513.130 and 513.140, we applied the
methodology for determining the
applicable ASPs, MFN Prices, and MFN
Drug Payment Amounts using historical
ASP-based payment limits,60 available
60 We used the 2019 Quarter 3 and Quarter 4 and
2020 Quarter 1 and Quarter 2 ASP data that align
with manufacturer-reported data based on sales
during 2019 to identify the applicable ASPs. The
ASP pricing files are posted at links available here:
https://www.cms.gov/Medicare/Medicare-Fee-for-
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international drug pricing information
from 2019 for the included countries,
and the MFN Model performance year 1
phase-in formula. Table 6 shows
illustrative data for applicable ASPs,
MFN Prices, and MFN Drug Payment
Amounts for one billing unit for the
HCPCS codes that are included on the
performance year 1 MFN Model Drug
HCPCS Codes List in Table 2. Actual
MFN Drug Payment Amounts per billing
unit for performance year 1, quarter 1,
and thereafter will be calculated as
specified in § 513.210. We will publish
the quarterly MFN Drug Payment
Amounts on a CMS website (such as the
MFN Model website), similar to how the
ASP Drug Pricing Files are posted
online prior to the start of the calendar
quarter. The performance year 1, quarter
1 MFN Drug Payment Amounts will be
published on a CMS website before the
start of the MFN Model.
Illustrative MFN Drug Payment
Amounts per billing unit are listed in
Table 6 by HCPCS code. For this
illustration, we partnered with ASPE,
which purchases licenses to data
products maintained by IQVIATM
(formerly known as Quintiles-IMS).
IQVIA’s proprietary MIDAS data set 61 is
a widely used source of drug sales and
volume data.
Service-Part-B-Drugs/McrPartBDrugAvgSalesPrice/
index.html.
61 https://www.iqvia.com/solutions/
commercialization/brand-strategy-andmanagement/market-measurement/Midas.
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MIDAS data contain estimates of drug
sales (called ‘‘Monetary Value ’’ within
the MIDAS data set) and volume (called
‘‘Quantity’’ within the MIDAS data set)
that are based on audits of drug
transactions in different countries and
distribution channels (for example,
retail pharmacies and hospitals). The
audits underlying the MIDAS data
collect sales and volume information at
the ex-manufacturer (that is, prices as
drugs are sold by manufacturers), exwholesaler, and/or retail levels. IQVIA
applies a set of country- and channelspecific assumptions on markups
between manufacturer, wholesale, and
retail prices to estimate ex-manufacturer
and retail sales. Sales information
within the database is stated in local
and U.S. currency, as of the transaction
date or current date, and are expressed
as ex-manufacturer, trade, and public
(retail) sales.62 MIDAS uses a variable
sales are: Manufacturer
Selling Price or Wholesaler Purchasing Price or
Price to Wholesaler (PTW). Trade sales are:
Wholesaler Selling Price or Pharmacy Purchase
Price or Price to Chemist (PTC). Public (retail) sales
are: Pharmacy Selling Price or Consumer Purchase
Price or Price to the Public (PTP).
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62 Ex-manufacturer
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called ‘‘Molecule List’’ (also called
‘‘Moleculelist’’) which identifies
scientific and nonproprietary names for
drug and biological products. Users
extract data from the MIDAS database
by selecting report filters, which are
values for various data fields included
in the database, such as ‘‘Molecule List’’
and ‘‘NFC123’’ (or ‘‘New Form Code,’’ a
3-digit code which identifies the dosage
form 63). The database has a standard
method for identifying drugs within the
U.S. and across countries, and a
standard method for identifying drug
forms. MIDAS data is updated monthly
and retains up to 12 years of history.
CMS obtained a MIDAS data extract
of available 2019 international drug
pricing information for the included
countries for the MFN Model drugs for
performance year 1 from ASPE. After
identifying the MFN Price for each drug,
we applied the phase-in formula for
performance year 1 (75 percent of the
applicable ASP and 25 percent of the
MFN Price) and applied the exceptions
in § 513.210(d) when no international
63 For more information on the New Form Codes
see: https://www.ephmra.org/classification/newform-codes/.
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drug pricing information was available
in the MIDAS data. In Table 6, the
illustrative MFN Prices, calculated
using available international drug
pricing sales and volume information at
the ex-manufacturer level, represent the
lowest of the GDP-adjusted countrylevel prices available in the single data
source we used. For a complete
discussion of how CMS used
international drug pricing information
available through IQVIA and CMS data
to calculate the illustrative applicable
ASPs, MFN Prices, and MFN Drug
Payment Amounts displayed in Table 6,
we refer readers to the supplemental
documentation available on the MFN
Model website.64 We also refer readers
to the Medicare Part B Drug Spending
Dash board 65 that can be used to search
for brand name or generic name; search
results present certain manufacturer
information when available.
BILLING CODE 4120–01–P
64 See: https://innovation.cms.gov/initiatives/
most-favored-nation-model/.
65 See: https://www.cms.gov/Research-StatisticsData-and-Systems/Statistics-Trends-and-Reports/
Information-on-Prescription-Drugs/MedicarePartB.
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We note that, as codified in
§ 513.210(d)(5), and described in section
III.E.10. of this IFC, the MFN Drug
Payment Amount will not exceed the
non-model drug payment amount for
line items submitted with the JG
modifier (or any successor modifier
used to identify drugs purchased under
the 340B program) after removing any
add-on amount, if applicable.
8. Timing of Data and MFN Drug
Payment Amount Calculations
As discussed in section III.E.4. of this
IFC, we will calculate the MFN Drug
Payment Amounts on a calendar quarter
basis using the most recent ASP and
correlated international drug pricing
information (that is, data from the
highest level of hierarchy available).
Under the reporting requirements
outlined in section 1927(b)(3)(A)(iii),
manufacturers that report ASPs are
required to submit them to CMS no later
than 30 days after the last day of the
previous quarter. CMS uses these data to
calculate the ASP-based Medicare
payment amounts for the next calendar
quarter. As a result, there is a twoquarter lag between the time when sales
reflected in the ASP occur and the time
when these sales become the basis for
Medicare payment amounts.
We will use international drug pricing
information from the same time period
(that is, the same calendar quarter), if
available in accordance with the
hierarchy specified in § 513.140(c)(3), in
order to align information across the
ASP Drug Pricing files and the data
sources for international drug pricing
information that we will use. This
approach will consistently correspond
to the two-quarter lag used for the ASP
pricing files when an international drug
pricing information data source at the
highest level of the hierarchy specified
in § 513.140(c)(3) is available. Table 7
illustrates how the information we will
use to calculate the MFN Drug Payment
Amounts for each calendar quarter
during performance year 1 using data
from the applicable ASP calendar
quarter will align when an international
drug pricing information data source at
the highest level of the hierarchy
specified in § 513.140(c)(3) is available.
We will use the same approach for each
performance year.
TABLE 7—ALIGNMENT OF PERFORMANCE YEAR CALENDAR QUARTERS FOR ASP AND MFN PRICE DATA BASED ON
JANUARY 2021 MODEL START
1
1
1
1
Performance year
Performance year calendar
quarter
ASP pricing file for calendar
quarter
.................................
.................................
.................................
.................................
2021,
2021,
2021,
2021,
2021,
2021,
2021,
2021,
Quarter
Quarter
Quarter
Quarter
1
2
3
4
..................
..................
..................
..................
Quarter
Quarter
Quarter
Quarter
1
2
3
4
..................
..................
..................
..................
Applicable ASP calendar
quarter
2020,
2020,
2021,
2021,
Quarter
Quarter
Quarter
Quarter
3
4
1
2
..................
..................
..................
..................
MFN price for calendar
quarter*
2020,
2020,
2021,
2021,
Quarter
Quarter
Quarter
Quarter
3
4
1
2
*When an international drug pricing information data source at the highest level of the hierarchy specified in § 513.140(c)(3) is available.
For example, for the initial
calculations to calculate payment
amounts for the start of the MFN Model
on January 1, 2021, the beginning of the
first calendar quarter in 2021, we will
use the January 2021 ASP Pricing File
(which will be based on manufacturers’
ASP for the third quarter of 2020, from
July 1, 2020, to September 30, 2020) and
international drug pricing information
for the third quarter of 2020, from July
1, 2020, to September 30, 2020. For each
subsequent calendar quarter for a
performance year, the MFN Drug
Payment Amount will be established by
calculating the MFN Price based on
more recent international drug pricing
information, using data for the
applicable ASP calendar quarter, if
available, as illustrated in Table 7, and
calculating the MFN Drug Payment
Amount.
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9. Adjustments to Phase-In Formula and
Incentives for Manufacturers To
Address Rising U.S. Drug Prices
In response to the October 2018
ANPRM, we received several comments
asking that we consider including
model design features to address
potential spillover effects and costshifting to the commercial market and
Medicare payment outside of the model
geographic area. The commenters
requested that CMS carefully consider
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the potential impacts of a potential
model on other markets—including the
potential for cost-shifting to other
segments of the Medicare program, the
Medicaid program, and the commercial
market. The commenters recommended
that in order to avoid unintended
consequences and cost-shifting, CMS
should closely monitor prices for
included drugs and consider additional
policies or actions if drug prices in other
markets rise above certain pricing
thresholds (for example, above the
Consumer Price Index (CPI) or
inflation).
We appreciate these concerns, as it is
possible that, in response to the MFN
Model, manufacturers may take steps to
increase U.S. prices outside of the MFN
Model, such as in the commercial and
Medicare Advantage markets, which
may be seen in increases in
manufacturers’ ASPs. In response to the
concerns expressed in the October 2018
ANPRM comments and to minimize the
possibility of a spillover impact on
beneficiaries outside of the MFN Model,
we will make adjustments to the phasein formula in order to mitigate costshifting in the market and incentivize
manufacturers of MFN Model drugs to
maintain stable ASPs of MFN Model
drugs to minimize the potential for
spillover impacts. In addition to
creating spillover impacts, rapid
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increases in ASP that outstrip not only
U.S. inflation but also changes in
international prices over time would
reduce our ability to test the phase-in of
the MFN Price over time, as the MFN
Price’s contribution to the MFN Drug
Payment Amount could be obscured by
a significant increase in the MFN Model
drug’s ASP.
As discussed in section III.E.5. of this
IFC, we will phase-in the MFN Prices to
allow MFN participants time to adjust to
the MFN Model payment amounts and
processes. Calculating the MFN Prices
and MFN Drug Payment Amounts each
calendar quarter will allow
manufacturers to address the large
difference between prices in the U.S.
and in other countries for MFN Model
drugs during the course of the MFN
Model and serves as an incentive for
manufacturers to refrain from raising
U.S. prices faster than a reasonable
inflation allowance. Furthermore, as
discussed in section III.M. of this IFC,
we are waiving requirements of section
1847A in order to exclude units of MFN
Model drugs from the calculation of the
manufacturer’s ASP. However, if these
incentives prove to be insufficient to
deter manufacturers from raising U.S.
prices for MFN Model drugs faster than
a reasonable inflation allowance, we
will adjust the calculation of the MFN
Drug Payment Amount by adjusting the
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phase-in formula for MFN Model drugs
where such concerns are observed.
Specifically, to preserve the integrity
of the model test as described
previously, we will make an adjustment
to the phase-in formula for an MFN
Model drug if the applicable ASP or
monthly U.S. list price (defined as
Wholesale Acquisition Cost (WAC)
available in a U.S. drug pricing
compendium or if WAC is not available,
other available list prices, such as
Average Wholesale Price (AWP)
available in a U.S. drug pricing
compendium) increases faster than both
inflation and the MFN Price. CMS will
accelerate the phase-in of the MFN Price
by 5 percentage points at the next
quarterly update for each MFN Model
drug with: (1) A greater cumulative
percentage increase in either the
applicable ASP 66 or any monthly U.S.
list price for any of the NDCs assigned
to the MFN Model drug’s HCPCS code
compared to the cumulative percentage
increase in the Consumer Price Index
for All Urban Consumers (CPI–U) 67
based on all items in U.S. city average
and not seasonally adjusted; and (2) a
greater cumulative percentage increase
in either the applicable ASP or any
monthly U.S. list price for any of the
NDCs assigned to the MFN Drug’s
HCPCS code compared to the
cumulative percentage increase in the
MFN Price. To apply these conditions
for an MFN Model drug, we will
identify the cumulative percentage
increase from a baseline to the
applicable ASP calendar quarter. For all
MFN Model drugs with an applicable
ASP for the first quarter of performance
year 1, we will set the baseline as the
ASP calendar quarter for the applicable
ASP for the first quarter of performance
year 1 (that is, the third calendar quarter
of 2020 (July 2020 through September
2020)). For all MFN Model drugs that do
not have an applicable ASP for the first
quarter of performance year 1 (for
example, a drug that is first marketed in
the U.S. after the start of the model), the
baseline will be the ASP calendar
quarter for the first applicable ASP
based on the manufacturer’s average
sales price for that MFN Model drug
that occurs after the third quarter of
2020. For example, the baseline for an
MFN Model drug with its first
applicable ASP based on the
manufacturer’s average sales price
occurring in the second quarter of
performance year 1 (that is, April 2021
66 We note that the manufacturers’ ASPs will be
based on non-model sales only as codified in
§ 513.600(b) and as discussed in section III.M. of
this IFC.
67 All references to CPI–U are based on all items
in U.S. city average and not seasonally adjusted.
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through June 2021) will have a baseline
of the fourth calendar quarter of 2020
(October 2020 through December 2020).
The cumulative percentage change
will be calculated from the end of the
baseline to the end of the applicable
ASP calendar quarter. We will apply the
adjustment to the phase-in formula
similarly for all MFN Model drugs
regardless of when the MFN Model drug
is added to the MFN Model Drug
HCPCS Codes List.
Further, if both conditions are not
met, such as the cumulative percentage
increase in any monthly U.S. list prices
for the NDCs assigned to the MFN
Drug’s HCPCS code outpaces the
cumulative percentage increase in CPI–
U but is less than the cumulative
percentage increase in the MFN Price,
then the trigger conditions will not be
met and the phase-in formula will not
be accelerated. If the cumulative
percentage change in the CPI–U or MFN
Price is negative, we will use zero as the
cumulative percentage increase in the
CPI–U or MFN Price, as applicable, for
the relevant quarter.
We will accelerate the phase-in
formula by 5 percentage points as we
believe this amount strikes a balance
between moving the MFN Drug Payment
Amount more quickly toward the MFN
Price while still retaining the stepwise
nature of the phase-in. As an example,
in the case that both trigger conditions
are met for an MFN Model drug during
the applicable ASP calendar quarter for
the second quarter of performance year
1, the phase-in formula would be 70
percent applicable ASP and 30 percent
MFN Price for that quarter and
remaining quarters in performance year
1, assuming both trigger conditions are
not met in the ASP calendar quarters for
the third and fourth quarter of
performance year 1.
We will apply the acceleration of the
phase-in formula for each calendar
quarter of the MFN Model where both
trigger conditions are met. That is, for
an MFN Model drug that is subject to
the accelerated phase-in of the MFN
Price, we will further accelerate the
phase-in of the MFN Price by an
additional 5 percentage points at the
next quarterly update if the cumulative
percentage increase in the applicable
ASP or any of the monthly U.S. list
prices for the NDCs assigned to the MFN
Model drug’s HCPCS code continues to
be greater than the cumulative
percentage increase in the CPI–U and
MFN Price. In the previous example, if
both of the trigger conditions were met
for the same MFN Model drug during
the applicable ASP calendar quarter for
quarters 3 and 4 of performance year 1,
the phase-in formula would be 65
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percent applicable ASP and 35 percent
MFN Price for quarter 3 of performance
year 1, and 60 percent applicable ASP
and 40 percent MFN Price for quarter 4
of performance year 1. The accelerated
phase-in of the MFN Price will not be
reversed, but will remain in place for
the duration of the model performance
period for that drug, even if the
manufacturer lowers its ASP and U.S.
list prices after the accelerated phase-in
is in effect.
Further, after the full phase-in of the
MFN Price is reached, if both of the
trigger conditions are met, there will be
a decrease in MFN Model Drug Payment
Amount equal to the largest difference
in the cumulative percentage increase in
the applicable ASP or any of the
monthly U.S. list prices for the NDCs
assigned to the MFN Model drug’s
HCPCS code compared to the
cumulative percentage increase in the
CPI–U and in the MFN Price. This
additional adjustment will lead to the
affected drug’s MFN Drug Payment
Amount falling below the MFN Price for
that drug. For example, for an MFN
Model drug, if 100 percent of the MFN
Price was already applied in the
calculation of the MFN Model Drug
Payment Amount for a quarter and its
applicable ASP cumulatively increased
by 14 percent, the largest cumulative
percentage increase of any of the
monthly U.S. list prices for the NDCs
assigned to the HCPCS code was 13
percent, the CPI–U cumulatively
increased by 12 percent, and the MFN
Price cumulatively increased by 11
percent, we would reduce the MFN
Drug Payment Amount for the quarter
(in this case, previously established as
to equal the MFN Price) by 3 percent
(that is, the difference between 14 and
11) of the MFN Price.
Any such additional adjustment will
apply for the duration of the model
performance period, unless a larger
additional adjustment is triggered. As
with the adjustment before the full
phase-in is reached, we will update the
calculation for the additional
adjustment for each additional calendar
quarter of the model. That is, for an
MFN Model drug that is subject to the
additional adjustment of the MFN Price,
each calendar quarter thereafter, we will
calculate the largest difference between
the cumulative percentage increase in
the applicable ASP or any of the
monthly U.S. list prices for the NDCs
assigned to the MFN Model drug’s
HCPCS code and the cumulative
percentage increase in CPI–U and in
MFN Price and increase the additional
adjustment if the result of the updated
calculation results in a larger additional
adjustment. CMS will not reduce the
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additional adjustment based on the
results of the updated calculation. We
believe this policy will serve as a strong
incentive for manufacturers to avoid
taking steps that could cause spillover
impacts and will help to address
commenters’ concerns.
10. Limitation on MFN Drug Payment
Amount To Protect Beneficiaries
To avoid potentially increasing
beneficiary cost-sharing or coinsurance,
we are codifying in § 513.210(b)(6) to
compare the MFN Price to the
applicable ASP in order to ensure that
beneficiaries are always paying the
lowest amount of coinsurance available.
If the applicable ASP is less than the
MFN Price, we will establish the MFN
Price as equal to the applicable ASP. In
addition, in § 513.210(a), we are
codifying that the allowed MFN Drug
Payment Amount will not exceed the
billed amount on the claim for the MFN
Model drug. In addition, to maintain
beneficiary protections for all claims
paid under the OPPS, we are codifying
in § 513.210(d)(4) that the MFN Drug
Payment Amount cannot exceed the
non-model drug payment amount for
line items submitted with the JG
modifier (or any successor modifier
used to identify drugs purchased under
the 340B program) after removing any
add-on amount, if applicable. We will
apply this limitation to line items
submitted with the JG modifier. We
refer readers to the Calendar Year (CY)
2021 OPPS/ASC Notice of Proposed
Rulemaking (CMS–1736–P) 68 (85 FR
48880) for a discussion of CMS’s
proposal for CY 2021 and subsequent
years to pay for drugs acquired under
the 340B program at ASP minus 34.7
percent, plus an add-on of 6 percent of
the product’s ASP, for a net payment
rate of ASP minus 28.7 percent based on
the results of the Hospital Acquisition
Cost Survey for 340B—Acquired
Specified Covered Drugs. If CMS
finalizes the proposed OPPS payment
policy to pay for drugs acquired under
the 340B program at ASP minus 34.7
percent, plus an add-on of 6 percent of
the product’s ASP, the MFN Drug
Payment Amount for an MFN Model
drug furnished by an MFN participant
and billed with the JG modifier will be
capped at ASP minus 34.7 percent. In
such cases, the MFN participant will
also receive the per-dose add-on
payment amount described in section
III.F. of this IFC.
In the CY 2021 OPPS/ASC Notice of
Proposed Rulemaking, CMS proposed in
the alternative to continue its current
68 https://www.govinfo.gov/content/pkg/FR-202008-12/pdf/2020-17086.pdf.
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policy of paying ASP minus 22.5
percent for 340B-acquired drugs. If CMS
finalizes this alternative proposal, the
MFN Drug Payment Amount for an
MFN Model drug furnished by an MFN
participant and billed with the JG
modifier will be capped at ASP minus
22.5 percent (85 FR 48890). In such
cases, the MFN participant will also
receive the per-dose add-on payment
amount described in section III.F. of this
IFC.
11. Method for Establishing MFN Drug
Payment Amounts for Drugs Added to
the MFN Model
We will add annually any top 50
drugs that are not already included on
the MFN Model Drug HCPCS Codes
List, after taking the exclusions in
§ 513.130(b) into account. In accordance
with§ 513.210, we will calculate the
MFN Price that will apply to drugs that
are added to the list of MFN Model
drugs and the applicable phase-in
formula for a given performance year
and adjustments will apply. We will
apply the applicable phase-in formula
for drugs that are added to the MFN
Model Drug HCPCS Codes List, in order
to simplify and maintain consistent
payment policies for all MFN
participants and MFN Model drugs. For
example, for a drug added as an MFN
Model drug for performance year 2, the
phase-in formula will be a blend of 50
percent of the ASP and 50 percent of the
MFN Price for the drug. Thus, Medicare
Part B drugs that will be added to the
MFN Model Drug HCPCS Codes List for
performance year 2 and beyond will
have an MFN Drug Payment Amount
that will start more heavily based on the
MFN Price than drugs that were
included in earlier performance years.
We believe this approach is appropriate
because the MFN Model seeks to test a
new payment methodology that takes
into account the discounts that other
countries enjoy and delaying the phasein of the MFN Price for drugs that will
be added to the MFN Model Drug
HCPCS Codes List for performance year
2 and beyond will not allow CMS to
fully evaluate the model payment test
for such drugs during the model
performance period.
For drugs added to the MFN Model
Drug HCPCS Codes List in a later
performance year, this approach could
result in a more significant change in
payment for the drug upon entry to the
model compared to drugs that are
included from the beginning of the
model. Although there is the potential
for a larger change in payment for drugs
that are added later in the model, we
believe that it is necessary to maintain
the same phase-in for all included drugs
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to enable us to test the full phase-in of
the MFN Price by performance year 4.
We also believe that MFN participants
are aware of which separately payable
Medicare Part B drugs have high annual
spending and therefore will have a basis
for assessing which drugs that are not
on the MFN Model Drug HCPCS Codes
List in performance year 1 are more
likely be added to the MFN Model Drug
HCPCS Codes List in a later
performance year. For future years, we
seek comment on whether additional
information that CMS could provide
would be helpful to MFN participants
for their planning purposes, for example
drug utilization reports developed
through the model monitoring activities
that CMS could make available on the
model website.
12. Payment Exceptions for MFN Model
Drugs in Short Supply
Rather than broadly excluding drugs
that are in short supply from the model,
we will keep MFN Model drugs in the
model while they are in short supply,
but revert the MFN Drug Payment
Amount to the applicable ASP, which
could be the amount determined under
section 1847A(e) of the Act if the
conditions set forth in that provision are
met, beginning with the first day of the
next calendar quarter after the date on
which the MFN Model drug is reported
as ‘‘Currently in Shortage’’ by FDA, as
available on these websites: https://
www.accessdata.fda.gov/scripts/
drugshortages/ and https://
www.fda.gov/vaccines-blood-biologics/
safety-availability-biologics/cberregulated-products-current-shortages,
and continuing for subsequent calendar
quarters as warranted. Once the MFN
Model drug is no longer reported as
‘‘Currently in Shortage’’ by FDA, the
MFN Model payment will resume the
first day of the next quarter after the
date on which it is no longer reported
in shortage. For example, as noted in
section III.D.2. of this IFC, one of the
HCPCS codes with high aggregate 2019
Medicare Part B total allowed charges
(J1569, Gammagard liquid infusion)
represents a drug that is currently on the
FDA shortages list. If this HCPCS code
were to be included on the MFN Model
Drug HCPCS Codes List and remain on
the FDA shortages list, the MFN Drug
Payment Amount will be the applicable
ASP until the first day of the next
quarter of the model performance period
after it is no longer reported as
‘‘Currently in Shortage’’ by FDA.
However, we note that we are excluding
HCPCS codes that describe intravenous
immune globulin from the MFN Model
Drug HCPCS Codes List as discussed in
section III.D.2 of this IFC.
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13. Payment of Blood Clotting Factor
Furnishing Fee Under the MFN Model
Currently, payment for the blood
clotting factor furnishing fee under 42
CFR 410.63(c) is made along with
payment for the blood clotting factor.
Under the MFN Model, a HCPCS code
that is used to bill for a blood clotting
factor may be an MFN Model drug if
such HCPCS code is included on the
MFN Model Drug HCPCS Codes List. To
maintain the current payment approach
for the blood clotting factor furnishing
fee during the MFN Model, we are
codifying in § 513.210(e), that when
applicable, the blood clotting furnishing
fee under § 410.63(c) will be payable
along with the MFN Drug Payment
Amount. We believe this approach will
eliminate the need to establish different
billing instructions for MFN Model
drugs that are blood clotting factors.
F. MFN Model Alternative Add-On
Payment
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1. Overview of the Alternative Add-On
Payment
In the October 2018 ANPRM, we
sought public comment on testing an
alternative add-on payment to the
current system, required by section
1847A of the Act, under which
Medicare Part B pays a fee based on 6
percent of the ASP of the drug so that
the dollar amount of the add-on
increases with the price of the drug
rather than reflecting the service being
performed. In general, the amount of
add-on realized by providers and
suppliers has been described by
commenters as 4.3 percent as a result of
sequestration.69 In the October 2018
ANPRM, we described our belief
regarding how a potential model could
pay a drug add-on amount that would
be different from the current drug addon amount. We sought public comment
on potential ways to structure the
69 Stakeholders have reported that the add-on
percentage is slightly further reduced when the
OPPS beneficiary cost-sharing limitation applies.
Further, we note that current payments under the
OPPS for certain drugs when the drug is acquired
under the 340B program are made based on ASP–
22.5 percent and are not considered to include a
drug add-on payment amount. We refer readers to
to the Calendar Year (CY) 2021 OPPS/ASC Notice
of Proposed Rulemaking (CMS–1736–P) (85 FR
48880) for a discussion of CMS’s proposal for CY
2021 and subsequent years to pay for drugs
acquired under the 340B program at ASP minus
34.7 percent, plus an add-on of 6 percent of the
product’s ASP, for a net payment rate of ASP minus
28.7 percent based on the results of the Hospital
Acquisition Cost Survey for 340B-Acquired
Specified Covered Drugs. We also refer readers to
the alternative proposal in the CY 2021 OPPS/ASC
Notice of Proposed Rulemaking (85 FR 48890) to
continue the current policy of paying ASP–22.5
percent for 340B drugs and biologicals under the
OPPS.
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alternative add-on, including but not
limited to: An amount based on drug
class, the physician’s specialty, or the
practice’s historical billing patterns,
with a possible bonus pool tied to
clinically appropriate utilization. We
requested feedback on several design
topics, such as how we could best
define and determine the alternative
add-on payment amount, whether CMS
should develop an encounter-based or
monthly add-on payment approach, and
potential inclusion of a quality bonus
pool to incentivize evidence-based care.
We stated that our goal was to maintain
relative stability in provider and
supplier revenue through an alternative
drug add-on payment for furnishing
drugs that removes the current
percentage-based drug add-on
payments.
In response to the October 2018
ANPRM, we received feedback from a
number of stakeholder groups on the
structuring of an alternative add-on
payment. Overall, there was no
consensus on the best approach to
designing an alternative add-on
payment, though several commenters
supported calculating the alternative
add-on payment in such a way that
model participants would be held
harmless. Some commenters supported
the idea of testing an alternative add-on
payment that is not tied to increases in
drug prices over time, with one
commenter noting that this could
promote revenue stability. One
commenter noted an approach that
varies the alternative add-on payment
between different drugs would risk
creating perverse incentives in
prescribing decisions between
alternative treatment options. Several
commenters supported a flat fee with
more than one tier. Several commenters
expressed concern about linking a
bonus pool to prescribing lower cost
drugs. One commenter opposed
reducing the add-on amount to allow for
a bonus pool.
After considering the comments we
received, we were persuaded that
potential model requirements to qualify
for a modest quality bonus would be
challenging and may be burdensome for
MFN participants to implement and
adhere to consistently for all MFN
beneficiaries, and would add potential
financial risk for MFN participants,
which is not necessary for purposes of
testing an alternative add-on payment
approach under the MFN Model. Thus,
we are not including a quality bonus in
the MFN Model. We were also
persuaded that the alternative add-on
should be designed in as straightforward
a manner as possible to minimize
administrative burden for MFN
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participants and potential confusion for
beneficiaries.
We will pay MFN participants a
single add-on payment amount per dose
of an MFN Model drug; this payment
will not vary based on the amount of
drug furnished in a dose, billing units
billed on the claim line, or by MFN
participant or specialty. The goals for
the model’s approach to the alternative
add-on payment are to test an
innovative way to pay the add-on
portion of the drug payment, boost addon revenue for MFN participants on
average based on historical overall addon revenue, create an incentive to
encourage appropriate drug utilization
by breaking the link between the
manufacturer’s drug price and the
calculation of the Medicare Part B
payment for the add-on amount, and
remove or reduce the incentive to
furnish higher-cost drugs inherent in the
current methodology.
With the MFN alternative add-on
payment, we will test a single add-on
payment amount that will paid per
dose, where ‘‘dose’’ for the purposes of
the MFN alternative add-on payment is
defined as the number of HCPCS billing
units reported on a claim line 70 (also
called service line or line item). We are
codifying this alternative add-on
payment at § 513.220. We will waive
beneficiary cost-sharing for the add-on
payment. As such, the add-on approach
will test a separate standardized add-on
payment amount per dose that is not
tied to the Medicare Part B payment
amount for a drug. We will start with an
amount that is calculated based on
6.1224 percent of historical applicable
ASPs for 2019 final action claim lines
for the selected MFN Model drugs for
the beginning of performance year 1 as
further described in § 513.220, trended
forward using an inflationary
adjustment for the start of performance
year 1. With this approach, the per-dose
add-on payment amount will be
calculated once at the beginning of the
model and will not be recalculated as
the MFN Model Drug HCPCS Codes List
changes. For each calendar quarter
thereafter, beginning with performance
year 1, quarter 2, we will update the
per-dose add-on payment amount using
an inflation factor.
For the MFN Model drugs for the
beginning of performance year 1 that are
biosimilar biological products, we will
use 6.1224 percent of the historical
applicable ASPs for the reference
biological product in the calculation of
the per-dose add-on amount rather than
6.1224 percent of the historical
70 An exception is when a claim line is billed
with the modifier JW, indicating discarded drug.
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applicable ASPs for the biosimilar
biological product to align with the
determination of the add-on amount to
such products under section 1847A.
Based on the performance year 1 MFN
Model Drug HCPCS Codes List in Table
2, this applies to Q5111 (Injection,
udenyca 0.5 mg).
We selected 6.1224 percent because
that amount results in an add-on pool
that will allow MFN participants to
realize, on average, a 6 percent add-on
per dose after sequestration, which
generally applies.71 In the absence of
actual drug acquisition costs for eligible
providers and suppliers, we believe it is
appropriate to use an amount for the
add-on pool that represents, on average,
a 40 percent increase compared to 4.3
percent of ASP in use in the baseline
period to achieve a goal of the model to
provide increased add-on revenue for
MFN participants on average.
2. Per-Dose Add-On Payment Amount
Methodology
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a. Calculation of the Single Per-Dose
Add-On Payment Amount
In § 513.220(b), we specify how we
calculated a single per-dose add-on
payment amount for the start of the
MFN Model. Using 2019 historical
claims data, we calculated a per-dose
add-on payment amount by applying
the applicable ASP (that is, the payment
amount determined in accordance with
section 1847A of the Act for a quarter
minus the applicable add-on
percentage) to the identified 2019
claims lines, based on the calendar
quarter in which the claim’s date of
service falls, which corresponds to the
manufacturer-reported ASPs from two
calendar quarters prior, with an
exception for biosimilar biological
products as described previously. We
used all 2019 Medicare Part B FFS
claims lines for separately paid drugs
(by HCPCS code) included on the MFN
Model HCPCS Codes List for the
beginning of performance year 1 that
were furnished by eligible Medicareparticipating providers and suppliers
(that is, entities that are eligible to be an
MFN participant). We excluded claims
submitted by excluded providers and
suppliers described in § 513.100(c)
(such as CAHs, and cancer hospitals) as
well as certain claims described in
§ 513.100(d) (such as claims processed
by the DME MAC), as applicable in
2019, as well as claims where Medicare
71 Note
that Section 3709 of the Coronavirus Aid,
Relief, and Economic Security (CARES) Act
temporarily suspends Medicare sequestration from
May 1, 2020 to December 31, 2020. Available at:
https://www.govinfo.gov/content/pkg/BILLS116hr748enr/pdf/BILLS-116hr748enr.pdf.
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was not the primary payer. We included
all relevant claim lines for an MFN
Model drug with an allowed charge
greater than zero dollars in the
calculation. As we used nearly all 2019
claims for drugs included on the MFN
Model HCPCS Codes List for the
beginning of performance year 1
furnished from any eligible Medicareparticipating provider or supplier, we
believe that one calendar year provided
sufficient data for purposes of
calculating a single per-dose add-on
payment amount. Calendar year 2019
represents the same baseline year that
we used to select the MFN Model drugs
for the beginning of performance year 1,
as identified in Table 2.
Once all relevant 2019 claim lines
were identified for each drug (by HCPCS
code) on the MFN Model HCPCS Codes
List for the beginning of performance
year 1, we multiplied the number of
HCPCS units billed on each claim line
by 6.1224 percent of the 2019 applicable
ASP (which we define as the payment
amount determined in accordance with
1847A of the Act less the applicable
add-on percentage for the MFN Model
drug’s HCPCS code) for the calendar
quarter that matches the claim line’s
date of service and then summed across
all claim lines for that drug to yield a
total add-on spending amount for that
drug. For biosimilar biological products,
we used the applicable ASP for the
reference biological product.
Then we pooled together the total
add-on spending amounts for all drugs
on the MFN Model HCPCS Codes List
for performance year 1 and the total
number of claim lines for those drugs
(excluding claim lines billed with the
JW modifier). Lastly, we calculated the
per-dose add-on payment amount as the
total pooled add-on spending amount
divided by the total pooled number of
claim lines.
Using the drugs (by HCPCS code)
included on the performance year 1
MFN Model Drug HCPCS Codes List in
Table 2, available 2019 claims data
subject to the exclusions and exception
previously noted, and applicable ASPs
from 2019, we calculated a single perdose add-on payment amount in the
amount of $146.55. This amount
represents the single per-dose add-on
payment amount for a dose of any MFN
Model drug prior to application of the
inflationary factor as described in
section III.F.2.b. of this IFC.
b. Trending the Single Per-Dose Add-On
Payment Amount Forward Each
Calendar Quarter During the MFN
Model
We will trend forward the single perdose add-on payment amount each
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calendar quarter during the MFN Model
to account for inflation over time by
using a cumulative inflationary factor as
described in this section of this IFC. We
will not use changes in ASP or MFN
Drug Payment Amount to trend forward
the single per-dose add-on payment
amount to align with our intention to
test the removal of the link between a
drug’s add-on payment and its price.
As specified in § 513.220(b)(7), after
calculating the single per-dose add-on
payment amount, we multiplied the
single per-dose add-on payment amount
($146.55) by an inflationary factor,
which equals the percentage increase in
the CPI–U from the midpoint of the
baseline year (2019) through the first
month of the calendar quarter prior to
the start of the model (that is, the
percentage increase in CPI–U from July
2019 through October 2020). The
resulting per-dose alternative add-on
payment amount for the first calendar
quarter of performance year 1 (January
1, 2021 through March 31, 2021) is
$148.73.
To calculate the per-dose alternative
add-on payment amount for each
subsequent calendar quarter during the
model performance period, as specified
in § 513.220(c), we will multiply the
performance year 1, quarter 1 alternative
add-on payment amount by a
cumulative inflation factor that will
ensure the amount will remain equal to
or greater than the alternative add-on
payment amount calculated for
performance year 1, quarter 1. We will
calculate a cumulative inflation factor as
equal to the percentage increase in the
CPI–U from October 2020 through the
first month after the end of the
applicable ASP calendar quarter. If the
cumulative percentage change in the
CPI–U is negative, we will use an
inflation factor of 1. For example, the
cumulative inflation factor for
performance year 1, quarter 2 (that is,
April 1, 2021 through June 30, 2021)
will be the percentage increase in the
CPI–U from October 2020 through
January 2021. Similarly, the cumulative
inflation factor for performance year 1,
quarter 3 will be the percentage increase
in the CPI–U from October 2020 through
April 2021.
As discussed in section III.G. of this
IFC, MFN participants will use a new
HCPCS code (M1145, MFN drug add-on,
per dose) to bill for and receive the
alternative add-on payment amount for
each dose of an MFN Model drug that
is billed on the claim.
3. Discussion of the Per-Dose Add-On
Payment Approach
The per-dose add-on payment amount
approach will test an alternative way to
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calculate the add-on payment that is not
tied to the sales price of the drug that
is furnished. This approach also aims to
boost add-on revenue, on average, for
MFN participants by setting the perdose add-on payment amount based on
6.1224 percent of historical ASP
payment allowances trended forward for
inflation. However, the impact on MFN
participants will vary based on the MFN
participant’s prescribing patterns,
including the amount and types of MFN
Model drugs they furnish to Medicare
FFS beneficiaries.
Compared with the current add-on
payment policy, on an average per dose
basis based on 2019 historical claims,
the single per-dose add-on approach
will initially decrease add-on payments
for MFN Model drugs with relatively
higher historical applicable ASP-based
payment amounts per dose and increase
add-on payments for MFN Model drugs
with relatively lower historical
applicable ASP-based payment amounts
per dose. Average 2019 historical addon payment amounts per dose for the
MFN Model drugs for performance year
1 ranged from $10.44 to $2,575.47 per
average dose for a drug. Based on 2019
claims, on average, a single per-dose
add-on payment amount, calculated as
described in this IFC and after
sequestration is applied, will represent
an increase in the add-on payment
amount for 70 percent of doses on
average compared to the effective
historical add-on amount of 4.3 percent
of the applicable ASP after
sequestration.
To examine the potential impact of
the single per-dose add-on approach on
MFN participants using 2019 claims
data, we considered the overall
potential change in the add-on payment
amount at the eligible entity level,
specialty level, and type of provider and
supplier. That is, for this entity level
analysis, we grouped 2019 claim lines
for the drugs (by HCPCS code)
identified in Table 2 based on the
provider’s or supplier’s CMS
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Certification Number (‘‘CCN’’) or
Taxpayer Identification Number
(‘‘TIN’’). To examine the potential
impact of the single per-dose add-on
payment amount at the specialty level,
we assigned claims to a specialty
category based on the primary specialty
of the National Provider Identifier (NPI)
associated with the furnishing of the
drug as listed in the Medicare Provider
Enrollment, Chain, and Ownership
System (PECOS). Eligible providers
were assigned to the specialty that was
most frequently associated with their
2019 claims for the drugs (by HCPCS
code) identified in Table 2. We also
used the type of bill to examine the
potential impacts on various types of
providers and suppliers.
These analyses highlight that different
subsets of providers and suppliers will
potentially gain (or lose) under the
single per-dose add-on approach. For
340B covered entities that were paid
under the OPPS during calendar year
2019, the entirety of the alternative addon payment amount represent an
increase in payment when drugs are
acquired under the 340B program. Thus,
we removed these entities from the
following analyses.
To explore the potential entity level
change in the add-on amount for the
single per-dose add-on payment
approach, we assigned each CCN or TIN
to only one specialty based on the
specialty code with the highest total
allowed spending for the entity’s claim
lines, regardless of setting (for example,
hospitals, ASCs, and physician office).
We also assigned each specialty a value
of ‘‘low,’’ ‘‘medium,’’ or ‘‘high,’’ based
on the percentage of its Medicare
revenue that is related to Part B drugs,
such that ‘‘high’’ means the specialty’s
drug revenue is more than 50 percent of
its total Medicare revenue, ‘‘medium’’
means the specialty’s drug revenue is 25
to 50 percent of its total Medicare
revenue, and ‘‘low’’ means the
specialty’s drug revenue is less than 25
percent of its total Medicare revenue.
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Based on the single per-dose add-on
payment amount of $146.55 (prior to the
application of the inflationary factor
that applies during the model) and
using 2019 drug utilization, MFN
participants will fare, on average, 40
percent better overall across all
specialties with the per-dose add-on
payment amount than they did
historically based on 4.3 percent of ASP
after sequestration. Some MFN
participants will see more than a 40
percent increase in revenue related to
the MFN add-on payment amount
compared to their 2019 historical Part B
drug claims, and others will see less
than a 40 percent increase, including
some who will see a reduction in addon revenue. Based on our analysis, in
general, physician practices will be
better off under the per-dose add-on
payment approach than hospital
outpatient departments, and single
specialty practices will be better off than
multi-specialty practices. Table 8 shows
the estimated variation in impacts for
the top specialties by comparing 2019
baseline add-on payments based on 4.3
percent of the applicable ASP with a
post-sequestration single per-dose addon payment amount (that is, for this
comparison, we used the per-dose addon payment amount prior to the
application of the inflationary factor
($146.55) and applied the effects of
sequestration for this comparison). The
Entity-Level Percentage Change By
Percentile portion of Table 8 shows the
distribution of entities based on size of
the difference between their 2019
baseline add-on payments (based on 4.3
percent of the applicable ASP) and the
single per-dose add-on amount (postsequestration). Each row shows the size
of the impact for the given specialty.
The 5th percentile will experience the
largest negative impact whereas the 95th
percentile will experience the largest
positive impact.
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Table 8, all but 9 of the top 35
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specialties (in terms of overall 2019
allowed dollars) impacted by the MFN
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Model will on average see increases in
add-on revenue compared to 4.3 percent
of the applicable ASP with a single
payment amount (the exceptions are
hematology/oncology, medical
oncology, neurology, hematology,
gastroenterology, gynecological/
oncology, infectious disease,
hematopoietic cell transplantation &
cellular therapy, and dermatology). At
the 25th percentile, 57 percent of the
entities will see increased add-on
revenue for the top 35 specialties with
the single per-dose add-on payment
amount; whereas at the 50th percentile,
83 percent of the entities will see
increased add-on revenue for the top 35
specialties with the single per-dose addon payment amount. Please note that
some of the large percentage increases
seen shown in the 95th percentile
column are likely driven by the small
volume of drugs furnished by entities in
this percentile.
We observed that volume is not
consistently associated with whether an
entity will be better or worse off under
the per-dose add-on payment approach
when we look at the single per-dose
add-on amount approach for the top five
specialties in terms of total aggregate
Medicare spending on MFN Model
drugs in 2019: internal medicine,
hematology/oncology, ophthalmology,
rheumatology, and medical oncology.
When we specifically looked at the top,
middle, and bottom of a distribution of
all entities based on how much better or
worse off each entity will be under the
per-dose add-on payment amount
compared to their add-on revenue
(based on their 2019 claims), we found
that entities in the top 5 percent (that is,
those that will do the best) had very low
volume (that is, few claims for these
drugs in 2019 claims). Entities in the
bottom 5 percent (that is, those that will
do the worst) tended to have lower
volume than the middle 10 percent,
though volume was highest in the
bottom 5 percent of entities in the
internal medicine and ophthalmology
specialties. Overall, entities that will be
worse off compared to their add-on
revenue (based on their 2019 claims)
under the per-dose add-on payment
approach tended to furnish more drugs
with higher drug add-on payment
amounts per dose more frequently than
the entities that will be better off. We
estimate that similar impacts will be
experienced across the performance
years unless ASPs for MFN Model drugs
rise faster than inflation, in which case
the overall increase in add-on revenue
compared to non-model add-on revenue
will diminish over time.
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4. Beneficiary Cost-Sharing
Responsibilities
In response to the October 2018
ANPRM, which suggested continuing
beneficiary cost-sharing for the
alternative add-on payment, some
commenters suggested that CMS should
ensure any alternative add-on payment
does not increase out-of-pocket costs for
beneficiaries. Other commenters noted
that an alternative add-on payment
could be confusing to beneficiaries since
currently they pay cost-sharing based on
a single amount, versus separate
amounts, such as the MFN Model Drug
Payment Amount and alternative addon that we are including in the MFN
Model. We appreciate these
commenters’ feedback.
To support reducing out-of-pocket
drug costs and minimizing potential
confusion for MFN beneficiaries related
to the alternative add-on payment
amount, and decreasing administrative
burden for MFN participants, we will
waive beneficiary cost-sharing
(coinsurance and deductible amounts)
on the portion of the allowed MFN
Model Payment amount that is based on
the alternative add-on payment. Under
the MFN Model, the MFN Drug Payment
Amount will be subject to beneficiary
coinsurance and the annual deductible
amount. MFN participants will continue
to collect beneficiary cost-sharing
applicable to the portion of the allowed
payment amount that is based on the
MFN Drug Payment Amount. For the
alternative add-on, Medicare will pay
the entire allowed payment amount that
is based on the alternative add-on
payment to ensure that beneficiaries do
not experience an increase in costsharing under the MFN Model as a
result of testing an alternative add-on
amount. That is, beneficiaries will not
owe any coinsurance or amount for the
annual deductible for the per-dose addon payment amount.
G. Billing and Claims Processing
Approach
We intend to issue model-specific
claims submission instructions that
MFN participants will be required to
follow. Currently, for separately payable
Part B drugs, providers and suppliers
submit separate claim lines for each
drug. Among the information included
in each claim line for the applicable bill
type, providers and suppliers specify
the appropriate HCPCS code to indicate
the drug that was furnished, the number
of billing units to indicate the total
amount of the drug that was furnished,
billing code modifiers as necessary, and
a billing amount (or charge). In general,
providers and suppliers routinely use
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one claim line to bill for a furnished
drug dose, and using billing modifiers
when doing so may be necessary to
comply with billing instructions. In
certain situations, a second claim line
may be necessary to report the amount
of drug that was furnished, for example,
when the number of billing units
necessary to indicate the dosage given
exceeds the character size of the units
field or when appropriately discarded
drug is billed. When applicable, a
separate line item is billed with the
modifier JW to identify the amount of
unused drugs (or biologicals) from
single use vials or single use packages
that was appropriately discarded. The
Medicare claims processing system
calculates payment for the amount of
discarded drug when the modifier JW is
present. MFN participants will be
required to submit a separate claim line
using a new model-specific HCPCS code
(M1145, MFN drug add-on, per dose) to
bill for and receive the alternative addon payment amount for each dose of an
MFN Model drug that is billed on the
claim. The MFN participant will
indicate in the units field of the claim
line with HCPCS code M1145 the
number of doses of a separately payable
MFN Model drug that are billed on the
claim. To do so, the MFN participant
will count the number of claim lines
with a HCPCS code that is included on
the applicable MFN Model Drug HCPCS
Codes List (based on the date of service),
including all claim lines when the
number of billing units necessary to
indicate the dosage given exceeds the
character size of the units field and the
claim has more than one claim line for
such MFN Model drug (we note that this
is expected to be a rare situation), and
excluding the number of claim lines
billed with the JW modifier. This
approach will allow the Medicare
claims processing system to apply the
alternative add-on payment amount for
each dose, and not apply beneficiary
cost-sharing to the alternative add-on
payment amount. MFN participants will
still bill for wastage as they otherwise
would, using a separate claim line and
the JW modifier, and the payment for
such claim lines will be based on the
MFN Drug Payment Amount (the
alternative add-on payment amount is
not applicable to such claim lines).
This billing and claims processing
approach will initiate from the MFN
participant’s billing system and will
establish a clear mechanism for MFN
participants to track when the
alternative add-on amount was billed
and paid. This approach will simplify
Medicare claims processing changes for
the MFN Model. However, this
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approach may increase administrative
burden for MFN participants and
requires MFN participants to count the
number of claim lines for MFN Model
drugs included on a claim, indicate this
number in the units field of the claim
line for the alternative add-on (using
HCPCS code M1145), and submit a
billing amount (or charge) on the claim
line for the alternative add-on. In
addition, the alternative add-on
payment amount will be updated
quarterly. Because Medicare allows the
lesser of the applicable payment amount
or the billed amount, MFN participants
will have to ensure that they submit an
appropriate billing amount (or charge)
for the alternative add-on for the
applicable quarter. Because the same
HCPCS code will be used to bill for the
alternative add-on for all MFN Model
drugs, we believe this approach
minimizes, but does not eliminate, the
additional administrative burden for
MFN participants.
We are waiving program requirements
in section 1833(a)(1)(S), section
1833(a)(1)(G) and section 1833(t) of the
Act, respectively to allow flexibility in
the way in which claims subject to the
MFN Model payment will be processed.
Section 1833(a)(1)(S) of the Act specifies
that the Medicare payment for drugs
and biologicals not paid on a cost or
prospective payment basis is 80 percent
of the lesser of actual charge or the
amount established in section 1842(o) of
the Act. Similarly, section 1833(a)(1)(G)
of the Act specifies that the amounts
paid with respect to facility services
furnished in connection with certain
surgical procedures and with respect to
services furnished to an individual in an
ASC shall be 80 percent of the lesser of
the actual charge for the services or the
amount determined by the Secretary
under such revised payment system.
Section 1833(t) of the Act specifies how
payment under the OPPS is calculated
including beneficiary copayment.
Specifically, we are waiving these
program requirements to the extent
necessary to allow the total allowable
model payment for the service as
specified in § 513.210 and § 513.220
(that is, the sum of the allowed MFN
Drug Payment Amount and the allowed
alternative add-on payment amount)
and to not apply beneficiary costsharing to the alternative add-on
payment amount.
H. Quality Measures
The October 2018 ANPRM stated our
intention to include quality measures as
part of the potential IPI Model, and our
interest in several categories of potential
measures, specifically: patient
experience measures, medication
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management measures, medication
adherence measures, and measures
related to patient access and utilization.
We sought public input on ways to
assess quality of care for purposes of
real-time monitoring of utilization,
hospitalization, mortality, shifts in siteof-service and other important
indicators of patient access and
outcomes, without requiring providers
or suppliers to report additional data.
We received numerous comments in
response to the October 2018 ANPRM
on this topic. Several commenters
expressed concern that testing
alternative payments for Part B drugs in
general may impact beneficiaries’ access
to care and may impact the overall
patient experience of care. Some
commenters requested that any quality
measurement not add burden to model
participants. Some commenters also
discussed the importance of adherence
to nationally recognized clinical
guidelines in treatment decisions,
stating that adherence to nationally
recognized clinical guidelines would
reduce drug spending while also
maintaining and possibly increasing
quality of care.
We appreciate the public feedback on
ways we could structure a model to
enhance and monitor quality of care. In
the MFN Model, we will implement
robust monitoring activities, such as
analyzing claims data, using patient
survey data, and site visits, to identify
any unintended consequences and
ensure that MFN beneficiaries’ access to
medications is not impeded and that
quality of care is preserved or enhanced.
Further, we believe the following
principles are appropriate for a quality
measurement approach for the MFN
Model: (1) Use quality measures for the
purpose of monitoring quality of care
and beneficiary access to treatment and
experience with care; (2) avoid
unnecessary participant reporting
burden as many providers and suppliers
are currently reporting quality measures
to other programs and payers, for
example, the MFN Model should use
claims-based measures where
appropriate; and (3) establish standards
for adding quality measures, if
necessary, during the model. We believe
that this approach will allow CMS to
test the MFN Model’s alternative drug
payment methodology, while creating a
safeguard for beneficiary access and
quality of care, as well as a means to
monitor patient access and quality of
care. We are also sensitive to concerns
regarding adding administrative burden
to MFN participants and beneficiaries
and, thus, seek to minimize burden on
them. As such, in § 513.400(b)(1) we
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will collect only one quality measure,
focused on patient experience, to help
better understand the impact of the
MFN Model on beneficiary access and
quality of care. This survey will be
fielded by CMS to avoid any quality
measure reporting burden for MFN
participants, although there will be
reporting burden on beneficiaries. CMS
will also monitor for quality as outlined
in section III.I.4. of this IFC, including
monitoring access to medications
through rapid analysis of claims data,
using monthly claims extracts that will
provide frequent assessments of
beneficiary access to MFN Model drugs
and that complement existing methods
to receive, assess, and respond to
beneficiary and health care provider
feedback on the MFN Model.
For the patient experience focused
quality measure, we will use a patient
experience survey, which we will field
periodically to a sample of Medicare
beneficiaries, beginning in performance
year 1. The patient experience survey
will be administered to these
beneficiaries by a third party contractor
throughout the model performance
period. A sample of beneficiaries will be
surveyed regarding their experience of
care, access, or other issues they
experienced under the MFN Model, and
we may also sample beneficiaries who
are not in the MFN Model. Beneficiaries
will not be required to complete the
survey.
Survey results will be used to monitor
the impact of the MFN Model on MFN
beneficiaries’ care experience and
potentially to inform educational
materials for MFN participants. As is
outlined in section III.I.4. of this IFC,
claims data will also be monitored to
assess patient access and outcomes.
If during the model the patient
experience of care quality measure and
claims-based monitoring strategies are
found to be insufficient to adequately
measure the quality of care that MFN
beneficiaries are receiving or MFN
participants are providing, CMS may
specify additional measures to monitor
quality. If additional quality measures
are added, they will meet the following
criteria: (1) Additional measures would
be among one or more of the following
categories: Patient experience of care,
patient activation, shared decision
making, adherence, utilization, and
process measures; (2) Additional
measures would not add significant
burden to MFN participants or
beneficiaries; and (3) Additional
measures would utilize an instrument
that CMS has used previously in a
model to adjust payment or for
monitoring or evaluation. We are
codifying the inclusion of the patient
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experience quality measure and its use
as well as the criteria for adding
measures during the MFN Model in
§ 513.400.
I. Beneficiary Protections and
Monitoring Actions
We are interested in enhancing
protections for beneficiaries included in
the MFN Model. In addition to existing
beneficiary protections, we will actively
monitor the MFN Model to ensure it is
operating effectively and meeting the
needs of beneficiaries, providers and
suppliers, and the Medicare program.
We will coordinate with the Medicare
Beneficiary Ombudsman and other
customer facing components to ensure
that any MFN Model-related beneficiary
complaints, grievances, or requests for
information submitted are responded to
in an appropriate and timely manner,
per CMS protocol.
We believe it will also be necessary to
have additional protections in place in
the MFN Model to ensure that
beneficiaries retain their existing rights
and are not harmed by the model test.
Further, we believe it is important for
beneficiaries to know and understand
their rights as beneficiaries who are
receiving care from MFN participants.
We therefore believe it is necessary to
include certain policies regarding
beneficiary choice, appeals, and the
availability of services.
1. Beneficiary Freedom of Choice
A beneficiary’s ability to choose his or
her provider or supplier is an important
principle of Medicare fee-for-service
and is reflected in section 1802 of the
Act. We are codifying in § 513.410(a)
that any MFN participant must not
commit any act or omission, nor adopt
any policy that inhibits a beneficiary
from exercising his or her freedom to
choose to receive care from any
Medicare participating provider or
supplier or any provider or supplier
who has opted out of Medicare. We
believe these provisions are necessary to
ensure the MFN Model does not prevent
beneficiaries from the general rights and
guarantees provided under Medicare.
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2. Appeals Processes and Financial
Hardship Exemption
a. Appeals Processes
In § 513.410(b), we are codifying that
MFN beneficiaries and their assignees
will have access to the existing formal
claims appeals process under 42 CFR
part 405, subpart I. In other words, once
an MFN Model drug is furnished by an
MFN participant to a beneficiary and a
claim is submitted and processed for
payment, that claim will be eligible for
the current Medicare claims appeals
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processes. If a beneficiary receives an
MFN Model drug from an MFN
participant it does not mean that he or
she should lose this right, but instead
this right should necessarily be
applicable to included beneficiaries as it
would be if they were not a part of the
MFN Model.
b. Financial Hardship Exemption
To include financial protection for
physicians and other MFN participants,
specifically those who furnish
substantial amounts of MFN Model
drugs as part of the services they furnish
to Medicare FFS beneficiaries,
especially MFN Model drugs with the
greatest difference between the MFN
Price and the applicable ASP, we are
including a financial hardship
exemption codified in § 513.230. The
financial hardship exemption process
for MFN participants will be available
in the event unintended consequences
arise to ensure access to MFN Model
drugs for MFN beneficiaries and
financial protections for MFN
participants who are unable to obtain
MFN Model drugs at or below the MFN
Model Payment for such drugs and are
significantly affected by their
participation in the MFN Model.
The financial hardship exemption
process will occur independently of
existing Medicare claims processing and
appeals processes. In § 513.230(a), we
codify that a financial hardship
exemption for a performance year may
be granted to an MFN participant by
CMS, in its sole discretion and will not
be subject to appeal, when the
provisions in § 513.230 are met. This
means that a financial hardship
exemption, if granted, will be applied at
the MFN participant level (as defined in
§ 513.2). As further described in this
section of this IFC, a financial hardship
exemption will be limited to cases
where the MFN participant experienced
a financial loss.
Specifically, to be eligible for a
financial hardship exemption, the MFN
participant must submit its request for
a financial hardship exemption to CMS
in accordance with the submission
process that CMS will post on the MFN
Model website prior to October 1, 2021,
and in the form and manner and with
the content that will be specified by
CMS, including without limitation the
requirements specified in § 513.230(b).
Such requests must be submitted to
CMS within 60 calendar days following
the end of the performance year for
which the MFN participant seeks a
financial hardship exemption. The MFN
participant must include the following
in its request for a financial hardship
exemption:
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• Evidence of methods used to obtain
each MFN Model drug that was
furnished by the MFN participant
during the performance year to any
patient;
• Average net acquisition cost for
each MFN Model drug (inclusive of all
on-invoice prices and price reductions,
off-invoice discounts, any adjustments
thereto, and any other price concessions
related to the purchase of the MFN
Model drug) that was furnished by the
MFN participant during the
performance year to MFN beneficiaries;
• Average net acquisition cost for
each MFN Model drug (inclusive of all
on-invoice prices and price reductions,
off-invoice discounts, any adjustments
thereto, and any other price concessions
related to the purchase of the MFN
Model drug) that was furnished by the
MFN participant during the
performance year to patients who were
not MFN beneficiaries;
• Statement of any remuneration
received by the MFN participant from
manufacturers of MFN Model drugs,
wholesalers, and distributors that is not
reflected in the MFN participant’s
average net acquisition costs with a
justification of why such remuneration
should not be treated as a price
concession related to the purchase of an
MFN Model drug;
• Administrative information,
including: MFN participant’s name, TIN
or CCN (as applicable), contact name,
phone number, and email address; and
• The MFN participant’s attestation
that—
++ It experienced a reduction in
Medicare Part B FFS payments for
separately payable drugs on a per
beneficiary basis during the
performance year as compared to the
prior year (that is, the four calendar
quarters immediately preceding the
performance year) due to its inability to
obtain one or more of the MFN Model
drugs at or below the MFN Model
Payments for such drugs during the
performance year;
++ It has not received and will not
receive any remuneration from
manufacturers of MFN Model drugs,
wholesalers, and distributors related to
the purchase of an MFN Model drug
that was furnished by the MFN
participant during the performance year
that is not reflected in the MFN
participant’s submission; and
++ Its submission is true, accurate,
and complete.
In addition, MFN participants must
use a template that CMS will post on the
MFN Model website for submission of
their net acquisition costs for MFN
Model drugs and administrative
information. This template will be
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similar to the template CMS provided
for the 2020 Hospital Survey for
Specified Covered Outpatient Drugs
(SCODs) Average Acquisition Cost.72
The MFN participant will submit the
other required materials to CMS along
with the template.
In § 513.230(c), we codify the
standards that CMS will use to
determine if an MFN participant is
granted a financial hardship exemption.
Specifically, to be eligible for the
financial hardship exemption, we codify
in § 513.230(c)(2)(i) that the MFN
participant must submit a timely,
complete request for a financial
hardship exemption in accordance with
the requirements specified in
§ 513.230(b) that in the sole discretion
of CMS demonstrates all of the
following:
• The MFN Participant exhausted all
reasonable methods to obtain the MFN
Model drugs at or below the MFN
Model Payments for such drugs during
the performance year.
• The MFN participant’s average net
acquisition cost for each MFN Model
drug (including on- and off-invoice
discounts or adjustments) that was
furnished by the MFN participant
during the performance year to patients
who were not MFN beneficiaries was
not less than the MFN participant’s
average net acquisition costs for such
MFN Model drug (including on- and offinvoice discounts or adjustments) that
was furnished by the MFN participant
during the performance year to MFN
beneficiaries.
• Any remuneration the MFN
participant received from manufacturers
of MFN Model drugs, wholesalers, and
distributors that was not reflected in the
MFN participant’s average net
acquisition costs was not a price
concession related to the purchase of an
MFN Model drug.
In addition, in § 513.230(c)(2)(ii), we
are codifying that the agency in its sole
discretion must also determine that the
MFN participant’s excess reduction
amount per beneficiary (as determined
by CMS in accordance with
§ 513.230(d)(6)) is greater than zero.
That is, the MFN participant must have
experienced a reduction in Medicare
FFS allowed charges for separately
payable Medicare Part B drugs on a per
beneficiary basis during the
performance year as compared to the
prior year (that is, the four calendar
quarters immediately preceding the
performance year) that is greater than 25
72 The template for the 2020 Hospital Survey for
Specified Covered Outpatient Drugs (SCODs)
(CMS–10709; OMB 0938–1374) available at: https://
www.cms.gov/Medicare/Medicare-Fee-for-ServicePayment/HospitalOutpatientPPS/index.
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percent of the MFN participant’s total
Medicare Part A and Medicare Part B
FFS allowed charges on a per
beneficiary basis during the prior year.
We are establishing a threshold of 25
percent of the MFN participant’s total
Medicare Part A and Medicare Part B
FFS allowed charges on a per
beneficiary basis as a criterion to qualify
for the financial hardship exemption
because the exemption is designed to be
limited to MFN participants that
experience a significant year-to-year
reduction in total allowed charges as a
result of the MFN Model. We believe
this threshold will protect MFN
participants from significant financial
hardship under the MFN Model while
also preserving the model test of
aligning payment for Medicare Part B
drugs with the lowest international
prices using a phase-in approach.
Incomplete financial hardship
exemption requests will not be
considered by CMS.
In § 513.230(d), we are codifying how
CMS will calculate the MFN
participant’s excess reduction amount
per beneficiary. CMS will calculate the
MFN participant’s excess reduction
amount per beneficiary using available
final action claims data that are
estimated to be more than 90 percent
complete (claims are generally complete
within 2 months after the service
month) where Medicare was the
primary payer, as determined by CMS.
This approach will not include nonclaims based payments or other
transactions, for example, performancebased payment or repayments. CMS will
calculate, for dates of service within the
performance year, the MFN participant’s
total allowed charges for separately
payable Medicare Part B drugs, and the
total number of beneficiaries that had at
least one claim for a service furnished
by the MFN participant with a Medicare
Part A or Medicare Part B allowed
charge greater than $0. Then, CMS will
divide the MFN participant’s total
allowed charges for separately payable
Medicare Part B drugs for dates of
service within the performance year by
the total number of beneficiaries that
had at least one claim for a service
furnished by the MFN participant with
a Medicare Part A or Medicare Part B
allowed charge greater than $0 with a
service date within the performance
year. CMS will repeat this calculation
using the available claims data for the
prior year, to calculate the MFN
participant’s average per beneficiary
total allowed charges for separately
payable Medicare Part B drugs for the
prior year. Then, CMS will subtract the
MFN participant’s average per
beneficiary total allowed charges for
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separately payable Medicare Part B
drugs for the performance year from the
MFN participant’s average per
beneficiary total allowed charges for
separately payable Medicare Part B
drugs for the prior year. This difference
will then be compared to 25 percent of
the MFN participant’s average per
beneficiary total allowed charges for all
Medicare Part A and Part B claims with
dates of service within the prior year,
using subtraction as described in
§ 513.230(d)(6). The latter quantity will
be calculated by identifying 25 percent
of the MFN participant’s total allowed
charges for all Medicare Part A and Part
B claims with dates of service within
the prior year, then dividing this
amount by the total number of
beneficiaries that had at least one claim
for a service furnished by the MFN
participant with a Medicare Part A or
Medicare Part B allowed charge greater
than $0 with a date of service within the
prior year. If the resulting amount,
called the excess reduction amount per
beneficiary, is greater than zero, then
the MFN participant will meet this
eligibility criterion for the financial
hardship exemption.
In § 513.230(e)(1), we are codifying
that if CMS in its sole discretion grants
a financial hardship exemption to an
MFN participant for a performance year,
CMS shall provide to such MFN
participant, a reconciliation payment for
the performance year. To calculate the
reconciliation amount for the MFN
participant, CMS will multiply the
excess reduction amount per beneficiary
by the total number of beneficiaries that
had at least one claim for a service
furnished by the MFN participant with
a Medicare Part A or Medicare Part B
allowed charge greater than $0 with a
service date within the performance
year.
The reconciliation payment amount
will be paid by a CMS contractor using
Medicare Part B funds as soon as
practical after CMS notifies the MFN
participant of CMS’s decision regarding
the MFN participant’s financial
hardship exemption request and the
amount of the reconciliation payment, if
any, to be made to the MFN participant.
In § 513.230(e)(2), we are codifying that
there will be no appeal of the amount
of the reconciliation payment, if any, to
be made to the MFN participant. In
addition, the reconciliation payment
amount will not be subject to
beneficiary cost sharing (including any
deductible or coinsurance) because the
reconciliation payment will not be tied
to specific beneficiary claims,
beneficiaries will have been responsible
for 20 percent cost-sharing on the
allowed payment amounts for the
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Medicare Part B drugs they received
during the performance year, and steps
to seek additional cost-sharing from
beneficiaries would likely cause
significant confusion and burden for
beneficiaries and MFN participants.
We do not foresee that many MFN
participants will qualify for a
reconciliation payment for performance
year 1, because the estimated overall
reduction in Medicare Part B drug
payment during performance year 1 is 7
percent on average. This reflects the
MFN Price phase-in formula in section
III.E.5. of this IFC which will begin with
the MFN Price making up 25 percent of
the MFN Drug Payment Amount and the
alternative add-on payments in section
III.F. of this IFC will represent a 40
percent increase on average for MFN
participants relative to historical
Medicare add-on payments. Given the
financial hardship execption threshold
of 25 percent of the MFN participant’s
total Medicare Part A and Medicare Part
B FFS allowed charges on a per
beneficiary basis in the prior year will
be determined at the entity level, MFN
participants with a high proportion of
their overall Medicare payments related
to MFN Model drugs will be more likely
to qualify for the hardship exemption if
their Medicare Part B drug allowed
charges on a per beneficiary basis
during a performance year were to
decrease significantly compared to the
prior year. MFN participants that are
hospitals will likely have significant
Medicare Part A revenues and
purchasing abilities that will lessen the
likelihood that they will qualify for a
financial hardship exemption based on
their experience in the MFN Model
during performance year 1. Nonhospital MFN participants will be more
likely to potentially qualify in later
performance years.
For future years, we seek comment on
whether an alternative threshold might
better protect beneficiary access to MFN
Model drugs or mitigate impacts on
physicians and other MFN participants
under the MFN Model. For example, we
are interested in whether a uniform
threshold should be applied for all MFN
participants, and whether certain
physician specialties or types of MFN
participants would find the threshold
insufficient in protecting beneficiary
access to MFN Model drugs. For future
rulemaking, we also seek comment on
how CMS could refine the design of the
financial hardship exception to advance
the model goals to reduce program
expenditures and maintain or improve
quality of care.
CMS pledges to maintain
confidentiality of individual financial
hardship exemption requests to the
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extent provided by law. However, CMS
may make public descriptive
information about MFN participants
that are granted a financial hardship
exemption and the extent to which they
were unable to obtain MFN Model drugs
at or below the MFN Model Payment for
such drugs. We do not intend to make
such information available in an
individually identifiable manner.
3. Availability of Services
The MFN Model is designed to test
potential improvements to the delivery
of and payment for healthcare to reduce
Medicare expenditures while preserving
or enhancing the quality of care for
beneficiaries. As such, an important
aspect of testing models is that
beneficiaries must continue to have
access to and receive needed care.
In § 513.410(c), we are codifying that
MFN participants must not take any
action to select or avoid treating
beneficiaries based on their diagnoses,
care needs, income levels, or other
factors that would render them ‘‘at-risk
beneficiaries’’ as that term is defined at
42 CFR 425.20 (‘‘lemon dropping’’). We
will use monitoring to ensure that MFN
participants are complying with this
requirement. We believe that this is a
necessary precaution to protect
beneficiaries against potential
beneficiary selection bias from MFN
participants and ensure that MFN
beneficiaries retain access to medically
necessary treatment.
4. Monitoring and Compliance
Activities
Consistent with other CMS Innovation
Center models, CMS will implement a
monitoring program for the MFN Model
to ensure that the MFN Model is
implemented safely and appropriately.
Given that MFN participants will
receive model-specific payments and
access to payment rule waivers while
participating in the MFN Model, we
believe that enhanced compliance
review and monitoring of MFN
participants is necessary and
appropriate to ensure the integrity of the
MFN Model. In addition, as part of the
CMS Innovation Center’s assessment of
the impact of new models such as the
MFN Model, we have a special interest
in ensuring that model tests do not
interfere with ensuring the integrity of
the Medicare program. Our interests
include ensuring the integrity and
sustainability of the MFN Model and the
underlying Medicare program from both
a financial and policy perspective, as
well as protecting the rights and
interests of Medicare beneficiaries. For
these reasons, as a part of the models
currently being tested by the CMS
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Innovation Center, CMS or its
designee(s) monitors model participants
to assess compliance with model terms
and with other applicable program laws
and policies. We believe our monitoring
efforts help ensure that model
participants are furnishing medically
necessary covered services and are not
falsifying data, increasing program
costs, or taking other actions that
compromise the integrity of the model
or are not in the best interests of the
model, the Medicare program, or
Medicare beneficiaries.
In § 513.420, we are codifying a
framework for conducting compliance
monitoring activities for the MFN Model
that is consistent with the standard
practices in other CMS Innovation
Center models. Under the monitoring
policy at § 513.420(b), MFN participants
will be monitored to assess compliance
with the MFN Model requirements, to
determine the effects of the MFN Model
on MFN beneficiaries, providers,
suppliers, and on the Medicare program
and to facilitate real time identification
and response to potential issues.
Further, under § 513.420(a)(2), an MFN
participant will be required to notify
CMS within 15 calendar days after
becoming aware that the MFN
participant is under investigation or has
been sanctioned by the federal, state, or
local government, or any licensing
authority (including, without limitation,
the imposition of program exclusion,
debarment, civil monetary penalties,
corrective action plans, and revocation
of Medicare billing rights).
In § 513.420(b)(2), we are codifying
that when we are conducting
compliance monitoring and oversight
activities, CMS or our designees will be
authorized to use any relevant data or
information, including without
limitation Medicare claims submitted
for items or services furnished to MFN
beneficiaries. In § 513.420(b)(3), we are
codifying that MFN participants will be
required to cooperate with the model
monitoring and evaluation activities,
comply with the government’s right to
audit, inspect, investigate, and evaluate
any documents or other evidence
regarding implementation of the MFN
Model, and to retain and provide the
government with access to records.
In § 513.420(b)(1), we are codifying
that monitoring activities will include,
but will not be limited to: (1)
Documentation requests sent to the
MFN participant, including surveys and
questionnaires; (2) audits of claims data,
medical records, and other data from the
MFN participant; (3) interviews with
any individual or entity participating in
the MFN Model, including members of
the MFN participant’s leadership,
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management, and staff; (4) interviews
with beneficiaries and their caregivers;
(5) site visits to the MFN participant;
and (6) tracking complaints and appeals.
We believe these specific monitoring
activities, which align with those
currently used in other models being
tested by the CMS Innovation Center,
are necessary in order to ensure
compliance with the terms and
conditions of the MFN Model and to
protect beneficiaries from potential
harms that may result from activities of
an MFN participant, such as attempts to
reduce access to medically necessary
covered services or appropriate drugs.
We anticipate that monitoring of the
MFN Model activities will include
gathering and analyzing data captured
through the Ombudsman’s service, the
evaluation of the MFN Model, the
patient experience survey, and audits of
charts, claims data, medical records,
among other data as available. As
previously noted in this IFC, one
purpose of monitoring and analyzing
these data sources will be to provide
timely information about the effects of
the MFN Model on MFN beneficiaries,
providers, suppliers, and on the
Medicare program, and to facilitate real
time identification and response to
potential issues. We anticipate that
these findings will inform model
oversight and the potential need for
action to address identified issues.
In § 513.420(c), we outline parameters
for site visits. We will require that MFN
participants cooperate in periodic site
visits conducted by CMS or its designee.
Such site visits will be conducted to
facilitate the model implementation.
In order to operationalize this model,
CMS or its designee will provide the
MFN participant with no less than 15
calendar days advance notice of a site
visit, to the extent practicable.
Furthermore, to the extent practicable,
CMS will attempt to accommodate a
request that a site visit be conducted on
a particular date, but that the MFN
participant will be prohibited from
requesting a date that was more than 60
calendar days after the date of the initial
site visit notice from CMS. We believe
the 60-calendar day period will
reasonably accommodate MFN Model
participants’ schedules while not
interfering with the operation of the
MFN Model. Further, we will require
MFN participants to ensure that
personnel with the appropriate
responsibilities and knowledge
pertaining to the purpose of the site visit
be available during any and all site
visits. We believe this is necessary to
ensure an effective site visit and prevent
the need for unnecessary follow-up site
visits.
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Finally, CMS or its designee can
perform unannounced site visits to all
physical locations of MFN participants
at any time to investigate concerns
related to the health or safety of
beneficiaries or other patients or other
program integrity issues,
notwithstanding these provisions.
Further, nothing in part 513 will limit
CMS from performing other site visits as
allowed or required by applicable law.
We believe that, regardless of the model
being tested, CMS must always have the
ability to timely investigate concerns
related to the health or safety of
beneficiaries or other patients, or
program integrity issues, and to perform
functions required or authorized by law.
In particular, we believe that it will be
necessary for us to monitor, and for
MFN participants to be compliant with
our monitoring efforts, to ensure that
they are not denying or limiting the
coverage or provision of medically
necessary covered services to
beneficiaries in an attempt to change the
MFN Model results or their MFN Model
payments, including discrimination in
the provision of services to at-risk
beneficiaries (for example, due to
eligibility for Medicaid based on
disability).
We intend to monitor MFN
participants through any of the
previously described monitoring
activities (such as documentation
requests, audits of claims data, audits of
medical records, etc.) to ensure that
MFN Model drugs are not being
inappropriately billed (for example,
excessive doses or units). We anticipate
that this monitoring activity will
discourage MFN participants from
furnishing smaller and more frequent
doses of MFN Model drugs to
beneficiaries in order to maximize the
alternative add-on payments. If it is
found that an MFN participant has been
engaged in inappropriate billing, then
we will use applicable remedial actions
set forth in § 513.440(a)(2).
We may employ longer-term analytic
strategies to confirm our ongoing
analyses and detect more subtle or hardto-determine changes in care delivery
and beneficiary outcomes. Some
determinations of beneficiary outcomes
or changes in treatment delivery
patterns may not be able to be built into
ongoing claims analytic efforts and may
require longer-term study.
a. Reduced Access
We will monitor claims data from
MFN participants—for example, to
compare MFN participants’ case mix
relative to a pre-model historical
baseline to determine whether complex
patients are being systematically
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excluded. To the extent that the use of
a patient experience survey includes
items focused on access, we will
analyze these data as well to determine
whether MFN beneficiaries continue to
be able to access the right drug at the
right time. We will use these data to
promote transparency and develop an
understanding of the MFN Model’s
effects. We intend to review and audit
MFN participants if we have reason to
believe that they are compromising
beneficiary access to care.
We intend to conduct analyses of
claims data, such as monthly updates
and historic comparisons of trends
including drug utilization, program
spending, and prescribing patterns
(including observing for any shift to
compounded or other categories of
drugs that are not included in the MFN
Model) as well as changes in site of
service delivery, mortality, hospital
admissions, and other indicators present
in claims data. We will monitor
physician visits, days in a hospital, and
other services as part of the thorough
look at how MFN beneficiaries are
receiving care to determine whether any
treatment patterns are changing
systematically. We will use the
monitoring results to detect potential
issues with beneficiary access to care or
potential provider and supplier
payment issues.
b. Quality of Care Monitoring
We anticipate that quality monitoring
activities may include claims and
survey data analytics, site visits,
medical record review, and tracking
patient complaints and appeals. We will
also use the most recent claims data
available to track utilization and
beneficiary outcomes under the MFN
Model. We believe this type of
monitoring is important as we want to
ensure to the greatest extent possible
that patients continue to receive highquality care.
We believe that this set of monitoring
activities will allow us to promptly
identify any unintended consequences
of the MFN Model. We anticipate that
by identifying unintended potential
consequences of the MFN Model, that
we will then be able to determine
methods to address or alleviate those
potential consequences.
c. Remedying Improper Payment
We anticipate that our monitoring
activities may identify instances of
incorrect MFN Model payments. As
such, we are codifying that CMS is
authorized to correct model-specific
payments under § 513.420(d).
Specifically, under this section if CMS
discovers that it has made or received
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an incorrect model-specific payment
under the terms of the MFN Model, then
CMS may make payment to, or demand
payment from, the MFN participant.
Should these monitoring activities
identify a need for additional
protections, we will consider
appropriate action.
d. Compliance With Laws
MFN participants will remain subject
to all existing requirements and
conditions for Medicare participation as
set out in Federal statutes and
regulations and provider and supplier
agreements, unless waived under the
authority of section 1115A(d)(1) of the
Act solely for purposes of testing the
MFN Model. In § 513.420(a)(1), we
therefore require that MFN participants
must comply with all applicable laws
and regulations. We note that a law or
regulation is not ‘‘applicable’’ to the
extent that its requirements have been
waived under section 1115A(d)(1) of the
Act solely for purposes of testing the
MFN Model.
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5. Enforcement Authority and Remedial
Action
We are codifying at § 513.440(b) that
nothing contained in the terms of the
MFN Model or part 513 will limit or
restrict the authority of the HHS Office
of Inspector General (OIG) or any other
Federal Government authority,
including its authority to audit,
evaluate, investigate, or inspect the
MFN participant.
It is necessary for CMS to have the
ability to impose remedial actions to
address non-compliance with the
requirements of the MFN Model and to
ensure that the MFN Model does not
interfere with the program integrity
interests of the Medicare Program. Thus,
in § 513.440(a)(1), CMS may take
remedial action against an MFN
participant if CMS determines, in CMS’
sole discretion, that the MFN
participant—
• Has failed to comply with any
applicable Medicare program
requirement, rule, or regulation;
• Has failed to comply with any of
the terms of the MFN Model, including
applicable requirements of part 513;
• Systematically engaged in the under
delivery or over delivery of an MFN
Model drug;
• Has taken any action that threatens
the health or safety of an MFN
beneficiary or other patient;
• Has undergone a change of control
that presents a program integrity risk;
• Has submitted false data or made
false representations, warranties,
certifications or attestations in
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connection with any aspect of the MFN
Model;
• Has avoided at-risk beneficiaries, as
this term is defined in § 425.20;
• Has avoided patients on the basis of
payer status;
• Is subject to any sanctions or final
actions of an accrediting organization or
a Federal, State, or local government
agency;
• Takes any action that CMS
determines for program integrity reasons
is not in the best interests of the MFN
Model, or the Medicare program, or fails
to take any action that CMS determines
for program integrity reasons should
have been taken to further the best
interests of the MFN Model or Medicare
program;
• Is subject to investigation or action
by HHS (including the HHS Office of
the Inspector General (OIG)) or the
Department of Justice due to an
allegation of fraud or significant
misconduct, including being subject to
the filing of a complaint, filing of a
criminal charge, being subject to an
indictment, being named as a defendant
in a False Claims Act qui tam matter in
which the Federal Government has
intervened, or similar action;
• Is the subject of administrative
enforcement action imposed by CMS; or
• Has failed to demonstrate improved
performance following any remedial
action imposed by CMS.
In § 513.440(a)(2), we are codifying
that if CMS determines that one or more
grounds for remedial action exists, CMS
may take one or more of the following
remedial actions:
• Notify the MFN participant of the
violation.
• Require the MFN participant to
provide additional information to CMS
or its designees.
• Require the MFN participant to
develop and implement a corrective
action plan in a form and manner and
by a deadline specified by CMS.
• Subject the MFN participant to
additional monitoring, auditing, or both.
• Remove the MFN participant from
the MFN Model;
• Recoup model-specific payments.
• Such other action as may be
permitted under the terms of § 513.420.
6. Audits and Record Retention
By virtue of participation in the MFN
Model, MFN participants will receive
model-specific payments and access to
payment rule waivers. We therefore
believe that CMS’ ability to audit,
inspect, investigate, and evaluate
records and other materials related to
participation in the MFN Model is
necessary and appropriate. In order to
expand a phase 1 model tested by the
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CMS Innovation Center, among other
things, the Secretary must first
determine that such expansion would
not deny or limit the coverage or
provision of benefits under the
applicable title for applicable
individuals. Thus, there is a particular
need for CMS to be able to audit,
inspect, investigate, and evaluate
records and materials related to
participation in CMS Innovation Center
models to allow us to ensure that the
model is not denying or limiting the
coverage or provision of benefits for
beneficiaries.
We note that there are audit and
record retention requirements under the
Medicare Shared Savings Program (42
CFR 425.314) and in current models
being tested under section 1115A (such
as under 42 CFR 510.110 for the CMS
Innovation Center’s Comprehensive
Care for Joint Replacement Model).
Building off those existing
requirements, in § 513.430(a), the
Federal Government, including, but not
limited to, CMS, HHS, and the
Comptroller General, or their designees,
have a right to audit, inspect,
investigate, and evaluate any documents
and other evidence regarding
implementation of the MFN Model.
Additionally, in order to align with the
policy of current models being tested by
the CMS Innovation Center, we are
codifying in §§ 513.430(b) and (c) that
MFN participants must—
• Maintain and give the Federal
Government, including, but not limited
to, CMS, HHS, and the Comptroller
General, or their designees, access to all
documents (including books, contracts,
and records) and other evidence
sufficient to enable the audit,
evaluation, inspection, or investigation
of the MFN Model, including without
limitation, documents and other
evidence regarding all of the following:
++ The MFN participant’s
compliance with the terms of the MFN
Model, including new subpart E of part
513.
++ Quality measure information and
the quality of services performed under
the terms of the MFN Model, including
new subpart E of part 513.
++ Patient safety.
++ The accuracy of model-specific
payments under the MFN Model.
++ Utilization of items and services
furnished under the MFN Model.
++ Any other program integrity
issues.
• Maintain the documents and other
evidence for a period of 6 years from the
last payment received by the MFN
participant under the MFN Model or
from the date of completion of any
audit, evaluation, inspection, or
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investigation, whichever is later,
unless—
++ CMS determines there is a special
need to retain a particular record or
group of records for a longer period and
notifies the MFN participant at least 30
calendar days before the normal
disposition date; or
++ There has been a termination,
dispute, or allegation of fraud or similar
fault against the MFN participant in
which case the records must be
maintained for an addition 6 years from
the date of any resulting final resolution
of the termination, dispute, or allegation
of fraud or similar fault.
If CMS notifies the MFN participant
of the special need to retain records or
group of records at least 30 calendar
days before the normal disposition date,
the records must be maintained for such
period of time determined by CMS.
J. Interaction With Other Models and
Programs
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1. Approach for Overlap With Other
Models
In designing each CMS Innovation
Center model, CMS considers potential
overlap between a new model and other
ongoing and potential models and
programs. Based on the type of overlap,
such as health care provider or
beneficiary, operating rules may be
established for whether or not health
care providers and beneficiaries can be
part of both models as well as how to
handle overlap when it occurs. These
policies help to ensure that the
evaluation of model impact is not
compromised by issues of model
overlap and that double counting of
beneficiaries and dollars across different
models does not occur.
In response to the October 2018
ANPRM, several commenters expressed
concern regarding model overlap,
specifically with the Oncology Care
Model (OCM) and initiatives involving
accountable care organizations (ACOs).
Some commenters noted that OCM
participants should be excluded from
the potential IPI Model or excluded
from mandatory participation. Some
commenters also requested that ACO
initiatives take precedence in terms of
calculating shared savings as well as for
clarity on how overlap between ACO
initiatives and the potential IPI Model
would work.
We appreciate commenters’ request
for detailed information about model
overlap policies. In developing the MFN
Model, CMS conducted an internal
review of which models will have
potential overlap with the MFN Model.
As a result of our review, we expect
there will be situations where a
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Medicare beneficiary who receives an
MFN Model drug will also be assigned,
aligned, or attributed to another CMS
Innovation Center model or CMS
program. Overlap could also occur
among providers and suppliers at the
individual or organization level, for
example, a health care practitioner or a
physician group practice could
participate in multiple CMS Innovation
Center models and CMS programs
concurrently. Of note, some existing
models and programs will not have
overlap at the health care practitioner or
participant level due to the way in
which the model or program operates
and makes payments.
We believe that the MFN Model is
operationally compatible with existing
models and programs that provide
opportunities to improve care and
reduce spending, especially total cost of
care-focused CMS programs and
Innovation Center models. The MFN
Model will test an innovative way to
pay for Medicare Part B drugs that seeks
to address any existing incentives for
prescribing higher cost drugs and ways
to lower costs for beneficiaries and the
Medicare program; total cost of carefocused CMS programs and Innovation
Center models incentivize more
appropriate provision of care across
multiple clinical areas, including use of
Medicare Part B drugs; the MFN Model
addresses only use of certain Medicare
Part B drugs. To some degree, incentives
for inappropriate use of higher cost
drugs are reduced, and intended effects
of the MFN Model are already built into
total cost of care-focused models, so the
addition of the MFN Model should not
have further effects in those programs.
We do not plan to make adjustments to
the MFN Drug Payment Amount or
MFN alternative add-on payment due to
overlap between the MFN Model and
another model or program, unless such
model tests an alternative approach to
the add-on portion of payment for
Medicare Part B drugs as specified in
§ 513.220(d)(2). However, for certain
models and programs, adjustments to
those models and programs may be
necessary to account for payment
changes under the MFN Model.
Because the MFN Model will focus on
approximately 50 separately payable
Medicare Part B drugs, when claims are
considered from all beneficiaries
aligned with or assigned to some other
Innovation Center models or CMS
programs that focus on total cost of care,
such as the Medicare Shared Savings
Program, we do not expect that the MFN
Model will have a significant impact on
shared savings, total cost of care, or
other benchmarks and measures.
Therefore, changes to benchmarks,
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targets, and reconciliation
methodologies may not be necessary,
and will be determined by each other
model, program, or initiative as
appropriate.
However, we recognize that the
design of some other models, programs,
and initiatives could create unique
challenges at the organization, clinician,
or beneficiary level. As a result, we will
work with such models, programs, or
initiatives to resolve any potential
overlaps that could result in
overpayment of savings due to double
counting of the impact of a result that
could be attributed to the interventions
from two different models. For example,
OCM focuses on improved care
management and coordination for
Medicare beneficiaries with cancer who
receive chemotherapy during 6-month
episodes of care. An OCM practice has
the opportunity to receive a
performance-based payment if it
reduces the total cost of care in its OCM
episodes compared to a target. Based on
the performance year 1 MFN Model
Drug HCPCS Codes List, we anticipate
substantial overlap between MFN
participants and MFN beneficiaries with
OCM practices and OCM beneficiaries.
To avoid paying performance-based
payments in OCM that are due simply
to the drug payment change that will
occur under the MFN Model and not to
changes in care delivery, for OCM, we
will adjust reconciliation calculations
such that the drug payments included in
OCM episode expenditures will be
calculated as if the MFN Model were
not occurring. OCM participants will be
notified and provided with further
information through OCM’s typical
channels of communication.
As discussed in the section III.C.1. of
this IFC, CMMI has already waived
section 1833(t) of the Act for certain
acute care hospitals due to their
participation in models under section
1115A of the Act for which payment for
outpatient hospital services furnished to
Medicare FFS beneficiaries, including
MFN Model drugs, is made under such
model on a fully capitated or global
budget basis. For the first and second
quarters of performance year 1, we will
exclude these entities from the MFN
Model with limitation. That is, the acute
care hospitals that participate in another
CMS Innovation Center model under
which they are paid for outpatient
hospital services furnished to Medicare
FFS beneficiaries, including MFN
Model drugs, on a fully capitated or
global budget basis under a waiver
under such model of section 1833(t) of
the Act, such as the Maryland Total Cost
of Care Model and the Pennsylvania
Rural Health Model, will be excluded
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from the MFN Model. For the third
quarter of performance year 1 and
beyond, acute care hospitals that
participate in a CMS Innovation Center
model under which they are paid for
outpatient hospital services furnished to
Medicare FFS beneficiaries, including
MFN Model drugs, on a fully capitated
or global budget basis under a waiver
under such model of section 1833(t) of
the Act will be excluded from the MFN
Model if the parameters of the other
CMS Innovation Center model adjust for
the difference in payment for MFN
Model drugs between the MFN Model
and non-MFN Model drug payments
such that savings under the MFN Model
are incorporated into the other CMS
Innovation Center model’s parameters
(for example, the annual global budget)
for the duration of the MFN Model.
These exclusions will apply only during
the period of the hospital’s participation
in such model under which it is paid on
a fully capitated or global budget basis.
Upon termination of such participation
for any reason or if the model is revised
such that the waiver of section 1833(t)
of the Act no longer applies under such
model, the hospital—if it otherwise
meets the definition of MFN
participant—will be required to
participate in the MFN Model.
We anticipate model overlap may
occur between the MFN Model and
future CMS models or programs not yet
implemented. As discussed in section
III.F.5. of this IFC, if there are MFN
participants that concurrently
participate in a future CMS model that
also tests an alternative approach to the
add-on portion of payment for Part B
drugs, we will not make the MFN
alternative add-on payment to those
MFN participants for those MFN Model
drugs that overlap with the other model.
Instead, we will follow the other
model’s approach to making an
alternative add-on payment. We expect
this overlap policy will maintain the
intended financial effects of the MFN
Model, while allowing operational
compatibility with other models that
test alternative approaches to Medicare
Part B drug payment.
2. Quality Payment Program
The MFN Model will not qualify as an
Advanced APM under the Quality
Payment Program. Specifically, the
MFN Model does not require participant
health care providers to use CEHRT,
does not base payment to participant
health care providers on quality
measures, and does not satisfy the
financial risk criteria because it does not
involve requiring participating APM
Entities to bear risk for monetary losses
of more than nominal amounts under
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the APM and is not a Medical Home
Model expanded under section
1115A(c) of the Act. The MFN Model
also will not qualify as a MIPS APM,
because it does not hold participant
health care providers financially
accountable for both the cost and
quality of care provided to Medicare
beneficiaries.
K. Interaction With Other Federal
Programs
The MFN Model may have impacts on
other federal programs, such as
Medicaid, the 340B Program, the
Veterans Health Administration, the
Department of Defense, the Public
Health Service, the Coast Guard, and
Medicare.
1. Impact on Medicaid
a. Impact on Medicaid ‘‘Best Price’’
With respect to single source or
innovator multiple source drugs (which
Medicaid recognizes to include
biologicals), the term ‘‘Medicaid Best
Price’’ is the lowest price available from
the manufacturer during the rebate
period to any wholesaler, retailer,
provider, health maintenance
organization, non-profit entity or
governmental entity within the U.S.
with certain exclusions. That is, a
manufacturer’s best price determination
represents the lowest price available
from the manufacturer during a rebate
period (a quarter) to best price eligible
entities or purchasers in the U.S. only.
Since the MFN Drug Payment
Amount will be paid to MFN
participants for each MFN Model drug
as a Medicare payment, and it will not
be a ‘‘price available from the
manufacturer,’’ the MFN Drug Payment
Amounts themselves will not be
included in the manufacturer’s
determination of best price. However, in
order for MFN participants to purchase
MFN Model drugs at prices that does
not lead to financial loss, the
manufacturer will need to make
available prices that are competitive
with the MFN Drug Payment Amounts.
We expect that the MFN Drug Payment
Amounts will likely drive manufacturer
drug prices available to MFN
participants down over the course of the
model, and the model may indirectly
impact a manufacturer’s best price to
the extent that a manufacturers’ U.S.
best price will be lower than what it
would be otherwise. In other words, if
during the course of the MFN Model,
market forces result in manufacturers
reducing prices available to MFN
participants, such available prices to
MFN participants will be considered in
a manufacturer’s determination of best
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price and could potentially lower best
price and possibly increase Medicaid
rebates.
Specifically, if the manufacturer
lowers prices available to an MFN
participant at or below the MFN Drug
Payment Amount, such prices will be
considered in the manufacturer’s
determination of best price and may
reset the manufacturer’s best price if the
reduced price is lower than the
manufacturer’s best price that would
otherwise apply. This is particularly
possible because the MFN Drug
Payment Amount, which is expected to
be lower than the payment amounts for
the same drugs outside of the model,
will include the impact of pricing
outside of the U.S., which is typically
lower than prices in the U.S., and will
likely impact the prices made available
by the manufacturer in the U.S.
b. Impact on Average Manufacturer
Price (AMP)
AMP is defined at section 1927(k)(1)
of the Act. Generally, AMP is
determined based on the average price
paid to the manufacturer for a covered
outpatient drug in the U.S. by
wholesalers for drugs distributed to
retail community pharmacies and retail
community pharmacies that purchase
drugs directly from the manufacturer
with certain exclusions. Because the
MFN Model will focus on certain Part
B drugs that are furnished in the
outpatient setting and these drugs are
most likely injected or infused, the AMP
for an MFN Model drug is likely
determined using the AMP computation
for 5i drugs,73 which includes sales that
are not generally dispensed through
retail community pharmacies (see
section 1927(k)(1)(B)(i)(IV) of the Act,
42 CFR 447.504(d)), such as sales to
physicians, pharmacy benefit managers
(PBMs) and hospitals. Thus, a
manufacturer’s sales of MFN Model
drugs to MFN participants (or price paid
by MFN participants) will be included
in the AMP or 5i AMP. If, as described
in section III.K.1.a. of this IFC, the
manufacturer lowers prices available to
an MFN participant at or below the
MFN Drug Payment Amount, the
manufacturer’s AMP for an MFN Model
drug may be lower. If a drug’s AMP
decreases, it may result in potentially
lowering the applicable Medicaid drug
rebate paid (the rebate, in part, is based
on a percentage of AMP). However, the
MFN Model may also lower a
manufacturer’s best price for an MFN
Model drug as previously discussed.
The resulting effect on the Medicaid
73 Inhalation, infusion, instilled, implanted or
injectable drugs.
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drug rebate will depend upon the
relationship of any AMP change and
any best price change.
We also note that if the AMP for an
MFN Model drug is lowered it may be
more likely that, in accordance with
section 1847A of the Act, the Inspector
General may find that the ASP for an
MFN Model drug exceeds the AMP for
such drug, and that the circumstances in
which 103 percent of AMP is
substituted for ASP in CMS’s
determination of the non-model
payment allowance for such drug would
occur. We refer readers to section III.L.
of this IFC for a discussion of excluding
units of MFN Model drugs from
manufacturers’ ASP, which may also
increase the likelihood that the ASP for
an MFN Model drug will be greater than
the AMP for such drug.
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2. Interaction With 340B Program
The Health Resources and Services
Administration (HRSA) administers the
340B Drug Pricing Program that allows
certain hospitals and other health care
providers (‘‘covered entities’’) to obtain
discounted prices on ‘‘covered
outpatient drugs’’ (as defined at
1927(k)(2) of the Act) from drug
manufacturers. HRSA calculates a 340B
ceiling price for each covered outpatient
drug, which represents the maximum
price a manufacturer can charge a
covered entity for the drug that is
provided to an eligible patient. Several
types of hospitals as well as clinics that
receive certain federal grants from the
HHS may enroll in the 340B program as
covered entities. Such entities will be
included in the MFN Model and will be
subject to the MFN Model payment test.
That is, these 340B covered entities will
be MFN participants and receive the
MFN Drug Payment Amount and
alternative add-on payment. To the
extent these entities receive payment
under the model that is lower than their
current Medicare payment, there may be
fewer resources available for their 340B
program activities.
Under the MFN Model, MFN
participants will be paid for MFN Model
drugs according to the payment
approach discussed in section III.E. of
this IFC. If the MFN participant is a
340B covered entity, the drug portion of
the model payment will be the lower of
the MFN Drug Payment Amount or the
non-model payment amount paid to
340B covered entities for 340B drugs
under the OPPS for the MFN Model
drug for that corresponding calendar
quarter. The MFN alternative add-on
payment will be paid to MFN
participants that are 340B covered
entities in the same way as MFN
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participants that are non-340B covered
entities.
We are including certain 340B
covered entities in the MFN Model in
order to test the innovative payment
approach, including the alternative (perdose) add-on payment amount, broadly.
MFN participants that are 340B covered
entities may need to enhance their
direct contracting with manufacturers in
order to obtain MFN Model drugs
within the MFN Drug Payment Amount.
Our analyses estimate that 340B covered
entities will realize a total add-on
percentage amount of 4.5 percent in the
first year of the model due to the mix
of MFN Model drugs they historically
furnish. The amount of the alternative
add-on that 340B entities realize will be
an increase in revenue compared to
their historical baseline. However, these
entities will face the same or increased
burden from model participation. Thus,
we believe the modest increase in addon revenue that will be paid to these
entities through the alternative add-on
payment approach will potentially be
offset through higher facility costs for
acquiring included drugs (for example,
higher costs for direct contracting).
Programs that support vulnerable
Americans are a vital safety net. We
refer readers to section III.C. of this IFC
where we discuss providers and
suppliers that will be MFN participants.
We discuss potential impacts on 340B
covered entities in more detail in
section VI. of this IFC.
a. Impact on 340B Ceiling Price
Covered entities that enroll in the
340B Program can purchase covered
outpatient drugs at no more than a
‘‘ceiling price,’’ which is calculated as
AMP minus Medicaid unit rebate
amount. We note that a ceiling price is
just a ceiling; some 340B hospitals can
obtain covered outpatient drugs at less
than the ceiling price. Since the
Medicaid unit rebate amount is based
partly on AMP minus best price, to the
extent the MFN Model affects a drug’s
AMP and best price, the 340B prices
will be affected. We discuss the
potential impacts on a drug’s AMP and
best price in section III.K.1. of this IFC.
3. Interaction With Medicare
a. Medicare Part B
As discussed in section VI. of this
IFC, we believe the MFN Model will
result in lower Medicare spending for
MFN Model drugs, including lower
program spending and lower beneficiary
cost-sharing, and in overall reduced
Medicare Part B Trust Fund
expenditures, which in turn will lower
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Medicare FFS expenditures and
beneficiaries’ Part B premiums.
As discussed in section III.K. of this
IFC, manufacturers’ ASPs for MFN
Model drugs may be higher or lower
than they otherwise would be absent the
MFN Model. In turn, non-model
Medicare Part B FFS payment for MFN
Model drugs could be higher or lower.
We are excluding from the calculation
of the manufacturer’s ASP any units of
an MFN Model drugs furnished to MFN
beneficiaries and billed by MFN
participants. Thus, during the MFN
Model, manufacturers’ ASPs for MFN
Model drugs could be higher or lower
than they might be absent the model,
resulting in Medicare payments to
providers and suppliers that are not
MFN participants that would be higher
or lower than what the payments would
have been absent the model.
We note that if the AMP for an MFN
Model drug is lowered it may be more
likely that, in accordance with section
1847A of the Act, the Inspector General
may find that the ASP for an MFN
Model drug exceeds the AMP for such
drug, and that the circumstances in
which 103 percent of AMP is
substituted for ASP in CMS’s
determination of the non-model
payment allowance for such drug would
occur.
b. Medicare Advantage
Medicare Advantage (MA) plans will
not be MFN participants. We note that
when MA plans pay non-contracted, out
of network providers who have
administered an MFN model drug to an
enrollee, the amount paid will be based
on the non-model Medicare FFS
payment amount (that is, the amount
that MA plans pay to these providers
will not be the MFN Model payment
amounts).
As discussed in section VI. of this
IFC, we expect the MFN Model will
lower overall Medicare FFS
expenditures; that is, Medicare Part B
MFN Drug Payment Amounts will be
lower than such payment would be
absent the model, the Medicare Part B
alternative add-on payments will be
greater than such payment would be
absent the model, there could be
increases in Medicare Part A spending,
and taken together the model will result
in an overall reduction in Medicare
expenditures. The overall decrease in
Medicare FFS expenditures will be
considered in determining the historical
FFS claims experience for calculating
the rates for plan service areas.
Payments to Medicare Advantage
Organization plans are anticipated to be
lower than they would be absent the
model. At a high level, the FFS
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component of the non-ESRD MA rates is
based on the product of the projected
national per-capita spending and a
county-level relative cost index. Thus,
the MA ratebook calculations will
reflect changes in actual FFS spending
due to the impact of the MFN Model.
We note that this approach is consistent
with treatment of payments made under
other CMS Innovation Center models
and the Medicare Shared Savings
Program.
As discussed in more detail in section
VI. of this IFC, we estimate that total
payments to MA plans over the 7-year
course of the model will be substantially
lower as a result of reduced FFS
spending under the MFN Model, that is,
total payments to MA plans may be
approximately $49.6 billion lower in the
OACT estimate and $28.5 billion lower
in the ASPE estimate. We note that there
is much uncertainty around the
assumptions for these estimates.
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L. Exclusion of Certain MFN Model
Sales From Manufacturers’ Calculation
of ASP for MFN Model Drugs
In accordance with sections 1847A
and 1927(b)(3)(A)(iii) of the Act,
manufacturers 74 75 submit ASP data for
their products to CMS on a quarterly
basis. The manufacturer’s ASP is based
on sales to all purchasers in the U.S.
with limited exceptions (that is,
exclusions are limited to sales exempt
from best price (as defined in section
1927(c)(1)(C)(i) of the Act), sales at a
nominal charge, and units sold to a CAP
vendor), and is net of discounts such as
volume discounts, prompt pay
discounts, cash discounts, free goods
that are contingent on any purchase
requirement, chargebacks, and rebates
(other than certain rebates specified in
section 1927 of the Act). Specific ASP
reporting requirements are set forth in
section 1927(b)(3) of the Act. In
accordance with sections 1847A and
1927(b)(3) of the Act, manufacturers
74 For the purposes of reporting under section
1847A of the Act, the term ‘‘manufacturer’’ is
defined in section 1927(k)(5) of the Act and means
any entity engaged in the production, preparation,
propagation, compounding, conversion or
processing of prescription drug products; either
directly or indirectly by extraction from substances
of natural origin, or independently by means of
chemical synthesis, or by a combination of
extraction and chemical synthesis; or in the
packaging, repackaging, labeling, relabeling, or
distribution of prescription drug products. The term
manufacturer does not include a wholesale
distributor of drugs or a retail pharmacy licensed
under State law. However, manufacturers that also
engage in certain wholesaler activities are required
to report ASP data for those drugs that they
manufacture. Note that the definition of
manufacturers for the purposes of ASP data
reporting includes repackagers.
75 Manufacturer is also defined in 42 CFR
447.502.
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report most ASP data by National Drug
Code (NDC), which identifies products
in terms of the labeler, product, and
package size and type. The reported
ASP data are used to establish the
Medicare payment amounts. In general,
Medicare’s payment limit for most
separately payable Part B drugs is based
on the methodology in section 1847A of
the Act, that is, 106 percent of the
volume-weighted average of
manufacturers’ ASP for a drug (at the
billing and payment code level), and is
updated quarterly. The payment
requirements in section 1847A of the
Act will be waived for purposes of
testing the MFN Model as discussed in
section III.M.1. of this IFC, but will
continue to apply outside of the model
as discussed in this section.
Section 1115A of the Act authorizes
the CMS Innovation Center to test
innovative payment and service
delivery models to reduce program
expenditures, while preserving or
enhancing the quality of care furnished
to beneficiaries. The MFN Model will
test an alternative approach for
determining Medicare’s payment limit
for MFN Model drugs, which will phase
down the Medicare payment amount for
selected Part B drugs to more closely
align with available international prices,
and test an alternative add-on payment.
Under the MFN Model, the model’s
payment test will apply when Medicare
makes separate payment for an MFN
Model drug that was furnished on an
outpatient basis by an MFN participant
to an MFN beneficiary within the
model’s nationwide geographic area.
In designing the MFN Model, we
considered ways to mitigate potential
impacts on manufacturers’ ASPs
stemming from price concessions given
to MFN participants for purchases
related to the MFN Model and on
Medicare payment for units of MFN
Model drugs that are not subject to the
MFN Model payment test. For example,
sales to MFN participants may include
larger price concessions than are typical
today, resulting in lower net sales prices
as compared to what net sales prices
would be absent the MFN Model. As
such, the manufacturer’s ASP for an
MFN Model drug, which will reflect the
average price for all non-excluded
sales—including sales to MFN
participants to the extent applicable—
may be lower than the manufacturer’s
ASP would be absent the MFN Model.
Because CMS will base the non-model
Medicare payment limit for an MFN
Model drug on 106 percent of the
manufacturer’s ASP, payment to
providers and suppliers for such drug
outside of the model may be lower than
it otherwise would be absent the MFN
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Model. To conduct the MFN Model test
it is necessary to minimize this potential
spillover effect for providers and
supplier that are not MFN participants
to best observe the impacts of the
payment change. Thus, we will exclude
from the calculation of the
manufacturer’s ASP any units of MFN
Model drugs billed by MFN participants
where the MFN Drug Payment Amount
is based on available international drug
pricing information and Medicare Part B
is the primary payer. policy will only
apply when the MFN Price is based on
available international drug pricing
information. That is, the policy will not
apply when there is no available
international drug pricing information
and the MFN Price is equal to the
applicable ASP because there will be no
concern for spillover impacts in such
cases. We are waiving requirements of
section 1847A of the Act as necessary to
exclude such units of MFN Model drugs
from the calculation of the
manufacturer’s ASP. We will also
indicate the MFN Drug Payment
Amounts that are (and are not, when
applicable) based on available
international drug pricing information
within the quarterly MFN Model drug
pricing files posted on a CMS website.
This approach is responsive to
comments we received in response to
the October 2018 ANPRM. Several
commenters requested clarification
about how sales for purposes of the
model would be taken into account in
computing the ASP under section
1847A of the Act. Some commenters
who expressed concern about potential
spillover effects of the potential model
payment test recommended that
purchases made for use under the
potential model be excluded from the
ASP calculation. Based on our
interactions with stakeholders,
particularly those with experience
operating chargebacks related to the
340B program, we believe our exclusion
of units of MFN Model drugs that are
billed by MFN participants and have the
MFN Drug Payment Amount paid by
Medicare from manufacturers’ ASPs
will be feasible. Manufacturers have
existing processes and tools to exclude
various prices from the calculation of
their ASPs, and excluding certain MFN
Model related units of MFN Model
drugs could be similar.
Distribution management systems are
employed throughout the drug
distribution system to order drugs, track
sales and shipments, trace custody,
manage price and customer lists, record
financial transactions, and support other
industry processes. Separate purchasing
accounts are often used to align with
purchasing arrangement terms, and
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through a process called the
‘‘chargeback process,’’ manufacturers
reduce the final drug prices to
wholesalers and other distributors to
reflect the purchasing terms and
contract prices that apply to the end
purchaser. End purchasers of drugs who
purchase under more than one contract
use virtual inventory or replenishment
purchasing tools or business processes
to manage their purchases under their
various contract arrangements. For
example, a provider or supplier that
belongs to more than one group
purchasing organization could use such
tools or business processes to track drug
purchasing, maintain records toward
volume targets and, should the need to
return a product occur, conduct returns.
However, based on stakeholder
feedback, we understand that all MFN
participants are unlikely to have such
tools in place. Hospitals, particularly
those that participate in the 340B
program, are more likely to currently
have these tools compared to other
hospitals, physician offices and ASCs.
Thus, manufacturers may establish
mechanisms to obtain information from
MFN participants about the number of
units of MFN Model drugs that were
furnished to MFN beneficiaries and for
which payment under § 513.210 was
allowed, which would increase MFN
participants’ activities related to the
model.
CMS also seeks to minimize the
potential for excessive increases in nonmodel Medicare drug payment amounts
during the MFN Model. For example,
during the model, manufacturers’ ASPs
may increase causing a concomitant
increase in non-model Medicare drug
payment amounts outside of the model
if: (1) The policy that manufacturers not
include units of an MFN Model drug
billed by MFN participants where the
MFN Drug Payment Amount is paid by
Medicare and Medicare Part B is the
primary payer in the manufacturer’s
ASP for the MFN Model drug results in
higher ASPs; or (2) manufacturers raise
drug prices or lower existing discounts
for U.S. sales that are not subject to the
model’s payment test. Because
manufacturers will continue to have the
ability to set their own drug prices, as
a behavioral response to the MFN
Model, manufacturers could raise prices
for MFN Model drugs in the United
States in part to make up for price
concessions that may be given to model
participants.
We believe the policy for
manufacturers not to include in the
manufacturer’s ASP units of an MFN
Model drug administered to an MFN
beneficiary and billed by MFN
participants where the MFN Drug
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Payment Amount applied by Medicare
is based on available international drug
pricing information and Medicare is the
primary payer will minimize the
potential for manufacturers to choose to
increase purchase prices for non-model
participants and for MFN participants’
purchases of MFN Model drugs for use
outside of the MFN Model.
Additionally, we believe that the
adjustments to the MFN Price phase-in,
as described in section III.E. of this IFC,
will also minimize the potential for
manufacturers to increase prices for
non-model participants and non-model
purchases. We also believe this policy is
necessary for a rigorous test of the
model payment for MFN drugs because
price concessions tied to the model will
not lower Medicare payment when MFN
Model drugs are purchased for use
outside the model, which would limit
our ability to observe the impacts of the
payment change.
We will not collect the number of
units that manufacturers exclude from
ASP as part of their ASP submission to
CMS to avoid establishing a new data
collection effort and to minimize
administrative burden for
manufacturers.
As an alternative approach, we
considered whether manufacturers
should exclude from the manufacturer’s
ASP for the MFN Model drug price
concessions on units of an MFN Model
drug billed by MFN participants where
the MFN Drug Payment Amount applied
by Medicare is based on available
international drug pricing information
and Medicare is the primary payer. We
believe that excluding from the
manufacturer’s ASP price concessions
on units of an MFN Model drug billed
by MFN participants where the MFN
Drug Payment Amount applied by
Medicare is based on available
international drug pricing information
and Medicare is the primary payer, and
not excluding the manufacturer’s ASP
the units of an MFN Model drug billed
by MFN participants where the MFN
Drug Payment Amount is applied by
Medicare is based on available
international drug pricing information
and Medicare is the primary payer
would inappropriately raise the ASP.
We believe this is the case because those
units would likely be factored into the
manufacturer’s ASP calculation as
undiscounted sales. Thus, this
approach, while it may be less complex,
would likely lead to inappropriately
higher Medicare payment outside of the
model.
We are waiving requirements in
section 1847A(c) to the extent necessary
to exclude from the calculation of the
manufacturer’s ASP any units of an
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MFN Model drug administered to an
MFN beneficiary and billed by MFN
participants where the MFN Drug
Payment Amount applied by Medicare
is based on available international drug
pricing information and Medicare is the
primary payer. Consistent with section
1847A(c)(5) of the Act, we will issue
program instructions to further describe
how the waiver will impact
manufacturers’ calculation of the
manufacturer’s ASP. For example, we
envision that manufacturers will take
reasonable steps and make reasonable
assumptions to exclude applicable
units. We note that all other existing
statutory requirements and regulations
will continue to apply. For example,
manufacturers who misrepresent or fail
to report manufacturer ASP data will
remain subject to civil monetary
penalties, as applicable and described in
sections 1847A and 1927(b) of the Act
and codified in regulations at § 414.806.
M. Program Waivers and Model
Termination
1. Waivers of Medicare Program
Requirements for Purposes of Testing
the Model
We will test the MFN Model under
the authority of section 1115A of the
Act and waive certain Medicare
program requirements as necessary
solely for purposes of testing the model.
Under section 1115A(d)(1) of the Act,
the Secretary may waive the
requirements of Titles XI and XVIII and
of sections 1902(a)(1), 1902(a)(13),
1903(m)(2)(A)(iii), and 1934 of the Act
(other than subsections (b)(1)(A) and
(c)(5) of such section) as may be
necessary solely for purposes of carrying
out section 1115A of the Act with
respect to testing models described in
section 1115A(b) of the Act. The
purpose of these waivers will be to
allow Medicare to test the MFN Model
described in this IFC, with the goal of
reducing Medicare expenditures while
improving or maintaining the quality of
beneficiaries’ care.
In § 513.500, we waive program
requirements that are necessary solely
for purposes of testing the MFN
Model—
• Sections 1833(t)(6) and 1833(t)(14)
of the Act and 42 CFR 419.62 and
419.64 related to Medicare payment
amounts for drugs and biologicals under
the OPPS as necessary to permit testing
of an adjusted payment amount for MFN
Model drugs using the pricing
approaches described in this IFC;
• Section 1833(i)(2)(D) of the Act
related to Medicare payment to ASCs for
drugs and biologicals as necessary to
permit testing of an adjusted payment
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amount for MFN Model drugs using the
pricing approaches described in this
IFC;
• Sections 1847A(b) and 1847A(c) of
the Act and 42 CFR 414.904 and
414.802 related to use of the ASP-based,
WAC-based, or other applicable
payment methodology and calculation
of manufacturers’ ASP as necessary to
permit testing of an adjusted payment
for MFN Model drugs and to exclude
certain units of MFN Model drugs from
manufacturers’ ASPs;
• Section 1833(a)(1) of the Act related
to Medicare payment portion of the
allowed payment amount for an
included MFN Model drug that is
determined under § 513.220 as
necessary to permit testing of an
innovative payment approach for the
alternative add-on payment amount;
• Section 1833(a)(1)(S) related to
Medicare payment for drugs and
biologicals at 80 percent of the lesser of
actual charge or the amount established
in section 1842(o) of the Act as
necessary to allow CMS to not apply
beneficiary cost-sharing to the
alternative add-on payment amount;
• Section 1833(a)(1)(G) of the Act
related to the amounts paid with respect
to facility services furnished in
connection with certain surgical
procedures and with respect to services
furnished to an individual in an ASC
shall be 80 percent of the lesser of the
actual charge for the services or the
amount determined by the Secretary
under such revised payment system as
necessary to allow CMS to not apply
beneficiary cost-sharing to the
alternative add-on payment amount;
• Section 1833(t) of the Act related to
how Medicare payment under the OPPS
is calculated including beneficiary
copayment to allow CMS to not apply
beneficiary cost-sharing to the
alternative add-on payment amount;
and
• Section 1833(t)(9)(B) of the Act
related to the requirement that Medicare
account for adjustments to ensure that
the amount of expenditures under the
OPPS for the year does not increase or
decrease from the estimated amount of
expenditures under the OPPS that
would have been made if the
adjustments had not been made (that is,
OPPS budget neutrality). CMS intends
to continue to maintain budget
neutrality under the OPPS as it
currently does, including as described
in 42 CFR 419.32(d)(1). This includes
continuing to use the applicable
payment amount for each separately
payable drug under that payment
system, rather than the MFN Drug
Payment Amount and alternative addon payment amount. CMS may consider
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using volume for drugs included in the
MFN Model for purposes of the budget
neutrality calculations under the OPPS
beginning in 2022, but would utilize the
applicable OPPS payment amount for
the drug or biological, rather than the
MFN Drug Payment Amount. We
believe a waiver of the OPPS budget
neutrality requirements for Part B drugs
furnished under the MFN Model is
necessary solely for purposes of testing
the MFN Model because if reductions in
Medicare Part B drug expenditures were
redistributed through the OPPS budget
neutrality process to non-drug Part B
services under the OPPS, the model
would change pricing for numerous
other services that are not related to Part
B drugs. This would make it difficult to
determine the independent impact of a
change in Part B drug payment levels to
MFN Model pricing if there is also a
corresponding change in the payment
amount for all non-drug hospital
outpatient items and services as a result
of the OPPS budget neutrality
requirements.
Our intent is to include a waiver for
all program requirements in title XVIII
of the Act as may be necessary solely to
test separate payment for MFN Model
drugs furnished to MFN beneficiaries by
MFN participants. To the extent that
MFN participants receive separate
payment for MFN Model drugs under
program requirements that we have not
listed in § 513.500, we waive such
requirements as necessary to effectuate
part 513.
2. Model Termination
CMS may terminate the MFN Model
for reasons including, but not limited to,
the following: CMS determines that it
no longer has the funds to support the
model; or CMS terminates the model in
accordance with section 1115A(b)(3)(B)
of the Act. As provided by section
1115A(d)(2) of the Act, termination of
the model under section 1115A(b)(3)(B)
of the Act is not subject to
administrative or judicial review. We
are codifying these policies in
§ 513.1000.
N. Evaluation
We will conduct an evaluation of the
MFN Model, as required under section
1115A(b)(4) of the Act. The evaluation
of the MFN Model will include an
analysis of the quality of care furnished
under the model and the changes in
spending under Medicare by reason of
the model.
There will be several populations of
interest for the MFN Model evaluation.
A population of interest for the
evaluation will be Medicare
beneficiaries who are likely to receive
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one of the MFN Model drugs based on
recent diagnoses and/or prior treatment.
One possible prescriber behavior change
due to the MFN Model could be shifts
from prescribing MFN Model drugs to
other alternative Part B or Part D drugs
or vice versa. A population defined by
recent diagnoses and/or prior treatment
will capture the model’s impact on
beneficiaries affected by these
prescribing behavioral changes due to
the model. Other populations such as,
but not limited to, MFN Model drug
users and subgroups of particular
patient populations (for example,
cancer, rheumatoid arthritis,
ophthalmologic conditions) will be
considered in the evaluation.
For each of the populations of
interest, we will create separate impact
estimates for two types of outcomes:
Medicare spending and drug/other
health care utilization. Medicare
spending will be examined in terms of
total Part B drug spending for MFN
Model drugs, total Part B drug spending
for any Part B drugs, total Parts A and
B spending, and potentially other
spending measures for specific types of
health care services (for example,
inpatient hospital spending). The
evaluation of the model’s impact on
quality of care will examine drug access,
measured by utilization (for example,
rates of any use and duration of use) of
both Part B (both MFN Model drug and
non-MFN Model drugs) and Part D
drugs. We will also examine non-drug
health care utilization that may change
as a result of the MFN Model to estimate
any impacts on access to care. Examples
of other non-drug health care utilization
include hospitalizations, emergency
department visits, and conditionspecific utilization related to a given
subgroup of beneficiaries. The impact
estimates will reflect the collective
effect of the MFN Model’s changes to
Medicare payments and beneficiary
cost-sharing for MFN Model drugs.
Because the MFN Model will be a
nationwide, mandatory model, we must
employ an evaluation design that does
not require an independent comparison
group to establish the counterfactual
(what would have happened in the
absence of the model). The term
‘‘interrupted time series’’ (ITS) refers to
the situation in which multiple
observations for the treatment group are
available both before and after the
intervention is implemented.76 ITS
models can be employed both with and
76 Wagner, A.K., Soumerai, S.B., Zhang, F. and
Ross-Degnan, D. (2002), Segmented regression
analysis of interrupted time series studies in
medication use research. Journal of Clinical
Pharmacy and Therapeutics, 27: 299–309. doi:
10.1046/j.1365–2710.2002.00430.x.
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without comparison groups, and be
used to imply causality without
comparison groups.77 The design is
used when data are available both for
the pre-intervention period and the
post-intervention period, and the
intervention takes place at a specific,
identifiable point in time.78 The timerelationship between the data points can
then be used to estimate treatment
effects. The trends from the preintervention period establish a baseline
that is used to project what would be
expected in the absence of the
intervention. The typical ITS approach
assumes linear trends before and after
the intervention, but ITS models can be
made more general to address potential
non-linear trends.79 80 Intervention
effects are demonstrated when
observations gathered after the
intervention start period deviate from
the baseline projections.
Using this design for evaluating the
effects of an intervention—that is,
implying a causal relationship between
the intervention and its target
outcomes—relies on a strict set of
conditions. As previously described,
when there is no comparison group, the
counterfactual is established as the
continuation of the pre-intervention
trend for the treated group. The
intervention impact is estimated as the
difference between the actual postintervention trend and the preintervention trend extended.
The most common statistical method
for analyzing ITS data is called
segmented regression.81 82 Segmented
regression focuses on two parameters,
the level (intercept) and the trend
(slope). For observations before the
model, we will have a level (intercept)
77 Sheingold, S., Bir, A, (2019), Evaluation for
Health Policy and Health Care: A Contemporary
Data Driven Approach, Sage Publications.
78 Bernal, J.L., Cummins, S., Gasparrin, A., (2017)
Interrupted time series regression for the evaluation
of public health interventions: A tutorial,
International Journal of Epidemiology, 2017, Vol.
46, No. 1: 348–355, doi: 10.1093/ije/dyw098.
79 Kontopantelis, E., Doran, T., Springate, D.A.,
Buchan, I Reeves, D, (2015), Regression based quasiexperimental approach when randomisation is not
an option: Interrupted time series analysis, BMJ
2015;350:h2750, doi: 10.1136/bmj.h2750.
80 Valsamis, E.M., Ricketts, D., Husband, H., and
Rogers, B.A. (2019), Segmented linear regression
models for assessing change in retrospective studies
in healthcare. Computational and Mathematical
Methods in Medicine. doi: 10.1155/2019/9810675.
81 Wagner, A.K., Soumerai, S.B., Zhang, F. and
Ross-Degnan, D. (2002), Segmented regression
analysis of interrupted time series studies in
medication use research. Journal of Clinical
Pharmacy and Therapeutics, 27: 299–309. doi:
10.1046/j.1365–2710.2002.00430.x.
82 Valsamis, E.M., Ricketts, D., Husband, H., and
Rogers, B.A. (2019), Segmented linear regression
models for assessing change in retrospective studies
in healthcare. Computational and Mathematical
Methods in Medicine. doi: 10.1155/2019/9810675.
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and trend (slope). After the model
begins, the data may exhibit changes in
any one of these features. The
fundamental idea behind segmented
regression is to estimate a regression
specification with a linear trend for the
data points before the model and
estimate a regression specification with
a linear trend for the data points after
the model start. The level and trend
before and after the model start will
then be compared. We will use quarterly
observations for the pre- and postmodel start time periods ending with
the most recent data that will be
currently available. Given the MFN
Model design, we provide our
specification in this section of this IFC
for the longitudinal regression using a
more general specification of the trends
to capture the non-linear nature of the
data.
In the longitudinal regression
equation provided in this section of this
IFC, the vector Xit consists of factors that
will change from the pre-model time
period to the model performance period
and may include, but is not necessarily
limited to, the medical care component
of the Consumer Price Index (CPI–U),
national unrelated policy changes,
economic factors (for example,
unemployment rate). The unit of
analysis (for example, a hospital referral
region (HRR) as defined by the
Dartmouth Atlas 83 or beneficiary) on
which the quarterly observations are
measured will be allowed to vary in
order to estimate the model’s impact at
these different levels of aggregation. The
anticipated statistical model
specification includes a polynomial
time trend variable f(t) to account for
trends in spending and utilization over
time. In addition, the statistical model
includes separate indicator variables
(It=k) for each of the model performance
period quarters, which will allow for
estimates of the model’s impact in each
performance period quarter relative to
the entire pre-period after adjusting for
the time trend and other factors.
Yit = b0 + b1 · Xit + b2 · f(t) + a1 · It=1
+ a2 · It=2 + a3 · It=3 + a4 · It=4 + . . .
+ uit
Where:
Yit = outcome (see the previous section for
cost and utilization measures), for a
particular unit of analysis in a specific
quarter
Xit = vector of adjustment factors
f(t) = polynomial function to account for time
trend
It=k = denotes an indicator for time period k
(all after model implementation)
uit = unaccounted variation
83 https://www.dartmouthatlas.org/faq/#research-
methods-faq.
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i = unit of analysis (for example, beneficiary,
HRR)
t = time quarter (¥12, ¥11 . . . 0, 1, 2, 3
. . .) using a 3 year pre-model time
period, with 0 indicating the start of the
model
b0, b1, b2, a1 . . . . an are the statistical model
coefficients
b0 = the statistical model intercept
b1 = vector of estimates for the adjustment
factors
b2 = estimate of the time trend f(t) across the
pre-period and model performance
period
a1 thru an = estimate of change per model
performance period quarter (t) relative to
entire pre-period
With the statistical model
specification as previously described, in
an initial, exploratory data assessment,
the null hypothesis (Ho: a1 = a2 = a3 =
a4 = . . . = an = 0) will be that there is
no change in each of the model
performance period quarters when
compared to the pre-period after
adjusting for the time trend and the
other factors. The corresponding
alternate hypothesis (Ha: a1 or a2 or a3
or a4 or . . . an ≠ 0) will be that any of
the model performance period quarters
is statistically significantly different
than the pre-model time period,
suggesting that the model either
positively or negatively impacted
Medicare spending and quality of care
in at least one model performance
period quarter. These null and alternate
hypotheses will apply to each outcome
and population of interest.
The assessment just described will
not directly indicate success or failure
of the model. CMS will need to observe
a consistent statistically significant
directional pattern over multiple
consecutive time periods for the
outcome and population of interest in
order to draw sound conclusions about
the model’s impact. Based on a
combination of results from exploratory
data assessment and policy goals, CMS
will set a hypothesis that encompasses
the chosen outcome and population of
interest. This hypothesis will be tested
using data that is different from what
was used in the exploratory
assessment—for instance, due to being
gathered later in time or consisting of a
different randomly assigned subset of
contemporaneous data.
Statistical inference will be conducted
using cluster-robust standard errors.84
Cluster-robust standard errors account
for serial correlation as well as spatial
correlation within geographies (such as
an HRR). We will conduct hypothesis
testing using an alpha-level of 5 percent
84 Cameron, A.C., & Miller, D.L. (2015). A
practitioner’s guide to cluster-robust inference.
Journal of Human Resources, 50(2), 317–372.
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and CMS will report the p-value and
standard error to allow for inferences at
other alpha-levels.
As an illustration of a potential
subgroup analysis and the expected
changes that could be detected in the
MFN Model evaluation, CMS identified
two groups of Medicare cancer patients
using 2018 data. CMS defined the first
narrower group as Medicare cancer
patients who received an MFN Model
drug. CMS defined the second broader
group as Medicare cancer patients who
either received an MFN Model drug or
would have been considered eligible to
receive an MFN Model drug.
Specifically, CMS estimated that in
2018 approximately 400,000 Medicare
beneficiaries were being treated for the
most prevalent cancer types (that is,
colorectal, endometrial, breast, lung,
prostate, and certain forms of leukemia
and lymphoma) and received an MFN
Model drug. These 400,000 Medicare
beneficiaries were identified using the
inclusion and exclusion criteria for the
model, including the use of an MFN
Model drug. Cancer treatment was
determined by the utilization of Part B
and/or Part D cancer drugs and the
presence of cancer diagnosis codes on
Parts A and B claims. A subgroup
analysis that requires MFN Model drug
use, as in the narrower definition that
identified 400,000 Medicare
beneficiaries being treated for cancer
and who received an MFN Model drug,
would exclude cancer patients using an
alternative non-MFN Model drug cancer
therapy. A broader cancer population
definition based on any Part B and/or
Part D cancer drug use or just an
incident cancer diagnosis based on new
evidence of diagnosis codes on Parts A
and B claims in the current year would
capture the model’s impact on
beneficiaries affected by prescribing
behavioral changes due to the model.
This second broader cancer subgroup
population definition applied to
approximately 1.1 million Medicare
beneficiaries in 2018.
CMS believes that looking for
unintended consequences will be
critical for the monitoring and
evaluation of the MFN Model. In the
narrower definition of the cancer
subgroup, CMS expects that
approximately 100,000 Medicare cancer
patients who receive a MFN Model drug
will be eligible for inclusion in the
quarterly evaluation analysis. In the
broader cancer subgroup population,
CMS expects that approximately
280,000 Medicare cancer patients will
be included in the quarterly evaluation
analysis. With a nationwide MFN Model
(and the assumptions of an alpha-level
of 5 percent and power of 80 percent),
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CMS will have the sample sizes needed
in these two populations to detect small
changes in Medicare total cost of care
(approximately a 1 percent change),
drug access, and other important
measures of quality of care. With
multiple quarterly assessments of the
impact of the model on subgroup
populations, CMS will be able to
intervene early in the model’s
performance period should any
potential unintended consequences be
detected in the potential subgroups of
interest. Although CMS uses the cancer
subgroup patient population in the
previously discussed example, we
recognize that other patient populations
(for example, patients diagnosed with
rheumatoid arthritis and wet macular
degeneration) and certain types of
providers could be differentially
impacted by the MFN Model. These
other patient and provider subgroups
will be of interest in the evaluation. The
model’s impact on the Medicaid
program and commercial insurance
(including Medicare Advantage)
population is also of interest.
The evaluation will explore the
experiences of MFN participants
(beneficiaries and providers) and other
stakeholders affected by the changes in
payment and conditions included in the
model. In particular, CMS will
interview MFN participants and
beneficiaries, either by focus groups,
surveys, or one-on-one stakeholder
interviews, to assess the model’s
influence on access to and quality of
care, and administrative burden from
their perspectives. Further, CMS intends
to ask beneficiaries about their total out
of pocket costs under the MFN Model to
determine if those costs were reduced.
MFN participants will be asked for their
opinions about the MFN Model’s
payment changes to the drug and addon payment amounts separately. The
evaluation will also include qualitative
analyses of primary data collected from
MFN participants and beneficiaries. The
results of the qualitative analyses will
be used to provide additional context
for the results of the quantitative
analyses on health care spending and to
help further explain the observed
changes.
Evaluation reports detailing the
results and findings will be developed
and publicly posted on the CMS
website. The evaluation reports will
include the results of the quantitative
and qualitative analyses of the MFN
Model’s impact on spending and quality
of care and the model’s implementation
as described in this section. The
evaluation reports covering the earlier
performance years of the MFN Model
will be used in the decision making
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process on whether or not to continue
the MFN Model into performance years
5 to 7.
The evaluation may require that MFN
participants collect and submit
additional data specifically for the
evaluation (please see § 513.100(e) and
§ 513.100(f)). Such requirements for
additional data to carry out model
evaluation will be in compliance with
42 CFR 403.1110(b), which requires
entities participating in the testing of a
model under section 1115A to collect
and report such information, including
protected health information (as defined
at 45 CFR 160.103), as the Secretary
determines is necessary to monitor and
evaluate the model.
O. Limitations on Review
In § 513.450, we are codifying the
preclusion of administrative and
judicial review under section
1115A(d)(2) of the Act. Section
1115A(d)(2) of the Act states that there
is no administrative or judicial review
under section 1869 or 1878 of the Act
or otherwise for the all of the following:
• The selection of models for testing
or expansion under section 1115A of the
Act.
• The selection of organizations, sites,
or participants to test models selected.
• The elements, parameters, scope,
and duration of such models for testing
or dissemination.
• Determinations regarding budget
neutrality under section 1115A(b)(3) of
the Act.
• The termination or modification of
the design and implementation of a
model under section 1115A(b)(3)(B) of
the Act.
• Determinations about expansion of
the duration and scope of a model under
section 1115A(c) of the Act, including
the determination that a model is not
expected to meet criteria described in
paragraph (1) or (2) of such section.
We interpret the preclusion from
administrative and judicial review
regarding the CMS Innovation Center’s
selection of organizations, sites, or
participants to test models selected to
preclude from administrative and
judicial review CMS’ selection of an
MFN participant, as well as CMS’
decision to terminate an MFN
participant, as these determinations are
part of CMS’ selection of participants for
CMS Innovation Center model tests.
We interpret the preclusion from
administration and judicial review
regarding the elements, parameters,
scope, and duration of models for
testing or dissemination to preclude
from administrative and judicial review
the following CMS determinations made
in connection with the MFN Model:
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• The selection of the model
geographic area for the MFN Model by
CMS;
• The selection of MFN Model drugs
by CMS; and
• The selection of included
international data, including selection
of countries, international drug pricing
databases, and international drug
pricing information.
In addition, we interpret the
preclusion from administrative and
judicial review regarding the elements
of the MFN Model to preclude from
administrative and judicial review the
methodology for determining MFN
Prices, MFN Drug Payment Amounts,
Alternative Add-on Amounts, and
reconciliation payments related to
financial hardship exemptions.
V. Collection of Information
Requirements
As stated in section 1115A(d)(3) of the
Act, Chapter 35 of title 44, United States
Code, shall not apply to the testing and
evaluation of CMS Innovation Center
Models. As a result, the information
collection requirements contained in
this IFC need not be reviewed by the
Office of Management and Budget.
However, costs incurred through
information collections are included in
section VI.C.5. of this IFC.
V. Response to Comments
Because of the large number of public
comments we normally receive on
documents, we are not able to
acknowledge or respond to them
individually. We will consider all
comments we receive by the date and
time specified in the DATES section of
this preamble, and, when we proceed
with a subsequent document, we will
respond to the comments in the
preamble to that document.
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VI. Regulatory Impact Analysis
A. Statement of Need
This IFC is necessary to address the
current Medicare Part B payment system
for separately payable Medicare Part B
drugs, which has several features that
may be incentivizing avoidable costs
and causing greater utilization of higher
priced drugs. By testing ways to address
these payment issues, the MFN Model
seeks to improve quality of care, address
features of the current payment system
that may be incentivizing unnecessary
Medicare Part B drug spending and
utilization of high cost drugs, and
ensure that the Medicare program and
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its beneficiaries pay generally
comparable prices for Medicare Part B
drugs relative to certain other countries.
As detailed in section III of this IFC,
this IFC will establish a 7-year
nationwide MFN Model alternative
payment test for approximately 50
separately payable Medicare Part B
drugs furnished by certain providers
and suppliers. As discussed in section
III.C. of this IFC, MFN participants will
include Medicare-participating
providers and suppliers that furnish
MFN Model drugs, with certain
exclusions. Most of the MFN
participants will be: Physicians; nonphysician practitioners; supplier groups;
HOPDs (including on- and off-campus
outpatient provider-based departments,
but excluding cancer hospitals,
children’s hospitals, CAHs, and other
hospitals exempt from the OPPS); and
ASCs. When other providers and
suppliers that are not excluded bill for
separately payable MFN Model drugs
(for example, pharmacies and
independent diagnostic testing
facilities), they will be included in the
MFN Model as MFN participants; based
on 2018 Medicare Part B claims data,
their aggregate annual volume of
separately payable Part B drugs was less
than $3.6 million. MFN participants
will be subject to the participation
requirements described in section III. of
this IFC.
B. Overall Impact
We have examined the impacts of this
IFC, as required by Executive Order
12866 on Regulatory Planning and
Review (September 30, 1993), Executive
Order 13563 on Improving Regulation
and Regulatory Review (February 2,
2013), the Regulatory Flexibility Act
(RFA) (September 19, 1980, Pub. L. 96–
354), section 1102(b) of the Act, section
202 of the Unfunded Mandates Reform
Act of 1995 (UMRA) (March 22, 1995,
Pub. L. 104–4), Executive Order 13132
on Federalism (August 4, 1999), and the
Congressional Review Act (5 U.S.C.
804(2)), and Executive Order 13771 on
Reducing Regulation and Controlling
Regulatory Costs (January 30, 2017).
Executive Orders 12866 and 13563
direct agencies to assess all costs and
benefits of available regulatory
alternatives and, if regulation is
necessary, to select regulatory
approaches that maximize net benefits
(including potential economic,
environmental, public health and safety
effects, distributive impacts, and
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76235
equity). Section 3(f) of Executive Order
12866 defines a ‘‘significant regulatory
action’’ as an action that is likely to
result in a rule: (1) Having an annual
effect on the economy of $100 million
or more in any 1 year, or adversely and
materially affecting a sector of the
economy, productivity, competition,
jobs, the environment, public health or
safety, or state, local or tribal
governments or communities (also
referred to as ‘‘economically
significant’’); (2) creating a serious
inconsistency or otherwise interfering
with an action taken or planned by
another agency; (3) materially altering
the budgetary impacts of entitlement
grants, user fees, or loan programs or the
rights and obligations of recipients
thereof; or (4) raising novel legal or
policy issues arising out of legal
mandates, the President’s priorities, or
the principles set forth in the Executive
Order. This IFC triggers these criteria.
A regulatory impact analysis (RIA)
must be prepared for major rules with
economically significant effects ($100
million or more in any 1 year). We
estimate that this rulemaking is
‘‘economically significant’’ as measured
by the $100 million threshold and hence
also a major rule under the
Congressional Review Act. Accordingly,
we have prepared a RIA that, to the best
of our ability, reflects the economic
impact of the policies contained in this
IFC.
C. Detailed Economic Analysis
The MFN Model will test different
payment rates for certain separately
payable Medicare Part B drugs and their
associated drug add-on payment. The
payment rates for these Medicare Part B
drugs will be phased in over 4 years,
ultimately arriving at the lowest price
for a particular drug from a selected
group of countries. Eligible providers
and suppliers participating in the 340B
program will be paid the lesser of this
amount or the payment outside the
model for MFN Model drugs they
purchase under the 340B program. This
IFC includes a single alternative add-on
payment, with MFN participants
receiving an amount that represents 6
percent (after sequestration) of the
average sales price (ASP) baseline for
the initial set of included drugs trended
forward. The phased-in MFN Price
discount relative to applicable ASP is
shown in Table 9, assuming the
relationship remains constant.
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TABLE 9—MOST FAVORED NATION DISCOUNT FROM ASP BY CALENDAR YEAR
Calendar year
2021
2022
2023
2024
2025
2026
2027
MFN Price impact ................................................................
¥16%
¥33%
¥49%
¥65%
¥65%
¥65%
¥65%
The model will require participation
by eligible providers and suppliers for
the selected separately payable
Medicare Part B drugs included in the
model. Certain provider types, defined
previously in this IFC, will be excluded
from the model. We assume that acute
care hospitals that are paid for
outpatient hospital services on a fully
capitated or global budget basis under a
waiver under such model of section
1833(t) of the Act will be excluded from
the MFN Model.
Because current payment rates for
340B covered entities that are paid
under the OPPS (hereafter called 340B
providers) are different from those for
other providers and suppliers (hereafter
called non-340B providers), the impact
of the MFN Model varies between the
two provider types, and therefore OACT
and ASPE estimated the financial
impacts separately. Similarly, both
analyses calculated the impact of the
drug add-on payment separately from
the MFN Price impact. Since the drug
add-on payment inside the model will
not be subject to beneficiary cost
sharing, and will be an additional
payment to 340B covered entities, the
associated Medicare expenditures are
higher.
The baseline for these analyses is
shown in Table 10, separately for OPPS
340B providers, OPPS non-340B
providers, and physician settings. These
values include all drugs, exclude
providers and suppliers that are exempt
from the model, and assume that 53%
of the hospital outpatient claims will be
from 340B providers. These payments
were then adjusted for beneficiary
responsibility, add-on payments, and
federal payments relative to ASP. These
values are on a pre-COVID–19 basis, and
the baseline is not are adjusted for the
effects of the pandemic. Similarly, the
impact analysis does not include the
effects of the COVID–19 pandemic.
Many assumptions such as utilization,
mortality, and morbidity are more
uncertain than usual due to the
pandemic. The direction and magnitude
of the financial impact of the pandemic
on Part B drug spending is uncertain.
For example, higher mortality due to
COVID–19 could lead to lower drug
utilization. A COVID–19-related drug
discovery could lead to higher drug
utilization. Beneficiaries seeking
treatment for quality of life
improvement may defer care during the
pandemic.
TABLE 10—BASELINE EXPENDITURES FOR CLAIMS INCLUDED IN THE MFN MODEL
(In billions)
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2020
2021
2022
2023
2024
2025
2026
2027
2020–27
OPPS Non-340B Providers ..........................................
OPPS 340B Providers .................................................
Other Providers and Suppliers .....................................
$6.1
6.9
19.4
$6.7
7.6
21.2
$7.5
8.4
23.3
$8.3
9.4
25.7
$9.2
10.4
28.1
$10.1
11.4
30.8
$11.2
12.6
33.8
$12.3
13.9
37.0
$71.4
80.5
219.3
Total ......................................................................
32.4
35.5
39.2
43.4
47.6
52.4
57.5
63.2
371.3
As the model does not dictate the
price that a drug manufacturer must
charge an MFN participant, there are
many possible behavioral responses by
manufacturers, providers, suppliers, and
beneficiaries. Because the estimates are
highly sensitive to these behavioral
assumptions, OACT provided three
scenarios: (i) An OACT estimate; (ii) an
illustrative estimate based on pricingeffects only; and (iii) an additional
illustration under the assumption that
manufacturers will refuse to change
prices and MFN participants will be
unwilling to administer drugs for which
model payment will be below their
acquisition cost. ASPE also developed a
bottom-up estimate built from analysis
of the IFC’s likely potential effects on
different types of separately payable
Part B drugs.
To better understand the values
shown in the three OACT scenarios, the
ASPE estimate, and the policy of the
model, consider the following example.
Suppose the current ASP for a given
drug is $100. The total payment to the
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provider for this drug under the current
system is $104.30, inclusive of the
federal payment for the drug and the
add-on, beneficiary cost-sharing, and
net of sequestration. Now suppose the
MFN Price of this drug is also $100. The
total payment to the provider under the
model would be $104.40. Under the
model, the drug payment after
sequestration is unchanged ($98.40) but
the add-on increases from $5.90 to
$6.00.
1. OACT Estimate
Manufacturers could adopt several
strategies in response to the model, such
as (i) charging a lower price to providers
and suppliers inside the model; (ii)
refusing to adjust their price from the
non-model amounts; or (iii) altering the
availability and terms of their
international prices. Given that the
international price data represent a
challenge to their U.S. market revenues,
manufacturers are expected to devote
considerable resources to the third
option. This assumption is included in
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the OACT estimate as a different
discount relative to ASP compared with
the values in Table 9. For drugs with
significant use outside of Medicare,
manufacturers may be willing to
sacrifice utilization and revenue within
the model. For drugs that are used
primarily in the Medicare program,
manufacturers may believe that offering
some pricing relief is necessary to
preserve a significant portion of their
revenue.
Eligible providers and suppliers will
need to decide if the difference between
the amount that Medicare will pay and
the price that they must pay to purchase
the drugs would allow them to continue
offering the drugs. For 340B providers,
the payment rates in the first year will
match their payments outside the
model. Accordingly, no change to
utilization or costs is expected under
the model in the first year for 340B
providers. In later years, the impact
varies depending on the assumed
change to international price data. For
non-340B providers, some may be
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willing to provide the drugs under a
lower payment rate to retain utilization
on other associated services.
Should an eligible provider or
supplier be unable to offer access to the
included drugs, beneficiaries will be left
with several options. They could seek
access to the drugs by traveling to an
excluded provider or supplier, access
the drugs through a 340B provider in
the model, or forgo access.
It should be noted that this model
does not have a reliable precedent in the
U.S. market; consequently, there is an
unusually high degree of uncertainty in
these assumptions, particularly with
respect to the behavioral responses. To
illustrate this uncertainty, three
potential financial effects are included
in this analysis; a full range of potential
behavioral effects are presented under
an Extreme Disruption scenario where
non-340B utilization of affected drugs
drops to zero percent and under a
Pricing-Effects Only scenario where all
currently projected utilization is
assumed to be retained. The OACT
estimate reflects one reasonable set of
assumptions for potential changes in
manufacturer, provider, and supplier
behavior. Other estimates outside the
range of the three scenarios could be
reasonable as well, due to the wide
range of potential responses.
The OACT assumptions consider that
the separately payable Medicare Part B
drugs make up approximately 5 percent
of the overall U.S. prescription drug
market. Drug manufacturers could see
this model as an obstacle to their pricing
throughout the market, which could
cause strong resistance to the model.
The OACT assumptions reflect that
some manufacturers will adhere to their
current pricing instead of lowering sales
prices in response to the model. This
behavior may persist in spite of pricing
in other sectors of the market or other
countries that demonstrates an ability to
offer the drug at the model payment
rates, and would result in unmet
demand for these Medicare Part B drugs.
After considering the relative size of the
Medicare Part B market, the current
price control of drug manufacturers, the
size of the model price reductions, the
nature of the Medicare Part B drug
providers and suppliers, the flexibility
that manufacturers may have in
adjusting pricing and arrangements in
other countries, and many other factors,
actuarial judgment was applied to
determine the assumptions that are
reflected in the OACT estimate, as
shown in Table 11.
Beneficiaries lacking continued
availability of their drugs through their
current provider or supplier are
assumed to seek access outside the
model, to obtain their drugs through
340B providers, or to forgo access. The
schedule of the phase-in to the MFN
price gives manufacturers incentive to
adjust or reduce access to international
price data quickly. Accordingly,
manufacturers are assumed to raise the
published international prices
beginning in 2022 and to retain a 25percent MFN Price discount relative to
applicable ASP.
As a result of this expected behavior
from manufacturers, 340B provider
payments will see a 3-percent reduction
compared to the current Medicare
payment in 2022 and subsequent years.
This 3-percent reduction represents the
impact of the 25-percent MFN Price
discount relative to the OPPS payment
to 340B providers of ASP less 22.5
percent, as that is the current payment
formula for 340B providers. This
represents a relatively small price
change and is assumed to occur later in
the model, so will be more predictable
than the payment changes for non-340B
providers. As a result, manufacturers
and 340B providers are assumed to
come to an agreement to continue to
provide for all of their utilization.
Because all regions are covered under
the model, beneficiaries seeking a
provider outside of the model will be
limited to an excluded provider or
supplier, such as a critical access
hospital. Based on the historical trend of
drug spending by excluded providers
and suppliers as a percentage of total
Medicare Part B drugs, the OACT
estimate reflects only 1 percent of use
shifting to non-model providers.
Furthermore, because the OPPS
payment to 340B providers will be
reduced year two through year seven of
the model, and because their capacity is
limited, 10 percent of use is assumed to
shift to 340B providers. Other
utilization not covered by providers and
suppliers continuing to provide access
in the model or by excluded providers
and suppliers is assumed to be
utilization not covered by the Medicare
benefit.
TABLE 11—ASSUMPTIONS REFLECTED IN OACT ESTIMATE
2021
(%)
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Non-340B providers:
Behavior:
Continued Availability ........................................................................
Altered Availability:
Move to non-MFN ......................................................................
Move to 340B .............................................................................
No Access ..................................................................................
Total ....................................................................................
MFN Price impact ............................................................................................
340B providers:
Behavior:
Continued Availability ........................................................................
MFN Price impact ............................................................................................
Table 12 shows the estimated
financial impacts under the model
based on the assumptions in Table 11.
Medicare savings are estimated to be
$85.5 billion, net of the premium offset.
While there are significant savings as a
result of this model, a portion of the
savings is attributable to beneficiaries
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2022
(%)
Frm 00059
Fmt 4701
2024
(%)
2025
(%)
2026
(%)
2027
(%)
80
75
70
70
70
70
70
1
10
9
100
¥16
1
10
14
100
¥25
1
10
19
100
¥25
1
10
19
100
¥25
1
10
19
100
¥25
1
10
19
100
¥25
1
10
19
100
¥25
100
0
100
¥3
100
¥3
100
¥3
100
¥3
100
¥3
100
¥3
not accessing their drugs through the
Medicare benefit, along with the
associated lost utilization. This estimate
does not capture any impacts to other
program costs as a result of lower
utilization. This estimate is on a preCOVID–19 basis, and is not adjusted for
the effects of the pandemic.
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(%)
Sfmt 4700
To the extent that manufacturers
discount their products for Medicare
sales, there may be a reduction in
Medicaid Best Price or AMP.
Reductions in Best Price could result in
increased Medicaid rebates and thus
lower Medicaid costs. However,
reductions in AMP generally result in
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lower statutory and inflationary rebates
under the Medicaid program. Therefore,
if the manufacturer discounts a drug so
that it is closer to the Medicaid best
price, there is a possibility of increased
Medicaid costs as a result of the model.
Furthermore, the effects on AMP may be
reduced or eliminated, if manufacturers
respond by increasing prices in the
private health insurance market. These
estimates do not include secondary
impacts to other sectors of the market as
a result of the changes in Medicare
payments under the model in part due
to the significant uncertainty around
manufacturer pricing behavior in
response to this model.
TABLE 12—ESTIMATED FINANCIAL IMPACT OF MFN MODEL
(In billion dollars)
2021
Drug price reduction:
FFS impact * .........................................................................
Gross impact (FFS+MA) ** ...................................................
Net of premium offset *** ......................................................
Medicaid impact ....................................................................
Federal ...........................................................................
State ..............................................................................
Drug add-on payment:
FFS impact ...........................................................................
Gross impact (FFS+MA) .......................................................
Net of premium offset ...........................................................
Medicaid impact ....................................................................
Federal ...........................................................................
State ..............................................................................
Total impact:
FFS impact ...........................................................................
Gross impact (FFS+MA) .......................................................
Net of premium offset ...........................................................
Medicaid impact ....................................................................
Federal ...........................................................................
State ..............................................................................
2022
2023
2024
2025
2026
2027
2021–27
¥4.7
¥4.7
¥3.5
¥0.4
¥0.2
¥0.2
¥7.5
¥7.5
¥5.6
¥0.6
¥0.3
¥0.2
¥9.3
¥17.6
¥13.2
¥1.3
¥0.8
¥0.6
¥10.2
¥19.5
¥14.6
¥1.5
¥0.8
¥0.6
¥11.2
¥21.6
¥16.2
¥1.6
¥0.9
¥0.7
¥12.3
¥24.0
¥18.0
¥1.8
¥1.0
¥0.8
¥13.5
¥26.5
¥19.9
¥2.0
¥1.1
¥0.9
¥68.7
¥121.4
¥91.1
¥9.1
¥5.2
¥3.9
0.6
0.6
0.4
¥0.1
¥0.1
0.0
0.6
0.6
0.4
¥0.1
¥0.1
0.0
0.5
1.0
0.7
¥0.1
¥0.1
0.0
0.6
1.1
0.8
¥0.1
¥0.1
¥0.1
0.6
1.2
0.9
¥0.1
¥0.1
¥0.1
0.7
1.4
1.0
¥0.1
¥0.1
¥0.1
0.8
1.5
1.2
¥0.2
¥0.1
¥0.1
4.4
7.4
5.6
¥0.8
¥0.5
¥0.4
¥4.1
¥4.1
¥3.1
¥0.4
¥0.3
¥0.2
¥7.0
¥7.0
¥5.2
¥0.7
¥0.4
¥0.3
¥8.8
¥16.6
¥12.4
¥1.4
¥0.8
¥0.6
¥9.6
¥18.4
¥13.8
¥1.6
¥0.9
¥0.7
¥10.6
¥20.4
¥15.3
¥1.8
¥1.0
¥0.8
¥11.6
¥22.6
¥16.9
¥1.9
¥1.1
¥0.8
¥12.7
¥25.0
¥18.7
¥2.1
¥1.2
¥0.9
¥64.4
¥114.0
¥85.5
¥9.9
¥5.7
¥4.3
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* Projected spending impact in the traditional Medicare FFS program under the model.
** Projected spending impact in both Medicare FFS and Medicare Advantage (MA).
*** Premium offset represents the change in the Part B premium income that would result from the change in Part B drug expenditures.
These impacts are based on the
President’s Fiscal Year 2021 Budget
baseline for Medicare Part B drugs,
including those dispensed by 340B
providers. Due to rounding, the sum of
values in the table may differ slightly
from the total results in the table. In
addition to the behavioral assumptions
in Table 11, these estimates reflect a
number of other technical assumptions,
including the following:
• Amounts illustrate the potential
impact on Medicare Part B drug
spending, assuming the reductions are
achievable and realized.
• Amounts are presented by calendar
year and are based on the date the
service is incurred and have therefore
not been adjusted to reflect when
payment is made.
• The model runs from January 1,
2021 through December 31, 2027. If any
of the provisions of this rule are not
effective on January 1, 2021, the impacts
will differ.
• The model will include the top 50
Medicare Part B drugs with the highest
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Jkt 253001
spending each year and will account for
roughly 73 percent of Medicare Part B
drug spending in each affected year.
• All included providers and
suppliers receive an add-on payment of
6 percent (after sequestration) of the
average sales price (ASP) and this addon payment is not subject to beneficiary
cost sharing.
• The impacts reflect changes to
payments to Medicare Advantage plans
starting in 2023.
• The premium offset is 25 percent of
the gross impact.
• The Medicaid impact represents the
portion of beneficiary cost sharing paid
on behalf of dual-eligible beneficiaries
(split 57 percent/43 percent between
Federal and State).
• The Medicaid impact does not
account for the potential impacts to
AMP or Best Price in the Medicaid
program.
a. Pricing Effects Only Illustration
As mentioned previously, there is
much uncertainty around the behavioral
PO 00000
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assumptions underlying the estimated
financial impacts. To show the effects of
the model absent any provider or
beneficiary behavioral responses, OACT
calculated the impacts of the payment
changes alone. These values reflect the
pricing changes inside the model, as
shown in Table 9, and the assumption
that manufacturers and MFN
participants are able to continue to
provide access to all drugs. Again,
because 340B providers will receive the
lesser of the model payment amount or
the amount outside the model for the
drug, no impact to their costs is
expected for the first year. Results for
this illustration are shown in Table 13,
and they reflect the same technical
assumptions as the OACT estimate. The
net impact on Medicare after the
premium offset is a savings of $155.6
billion over the 7-year period, and none
of the impact would be due to lost
utilization.
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76239
TABLE 13—ESTIMATED IMPACT OF PRICING EFFECTS ONLY ILLUSTRATION
(In billion dollars)
2021
Drug price reduction:
FFS impact * .........................................................................
Gross impact (FFS+MA) ** ...................................................
Net of premium offset *** ......................................................
Medicaid impact ....................................................................
Federal ...........................................................................
State ..............................................................................
Drug add-on payment:
FFS impact ...........................................................................
Gross impact (FFS+MA) .......................................................
Net of premium offset ...........................................................
Medicaid impact ....................................................................
Federal ...........................................................................
State ..............................................................................
Total impact:
FFS impact ...........................................................................
Gross impact (FFS+MA) .......................................................
Net of premium offset ...........................................................
Medicaid impact ....................................................................
Federal ...........................................................................
State ..............................................................................
2022
2023
2024
2025
2026
2027
2021–27
¥3.1
¥3.1
¥2.4
¥0.2
¥0.1
¥0.1
¥7.3
¥7.3
¥5.5
¥0.5
¥0.3
¥0.2
¥13.1
¥24.7
¥18.5
¥1.9
¥1.1
¥0.8
¥20.1
¥38.5
¥28.9
¥2.9
¥1.6
¥1.2
¥23.0
¥44.4
¥33.3
¥3.3
¥1.9
¥1.4
¥25.3
¥49.2
¥36.9
¥3.7
¥2.1
¥1.6
¥27.7
¥54.5
¥40.9
¥4.1
¥2.3
¥1.8
¥119.7
¥221.8
¥166.4
¥16.6
¥9.5
¥7.2
0.9
0.9
0.7
¥0.1
0.0
0.0
1.0
1.0
0.7
¥0.1
¥0.1
0.0
1.1
2.0
1.5
¥0.1
¥0.1
0.0
1.2
2.2
1.7
¥0.1
¥0.1
0.0
1.3
2.5
1.9
¥0.1
¥0.1
¥0.1
1.4
2.8
2.1
¥0.1
¥0.1
¥0.1
1.6
3.1
2.3
¥0.1
¥0.1
¥0.1
8.3
14.4
10.8
¥0.8
¥0.5
¥0.3
¥2.3
¥2.3
¥1.7
¥0.3
¥0.2
¥0.1
¥6.4
¥6.4
¥4.8
¥0.6
¥0.4
¥0.3
¥12.0
¥22.7
¥17.0
¥2.0
¥1.1
¥0.8
¥19.0
¥36.3
¥27.2
¥3.0
¥1.7
¥1.3
¥21.7
¥41.9
¥31.5
¥3.5
¥2.0
¥1.5
¥23.9
¥46.5
¥34.9
¥3.8
¥2.2
¥1.6
¥26.2
¥51.4
¥38.6
¥4.2
¥2.4
¥1.8
¥111.4
¥207.4
¥155.6
¥17.4
¥9.9
¥7.5
* Projected spending impact in the traditional Medicare FFS program under the model.
** Projected spending impact in both Medicare FFS and Medicare Advantage (MA).
*** Premium offset represents the change in the Medicare Part B premium income that would result from the change in Medicare Part B
expenditures.
b. Extreme Disruption Illustration
To cover the spectrum of possible
outcomes, the impact of a greater
behavioral response from manufacturers
and MFN participants was also
considered. Under this scenario, it is
assumed that non-340B providers and
suppliers will not be able to obtain any
of the current drugs inside the model.
All non-340B utilization will then be
divided among the three beneficiary
choices of traveling to an excluded
provider or supplier, using a 340B
provider, or forgoing access. Because
there are a small number of excluded
providers and suppliers, OACT assumed
they only have capacity for a 25 percent
increase in utilization. Additionally,
manufacturers are assumed to not
change the international prices; as a
result, 340B providers will have
reduced reimbursement beginning in
2022, when the MFN Price dips below
the baseline payment of ASP less 22.5
percent—leading to reduced beneficiary
access through 340B providers as well.
The financial hardship exemption could
possibly apply under this scenario, but
as this payment is retrospective and the
losses prior to the payment would be
severe, it is unclear whether providers
will be in a position to request the
exemption.
The illustrative results under these
assumptions are shown in Table 14.
They weredeveloped with the same
technical assumptions listed under the
OACT estimate. The overall impact of
the model would be a substantial
savings to Medicare of $286.3 billion,
but nearly half of that impact would be
due to lost utilization.
TABLE 14—ESTIMATED IMPACT OF EXTREME DISRUPTION ILLUSTRATION
jbell on DSKJLSW7X2PROD with RULES2
(In billion dollars)
Drug price reduction:
FFS impact * .........................................................................
Gross impact (FFS+MA) ** ...................................................
Net of premium offset *** ......................................................
Medicaid impact ....................................................................
Federal ...........................................................................
State ......................................................................................
Drug add-on payment:
FFS impact ...........................................................................
Gross impact (FFS+MA) .......................................................
Net of premium offset ...........................................................
Medicaid impact ....................................................................
Federal ...........................................................................
State ..............................................................................
Total impact:
FFS impact ...........................................................................
Gross impact (FFS+MA) .......................................................
Net of premium offset ...........................................................
Medicaid impact ....................................................................
Federal ...........................................................................
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2021
2022
2023
2024
2025
2026
2027
¥17.6
¥17.6
¥13.2
¥1.3
¥0.8
¥0.6
¥21.2
¥21.2
¥15.9
¥1.6
¥0.9
¥0.7
¥26.9
¥50.9
¥38.2
¥3.8
¥2.2
¥1.6
¥30.5
¥58.4
¥43.8
¥4.4
¥2.5
¥1.9
¥33.7
¥65.0
¥48.7
¥4.9
¥2.8
¥2.1
¥37.0
¥72.0
¥54.0
¥5.4
¥3.1
¥2.3
¥40.6
¥79.7
¥59.8
¥6.0
¥3.4
¥2.6
¥207.5
¥364.8
¥273.6
¥27.4
¥15.6
¥11.8
¥0.6
¥0.6
¥0.5
¥0.1
¥0.1
0.0
¥0.8
¥0.8
¥0.6
¥0.1
¥0.1
0.0
¥1.2
¥2.3
¥1.8
¥0.1
¥0.1
0.0
¥1.5
¥2.8
¥2.1
¥0.1
¥0.1
¥0.1
¥1.6
¥3.1
¥2.3
¥0.1
¥0.1
¥0.1
¥1.8
¥3.4
¥2.6
¥0.1
¥0.1
¥0.1
¥1.9
¥3.8
¥2.9
¥0.2
¥0.1
¥0.1
¥9.4
¥16.9
¥12.7
¥0.8
¥0.5
¥0.4
¥18.2
¥18.2
¥13.7
¥1.4
¥0.8
¥22.0
¥22.0
¥16.5
¥1.7
¥1.0
¥28.2
¥53.2
¥39.9
¥3.9
¥2.2
¥32.0
¥61.2
¥45.9
¥4.5
¥2.6
¥35.3
¥68.1
¥51.1
¥5.0
¥2.9
¥38.7
¥75.5
¥56.6
¥5.5
¥3.2
¥42.5
¥83.5
¥62.6
¥6.1
¥3.5
¥217.0
¥381.7
¥286.3
¥28.2
¥16.1
Fmt 4701
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76240
Federal Register / Vol. 85, No. 229 / Friday, November 27, 2020 / Rules and Regulations
TABLE 14—ESTIMATED IMPACT OF EXTREME DISRUPTION ILLUSTRATION—Continued
(In billion dollars)
2021
State ..............................................................................
¥0.6
2022
¥0.7
2023
¥1.7
2024
¥1.9
2025
¥2.2
2026
¥2.4
2027
¥2.6
2021–27
¥12.1
* Projected spending impact in the traditional Medicare FFS program under the model.
** Projected spending impact in both Medicare FFS and Medicare Advantage (MA).
*** Premium offset represents the change in the Medicare Part B premium income that would result from the change in Medicare Part B
expenditures.
c. Additional Considerations
Because the model will make
substantial changes to payment for
Medicare Part B drugs, there are many
other potential responses not considered
in this analysis. It is possible that
manufacturers could increase prices for
non-Part B drugs, which would affect
both private market and Part D
expenditures, although that potential
impact has not been quantified for this
estimate. It is also possible that moving
to a flat add-on payment from a
percentage of drug cost will have
additional effects, which are not
considered in the OACT analysis. The
analysis is on a pre-COVID–19 basis,
and neither the baseline nor the impact
analysis are adjusted for the effects of
the pandemic.
jbell on DSKJLSW7X2PROD with RULES2
2. ASPE Estimate
The behavioral responses of
manufacturers, providers, suppliers, and
beneficiaries to the MFN Model are
critical to estimating its impact on key
outcomes. Lack of direct experience
with policies such as the MFN Model,
however, results in great uncertainty for
making these behavioral assumptions.
For a robust approach, ASPE made a
number of assumptions based on
published literature and expert
consensus, and applied such
assumptions on a drug-by-drug basis.
Please note that ASPE has not adjusted
the assumptions and estimates based on
the effects of the COVID–19 pandemic.
The behavioral assumptions in this
approach first address manufacturers’
responses in the international market
that might increase MFN Prices; and
then the potential responses to the MFN
Drug Payment Amounts by the
manufacturers and providers and
suppliers that purchase MFN Model
drugs and submit a claim to Medicare
after administering such drugs to
beneficiaries. In general, these
assumptions represent the proposition
that manufacturers prefer to sell their
products, even at lower prices, as long
as net revenues (net sales prices minus
production and distribution costs)
remain positive; and that providers and
suppliers are committed to maintaining
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effective treatments for beneficiaries
either by negotiating lower prices,
accepting reduced revenue, or finding
effective Medicare Part B or Part D
alternative treatments.
To assess the likelihood of each of the
alternative manufacturer responses to
the MFN Model, ASPE reviewed
published literature on the impacts and
interviewed a small cohort of experts
regarding the potential impacts.
Published literature suggests that when
a large country establishes an
international reference price, smaller
reference countries experience price
increases and longer launch delays for
new products.85 ASPE’s conversations
with experts suggested that as a result
of the MFN Model, prices in other
countries could increase at the exmanufacturer level, potentially up to
current ASP levels, and manufacturers
could change formulations of MFN
Model drugs to lessen the impact of the
model. The experts generally believe
that manufacturers will be able to price
discriminate between the Medicare Part
B market and other markets within the
U.S. Potential utilization impacts will
thus be limited to Medicare Part B
beneficiaries, as payments to providers
and suppliers for drugs provided to
other patients will not be affected by the
model.
Considering this information, ASPE
made a series of assumptions for a base
analysis. First, ASPE considered a static
group of 50 drugs for this analysis.
Based on the literature and interviews
with experts, ASPE assumed
manufacturers of newly launched brand
products that become MFN Model drugs
would adjust their international pricing
strategies so that the MFN Payment
Amount will be equal to ASP absent of
the MFN Model. This assumption does
not necessarily mean that net
international prices (ex-manufacturer
sales prices minus the value of rebates
or other financial concessions) will be
equal to the ASP. In addition, ASPE
85 Patricia M. Danzon, ‘‘The Economics of the
Biopharmaceutical Industry’’, in Sherry Glied and
Peter C. Smith (eds.), The Oxford Handbook of
Health Economics, Oxford University Press 2011,
pp. 520–554.
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assumed that manufacturers of currently
marketed drugs outside but near the top
50 Medicare Part B drugs based on
annual allowed charges (with certain
exclusions and exemptions) will lower
their U.S. prices in an attempt to
prevent them from becoming MFN
Model drugs. To compensate for this
response, ASPE assumed that
manufacturers will increase prices for
non-MFN Model drugs. Since
companies often sell many different
drugs, ASPE assumed they will have
some flexibility to allocate discounts
between different drugs to ensure no
currently marketed non-MFN Model
drugs enter the top 50 while
maintaining near constant revenues. In
some cases, there are relatively new
drug products that may not have
launched or may be recently launched
in the included countries that may enter
the top 50. In those cases, ASPE
assumed the manufacturers will reevaluate their international pricing
strategies to ensure the MFN Price is
comparable to ASP absent of the MFN
Model. ASPE assumed that these
changes to U.S. prices of non-MFN
Model drugs will ultimately fully offset
one another in terms of Medicare Part B
drug spending as well.
For the 50 MFN Model drugs, the
MFN Price ultimately depends on the
prices for the drugs in the included
countries. The exact mechanisms in
which prices are determined in
included countries differ by country and
sometimes by product. These
mechanisms include national (or subnational tendering 86), therapeutic-level
reference pricing, international
reference pricing, cost-effectiveness
analysis, and negotiation. These
mechanisms generally result in lower
observed prices in other countries
compared to the U.S., and these
differences tend to be larger for products
that have more competition than in the
U.S. (such as more biosimilar
competition) or have only a marginally
better clinical profile than a cheaper
86 Tendering is a formal procedure to purchase
medications using competitive bidding for a
particular contract.https://www.ncbi.nlm.nih.gov/
pmc/articles/PMC5628685/.
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Federal Register / Vol. 85, No. 229 / Friday, November 27, 2020 / Rules and Regulations
therapy. Since the U.S. price under this
model depends on the prices in other
countries, the model will likely result in
increased observed prices in other
countries. This does not mean that net
prices will necessarily increase as
countries will try to find ways to
prevent spending increases while
limiting disruption in their drug
markets. In this analysis, ASPE
considered the potential impact at the
drug-level because the context of each
drug may determine the MFN Price.
ASPE modeled the pricing response to
the change in direct drug payment for
each of the 50 MFN Model drugs shown
in Table 6 of this IFC. ASPE assumed
that any changes in international sales
prices for included countries would not
occur until the beginning of the second
performance year of the MFN Model.
ASPE modeled the manufacturer pricing
response based on available 2019
international drug pricing information,
using the sales and volume data that
CMS used to calculate the MFN Prices
shown in Table 6 of this IFC. ASPE did
not model how manufacturers and
providers might take into account the
changes to the add-on.
If there was only one related brand for
the included countries,87 then ASPE
assumed the MFN Price for a drug will
increase to the average price of the drug
for the included countries plus 10
percent (with the cap of ASP). ASPE
made this assumption because at this
point the market size of the included
countries is roughly the size of the
Medicare Part B market for many of the
MFN Model drugs. ASPE applied this
approach to 34 of the 50 MFN Model
drugs. ASPE assumed that the MFN
Price will not likely increase by more
than this because, even if the net price
is constant for purchasers in the
included countries, these countries may
seek to avoid larger increases in
transaction prices. In the case of drugs
with no international spending in 2019,
ASPE assumed that the model would
have no impact. ASPE applied this
approach to 2 of the 50 MFN Model
drugs. When the MFN Price was
calculated based on international drug
pricing information for a country with
access to biosimilar products or a
competitor brand product that is not one
of the MFN Model drugs, ASPE
assumed smaller international price
increases because the MFN Model
would reduce the incentive for the
manufacturer of an MFN Model drug to
compete in those international markets.
This approach applied to 8 of the 50
87 For this analysis, we included available sales
and volume data for the brand drug manufacturer
and any parallel importers of the brand drug.
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MFN Model drugs. When the MFN Price
was calculated using international drug
pricing information for a non-innovator
unbranded product, ASPE assumed that
the MFN Price would not increase. This
assumption applied to 6 of the 50 MFN
Model drugs.
After analyzing price changes
internationally, ASPE analyzed the
potential for beneficiaries to switch to
other products with, for example, the
same active ingredient within the U.S.
and billed with HCPCS codes that are
not among the MFN Model drugs. First,
ASPE assumed that when a
manufacturer has multiple branded
products with different indications
represented by the same HCPCS code,
the manufacturer will work to obtain a
new HCPCS code for the product in
which Medicare Part B makes up a
smaller portion of its overall market. In
addition, the manufacturer will restrict
the amount of product sold that could
be billed under this new HCPCS code so
that such products will not become
included in the MFN Model. This
assumption applied to one of the MFN
Model drugs. ASPE also assumed that if
an MFN Model drug is available within
the U.S. in a formulation that will be
covered under Medicare Part D, the
manufacturer will work to shift 90
percent of the utilization from Medicare
Part B to Medicare Part D. This
assumption impacted 2 of the 50 MFN
Model drugs.
In addition to these assumptions,
ASPE made assumptions about potential
generic entry for some of the MFN
Model drugs. ASPE assumed that MFN
Model drugs with generic drugs
approved within the included countries
or currently subject to on-going
Paragraph 4 patent challenges would
have generic competition by
performance year 3. This assumption
impacted 6 of the 50 MFN Model drugs.
After examining the potential price
impacts and other utilization changes
described previously, ASPE examined
the potential for utilization impacts. In
general, economic theory and the
experts ASPE interviewed suggested
that manufacturers will adjust U.S.
prices to maintain sales as long as price
is greater than marginal costs of
producing and distributing the drug.
ASPE also assumed that manufacturers
will have substantial ability to price
discriminate—that is, adjust pricing for
Medicare-participating providers and
suppliers to reflect discounts for their
Medicare Part B patient share as
opposed to all patients. Nonetheless,
ASPE still considered the potential that
price discrimination will be less than
perfect for some drugs. In these cases, a
manufacturer might refuse to negotiate
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76241
lower prices for MFN beneficiaries if
doing so threatens its ability to sell in
other segments of the U.S. at a positive
margin. That is, would the loss in
revenues from selling for all purchasers
at a reduced price exceed the loss in
revenues from losing the MFN
beneficiary share of business for that
drug? To examine this issue, ASPE
estimated the Medicare Part B share of
each MFN Model drug compared with
the estimated U.S. market. If it seemed
likely that a manufacturer will have
higher revenues selling to all purchasers
at prices slightly above the MFN Drug
Payment Amount than not selling to
MFN participants for MFN beneficiary
use, ASPE assumed the manufacturer
will not restrict MFN beneficiaries’
access to an MFN Model drug under
Medicare Part B. This included
examining if the MFN Model drugs had
U.S. competitors. Since MFN
participants likely treat both Part B
beneficiaries and non-Part B
beneficiaries (including individuals
with employer, individual market, or
Medicaid coverage), an MFN participant
may select an alternative therapy
marketed by a competitor that can be
provided to both types of patients. As a
result, manufacturers will have an
incentive to work to maintain utilization
so long as the MFN Payment Amount is
not too low.
In cases where manufacturers might
refuse to lower U.S. prices sufficiently
to make it financially feasible for MFN
participants to furnish the drug and
receive the MFN Payment Amount,
ASPE examined whether there were
products that had similar therapeutic
effects to a MFN Model drug. ASPE
assumed that Medicare Part B
beneficiaries will be switched to the
potential alternative products. ASPE
made these assessments for each
performance year. ASPE assumed that
half of Medicare Part B beneficiaries
will continue accessing their current
drugs through 340B providers. Such
changes in drug utilization or service
providers will likely result in additional
burdens for patients. ASPE did not
quantify these impacts.
Additionally, for biological drugs for
which there are licensed biosimilar
products, ASPE assumed that there will
be at least one biosimilar manufacturer
that is willing to provide its product at
MFN payment levels if the reference
manufacturer would not supply this
drug. We note however that if reference
manufacturers are willing to sell at MFN
payment levels, providers may not have
any incentive to use biosimilar
products. The extent to which providers
may use biosimilar products will
depend on whether they are easier to
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Federal Register / Vol. 85, No. 229 / Friday, November 27, 2020 / Rules and Regulations
access instead of a product subject to
the model. The biosimilar
manufacturers will need to balance
those considerations with the possibility
that sufficiently large sales may also
result in that product becoming an MFN
Model drug. ASPE assumed any
utilization changes that occur will result
in zero net changes in spending. ASPE
made no assumptions about the
potential entry of biosimilar products
for reference products that currently do
not have biosimilar competition in the
U.S. or referenced countries.
The overall utilization impact is the
sum of the impacts for each of the 50
MFN Model drugs. These impacts
reflect, on a drug by drug basis, the
assumptions outlined previously.
Specifically, where estimates reduced
utilization, it reflects assumptions that
either manufacturers will be unwilling
to reduce prices to MFN participants,
viable substitute drugs are not available
for all affected patients, or both. In such
cases, ASPE assumed that half of the
impacted beneficiaries will be able to
still access the MFN Model drug
through a 340B provider.
ASPE calculated the potential impacts
of the MFN Model by calendar year.
ASPE assumed that at the end of the
MFN Model, there will be no continued
impacts because Medicare Part B
payments for MFN Model drugs will
immediately be based on non-model
payment policies at the end of the MFN
Model. Given the predictable 7-year
model performance period, ASPE
assumed manufacturers and MFN
participants will have sufficient time to
structure their agreements to ensure a
seamless transition after the end of the
MFN Model.
Table 15 summarizes the results of the
ASPE analysis.
TABLE 15—ASSUMPTIONS REFLECTED IN ASPE ESTIMATE
2021
(%)
Non-340B providers:
Behavior:
Continued Availability ........................................................................
Altered Availability:
Shift to other drugs .....................................................................
Move to 340B .............................................................................
No Access ..................................................................................
Total ....................................................................................
MFN Price impact ............................................................................................
340B providers:
Behavior:
Continued Availability ........................................................................
MFN Price impact ............................................................................................
jbell on DSKJLSW7X2PROD with RULES2
ASPE estimated the Medicare FFS
program impacts of the change from
ASP-based payment to MFN-based
payment.88 The Medicare FFS impact
includes changes in spending for
Medicare Parts B and D.
For patients that switch to 340B
providers, ASPE estimated the spending
change based on the difference in the
MFN Model payment for drugs acquired
under the 340B program and the current
Medicare Part B OPPS payment policy.
These impacts are generally
considered transfer impacts of the
model. To estimate these impacts, ASPE
took an approach similar to OACT.
88 An indirect benefit of this IFC may be reduced
distortions in the labor markets taxed to support the
Medicare Trust Fund. Such distortions are
sometimes referred to as marginal excess tax burden
(METB), and Circular A–94—OMB’s guidance on
cost-benefit analysis of federal programs, available
at https://www.whitehouse.gov/sites/
whitehouse.gov/files/omb/circulars/A94/a094.pdfsuggests that METB may be valued at roughly 25
percent of the estimated transfer attributed to a
policy change; the Circular goes on to direct the
inclusion of estimated METB change in
supplementary analyses. If secondary benefits—
such as reduced marginal excess tax burden is, in
the case of this IFC—are included in regulatory
impact analyses, then secondary costs must be as
well, in order to avoid inappropriately skewing the
net benefits results, and including METB only in
supplementary analyses provides some
acknowledgement of this potential imbalance.
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2022
(%)
Frm 00064
Fmt 4701
2024
(%)
2025
(%)
2026
(%)
2027
(%)
100.0
100.0
97.7
95.9
96.2
96.5
96.7
0.0
0.0
0.0
100
¥11.4
0.0
0.0
0.0
100
¥14.3
1.1
1.1
0.0
100
¥18.1
2.1
2.1
0.0
100
¥20.5
1.9
1.9
0.0
100
¥19.4
1.8
1.8
0.0
100
¥17.9
1.6
1.6
0.0
100
¥16.5
100
0
100
0
100
0
100
0
100
0
100
0
100
0
ASPE used the direct reduction in
Medicare Part B payments due to lower
MFN payment amounts and translated
that into transfers from the healthcare
system to the government, beneficiaries,
and Medicaid. In addition to the direct
effects of lower payments and
associated cost-sharing, the model
results in downstream transfers
associated with changes in Part B
premiums and government payments to
Medicare Advantage Plans. Like OACT,
ASPE estimated Medicaid impacts
based on changes to federal and state
shares of prescription drug costs for
dual eligibles but did not estimate
impacts on Medicaid that may result
from changes in net payments under the
Medicaid Drug Rebate Program.
Overall, the model results in changes
to federal spending in Medicare
(including Part B, and Part D) from the
model price and utilization impacts,
changes in federal and state spending on
Medicaid resulting from changes to the
governmental obligation of Medicare
cost-sharing for dual eligible
beneficiaries, and changes in federal
spending associated with add-on
payment changes in the model. The
model also results in changes to
beneficiary spending resulting from
changes in cost-sharing for drugs,
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(%)
Sfmt 4700
changes in beneficiary premiums, and
changes to cost-sharing associated with
the add-on payment. These transfers on
net balance out with reduced revenues
for healthcare providers (which may be
completely or mostly offset by the
reduced cost of acquiring drugs),
reduced revenues for pharmaceutical
manufacturers, and reduced revenues
for MA plans.
Based on our estimates of annual
impacts on prescription drug pricing
and annual add-on payments, ASPE did
not model any impacts from the
provider hardship payments. Eligibility
for the hardship exemption will be
based on year-over-year losses above 25
percent of total Medicare Part A and
Part B payments, including payments
for Medicare Part B drugs outside the
model and payments for Medicare Part
A and Medicare Part B services other
than prescription drugs. We expect that
few, if any, providers will have annual
losses above this level, and that those
who do may be insolvent and therefore
unable to obtain retrospective hardship
payments. We note in this regard that a
hypothetical provider could experience
revenue losses of 24.9 percent per year
in each of the model’s seven years,
resulting in an 86.5 percent loss of
revenue in Performance Year 7
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compared with the pre-model base year
and a 62.7 percent loss of revenue over
the seven-year demonstration period,
without qualifying for the hardship
payments in any year.
Table 16 shows the net transfer
impacts resulting from changes in
Medicare B, and D. According to the
ASPE estimate, this model would result
in a net reduction of $87.8 billion in
beneficiary, federal government, and
state government spending over the 7
years of the model.
TABLE 16—ESTIMATED TRANSFER IMPACT OF MFN MODEL—ASPE ESTIMATE
2021
Part B Drug Price Reduction:
Federal Government Spending ............................................
State Government Spending ................................................
Beneficiary Spending * ..........................................................
MA Plan Revenue .................................................................
Health Care System Revenue ** ..........................................
Part D Drug Switching:
Federal Government Spending ............................................
State Government Spending ................................................
Beneficiary Spending * ..........................................................
Health Care System Revenue ** ..........................................
Add-on Payment Impact:
Federal Government Spending ............................................
State Government Spending ................................................
Beneficiary Spending * ..........................................................
MA Plan Revenue .................................................................
Health Care System Revenue ** ..........................................
Total Impact:
Federal Government Spending ............................................
State Government Spending ................................................
Beneficiary Spending * ..........................................................
MA Plan Revenue .................................................................
Health Care System Revenue ** ..........................................
2022
2023
2024
2025
2026
2027
2021–27
¥2.4
¥0.1
¥1.4
0.0
¥4.0
¥3.4
¥0.1
¥2.0
0.0
¥5.5
¥8.4
¥0.4
¥5.0
¥4.8
¥8.9
¥10.0
¥0.4
¥5.9
¥5.9
¥10.5
¥10.3
¥0.4
¥6.2
¥6.1
¥10.9
¥10.7
¥0.5
¥6.4
¥6.5
¥11.1
¥10.8
¥0.5
¥6.4
¥6.5
¥11.1
¥56.0
¥2.4
¥33.4
¥29.8
¥61.9
0.0
0.0
0.0
0.0
0.0
0.0
0.0
0.0
0.3
0.0
0.1
0.5
0.3
0.0
0.1
0.5
0.3
0.0
0.1
0.5
0.3
0.0
0.1
0.5
0.3
0.0
0.1
0.5
1.7
0.1
0.7
2.5
0.2
0.0
¥0.1
0.0
0.0
0.2
0.0
¥0.1
0.0
0.0
0.4
0.0
¥0.1
0.2
0.0
0.3
0.0
¥0.1
0.3
0.0
0.4
0.0
¥0.1
0.3
0.0
0.4
0.0
¥0.1
0.3
0.0
0.4
0.0
¥0.1
0.3
0.0
2.2
¥0.3
¥0.5
1.3
0.1
¥2.2
¥0.1
¥1.6
0.0
¥3.9
¥3.2
¥0.2
¥2.1
0.0
¥5.5
¥7.7
¥0.4
¥4.9
¥4.6
¥8.4
¥9.3
¥0.4
¥5.9
¥5.6
¥10.0
¥9.7
¥0.5
¥6.1
¥5.8
¥10.3
¥10.0
¥0.5
¥6.3
¥6.2
¥10.6
¥10.0
¥0.5
¥6.3
¥6.2
¥10.6
¥52.1
¥2.5
¥33.2
¥28.5
¥59.3
* Beneficiary spending includes spending by beneficiary Medigap plans.
** Health care system revenue includes revenue accrued by health care providers, hospitals, pharmacies, and pharmaceutical manufacturers.
Based on this analysis, the model has
the potential to generate impacts
internationally. In particular, this model
may result in higher prices or longer
launch delays for new products in other
OECD countries. ASPE did not attempt
to quantify the impact of higher prices
on utilization or the impact of these
delays. The health effects of such delays
depend on which products experience
these delays and the potential
alternative treatments. In addition,
foreign governments may seek to
mitigate these impacts by accepting
higher prices for the products or
pursuing alternative price arrangements
that are less transparent.
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3. Aggregate Effects on the Market
There may be spillover effects in the
non-Medicare market, or even in the
Medicare market outside Part B as a
result of the MFN Model. Testing
changes in Medicare Part B drug
payment policy may have implications
for non-Medicare payers. During the
MFN Model, manufacturers’ ASPs may
increase or decrease, which may cause
the payment limits in the quarterly
Medicare ASP payment files to increase
or decrease. Other payers that align their
payments for drugs included in the
MFN Model with the quarterly Medicare
ASP payment files could therefore be
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impacted. Because the extent to which
other payers align with Medicare Part B
drug payments is unknown, we are not
able to quantify the potential impacts of
the MFN Model in this regard.
Private secondary payers that pay for
beneficiary cost-sharing, such as
Medigap plans and employer retiree
coverage, will likely be impacted by the
MFN Model. For MFN beneficiaries,
cost-sharing on MFN Model drugs
would be less than the amount that will
apply outside of the model. If
manufacturers generally raise drug
prices in response to the MFN Model,
the amount of cost-sharing paid by
beneficiaries and secondary payers may
increase; the opposite will occur if
manufacturers decrease drug prices.
Similarly, private primary insurers may
be impacted if manufacturers change
drug pricing as a result of the MFN
Model. Market-wide changes in drug
prices, including drugs not covered by
Medicare Part B, will impact any
individual who receives such drugs. In
addition, to the extent manufacturers
lower their overall prices for drugs,
manufacturers may realize lower
revenue as a result of the MFN Model.
It is possible that manufacturers will
increase international or domestic drug
prices, reduce marketing and other
expenses, or implement other efficiency
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measures to reduce their operating
costs. Given the uncertainty of
manufacturers’ potential behavioral
responses to the MFN Model, we are
unable to quantify these potential
spillover effects of the MFN Model. We
welcome comments on these potential
impacts and evidence on how this rule
could affect other payers, patients, and
drug manufacturers.
Some of this final rule’s important
tradeoffs occur over the long run. We
request comment on whether the drug
products affected by this IFC are likely
to be currently over- or underincentivized, including evidence from
the research literature on optimal patent
length, and on the effects of the IFC on
drug manufacturers’ incentives.
4. Estimated Effect and Burden of MFN
Model Changes on Medicare
Beneficiaries
We estimate that aggregate beneficiary
Medicare Part B cost-sharing within the
context of the MFN Model will decrease
as the MFN Drug Payment Amount will
not exceed 100 percent of the amount
that applies outside the MFN Model
(that is, the applicable ASP or WAC or
payment limit that applies to drug
acquired under the 340B program) and
that beneficiaries will not have a costsharing liability for the alternative drug
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add-on payment amount. Coinsurance
for most separately payable drugs is set
at 20 percent of the payment rates,
subject to limitation in the hospital
outpatient and ASC settings. To the
extent that prescribing patterns shift
toward lower cost drugs under the MFN
Model, in aggregate, beneficiaries could
benefit along with the Medicare
program. If prescribing patterns shift
toward Part D drugs, beneficiary costsharing may increase or decrease
depending upon the drugs they take,
which phase of the Part D benefit such
use occurs in, the beneficiary’s
eligibility for help with drug costs, and
their plan choice. In addition, as a result
of the MFN Model, we expect Medicare
Part B premiums to decrease.
Beneficiaries will benefit from 25
percent of any premium reduction that
may result as this is the portion of
annual premiums that beneficiaries pay.
If MFN participants choose not to
provide MFN Model drugs or prescribe
alternative therapies instead,
beneficiaries may experience access to
care impacts by having to find
alternative care providers locally,
having to travel to seek care from an
excluded provider, receiving an
alternative therapy that may have lower
efficacy or greater risks, or postponing
or forgoing treatment. There is
significant uncertainty with these
potential effects of the MFN Model.
CMS will carefully monitor for evidence
of these potential effects and conduct
beneficiary surveys to assess impacts of
the MFN Model on beneficiaries.
Given the uncertainty of these
impacts, we are unable to quantify these
potential effects of the MFN Model.
In section III.H. of this IFC, we
describe our intention to include quality
measures as part of the MFN Model, and
our plan to collect one quality measure,
focused on patient experience, to help
better understand the impact of the
MFN Model on beneficiary access and
quality of care. This information
collection will be one part of robust
monitoring activities to ensure that
MFN beneficiaries’ access to
medications and quality of care is
preserved or enhanced. We will use a
patient experience survey, which we
will field to a sample of MFN
beneficiaries, beginning in performance
year 1. We will include additional items
in the patient experience survey that
focus on patient access, to the extent
that valid and reliable items are
available. The patient experience survey
will be administered to these
beneficiaries by a third party contractor
throughout the model performance
period. Beneficiaries will not be
required to complete the survey.
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The patient experience survey will be
based on a standardized instrument,
designed to assess patients’ experiences
with health care providers and staff in
an ambulatory setting. We will use the
most current version of the instrument
plus additional survey questions as
applicable to meet CMS’s monitoring
needs.
Based on drug claims analyses and
the scope of the MFN Model, we assume
the patient experience survey will be
administered to 75,000 beneficiaries and
be completed by 30,000 beneficiaries
per year. The survey will take
approximately 30 minutes to complete.
Therefore, the annual total number of
hours for this information collection
will be 15,000 hours (30,000
beneficiaries times 0.5 hours per
beneficiary responding).
To derive average costs for
individuals we used data from the U.S.
Bureau of Labor Statistics’ May 2019
National Occupational Employment and
Wage Estimates for our salary estimate
(www.bls.gov/oes/current/oes_nat.htm).
We believe that the burden will be
addressed under All Occupations
(occupation code 00–0000) at $25.72 per
hour since the group of individual
respondents varies widely from working
and nonworking individuals and by
respondent age, location, years of
employment, and educational
attainment, etc. We are not adjusting
this figure for fringe benefits and
overhead since the individuals’
activities will occur outside the scope of
their employment. Therefore, the
estimated cost for this information
collection will be $385,800 (15,000
hours × $25.72). Beneficiaries will have
annual costs associated with responding
to the patient experience survey, which
we estimate will be $385,800 annually
during the model.
5. Estimated Effect and Burden on MFN
Participants and Manufacturers
MFN participants and drug
manufacturers will have administrative
costs related to adjusting to and
complying with the regulations. These
costs may include adjusting purchasing
arrangements, which for some affected
businesses may mean substantially
changing their pricing models and
engaging in negotiations with other
businesses; tracking units of MFN
Model drugs that are paid under the
MFN Model and excluded from
manufacturers’ ASPs; recordkeeping
requirements, which may require
acquisition of new tools and
information sharing; and adjusting to
any spillover effects. Additionally, MFN
participants may be subject to site visits
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for the purposes of monitoring the MFN
Model.
During the model performance period,
MFN participants must participate in
MFN Model monitoring and evaluation
activities in accordance with 42 CFR
403.1110(b), as the Secretary determines
is necessary to monitor and evaluate the
MFN Model, including without
limitation collecting and reporting of
information, including ‘‘protected
health information’’ as that term is
defined at 45 CFR 160.103. These
monitoring activities may include a
sample of site visits to verify any
monitoring concerns. We anticipate that
these monitoring and compliance
requirements will not diverge from
general monitoring requirements for
Medicare Part B providers. We believe
that these requirements do not add
additional burden or impose regulatory
impact on participants. The MFN Model
monitoring will likely include
beneficiaries and eligible providers and
suppliers completing surveys. Burden
for the patient survey is described
previously, and burden for any provider
and supplier survey will depend on the
length, complexity, and frequency of
surveys administered as needed to
ensure confidence in the survey
findings. We will make an effort to
minimize the length, complexity, and
frequency of any provider and supplier
surveys. A typical survey on average
requires about 20 minutes of the
respondent’s time. In other evaluations
of models where a survey is required,
the frequency of surveys varies from a
minimum of one round of surveys to
annual surveys. We estimate the burden
for annual surveys from clinicians,
assuming one per eligible provider and
supplier, will be 7 surveys [annual]
times 1⁄3 hour [20 min.] times $200
[median physician/surgeon hourly rate
plus fringe benefits] times 22,888
[eligible providers and suppliers] =
$10,702,429.
Finally, MFN participants may choose
to apply for a financial hardship
exemption that requires the submission
of a timely, complete request for a
financial hardship exemption. We think
that approximately 900 MFN
participants will submit a request for a
financial hardship exemption each
performance year of the model. We
expect that a medical health service
manager will need approximately 15
hours to compile the necessary
supporting documentation and submit a
complete financial hardship exemption
request. We estimate the burden for
applying for the financial hardship
exemption per year for all performance
year of the model will be 900 [number
of MFN participants that submit
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hardship exemption requests in each
performance year] times 15 hours times
$111 [medical health service manager
hourly rate plus fringe benefits] =
$1,498,500. Note, the financial hardship
exemption requests for performance
year 1 (2021) will be submitted in 2022,
and the requests for performance year 7
will occur in 2028.
We expect that manufacturers will
need to update their ASP reporting.
However, we expect the burden to be de
minimis compared to existing ASP
reporting requirements and can likely be
automated based on existing processes.
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6. Regulatory Review Cost Estimation
In order to comply with the regulatory
changes in this IFC, affected businesses
will need to review the rule and MFN
participants will need to review MFNspecific billing guidance on how to bill
for the alternative add-on payment. We
expect that a medical health service
manager reading 250 words per minutes
could review the rule in approximately
6 hours [(approximately 300 pages * 300
words/per page)/250 words per minute)/
60 minutes)]. We estimate 1 hour to
review the relevant MLN matters
publication and 2 hours to read MFN
Model billing guidance for a total of 3
hours of billing specific training. Since
all MFN participants have experience
billing HCPCS codes to Medicare, we do
not expect any additional specific
burden related to the alternative add-on
payment M code during model
implementation after the MFN-specific
billing guidance is reviewed. We
estimate the salary of a medical and
health service manager is $111 per hour,
using the wage information from the
2019 BLS including overhead and fringe
benefits (BLS occupation code 11–
9110). For each provider or supplier that
reviews the rule and MFN-specific
billing guidance, the estimated cost
based on the expected time and salary
of the person reviewing the rule is $999
($111 * 9 [6 hours for reviewing the rule
and 3 hours for billing training). We
estimate that the cost for providers and
suppliers to review this IFC and MFNspecific billing guidance will be
approximately $117.9 million (118,101
entities times $999).
7. Regulatory Flexibility Act (RFA)
The RFA requires agencies to analyze
options for regulatory relief for small
entities. For purposes of the RFA, small
entities include small businesses,
nonprofit organizations, and small
governmental jurisdictions. Most
hospitals, practitioners and most other
providers and suppliers are small
entities, either by nonprofit status or by
having annual revenues that qualify for
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small business status under the Small
Business Administration standards. (For
details, see the SBA’s website at https://
www.sba.gov/content/tablesmallbusiness-size-standards (refer to
the 620000 series)). Individuals and
states are not included in the definition
of a small entity. The RFA requires that
CMS analyze regulatory options for
small businesses and other entities
unless CMS certifies that a rule will not
have a significant economic impact on
a substantial number of small entities.
The analysis must include a justification
concerning the reason action is being
taken, the kinds and number of small
entities the rule affects, and an
explanation of any meaningful options
that achieve the objectives with less
significant adverse economic impact on
the small entities. The vast majority of
MFN participants are considered to be
small entities, based upon the SBA
standards. There are over twenty
thousand MFN model participants that
will be included or affected by the MFN
Model. Because many of the affected
entities are small entities, the analysis
and discussion provided in this section,
as well as elsewhere in this IFC is
intended to comply with the RFA
requirements regarding significant
impact on a substantial number of small
entities.
The RFA requires that a Regulatory
Flexibility Analysis (RFA) be prepared
if an IFC will have a ‘‘significant impact
on a substantial number’’ of small
entities. HHS interprets the statute as
mandating this analysis only if the
impact is adverse, though there are
differing interpretations. For purposes
of the RFA, most practitioners,
hospitals, and other providers and
suppliers are small entities, either by
nonprofit status or by having annual
revenues that qualify for small business
status under the Small Business
Administration standards (having
revenues of less than $7.5 million to
$38.5 million in any 1 year). For details,
see the Small Business Administration’s
‘‘Table of Small Business Size
Standards’’ at https://www.sba.gov/
document/support—table-sizestandards. The rule of thumb used by
HHS for determining whether an impact
is ‘‘significant’’ is an adverse effect
equal to 3 percent or more of total
annual revenues. Because the majority
of providers/suppliers in the U.S.
qualify as ‘‘small,’’ and this model
includes all eligible providers/suppliers
that submit claims for separately
payable Medicare Part B drugs, we
expect the majority of MFN participants
to be small entities. However, some of
these small entities may not administer
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76245
Medicare Part B drugs and will not be
MFN participants.
There are a number of providers and
suppliers, including various physician
specialties, that will see reduced drug
component payments of 3 percent or
more in performance year 1. Please refer
to Table 3 to see the number of entities
impacted, as well as the types of
providers and suppliers that will be
most likely impacted by the rule. Lower
MFN Model drug payments will likely
be a fraction of these entities’ total
revenues, taking into account nonMedicare patients and all other services
provided. Moreover, the alternative addon payments could offset such
reductions to some extent, as described
in section III.F. of this IFC. We
considered potential impacts on small
entities; we expect that the model’s
impact on an MFN participant’s revenue
will be driven by the proportion of
Medicare payments to the MFN
participant that is related to
administering Medicare Part B drugs
rather than its size. Further, to provide
financial protection for MFN
participants, we are including a
financial hardship exemption for MFN
participants (regardless of size) that
experience significant financial
hardship as a result of the model test,
as described in section III.I.2. of this
IFC. It is likely that many, if not all,
included providers and suppliers will
see an overall decrease in revenue for
MFN Model drugs of 3 percent or more
over the course of the model.
Accordingly, we have determined that a
Regulatory Flexibility Analysis (RFA) is
required. This RIA, together with the
preamble, constitutes the required
analysis.
As a result of the model, we expect
total allowed charges for Medicare Part
B drugs for small entities to go down
commensurate with the phase-in of the
MFN Price in the calculation of the
MFN Drug Payment Amount (Year 1: 75
percent applicable ASP and 25 percent
MFN Price; Year 2: 50 percent
applicable ASP and 50 percent MFN
Price; etc.). Although the alternative
add-on payment was designed to hold
MFN participants harmless based on
current revenue to the greatest extent
possible, as shown in Table 8, some
specialties will benefit from a higher
aggregate add-on payment amount,
while for other specialties some portion
of such specialties will have a decrease
in aggregate add-on payment. We
estimate that MFN participants, on
average, will see an approximate 40
percent increase in historical revenue
related to the alternative add-on portion
of the MFN Model payments, which
will total approximately $4.4 billion in
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the OACT estimate and $2.2 billion in
the ASPE estimate over the 7-year
model. In these estimates, the total
Medicare FFS impact, as indicated in
Tables 12 and 16, would be a reduction
of approximately $85.5 billion in
Medicare FFS spending in the OACT
estimate and a majority of the $52.1
billion in reduced federal spending in
the ASPE estimate over the 7-year
model, and will apply mainly to urban
and non-340B MFN participants. We
note that there is much uncertainty
around the assumptions for these
estimates. Finally, we have and will
continue to take steps to minimize the
impact of this IFC on administrative and
reporting burdens for small businesses.
We welcome comments on our estimate
of significantly affected providers and
suppliers and the magnitude of
estimated effects. We also welcome
comments on adjustments to the MFN
Model that could be considered for
future rulemaking while preserving the
innovative approach to payment in the
MFN Model.
8. Effects on Small Rural Hospitals
Section 1102(b) of the Act requires
CMS to prepare a regulatory impact
analysis if a rule may have a significant
impact on the operations of a substantial
number of small rural hospitals. This
analysis must conform to the provisions
of section 604 of the RFA. For purposes
of section 1102(b) of the Act, we define
a small rural hospital as a hospital that
is located outside of a metropolitan
statistical area and has 100 or fewer
beds. We estimate that this IFC will
have a significant impact on small rural
hospitals.
As described in section III.C. of this
IFC, we will exclude CAHs from the
types of providers and suppliers that
will be MFN participants. Slightly less
than 10 percent ($3.35 billion) of total
Medicare Part B drug allowed charges in
2019 are associated with rural providers
and suppliers (other than CAHs) based
on claims with ZIP codes associated
with areas that are not assigned to
metropolitan core based statistical areas
(CBSA) identified by the Office of
Management and Budget; of that
amount, less than 0.015 percent ($4.87
million) is for drugs furnished in the
U.S. territories outside of the
metropolitan areas of Puerto Rico. These
rural entities will experience drug
payment reductions and overall
payment reductions similar to urban
entities under the MFN Model.
9. Unfunded Mandates Reform
Section 202 of the Unfunded
Mandates Reform Act of 1995 (UMRA)
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also requires that agencies assess
anticipated costs and benefits before
issuing any rule whose mandates
require spending in any 1 year of $100
million in 1995 dollars, updated
annually for inflation. In 2020, that
threshold is approximately $156
million. This IFC does not mandate any
spending by State, local, or tribal
governments, or by the private sector,
and hence an UMRA analysis is not
required.
10. Federalism
Executive Order 13132 establishes
certain requirements that an agency
must meet when it promulgates a final
rule that imposes substantial direct
costs on State and local governments,
preempts state law, or otherwise has
Federalism implications. We have
examined the provisions in the MFN
Model included in this IFC in
accordance with Executive Order 13132,
and have determined that they will not
have a direct effect on state, local or
tribal governments, preempt state law,
or otherwise have a Federalism
implication.
D. Reducing Regulation and Controlling
Regulatory Costs
Executive Order 13771, titled
Reducing Regulation and Controlling
Regulatory Costs, was issued on January
30, 2017, and requires that the costs
associated with significant new
regulations ‘‘shall, to the extent
permitted by law, be offset by the
elimination of existing costs associated
with at least two prior regulations.’’
This IFC is considered an E.O. 13771
regulatory action. Details on the
estimated costs of this IFC can be found
in the preceding and subsequent
analyses.
E. Alternatives Considered
This IFC contains a range of policies.
It also provides descriptions of the
statutory provisions that are addressed,
identifies the final policies, and
presents rationales for our policies and,
where relevant, alternatives that we
considered in section III of this IFC.
Several alternatives we considered
included: (1) The parameters included
in this IFC; (2) variations of certain
parameters included in this IFC, such as
lengthening the phase-in of the MFN
Price (described in section III.E.8. of this
IFC) to occur over 5–7 performance
years, limiting the model performance
period to 5 performance years,
expanding or limiting the Medicare Part
B drugs that would be eligible for
inclusion in the MFN Model and a
different geographic area; (3) the
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parameters in the October 2018 ANPRM
for a potential IPI Model for Medicare
Part B Drugs; 89 and (4) not
implementing the model. In addition,
when developing the parameters for the
October 2018 ANPRM and this IFC, we
noted that there are a range of methods
to implement external reference pricing,
and these different approaches would
affect the impact of the model.90 91 In
examining potential variations of certain
parameters included in this IFC, we
considered potential differences such
variations would have on the impacts
presented in sections VI.C.1. and VI.C.2.
of this IFC. We note that a potential
model design with a longer MFN Price
phase-in would have a lower estimate of
overall Medicare savings; for example, a
7-year phase-in of the MFN Price over
a 7-year model performance period
would reduce estimates of Medicare
savings in the OACT estimate by
approximately 25 percent. As noted in
section III.E.5. of this IFC, our policy is
to phase-in the MFN Price more quickly
during the initial years to allow CMS to
test the full phase-in of the MFN Price.
In considering the scope of the model,
we actively assessed whether to pursue
a smaller geographic scope. As we
discuss in section III.C.3. of this IFC, we
reviewed the comments that we
received on the October 2018 ANPRM,
where we considered 50 percent of the
country in a model. We weighed
whether the ability to have a research
design where we would compare
changes in drug spending and
utilization relative to a comparison
group, a design that CMS uses
frequently in its models, would
outweight the concerns we highlight in
section III.C.3. of this IFC. We
ultimately concluded that operational
concerns such as administrative
complexity as well as the risk to model
integrity associated with a limited
geographic scope, as described in
section III.C.3. of this IFC, necessitate a
test with a nationwide scope using a
different evaluation design.
The estimates for the impact of this
IFC show a substantial reduction in
Medicare Part B spending over a 7-year
model.
89 https://www.federalregister.gov/documents/
2018/10/30/2018-23688/medicare-programinternational-pricing-index-model-for-medicarepart-b-drugs.
90 https://jasmin.goeg.at/432/1/EURIPID_
GuidanceDocument_V8.1_310718.pdf.
91 https://ec.europa.eu/health/sites/health/files/
systems_performance_assessment/docs/
pharmaproductpricing_frep_en.pdf.
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As required by OMB Circular A–4
under Executive Order 12866 (available
at https://
obamawhitehouse.archives.gov/omb/
circulars_a004_a-4/) in Tables 17 and 18
we have prepared two accounting
statements, based on the OACT and
ASPE estimates respectively, showing
the classification of transfers, benefits,
and costs associated with the provisions
in this IFC. The transfer from
beneficiaries to providers and MA plans
represents the premium change
attributable to the drug price, i.e., the
difference between the gross impact and
the net impact in the drug price section
of Table 12. The accounting statement
in Table 17 is based on estimates
92 https://www.federalregister.gov/documents/
2018/10/30/2018-23688/medicare-program-
international-pricing-index-model-for-medicarepart-b-drugs.
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F. Accounting Statements and Tables
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provided in this regulatory impact
analysis in Table 12 and the accounting
statement in Table 18 is based on
estimates in Table 16. Tables 17 and 18
include the estimated effect and burden
estimates on beneficiaries outlined in
section VI.C.4. of this IFC and on
participants and manufacturers in
section VI.C.5. of this IFC. The costs
shown in Table C18 reflect additional
medical expenses incurred as a result of
the potential loss of access to certain
drugs for some beneficiaries in the
ASPE estimate.
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In comparison, the parameters
considered in the October 2018 ANPRM
were estimated to result in a less
substantial reduction in Medicare Part B
spending over a 5-year model.92 The
alternative of not implementing the
model would not have an impact
compared to existing policy.
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G. Conclusion
The changes in this IFC will affect
providers and suppliers that furnish
separately payable Medicare Part B
drugs in the outpatient setting for which
annual Medicare FFS spending is high.
These providers and suppliers are
mostly physicians (including physician
practices), non-physician practitioners,
supplier groups, HOPDs (including onand off-campus outpatient providerbased departments, but excluding
cancer hospitals, children’s hospitals
and CAHs), and ASCs. We estimate that
the effect of the MFN Model on
providers and suppliers willvary,
depending on their type, location, what
drugs they furnish, their clinical
patterns, and the alternative add-on
payment for the MFN Model. We
estimate that eligible providers and
suppliers will experience a decrease in
overall payment related to the MFN
Model. We estimate that beneficiaries
who receive included drugs from MFN
participants will experience a decrease
in cost-sharing, however, some
beneficiaries’ providers and suppliers
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may choose not to offer access to the
MFN Model drugs, causing these
beneficiaries to seek alternative
providers, treatment alternatives, or
forgo access. The financial hardship
exemption is designed to mitigate this
risk.
The changes in this IFC will also
affect MA organizations, drug
manufacturers, primary and secondary
payers, and potentially non-Medicare
patients. MA organizations will
experience lower payments as a result of
the MFN Model because the MA
ratebook calculations will reflect
changes in actual FFS spending due to
the impact of the model. Drug
manufacturers may have lower revenue,
depending upon their behavioral
response to the MFN Model. Other
payers, including State Medicaid
Programs, and patients who take
prescription drugs may experience
direct or indirect spillover effects that
may increase or decrease their costs. In
addition, as shown in Tables 12 and 16,
the changes we are adopting in this IFC
will reduce state and federal Medicaid
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spending and beneficiary spending on
Medicare premiums.
In accordance with the provisions of
E.O. 12866, this IFC was reviewed by
the Office of Management and Budget.
VII. Waiver of Proposed Rulemaking
and Delay in Effective Date
Under 5 U.S.C. 553(b) of the
Administrative Procedure Act (APA),
the agency is required to publish a
notice of the proposed rule in the
Federal Register before the provisions
of a rule take effect. Similarly, section
1871(b)(1) of the Act requires the
Secretary to provide for notice of the
proposed rule in the Federal Register
and provide a period of not less than 60
days for public comment. Section
553(b)(B) of the APA provides for
exceptions from the notice and
comment requirements; in cases in
which these exceptions apply, section
1871(b)(2)(C) of the Act provides for
exceptions from the notice and 60-day
comment period requirements of the Act
as well. Section 553(b)(B) of the APA
and section 1871(b)(2)(C) of the Act
authorize an agency to dispense with
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normal rulemaking requirements for
good cause if the agency makes a
finding that the notice and comment
process is impracticable, unnecessary,
or contrary to the public interest.
High drug prices in the U.S. have
serious economic and health
consequences for beneficiaries in need
of treatment. Increasing premiums, outof-pocket costs in both Part B and Part
D, and increases in drug prices are
causing beneficiaries to divert scarce
resources to pharmaceutical treatments
and away from other needs, or
prompting them to skip doses of their
medications, take less than the
recommended doses, or abandon
treatment altogether.93 94 In Medicare
Part B, drug spending increased by over
9 percent between 2009 and 2017. Over
two thirds of that increase in spending
was based on increases in drug prices
alone, and only one third due to
increases in utilization.95 Prices of
certain drugs have increased by doubledigit percentages over time.96 These
dramatic increases are on prices where
the U.S. already pays significantly more
than other countries.97 When CMS
announced the 2020 Part B Premiums
and Deductibles, we noted that the
increases in Part B premiums and
deductibles was largely due to rising
spending on physician-administered
drugs.98
With more than 25 million Medicare
beneficiaries living at or below 200
percent of the Federal Poverty Line
(FPL),99 high drug prices could lead to
93 Kirzinger A, Neuman T, Cubanski J, Brodie M.
Data Note: Prescription Drugs and Older Adults,
Aug 09, 2019, Kaiser Family Foundation https://
www.kff.org/health-reform/issue-brief/data-noteprescription-drugs-and-older-adults/.
94 Kirzinger A, Lopes L, Wu B, Brodie M. KFF
Health Tracking Poll—February 2019: Prescription
Drugs, Kaiser Family Foundation, Mar 01, 2019,
https://www.kff.org/health-costs/poll-finding/kffhealth-tracking-poll-february-2019-prescriptiondrugs/.
95 Medicare Payment Advisory Commission,
Report to Congress ‘‘Chapter 3: Medicare payment
strategies to improve price competition and value
for Part B drugs,’’ June 2019, https://
www.medpac.gov/docs/default-source/reports/
jun19_ch3_medpac_reporttocongress_
sec.pdf?sfvrsn=0.
96 Hernandez I, San-Juan-Rodriguez A, Good CB,
Gellad WF. Changes in List Prices, Net Prices, and
Discounts for Branded Drugs in the US, 2007–2018.
JAMA. 2020;323(9):854–862. doi:10.1001/
jama.2020.1012.
97 Comparison of U.S. and International Prices for
Top Medicare Part B Drugs by Total Expenditures’’
https://aspe.hhs.gov/pdf-report/comparison-us-andinternational-prices-top-medicare-part-b-drugstotal-expenditures.
98 CMS Newsroom. 2020 Medicare Parts A & B
Premiums and Deductibles. https://www.cms.gov/
newsroom/fact-sheets/2020-medicare-parts-bpremiums-and-deductibles.
99 Schoen C, Davis K, Willink A, Medicare
Beneficiaries’ High Out of Pocket Costs: Cost
Burdens by Income and Health Status,
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improper medication adherence or
skipped treatment. The consequences of
these behaviors can result in poor
clinical outcomes for chronic disease
management.100 The COVID–19
pandemic has rapidly exacerbated these
problems. The risk of severe illness from
COVID–19 increases with age and the
presence of chronic illnesses, putting
many older adults at the highest risk
levels.101 102 This is of particular
concern given that 84 percent of
individuals over the age of 65 having at
least one chronic health condition, and
more than 53 million adults over the age
of 65 are enrolled in Medicare.103 104
With adults 65 and older comprising 8
out of 10 COVID–19 deaths reported in
the U.S., COVID–19 has
disproportionately impacted Americans
65 or older.105
Furthermore, the COVID–19
pandemic has led to historic levels of
unemployment in the U. S., with both
the unemployment rate and number of
unemployed persons remaining nearly
twice their Feburary (pre-pandemic)
numbers.106 The COVID–19 pandemic
has also led to an increase in food
prices, straining budgets for many of
America’s seniors, particularly those
who live on fixed incomes,107 such as
the 6 million Medicare fee-for-service
Commonwealth Fund, May 12, 2017, https://
www.commonwealthfund.org/publications/issuebriefs/2017/may/medicare-beneficiaries-high-outpocket-costs-cost-burdens-income?redirect_
source=/publications/issue-briefs/2017/may/
medicare-out-of-pocket-cost-burdens.
100 https://www.cdc.gov/mmwr/volumes/66/wr/
mm6645a2.htm.
101 https://www.cdc.gov/coronavirus/2019-ncov/
need-extra-precautions/older-adults.html#:∼:text=
Risk%20for%20Severe%20Illness%20
Increases%20with%20Age&text=The%20
greatest%20risk%20for%20severe%2cas%20
having%20underlying%20medical%20conditions.
102 https://www.cdc.gov/coronavirus/2019-ncov/
need-extra-precautions/people-with-medicalconditions.html.
103 National Council on Aging, https://
www.ncoa.org/economic-security/moneymanagement/debt/senior-debt-facts/.
104 MMCO Statistical & Analytic Reports,
Managed Care Enrollment Trends (2006–2018 Data),
https://www.cms.gov/Medicare-MedicaidCoordination/Medicare-and-MedicaidCoordination/Medicare-Medicaid-CoordinationOffice/Analytics.
105 https://www.cdc.gov/coronavirus/2019-ncov/
need-extra-precautions/older-adults.html#:∼:text=
Risk%20for%20Severe%20Illness%20
Increases%20with%20Age&text=The%20
greatest%20risk%20for%20severe%2cas%20
having%20underlying%20medical%20conditions.
106 U.S. Bureau of Labor Statistics. Economic
News Release.The Employment Situation—October
2020. November 06, 2020. https://www.bls.gov/
news.release/empsit.nr0.htm.
107 54 million people in America face food
insecurity during the pandemic. It could have dire
consequences for their health. AAMC. October 15,
2020. https://www.aamc.org/news-insights/54million-people-america-face-food-insecurity-duringpandemic-it-could-have-dire-consequences-their.
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76249
beneficiaries without supplemental
coverage and over 12 million
beneficiaries dually eligible for
Medicare and Medicaid.108 109 110
Already facing increased financial
burden, this population is in need of
urgent relief from high drug prices in
order to prevent stinting on care and
alleviate general financial instability
worsened by the COVID–19 pandemic.
This need is exacerbated in
communities of color and among
women, wherein Black, Latino, and
Hispanic adults face higher economic
insecurity than their white
counterparts.111 The economic
disruptions caused by the COVID–19
pandemic have increased the burdens
placed on America’s seniors and other
Medicare Part B beneficiaries and given
rise to an urgent need for swift action to
reduce drug prices. Though we have
seen some positive economic and
employment trends since the initial
peak in April,112 we are currently seeing
a new surge in COVID–19 cases that
may lead to additional hardship and
requires immediate action.113 As such,
we find that there is good cause to
waive the notice and comment
requirements under sections 553(b)(B)
of the APA and section 1871(b)(2)(C)
because of the particularly acute need
for affordable Medicare Part B drugs
now, in the midst of the COVID–19
pandemic. Implementation of this
model will provide immediate relief to
Medicare beneficiaries through reduced
copays for MFN drugs due to lower drug
payments and no beneficiary costsharing on the alternative add-on
payment.
We also usually provide for a delay in
effective date under section 553(d) of
the APA and section 1871(e)(1)(B) of the
Act. However, such delay in effective
date may be waived for good cause,
108 MMCO Statistical & Analytic Reports,
Managed Care Enrollment Trends (2006–2018 Data),
https://www.cms.gov/Medicare-MedicaidCoordination/Medicare-and-MedicaidCoordination/Medicare-Medicaid-CoordinationOffice/Analytics.
109 An Overview of Medicare, Kaiser Family
Foundation, Feb 12, 2019, https://www.kff.org/
medicare/issue-brief/an-overview-of-medicare/.
110 Note: The number of Medicare beneficiaries
without supplemental insurance is from 2016 while
the dual eligible numbers are from 2018.
111 Center on Budget and Policy Priorities,
Tracking the COVID–19 Recession’s Effects on
Food, Housing, and Employment Hardships.
November 9, 2020. https://www.cbpp.org/research/
poverty-and-inequality/tracking-the-covid-19recessions-effects-on-food-housing-and.
112 U.S. Bureau of Labor Statistics. Economic
News Release.The Employment Situation- October
2020. November 06, 2020. https://www.bls.gov/
news.release/empsit.nr0.htm.
113 Center for Disease Control. COVID–19
Forecasts: Cases. https://www.cdc.gov/coronavirus/
2019-ncov/cases-updates/forecasts-cases.html.
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when such delay is impracticable,
unnecessary, or contrary to the public
interest, and the agency incorporates a
statement of the finding and a brief
statement of the reasons therefore in the
notice. We find that delaying
implementation of this IFC is contrary
to the public interest for the same
reasons that we find good cause to
waive prior notice and comment.
List of Subjects in 42 CFR Part 513
Administrative practice and
procedure, Health facilities, Medicare,
Reporting and recordkeeping
requirements.
■ For the reasons set forth in the
preamble and under the authority at 5
U.S.C. 301, the Centers for Medicare &
Medicaid Services amends 42 CFR
Chapter IV by adding part 513 to read
as follows:
SUBCHAPTER H—HEALTH CARE
INFRASTRUCTURE AND MODEL
PROGRAMS
PART 513—Most Favored Nation (MFN)
MODEL
Sec.
Subpart A—General Provisions
513.1 Basis, scope, and duration.
513.2 Definitions.
Subpart B—Inclusion in the Model
513.100 MFN Model payments and MFN
participants.
513.120 MFN Model geographic area.
513.130 MFN Model drugs, updates,
categories and exclusions.
513.140 Included international data.
Subpart D—[Reserved]
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Subpart E—Quality Strategy, Beneficiary
Protections, and Compliance Activities
513.400 Quality measures.
513.410 Beneficiary protections.
513.420 Monitoring and compliance
activities.
513.430 Audits and record retention.
513.440 Enforcement authority.
513.450 Limitations on review.
Subpart F—Waivers
513.500 Waivers of Medicare program
requirements for purposes of testing the
MFN Model.
Subparts G through J—[Reserved]
Subpart K—Model Termination
513.1000 Termination of the MFN Model.
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Subpart A—General Provisions
§ 513.1
Basis, scope, and duration.
(a) Basis. This part implements the
test of the Most Favored Nation (MFN)
Model under section 1115A of the Act.
Except as specifically noted in this part,
the regulations under this part do not
affect payment, coverage, program
integrity, or any other requirements that
otherwise apply to providers of services
and suppliers under this chapter.
(b) Scope. This part sets forth the
following:
(1) The types of providers and
suppliers required to participate in the
MFN Model and applicable
requirements.
(2) The beneficiaries included in the
MFN Model.
(3) The drugs included in the MFN
Model.
(4) The methodologies for establishing
Medicare payment amounts for and
making payments for MFN Model drugs,
including an alternative add-on
payment.
(5) Beneficiary protections.
(6) Beneficiary cost-sharing.
(c) Duration. The MFN Model has a
performance period of 7 performance
years. The first performance year
(performance year 1) begins on January
1, 2021, and the final performance year
ends on December 31, 2027, unless
sooner terminated in accordance with
§ 513.1000.
§ 513.2
Subpart C—Payment Process and
Methodology
513.200 Payment process and beneficiary
cost-sharing.
513.210 Model payment methodology for
MFN Model drugs.
513.220 Model alternative add-on payment.
513.230 Financial Hardship Exemptions,
Request Process, and Reconciliation
Payment.
VerDate Sep<11>2014
Authority: 42 U.S.C. 1302, 1315(a), and
1395hh.
Definitions.
For the purpose of this part the
following definitions are applicable
unless otherwise stated:
Add-on percentage means the
percentage above 100 percent.
Alternative add-on payment means
the payment described in § 513.220.
Applicable ASP means the payment
amount determined in accordance with
section 1847A of the Act for a quarter
minus the applicable add-on percentage.
ASP stands for average sales price.
ASP calendar quarter means the
period that is two calendar quarters
prior to the calendar quarter to which
the MFN Drug Payment Amount will
apply.
CCN stands for CMS Certification
Number.
Country-level price means the
unadjusted country-level price for an
MFN Model drug at the HCPCS code
level as calculated in accordance with
§ 513.210(b)(2).
CPI–U stands for Consumer Price
Index for All Urban Consumers based
on all items in U.S. city average and not
seasonally adjusted.
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Days means calendar days.
DME stands for Durable Medical
Equipment.
FDA stands for Food and Drug
Administration.
GDP stands for gross domestic
product.
GDP-adjusted country-level price
means the country-level price adjusted
by the GDP adjuster as calculated in
accordance with § 513.210(b)(4).
GDP adjuster means the countryspecific adjuster as calculated in
accordance with § 513.210(b)(3).
HCPCS stands for Healthcare
Common Procedure Coding System.
HCPCS code level means the specified
drug and amount described in the
HCPCS code long descriptor.
MAC stands for Medicare
Administrative Contractor.
Manufacturer’s average sales price
has the same meaning as under 42 CFR
Subpart J.
MFN stands for most favored nation.
MFN beneficiary means an individual
who is furnished an MFN Model drug
by an MFN participant and who, on the
date of service, is enrolled in Medicare
Part B, has Medicare as his or her
primary payer, and is not covered under
Medicare Advantage or any other group
health plan, including a United Mine
Workers of America health plan.
MFN Drug Payment Amount means
the portion of the total allowed payment
amount for an MFN Model drug
determined in accordance with
§ 513.210.
MFN Model drug means a separately
payable Medicare Part B drug or
biological described by a HCPCS code
included on the MFN Model Drug
HCPCS Codes List.
MFN Model Drug HCPCS Codes List
means the list of drugs included in the
MFN Model for a given calendar quarter
of a performance year established under
§ 513.130.
MFN participant means a Medicare
participating provider or supplier,
identified by its CCN or TIN, that is
required to participate in the MFN
Model in accordance with § 513.100(b).
MFN Model Payment means the total
payment to an MFN participant for an
MFN Model drug in accordance with
subpart C of this part, inclusive of the
MFN Drug Payment Amount and the
Alternative Add-on Payment.
MFN Price means the lowest GDPadjusted country-level price of the
countries specified in § 513.140(b) for
an MFN Model drug.
Model performance period means the
7-year period of time beginning on
January 1, 2021, through December 31,
2027.
NOC stands for not otherwise
classified.
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OIG stands for the Department of
Health and Human Services Office of
Inspector General.
Outpatient prospective payment
system (OPPS) means the payment
system for designated hospital
outpatient items and services and
certain Medicare Part B services
furnished to hospital inpatients when
Part A payment cannot be made as
defined by section 1833(t) of the Act.
Performance year means each 12month period beginning on January 1
and ending on December 31 during the
performance period for the MFN Model
specified in § 513.1(c).
Provider means a ‘‘provider of
services’’ as defined under section
1861(u) of the Act and codified at
§ 400.202 of this chapter.
Supplier means a supplier as defined
in section 1861(d) of the Act and
codified at § 400.202 of this chapter.
TIN stands for taxpayer identification
number.
WAC means wholesale acquisition
cost as defined at section 1847A(c)(6)(B)
of the Act.
Subpart B—Inclusion in the Model
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§ 513.100 MFN Model payments and MFN
participants.
(a) General. Subject to the exceptions
specified in paragraph (d) of this
section, the MFN Model payments
specified under this part apply only to
claims for an MFN Model drug
furnished to an MFN beneficiary by an
MFN participant.
(b) MFN participants. Subject to the
exclusions specified in paragraph (c) of
this section, the MFN Model requires
participation by each Medicare
participating provider and supplier that
submits a claim (except for claims
specified in paragraph (d) of this
section) for a separately payable drug
that is an MFN Model drug furnished to
an MFN beneficiary.
(c) Excluded providers and suppliers.
The following are excluded from
participation in the MFN Model:
(1) Children’s hospitals (defined
under section 1886(d)(1)(B)(iii) of the
Act).
(2) PPS-exempt cancer hospitals
(defined under section 1886(d)(1)(B)(v)
of the Act).
(3) Critical access hospitals (CAHs)
(defined under section 1820 of the Act).
(4) Indian Health Service (IHS)
facilities (as described in section 1880 of
the Act)), except when MFN Model
drugs are furnished and such service is
described in section 1880(e)(2)(B) of the
Act.
(5) Federally Qualified Health Centers
(FQHCs) (defined under section
1861(aa)(4) of the Act).
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(6) Rural Health Clinics (RHCs)
(defined under section 1861(aa)(2) of the
Act).
(7) Hospitals that are not subsection
(d) hospitals (as defined in section
1886(d)(1)(B) of the Act) and are paid on
the basis of reasonable costs subject to
a ceiling under section 1886(b) of the
Act.
(8) Extended neoplastic disease care
hospitals (defined in section
1886(d)(1)(B)(vi) of the Act).
(9) For the first quarter and second
quarter of performance year 1, acute
care hospitals that participate in any
model authorized under section 1115A
of Act for which payment for outpatient
hospital services furnished to Medicare
FFS beneficiaries, including MFN
Model drugs, is made under such model
on a fully capitated or global budget
basis under a waiver of section 1833(t)
of the Act.
(10) Beginning with the third quarter
of performance year 1, acute care
hospitals that participate in any model
authorized under section 1115A of Act
for which payment for outpatient
hospital services furnished to Medicare
FFS beneficiaries, including MFN
Model drugs, is made under such model
on a fully capitated or global budget
basis under a waiver of section 1833(t)
of the Act, where the parameters of such
model adjust for the difference in
payment for MFN Model drugs between
the MFN Model and non-MFN Model
drug payments such that savings under
the MFN Model are incorporated into
the other CMS Innovation Center
model’s parameters (for example, the
annual global budget) for the duration of
the MFN Model.
(d) Exceptions. The MFN Model
payments specified under this part do
not apply to any of the following:
(1) Claims for MFN Model drugs
furnished in the inpatient hospital
setting under those circumstances
where Part A would not pay for hospital
services.
(2) Claims for MFN Model drugs
administered during an inpatient
hospital stay or included on an
inpatient hospital claim.
(3) Claims administered by the DME
MACs as described in § 421.404(c)(2) of
this chapter.
(4) Claims paid under the End-Stage
Renal Disease Prospective Payment
System, including claims paid using the
transitional drug add-on payment
adjustment.
(e) MFN participant requirements
during the MFN Model. During the
model performance period described in
§ 513.1(c), MFN participants must do all
of the following:
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(1) Adhere to the beneficiary
protections requirements under
§ 513.410.
(2) Adhere to the MFN Model-specific
billing instructions requirements
established by CMS and the MAC
responsible for processing the MFN
participant’s claims, including without
limitation those described in § 513.200.
(3) Participate in MFN Model
monitoring and evaluation activities in
accordance with § 403.1110(b) of this
chapter, including collecting and
reporting information as the Secretary
determines is necessary to monitor and
evaluate the MFN Model, including
without limitation ‘‘protected health
information’’ as that term is defined at
45 CFR 160.103.
(f) MFN participant requirements after
the MFN Model. For 2 years after
termination of the MFN Model, MFN
participants must participate in MFN
Model monitoring activities as
described in § 513.420.
§ 513.120
MFN Model geographic area.
The MFN Model geographic area is all
states and U.S. territories.
§ 513.130 MFN Model drugs, updates,
categories and excluded drugs.
(a) MFN Model drugs. CMS creates
and periodically updates the MFN
Model Drug HCPCS Codes List as
described in this section. The MFN
Model Drug HCPCS Codes List
designates the MFN Model drugs, which
are subject to the MFN Model payments
specified in subpart C of this part.
(1) Initial MFN Model Drug HCPCS
Codes List. For the beginning of
performance year 1, CMS identifies the
top 50 drugs by HCPCS code with the
highest aggregate 2019 Medicare Part B
total allowed charges after making the
exclusions specified in paragraphs (b)(1)
and (b)(2) of this section, and adds the
remaining HCPCS codes, after updating
such HCPCS codes for any applicable
changes, to the MFN Model Drug
HCPCS Codes List. Final action claims
with dates of service within calendar
year 2019 and allowed charges greater
than $0 are used to determine aggregate
2019 Medicare Part B total allowed
charges.
(2) Annual Update of the MFN Model
Drug HCPCS Codes List. For the start of
each subsequent performance year,
using Medicare Part B total allowed
charge from the next subsequent
calendar year, CMS identifies the top 50
drugs by HCPCS code with the highest
aggregate Medicare Part B total allowed
charges, after making the exclusions
specified in paragraphs (b)(1) and (b)(2)
of this section, for the most recent full
calendar year, and adds any remaining
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HCPCS codes not already on the MFN
Model Drug HCPCS Codes List to the
MFN Model Drug HCPCS Codes List,
after updating such HCPCS codes for
any applicable changes, effective on the
first day of the performance year.
(3) Removal. No more frequently than
quarterly, CMS removes HCPCS codes
from the MFN Model Drug HCPCS
Codes List when CMS becomes aware
that all of the National Drug Codes
assigned to the HCPCS code have been
permanently withdrawn from the U.S.
market and the drug has been
permanently withdrawn from the U.S.
market, the specific HCPCS code
included on the MFN Model Drug
HCPCS Codes List is terminated with no
replacement code available or planned,
or an exclusion in paragraph (b)(1) of
this section applies.
(4) Maintenance. No more frequently
than quarterly, CMS revises HCPCS
codes on the MFN Model Drug HCPCS
Codes List as necessary to reflect
quarterly HCPCS code updates that are
applicable to the HCPCS codes on the
MFN Model Drug HCPCS Codes List,
including adding replacement codes for
HCPCS codes that were terminated.
(b) Exclusions. (1) The following are
excluded from the MFN Model:
(i) Vaccines specified in section
1861(s)(10) of the Act (influenza,
pneumococcal pneumonia, coronavirus
disease 2019 (COVID–19), and Hepatitis
B vaccines).
(ii) Radiopharmaceuticals.
(iii) Oral anticancer chemotherapeutic
agents described in section 1861(s)(2)(Q)
of the Act.
(iv) Oral anti-emetic drugs described
in 1861(s)(2)(T) of the Act.
(v) Oral immunosuppressive drugs
described in section 1861(s)(2)(J) of the
Act.
(vi) Compounded drugs.
(vii) Intravenous immune globulin
products.
(viii) Drugs billed with HCPCS codes
that describe a drug product that was
approved under an abbreviated new
drug application under section 505(j) of
the Federal Food, Drug, and Cosmetic
Act;
(ix) Drugs for which there is an
Emergency Use Authorization (EUA)
from FDA, or FDA approval, to treat
patients with suspected or confirmed
COVID–19; or
(x) Drugs billed using a not otherwise
classified (NOC) or not otherwise
specified (NOS) billing and payment
code.
(2) The following claims are excluded
from the determination of whether a
drug is to be included on the MFN
Model Drug HCPCS Codes List:
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(i) Professional claims with a place of
service code indicating a home setting,
including home, homeless shelter,
assisted living facility, group home,
temporary lodging, and custodial care
facilities.
(ii) Claims administered by the DME
MACs as described in § 421.404(c)(2) of
this chapter.
§ 513.140
Included international data.
(a) General. (1) CMS uses drug pricing
information from international data
sources, available to CMS at least 20
business days prior to the start of a
calendar quarter, meeting the
requirements in paragraph (c) of this
section for MFN Model drugs from
countries included in paragraph (b) of
this section.
(2) For purposes of selecting a data
source for each MFN Model drug for a
calendar quarter, CMS identifies
available international drug pricing
information data sources for the MFN
Model drug, by aligning the MFN Model
drug’s HCPCS code long description
(including dosage form) with the data
sources’ standardized method for
identifying scientific names or
nonproprietary names and dosage
formulations, as applicable.
(b) Non-U.S. member countries of the
Organisation for Economic Co-operation
and Development (OECD). (1) CMS uses
available international sales, volume,
and pricing data for countries that were
non-U.S. OECD member countries as of
October 1, 2020 with a GDP per capita
that is at least 60 percent of the U.S.
GDP per capita as determined by CMS
in accordance with this paragraph (b).
(2) Each country’s GDP per capita is
assessed using data available at the end
of the applicable ASP calendar quarter.
(3) Subject to the limitation specified
in paragraph (b)(4) of this section, the
GDP per capita for a country is the the
most recent estimate of GDP per capita
based on purchasing power parity for
that country available in the U.S.
Central Intelligence Agency (CIA) World
Factbook.
(4) The country’s GDP per capita and
U.S. GDP per capita selected from the
CIA World Factbook must be for the
same year.
(5) CMS identifies countries with a
GDP per capita that is at least 60 percent
of the U.S. GDP per capita by dividing
the GDP per capita for a country by the
U.S. GDP per capita and assessing the
results.
(c) Identification of international data
sources. (1) CMS obtains data from one
or more international drug pricing
information data sources for purposes of
identifying available international drug
pricing information for the countries
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specified in paragraph (b) of this
section.
(2) Such data sources must, as
determined by CMS—
(i) Utilize a standardized method for
identifying drugs across countries
within that data source, such as using
internationally recognized scientific and
nonproprietary product names;
(ii) Utilize a standard method for
identifying drug forms that at a
minimum distinguishes among
injectable, oral, and other forms of a
drug; and
(iii) Be maintained by an organization
that seeks to limit the lag inherent in
data to no more than 180 days from the
end of the calendar quarter for which
drug pricing information is compiled to
the time that the organization makes
such updates available to users of the
database.
(iv) Contains international drug
pricing information stated in U.S.
currency, such as the following:
(A) Sales data, which may be based on
ex-manufacturer prices (sometimes
called ex-factory prices) that represent
actual or calculated prices paid to the
manufacturer by wholesalers and other
distributors, or retail prices that
represent actual or calculated sales for
retail purchasers, or prices paid by other
purchasers in the distribution channels.
(B) Volume data (for example, number
of packages or units sold).
(C) List prices.
(v) Have mechanisms in place to
maintain, update, and correct, if
necessary, the information on
international drug pricing in the data
source on at least a quarterly basis.
(3) For each MFN Model drug for a
calendar quarter, CMS selects a data
source using the following hierarchy.
(i) The data source contains sales and
volume data for the applicable ASP
calendar quarter from at least one
country described in paragraph (b) of
this section.
(ii) The data source does not have
sales and volume data for the applicable
ASP calendar quarter, but contains sales
and volume data for any prior ASP
calendar quarter beginning on or after
October 1, 2019 from at least one
country described in paragraph (b) of
this section. If sales and volume data
from a prior ASP calendar quarter are
used, CMS uses sales and volume data
from the most recent ASP calendar
quarter for which both sales and volume
data are available.
(iii) The extracted data used by CMS
to determine the most recent MFN Price
used to calculate an MFN Drug Payment
Amount posted on the MFN Model
website.
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(iv) The data source contains exmanufacturer price data for the
applicable ASP calendar quarter from at
least one country described in
paragraph (b) of this section.
(v) The data source contains list price
data for the applicable ASP calendar
quarter from at least one country
described in paragraph (b) of this
section.
(vi) If there is more than one data
source for an ASP calendar quarter, for
each MFN Model drug, CMS selects the
data source at the highest level of the
hierarchy that contains information
from the highest number of countries
described in paragraph (b) of this
section and, if available, incorporates
discounts and rebates into its drug
pricing information, and uses this data
source to calculate the MFN Price as
described in § 513.210(b).
Subpart C—Payment Process and
Methodology
§ 513.200 Payment process and
beneficiary cost-sharing.
(a) General. For purposes of the MFN
Model, the allowed MFN Drug Payment
Amount does not exceed the billed
amount on the claim for the MFN Model
drug.
(b) Model-specific billing instructions.
MFN participants submit claims for
MFN Model drugs to the applicable
MAC in the form and manner specified
by CMS in model-specific billing
instructions.
(c) Beneficiary cost-sharing.
Beneficiary coinsurance does not apply
to the portion of the allowed payment
amount for an MFN Model drug that is
determined under § 513.220.
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§ 513.210 Model payment methodology for
MFN Model drugs.
(a) Payment amount. The total
allowed payment amount for an MFN
Model drug furnished to an MFN
beneficiary by an MFN participant on a
given date of service within a calendar
quarter is determined in accordance
with this section. The total allowed
payment equals—
(1) For each billing unit in the HCPCS
code descriptor of the MFN Model drug,
the MFN Drug Payment Amount
determined in accordance with
paragraphs (b), (c) and (d) of this
section, as applicable, where the
allowed MFN Drug Payment Amount
does not exceed the billed amount on
the claim for the MFN Model drug as
described in § 513.200(a); and
(2) The alternative add-on payment
determined under § 513.220.
(b) Calculation of the MFN Drug
Payment Amount with Available
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International Drug Pricing Data. CMS
selects an available international drug
pricing information data source
described in § 513.140(c) for at least one
country specified in § 513.140(b) for an
MFN Model drug, and calculates, in
advance of each calendar quarter for a
performance year, the applicable MFN
Drug Payment Amount for one billing
unit of an MFN Model drug using the
following steps:
(1) Available international drug
pricing data. (i) For the MFN Model
drug, using the data source selected in
accordance with § 513.140(c)(3) (except
for a data source described in
§ 513.140(c)(3)(iii)), CMS identifies
available international drug pricing data
for the MFN Model drug, by aligning the
MFN Model drug’s HCPCS code long
description (including dosage form)
with the data sources’ standardized
method for identifying scientific names
or nonproprietary names and dosage
formulations, as applicable. CMS
extracts available drug pricing data for
the countries specified in § 513.140(b)
from the selected international drug
pricing information data source. CMS
uses the extracted data that have
complete package size information and
only for dosage formulations that could
be described by the MFN Model drug’s
HCPCS code descriptor, as determined
by CMS. If a data source described in
§ 513.140(c)(3)(iii) is selected, CMS uses
such extracted data.
(ii) When international drug pricing
data with sales and volume data are
available, CMS excludes from the
calculation of the unadjusted countrylevel price under paragraph (b)(2) of this
section international drug pricing data
without both sales and volume data,
with less than $1,000 in quarterly sales
(expressed as U.S. currency), or with
less than 1,000 units in quarterly
volume.
(iii) CMS converts the extracted
volume data to the MFN Model drug’s
HCPCS code billing unit level, as
applicable.
(iv) CMS adjusts the extracted volume
data, as applicable, before converting
the extracted volume data to the MFN
Model drug’s HCPCS code billing unit
level when the data source shows the
package size of a drug product that is
inconsistent with the manufacturer’s
information about that product, as
determined by CMS.
(v) CMS limits the number of HCPCS
code billing units when—
(A) The package labeling indicates a
limited amount of drug is to be used
from the package; and
(B) The HCPCS code dosage is per
dose.
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(2) Calculate the unadjusted countrylevel price for the MFN Model drug by
country.
(i) Using the drug pricing data
extracted and adjusted in accordance
with paragraph (b)(1) of this section,
CMS calculates the unadjusted countrylevel price for the MFN Model drug by
country, using the calculation that is
applicable.
(ii) If an international drug pricing
information data source with sales and
volume data is used, the applicable
calculation is as follows:
(A) CMS sums the adjusted volume
data (as specified in paragraph (b)(1)(iii)
of this section) for the drug.
(B) CMS sums the total sales for the
drug (that remain after performing the
exclusions in paragraph (b)(1)(ii) of this
section).
(C) CMS divides the sum determined
in paragraph (b)(2)(ii)(B) of the section
by the sum determined in paragraph
(b)(2)(ii)(A) of this section, resulting in
an average price per unit of drug, where
the unit of drug is the same as the
HCPCS code billing unit.
(iii) If an international drug pricing
information data source with exmanufacturer or list prices is used, the
applicable calculation is as follows:
(A) For each extracted exmanufacturer or list price, CMS
calculates the number of HCPCS billing
units in the package by dividing the
amount of drug in the package by the
amount of drug represented in one
HCPCS billing unit.
(B) CMS divides the ex-manufacturer
or list price, as applicable, by the
number of HCPCS billing units in the
package, resulting in a price per unit of
drug where the unit of drug is the same
as the HCPCS code billing unit.
(C) CMS sums the price per unit of
drug calculated in paragraph
(c)(3)(iii)(B) of this section.
(D) CMS divides the sum calculated
in paragraph (c)(3)(iii)(C) of this section
by the number of ex-manufacturer or list
prices that were summed in paragraph
(c)(3)(iii)(C) of this section, resulting in
an average price per unit of drug where
the unit of drug is the same as the
HCPCS code billing unit.
(iv) CMS performs the applicable
calculation for each country specified in
§ 513.140(b) for which international
drug pricing information is available in
the selected data source.
(3) Calculate the GDP adjuster for
each country. (i) CMS calculates the
GDP adjuster by dividing the country’s
GDP per capita by the U.S. GDP per
capita for the same year.
(ii) In cases where the resulting ratio
exceeds 1.0, the GDP adjuster is set to
1.0.
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(iii) Subject to the limitations
specified in paragraph (b)(3)(iv) of this
section, the GDP per capita for a country
is the most recent estimate of GDP per
capita based on purchasing power parity
for that country available in the CIA
World Factbook at the end of the
applicable ASP calendar quarter.
(iv) Limitations. (A) The country’s
GDP per capita and U.S. GDP per capita
must be for the same year.
(B) The GDP per capita used must be
for the same year as the data used to
calculate the unadjusted country-level
price, if available, or the most recent
earlier year available.
(4) Apply the GDP adjuster to
calculate the GDP-adjusted countrylevel price. CMS applies the applicable
GDP adjuster identified in paragraph
(b)(3) of this section to each unadjusted
country-level price identified in
paragraph (b)(2) of this section to
calculate the GDP-adjusted countrylevel price by dividing each unadjusted
country-level price by the applicable
GDP adjuster.
(5) Identify the lowest GDP-adjusted
country-level price. CMS identifies the
lowest GDP-adjusted country-level price
for the MFN Model drug. Except as
provided in paragraph (b)(7) of this
section, the price identified is the MFN
Model drug’s MFN Price.
(6) Identify Applicable ASP. CMS
identifies the applicable ASP for the
applicable quarter.
(7) Compare the MFN Price to the
applicable ASP. CMS compares the
price determined in paragraph (b)(5) of
this section to the applicable ASP
identified in paragraph (b)(6) of this
section. The MFN Price equals the
applicable ASP if the applicable ASP is
less than the price determined in
paragraph (b)(5) of this section.
(8) Phase-in. CMS identifies the
applicable phase-in formula based on
the applicable performance year as
follows:
(i) Performance year 1: 75 percent
applicable ASP and 25 percent MFN
Price.
(ii) Performance year 2: 50 percent
applicable ASP and 50 percent MFN
Price.
(iii) Performance year 3: 25 percent
applicable ASP and 75 percent MFN
Price.
(iv) Performance year 4: 100 percent
MFN Price.
(v) Performance year 5: 100 percent
MFN Price.
(vi) Performance year 6: 100 percent
MFN Price.
(vii) Performance year 7: 100 percent
MFN Price.
(9) Final calculation steps. (i) CMS
applies the applicable phase-in formula
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to the applicable ASP and the MFN
Price. Subject to any applicable
adjustments as provided in paragraph
(d) of this section, the amount
determined in this paragraph is the
MFN Drug Payment Amount.
(ii) Subject to the limitation in
paragraph (b)(iii) in this section, CMS
recalculates the MFN Drug Payment
Amounts for prior quarters when
revised international drug pricing
information is available in the data
source that was used to calculate the
MFN Price and applicable ASP updates
are available from CMS. CMS
prospectively applies the recalculations
in the quarterly update following the
availability of revised international drug
pricing information and ASP updates.
(iii) MFN Drug Payment Amounts
may be recalculated for the prior four
calendar quarters of the model.
(c) Frequency of MFN Drug Payment
Amount updates. CMS updates the
MFN Drug Payment Amounts on a
calendar quarter basis. CMS publishes
the quarterly MFN Drug Payment
Amounts on the MFN Model website in
advance of the calendar quarter in
which the MFN Drug Payment Amounts
apply, along with any recalculated MFN
Drug Payment Amounts for prior
quarters.
(d) Exceptions. (1) Payment for MFN
Model drugs for which no international
drug pricing data are available. If, as of
the first calendar quarter during which
an MFN Model drug has been included
in the MFN Model Drug HCPCS Codes
List in accordance with § 513.130, no
international sales, volume or pricing
information meeting the requirements
described in § 513.140(c)—including
data used by CMS to determine the most
recent MFN Price used to calculate an
MFN Drug Payment Amount posted on
the MFN Model website—is available
from any country described in
§ 513.120(b) for any calendar quarter
beginning on or after October 1, 2019
through the applicable quarter, the MFN
Drug Payment Amount is the applicable
ASP.
(2) Payment for MFN Model drugs
that are in short supply. If an MFN
Model drug is reported as ‘‘Currently in
Shortage’’ by FDA, beginning with the
first day of the next calendar quarter
after the date on which it is reported in
shortage, the MFN Drug Payment
Amount is the applicable ASP. CMS
calculates payment in accordance with
paragraph (b) of this section as of the
first day of the calendar quarter after the
date upon which the drug is no longer
reported as ‘‘Currently in Shortage’’ by
FDA.
(3) Adjustment to phase-in formula.
(i) CMS accelerates the phase-in of the
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MFN Price by 5 percentage points at the
next quarterly update to calculate the
MFN Drug Payment Amount for the
MFN Model drug where both of the
following conditions are met:
(A) There is a greater cumulative
percentage increase in either the
applicable ASP or any of the monthly
U.S. list prices for the NDCs assigned to
the MFN Model drug’s HCPCS code
compared to the cumulative percentage
increase in the CPI–U.
(B) There is a greater cumulative
percentage increase in either the
applicable ASP or any of the monthly
U.S. list prices for the NDCs assigned to
the MFN Model drug’s HCPCS code
compared to the cumulative percentage
increase in the MFN Price.
(C) For purposes of paragraphs
(d)(3)(i)(A) and (B) of this section, the
cumulative percentage increase means
the cumulative percentage change from
the end of the baseline to the end of the
applicable ASP calendar quarter.
(D) The baseline in paragraph
(d)(3)(i)(C) of this section for an MFN
Model drug is the ASP calendar quarter
for the applicable ASP for the first
quarter of performance year 1. If there
is not an applicable ASP for the first
quarter of performance year 1 for an
MFN Model drug, the baseline for that
MFN Model drug is the ASP calendar
quarter for the first applicable ASP
based on the manufacturer’s average
sales price for that MFN Model drug
that occurs after the ASP calendar
quarter for the applicable ASP for the
first quarter of performance year 1.
(ii) For purposes of paragraph (d)(3)(i)
of this section, if the cumulative
percentage increase in CPI–U or MFN
Price is negative, CMS uses zero as the
cumulative percentage increase in
CPI–U or MFN Price, as applicable.
(iii) The application of an acceleration
of the phase-in formula continues for
the duration of the model performance
period.
(iv) CMS applies an additional
acceleration of the phase-in formula for
each calendar quarter where the
conditions specified in paragraph (i) are
met.
(4) Adjustment for rapid increases in
the applicable ASP or any monthly U.S.
list prices beyond inflation and MFN
Price after the full phase-in of the MFN
Price. If the conditions described in
paragraphs (d)(3)(i)(A) and (B) of this
section are met after the full phase-in of
the MFN Price for an MFN Model drug,
for each calendar quarter thereafter,
CMS decreases the MFN Drug Payment
Amount equal to largest difference in
the cumulative percentage increase in
the applicable ASP or any of the
monthly U.S. list prices for the NDCs
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assigned to the MFN Model drug’s
HCPCS code compared to the
cumulative percentage increase in the
CPI–U and in the MFN Price,
respectively, determined quarterly.
(5) Limitation on MFN Drug Payment
Amount. The MFN Drug Payment
Amount cannot exceed the non-model
drug payment amount for claim lines
submitted with the JG modifier (or any
successor modifier used to identify
drugs purchased under the 340B
program) after removing any add-on
amount, if applicable.
(e) Blood clotting factor furnishing
fee. When applicable, the blood clotting
furnishing fee under § 410.63(c) of this
chapter is payable along with the MFN
Drug Payment Amount.
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§ 513.220 Model alternative add-on
payment.
(a) Payment amount. (1) The total
allowed alternative add-on payment
amount for a separately payable dose of
an MFN Model drug furnished to an
MFN beneficiary by an MFN participant
on a given date of service within a
calendar quarter is determined in
accordance with this section.
(2) The total allowed alternative addon payment amount for a claim line
does not exceed the billed amount on
that claim line.
(b) Calculation of the per-dose
alternative add-on payment amount.
CMS calculates the per-dose alternative
add-on payment for performance year 1,
quarter 1 for MFN Model drugs using
the following steps:
(1) CMS identifies available Medicare
Part B fee-for-service final action claims
lines, with dates of service in 2019, for
drugs on the initial MFN Model HCPCS
Codes List described in § 513.130(a)(1),
excluding claims for providers and
suppliers specified in § 513.100(c), and
claims specified in § 513.100(d), that
were furnished by Medicareparticipating providers and suppliers,
have a separately paid allowed charge
greater than $0, and for which Medicare
Part B was the primary payer. If a
HCPCS code on the initial MFN Model
HCPCS Codes List was not in use during
any calendar quarter in 2019, CMS uses
the HCPCS code that was applicable for
the MFN Model drug during 2019.
(2) CMS identifies the applicable ASP
for each calendar quarter of 2019 for the
drugs (by HCPCS code as specified in
paragraph (b)(1) of this section)
included on the initial MFN Model
HCPCS Codes List. In the case of a
biosimilar biological product, the
applicable ASP for the reference
biological product is identified and used
in paragraph (b)(3) of this section.
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(3) CMS multiplies the number of
units billed for each claim line
described in paragraph (b)(1) of this
section by 6.1224 percent of the
applicable ASP identified in paragraph
(b)(2) of this section for the HCPCS code
on the claim line and date of service.
(4) CMS sums the products calculated
in paragraph (b)(3) of this section for all
claim lines for each MFN Model drug to
calculate the total add-on spending
amount for each MFN Model drug.
(5) CMS sums the amounts calculated
in paragraph (b)(4) of this section to
calculate the total pooled add-on
spending amount for all MFN Model
drugs.
(6) CMS divides the amount
calculated in paragraph (b)(5) of this
section by the total number of claim
lines retained in paragraph (b)(1) of this
section, excluding claim lines billed
with the JW modifier.
(7) CMS trends the amount calculated
in paragraph (b)(6) of this section
forward to the applicable ASP calendar
quarter for quarter 1 of performance year
1 using the percentage change in CPI–
U from July 2019 through October 2020.
(c) Frequency of alternative add-on
payment amount updates. For each
calendar quarter after quarter 1 of
performance year 1, CMS updates the
alternative add-on payment by applying
a cumulative inflation factor based on
the cumulative percentage change in
CPI–U from October 2020 through the
first month of the prior calendar quarter.
If the cumulative percentage change in
the CPI–U is negative, CMS uses an
inflation factor of 1.
(d) Limitation on the alternative addon payment. The alternate add-on
payment is not payable for claim lines
billed—
(1) With the JW modifier; or
(2) By MFN participants that receive
an alternative add-on payment for an
MFN Model drug under any other
model authorized by section 1115A of
the Act that tests an alternative
approach to the add-on portion of
payment for Medicare Part B drugs.
§ 513.230 Financial hardship exemptions,
request process, and reconciliation
payment.
(a) General. For purposes of the MFN
Model, a financial hardship exemption
for a performance year may be granted
to an MFN participant by CMS, in its
sole discretion and not subject to
appeal, when the provisions in this
section are met.
(b) Request for financial hardship
exemption. To be eligible for a financial
hardship exemption, the MFN
participant must submit a request for
financial hardship exemption in the
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form and manner and with the content
specified by CMS, including without
limitation the requirements of this
paragraph (b).
(1) Timing and form of request. The
MFN participant must submit its request
for a financial hardship exemption to
CMS in accordance the submission
process posted on the MFN Model
website and such request must be
submitted within 60 calendar days
following the end of the performance
year for which the MFN participant
seeks a financial hardship exemption.
(2) Request content. The MFN
participant’s request a financial
hardship exemption must include, at a
minimum, all of the following:
(i) Evidence of methods used to obtain
each MFN Model drug that was
furnished by the MFN participant
during the performance year to any
patient.
(ii) Average net acquisition cost for
each MFN Model drug (inclusive of all
on- and off-invoice discounts or
adjustments, and any other price
concessions related to the purchase of
the MFN Model drug) that was
furnished by the MFN participant
during the performance year to MFN
beneficiaries.
(iii) Average net acquisition cost for
each MFN Model drug (inclusive of all
on- and off-invoice discounts and
adjustments, and any other price
concessions related to the purchase of
the MFN Model drug) that was
furnished by the MFN participant
during the performance year to patients
who were not MFN beneficiaries.
(iv) Statement of any remuneration
received by the MFN participant from
manufacturers of MFN Model drugs,
wholesalers, and distributors that is not
reflected in the MFN participant’s
average net acquisition costs with a
justification of why such remuneration
should not be treated as a price
concession related to the purchase of an
MFN Model drug.
(v) Administrative information,
including: MFN participant’s name, TIN
or CCN (as applicable), contact name,
phone number, and email address.
(vi) The MFN participant’s attestation
that:
(A) The MFN participant experienced
a reduction in Medicare Part B FFS
payments for separately payable drugs
on a per beneficiary basis during the
performance year as compared to the
prior year (that is, the four calendar
quarters immediately preceding the
performance year) due to its inability to
obtain one or more of the MFN Model
drugs at or below the MFN Model
Payments for such drugs during the
performance year;
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(B) The MFN participant has not
received and will not receive any
remuneration from manufacturers of
MFN Model drugs, wholesalers, and
distributors related to the purchase of an
MFN Model drug that was furnished by
the MFN participant during the
performance year that is not reflected in
the MFN participant’s submission; and
(C) The MFN participant submission
is true, accurate and complete.
(c) Standard of review. (1) Incomplete
requests for a financial hardship
exemption, as determined by CMS, are
not reviewed.
(2) CMS grants a financial hardship
exemption to an MFN participant for a
performance year, if the agency in its
sole discretion determines the following
requirements have been met:
(i) The MFN participant submits a
timely, complete request for financial
hardship exemption in accordance with
the requirements of this section which
in the sole discretion of CMS
demonstrates all of the following:
(A) The MFN participant exhausted
all reasonable methods to obtain MFN
Model drugs at or below the MFN
Model Payment for such drugs during
the performance year.
(B) The MFN participant’s average net
acquisition cost for each MFN Model
drug (including invoices and off-invoice
discounts or adjustments) that was
furnished by the MFN participant
during the performance year to patients
who were not MFN beneficiaries was
not less than the MFN participant’s
average net acquisition costs for such
MFN Model drug (including invoices
and off-invoice discounts or
adjustments) that was furnished by the
MFN participant during the
performance year to MFN beneficiaries.
(C) Any remuneration the MFN
participant received from manufacturers
of MFN Model drugs, wholesalers, and
distributors that was not reflected in the
MFN participant’s average net
acquisition costs was not a price
concession related to the purchase of an
MFN Model drug.
(ii) The MFN participant’s excess
reduction amount per beneficiary (as
determined in paragraph (d)(6) of this
section), is greater than zero.
(d) Excess reduction amount per
beneficiary. CMS calculates the MFN
participant’s excess reduction amount
per beneficiary using available final
action claims data where Medicare was
the primary payer that is estimated to be
more than 90 percent complete in
accordance with the following steps:
(1) CMS calculates, separately for
dates of service within the performance
year and prior year, the MFN
participant’s total allowed charges for
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separately payable Medicare Part B
drugs, and the total number of
beneficiaries that had at least one claim
for a service furnished by the MFN
participant with a Medicare Part A or
Medicare Part B allowed charge greater
than $0.
(2) CMS divides the MFN
participant’s total allowed charges for
separately payable Medicare Part B
drugs for dates of service within the
performance year by the total number of
beneficiaries that had at least one claim
for a service furnished by the MFN
participant with a Medicare Part A or
Medicare Part B allowed charge greater
than $0 with a service date within the
performance year, to calculate the MFN
participant’s average per beneficiary
total allowed charges for separately
payable Medicare Part B drugs for the
performance year.
(3) CMS divides the MFN
participant’s total allowed charges for
separately payable Medicare Part B
drugs for dates of service within the
prior year by the total number of
beneficiaries that had at least one claim
for a service furnished by the MFN
participant with a Medicare Part A or
Medicare Part B allowed charge greater
than $0 with a service date within the
prior year, to calculate the MFN
participant’s average per beneficiary
total allowed charges for separately
payable Medicare Part B drugs for the
prior year.
(4) CMS subtracts the MFN
participant’s average per beneficiary
total allowed charges for separately
payable Medicare Part B drugs for the
performance year (as calculated in
paragraph (d)(2) of this section) from the
MFN participant’s average per
beneficiary total allowed charges for
separately payable Medicare Part B
drugs for the prior year (as calculated in
paragraph (d)(3) of this section).
(5) CMS calculates 25 percent of the
MFN participant’s total allowed charges
for all Medicare Part A and Part B
claims with dates of service within the
prior year and divides that amount by
the total number of beneficiaries that
had at least one claim for a service
furnished by the MFN participant with
a Medicare Part A or Medicare Part B
allowed charge greater than $0 with a
service date within the prior year, to
calculate 25 percent of the MFN
participant’s average per beneficiary
total allowed charges for all Medicare
Part A and Part B claims with dates of
service within the prior year.
(6) CMS subtracts 25 percent of the
MFN participant’s average per
beneficiary total allowed charges for all
Medicare Part A and Part B claims with
dates of service within the prior year (as
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calculated in paragraph (d)(5) of this
section) from the difference calculated
in paragraph (d)(4) of this section, to
calculate the MFN participant’s excess
reduction amount per beneficiary.
(e) Reconciliation payment. (1) If CMS
in its sole discretion grants a financial
hardship exemption to an MFN
participant for a performance year, CMS
provides such MFN participant a
reconciliation payment for the
performance year that equals the
amount calculated by multiplying the
excess reduction amount per beneficiary
specified in paragraph (d)(6) of this
section by the total number of
beneficiaries that had at least one claim
for a service furnished by the MFN
participant with a Medicare Part A or
Medicare Part B allowed charge greater
than $0 with a service date within the
performance year.
(2) The amount of a reconciliation
payment provided in accordance with
this section is—
(i) Not subject to appeal;
(ii) Not subject to beneficiary costsharing, including any deductible or
coinsurance; and
(iii) Made by CMS (or a CMS
contractor) as soon as practical.
Subpart D—[Reserved]
Subpart E—Quality Strategy,
Beneficiary Protections, and
Compliance Activities
§ 513.400
Quality measures.
(a) General. Quality measures do not
adjust model payments to MFN
participants and are used for monitoring
purposes.
(b) Collection of quality measures. (1)
CMS administers a patient experience
survey to a sample of beneficiaries who
receive an MFN Model drug. A sample
of non-MFN beneficiaries may also be
surveyed.
(2) If during the MFN Model CMS
determines that the quality measures
specified in paragraph (b) of this section
are not sufficient to adequately monitor
the quality of care that MFN
beneficiaries are receiving from MFN
participants or that MFN participants
are providing, CMS may specify
additional measures. CMS applies the
following criteria when specifying
additional quality measures:
(i) Additional measures are among
one or more of the following categories:
(A) Patient experience of care.
(B) Patient activation
(C) Shared decision making.
(D) Adherence.
(E) Utilization.
(F) Process measures.
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(ii) Additional measures will not add
significant burden to MFN participants
or beneficiaries.
(iii) Additional measures utilize an
instrument that CMS has used
previously in a model to adjust payment
or for monitoring or evaluation.
§ 513.410
Beneficiary protections.
(a) Beneficiary choice.
(1) MFN participants must not restrict
beneficiaries’ ability to choose to receive
care from any Medicare participating
provider or supplier or any provider or
supplier who has opted out of Medicare.
(2) The MFN participant must not
commit any act or omission, nor adopt
any policy that inhibits a beneficiary
from exercising his or her freedom to
choose to receive care from any
Medicare participating provider or
supplier or any provider or supplier
who has opted out of Medicare.
Notwithstanding the foregoing, MFN
participants may communicate to
beneficiaries the benefits of receiving
care from an MFN participant, if
otherwise consistent with the
requirements of this part and applicable
law.
(b) Appeals. An MFN beneficiary and
his or her assignees retain their right to
appeal claims in accordance with part
405 subpart I of this chapter.
(c) Availability of services. MFN
participants must not take any action to
select or avoid treating beneficiaries
based on their diagnoses, care needs,
income levels or other factors that
would render the beneficiary an ‘‘at-risk
beneficiary’’ as defined at § 425.20 of
this chapter.
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§ 513.420 Monitoring and compliance
activities.
(a) Compliance with laws. (1)
Agreement to comply. The MFN
participant must comply with all
applicable laws and regulations.
(2) Notification. The MFN participant
must notify CMS within 15 days after
becoming aware that the MFN
participant is under investigation or has
been sanctioned by the federal, state, or
local government, or any licensing
authority (including, without limitation,
the imposition of program exclusion,
debarment, civil monetary penalties,
corrective action plans, and revocation
of Medicare billing privileges).
(b) CMS monitoring and compliance
activities. (1) CMS conducts monitoring
activities to ensure compliance by MFN
participants with the terms of the MFN
Model, to obtain timely information
about the effects of the MFN Model on
MFN beneficiaries, providers, suppliers,
and on the Medicare program and to
facilitate real time identification and
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response to potential issues. Such
monitoring activities may include,
without limitation, the following:
(i) Documentation requests sent to the
MFN participant including, without
limitation, surveys and questionnaires.
(ii) Audits of claims data, medical
records, and other data from the MFN
participant.
(iii) Interviews with any individual or
entity participating in the MFN Model
including members of the MFN
participant’s leadership, management,
and staff.
(iv) Interviews with beneficiaries and
their caregivers.
(v) Site visits to the MFN participants,
performed in a manner consistent with
§ 513.420(c).
(vi) Tracking patient complaints and
appeals.
(2) In conducting monitoring and
oversight activities, CMS or its
designees may use any relevant data or
information including without
limitation, all Medicare claims
submitted for items or services
furnished to beneficiaries in the MFN
Model.
(3) The MFN participant must
cooperate with evaluation and
monitoring activities as may be
necessary to enable CMS to evaluate the
MFN Model in accordance with section
1115A(b)(4) of the Act and to conduct
monitoring activities under this section.
(c) Site visits. (1) To the extent
practicable, CMS or its designee
provides the MFN participant with no
less than 15 days advance notice of any
site visit. To the extent practicable, CMS
attempts to accommodate a request for
particular dates in scheduling site visits.
However, the MFN participant may not
request a date that is more than 60 days
after the date of the initial site visit
notice from CMS.
(2) The MFN participant must ensure
that personnel with the appropriate
responsibilities and knowledge
associated with the purpose of the site
visit are available during all site visits.
(3) Notwithstanding the foregoing,
CMS may perform unannounced site
visits at all physical locations of the
MFN participant at any time to
investigate concerns about the health or
safety of beneficiaries or other patients
or other program integrity issues.
(4) Nothing in this part must be
construed to limit or otherwise prevent
CMS from performing site visits
permitted or required by applicable law.
(d) Right to correct. If CMS discovers
that it has made or received an incorrect
model-specific payment under the terms
of the MFN Model, CMS may make
payment to, or demand payment from,
the MFN participant.
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§ 513.430
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Audits and record retention.
(a) Right to audit. The Federal
Government, including CMS, HHS, and
the Comptroller General, or their
designees, has the right to audit,
inspect, investigate, and evaluate any
documents and other evidence
regarding implementation of the MFN
Model.
(b) Access to records. MFN
participants must maintain and give the
Federal Government, including CMS,
HHS, and the Comptroller General, or
their designees, access to all such
documents and other evidence
sufficient to enable the audit,
evaluation, inspection, or investigation
of the implementation of the MFN
Model, including without limitation,
documents and other evidence
regarding the following:
(1) The MFN participant’s compliance
with the terms of the MFN Model,
including this subpart.
(2) Quality measure information and
the quality of services performed under
the terms of the MFN Model, including
this subpart.
(3) Patient safety.
(4) The accuracy of model-specific
payments made under the MFN Model.
(5) Utilization of items and services
furnished under the MFN Model.
(6) Other program integrity issues.
(c) Record retention. The MFN
participant must maintain the
documents and other evidence
described in paragraph (b) of this
section and other evidence for a period
of 6 years from the last payment
received by the MFN participant under
the MFN Model or from the date of
completion of any audit, evaluation,
inspection, or investigation, whichever
is later, unless—
(1) CMS determines there is a special
need to retain a particular record or
group of records for a longer period and
notifies the MFN participant at least 30
days before the normal disposition date;
or
(2) There has been a termination,
dispute, or allegation of fraud or similar
fault against the MFN participant, in
which case the records must be
maintained for an additional 6 years
from the date of any resulting final
resolution of the termination, dispute,
or allegation of fraud or similar fault.
§ 513.440
Enforcement authority.
(a) Remedial action—(1) Grounds for
remedial action. In addition to any other
grounds for remedial action that are
permitted under the terms of this part,
CMS may take one or more of the
remedial actions set forth in paragraph
(a)(2) of this section if CMS determines,
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in CMS’ sole discretion, that an MFN
participant:
(i) Has failed to comply with any
applicable Medicare program
requirement, rule, or regulation.
(ii) Has failed to comply with any of
the terms of the MFN Model, including
applicable requirements of this part.
(iii) Has systematically engaged in the
under delivery or over delivery of an
MFN Model drug.
(iv) Has taken any action that
threatens the health or safety of an MFN
beneficiary or other patient.
(v) Has undergone a change of control
that presents a program integrity risk.
(vi) Has submitted false data or made
false representations, warranties,
certifications or attestations in
connection with any aspect of the MFN
Model.
(vii) Has avoided at-risk beneficiaries,
as this term is defined in § 425.20 of this
chapter.
(viii) Has avoided patients on the
basis of payer status.
(ix) Is subject to sanctions or final
actions of an accrediting organization or
Federal, State, or local government
agency.
(x) Takes any action that CMS
determines for program integrity reasons
is not in the best interests of the MFN
Model or the Medicare program, or fails
to take any action that CMS determines
for program integrity reasons should
have been taken to further the best
interests of the MFN Model or Medicare
program.
(xi) Is subject to investigation by HHS
(including the HHS Office of Inspector
General (OIG)) or the Department of
Justice due to an allegation of fraud or
significant misconduct, including being
subject to the filing of a complaint,
filing of a criminal charge, being subject
to an indictment, being named as a
defendant in a False Claims Act qui tam
matter in which the Federal
Government has intervened, or similar
action;
(xii) Is the subject of administration
enforcement action imposed by CMS; or
(xiii) Has failed to demonstrate
improved performance following any
remedial action imposed under this
section.
(2) Taking remedial actions. If CMS
determines that one or more grounds for
remedial action described in paragraph
(a)(1) of this section exist, CMS make
take one or more of the following
remedial actions:
(i) Notifying the MFN participant of
the violation.
(ii) Requiring the MFN participant to
provide additional information to CMS
or its designees.
(iii) Requiring the MFN participant to
develop and implement a corrective
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action plan in a form and manner and
by a deadline specified by CMS.
(iv) Subjecting the MFN participant to
additional monitoring, auditing, or both.
(v) Removing the MFN participant
from the MFN Model.
(vi) Recouping model-specific
payments.
(vii) Other action as may be permitted
under the terms of this part.
(b) OIG authority. Nothing contained
in the terms of the MFN Model or this
part limits or restricts the authority of
the HHS Office of Inspector General or
any other Federal Government authority
or agency, including its authority to
audit, evaluate, investigate, or inspect
model participant for violations of any
statutes, rules, or regulations
administered by the Federal
Government.
§ 513.450
Limitations on review.
There is no administrative or judicial
review under sections 1869 or 1878 of
the Act or otherwise for any of the
following:
(a) The selection of models for testing
or expansion under section 1115A of the
Act.
(b) The selection of organizations,
sites, or participants, including MFN
participants, to test the MFN Model,
including a decision by CMS to remove
an MFN participant from the MFN
Model.
(c) The elements, parameters, scope,
and duration of such MFN Model for
testing or dissemination, including
without limitation all of the following:
(1) The selection of the model
geographic area for the MFN Model by
CMS.
(2) The selection of MFN Model drugs
by CMS.
(3) The selection of included
international data, including selection
of countries, international drug pricing
databases, and international drug
pricing data.
(d) Determinations regarding budget
neutrality under section 1115A(b)(3) of
the Act.
(e) The termination or modification of
the design and implementation of an
MFN Model under section
1115A(b)(3)(B) of the Act.
(f) Determinations about expansion of
the duration and scope of the MFN
Model under section 1115A(c) of the
Act, including the determination that
the MFN Model is not expected to meet
criteria described in paragraphs (c)(1) or
(2) of such section.
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Subpart F—Waivers
§ 513.500 Waivers of Medicare program
requirements for purposes of testing the
MFN Model.
CMS waives the Medicare program
requirements in the following
provisions that are necessary solely for
purposes of testing the MFN Model:
(a) Sections 1833(t)(6) and 1833(t)(14)
of the Act and §§ 419.62 and 419.64 of
this chapter related to Medicare
payment amounts for drugs and
biologicals under the hospital outpatient
prospective payment system (OPPS) as
necessary to permit testing of an
alternative payment amount for MFN
Model drugs.
(b) Section 1833(i)(2)(D) of the Act
related to Medicare payment to ASCs for
drugs and biologicals as necessary to
permit testing of an alternative payment
amount for MFN Model drugs.
(c) Sections 1847A(b) and 1847A(c) of
the Act and §§ 414.904 and 414.802 of
this chapter related to use of the ASPbased, WAC-based, or other applicable
payment methodology and calculation
of manufacturers’ ASP as necessary to
permit testing of an alternative payment
for MFN Model drugs and to exclude
certain units of MFN Model drugs from
manufacturers’ ASPs.
(d) Section 1833(a)(1) of the Act
related to Medicare payment portion of
the allowed payment amount for an
included MFN Model drug that is
determined under § 513.220 as
necessary to permit testing of an
innovative payment approach for the
alternative add-on payment amount.
(e) Section 1833(a)(1)(S) of the Act
related to Medicare payment for drugs
and biologicals is 80 percent of the
lesser of the actual charge or the
payment amount established in section
1842(o) of the Act as necessary to permit
testing of an innovative payment
approach for the total allowable MFN
Model payment as determined under
subpart C.
(f) Section 1833(a)(1)(G) of the Act
related to the amounts paid with respect
to facility services furnished in
connection with certain surgical
procedures and with respect to services
furnished to an individual in an ASC
must be 80 percent of the lesser of the
actual charge for the services or the
amount determined by the Secretary
under such revised payment system as
necessary to permit testing of an
innovative payment approach for the
total allowable MFN Model payment as
determined under subpart C.
(g) Section 1833(t) of the Act related
to how beneficiary copayment is
calculated under the OPPS as necessary
to permit testing of an innovative
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payment approach for the total
allowable MFN Model payment as
determined under subpart C of this part.
(h) Section 1833(t)(9)(B) of the Act
related to the requirement that Medicare
account for adjustments to ensure that
the amount of expenditures under the
OPPS for the year does not increase or
decrease from the estimated amount of
expenditures under the OPPS that
would have been made if the
adjustments had not been made.
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Subparts G through J—[Reserved]
Subpart K—Model Termination
§ 513.1000
Termination of the MFN Model.
(a) CMS may terminate the MFN
Model for reasons including, but not
limited to, the following:
(1) CMS determines that it no longer
has the funds to support the MFN
Model.
(2) CMS terminates the model in
accordance with section 1115A(b)(3)(B)
of the Act.
(b) As specified in section
1115A(d)(2) of the Act, termination of
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the model in accordance with section
1115A(b)(3)(B) of the Act is not subject
to administrative or judicial review.
Dated: November 18, 2020.
Seema Verma,
Administrator, Centers for Medicare &
Medicaid Services.
Dated: November 18, 2020.
Alex M. Azar II,
Secretary, Department of Health and Human
Services.
[FR Doc. 2020–26037 Filed 11–20–20; 4:15 pm]
BILLING CODE 4120–01–P
E:\FR\FM\27NOR2.SGM
27NOR2
]]>Agencies
[Federal Register Volume 85, Number 229 (Friday, November 27, 2020)]
[Rules and Regulations]
[Pages 76180-76259]
From the Federal Register Online via the Government Publishing Office [www.gpo.gov]
[FR Doc No: 2020-26037]
[[Page 76179]]
Vol. 85
Friday,
No. 229
November 27, 2020
Part II
Department of Health and Human Services
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Centers for Medicare & Medicaid Services
42 CFR Part 513
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Most Favored Nation (MFN) Model; Final Rule
��Federal Register / Vol. 85 , No. 229 / Friday, November 27, 2020 /
Rules and Regulations��
[[Page 76180]]
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DEPARTMENT OF HEALTH AND HUMAN SERVICES
Centers for Medicare & Medicaid Services
42 CFR Part 513
[CMS-5528-IFC]
RIN 0938-AT91
Most Favored Nation (MFN) Model
AGENCY: Centers for Medicare & Medicaid Services (CMS), HHS.
ACTION: Interim final rule with comment period.
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SUMMARY: This interim final rule with comment period (IFC) implements
the Most Favored Nation (MFN) Model, a new Medicare payment model under
section 1115A of the Social Security Act (the Act). The MFN Model will
test whether more closely aligning payment for Medicare Part B drugs
and biologicals (hereafter, referred to as ``drugs'') with
international prices and removing incentives to use higher-cost drugs
can control unsustainable growth in Medicare Part B spending without
adversely affecting quality of care for beneficiaries.
DATES: Effective date: These regulations are effective on November 27,
2020.
Comment date: To be assured consideration, comments must be
received at one of the addresses provided below, no later than 5 p.m.
on January 26, 2021.
ADDRESSES: In commenting, please refer to file code CMS-5528-IFC.
Because of staff and resource limitations, we cannot accept comments by
facsimile (FAX) transmission.
Comments, including mass comment submissions, must be submitted in
one of the following three ways (please choose only one of the ways
listed):
1. Electronically. You may submit electronic comments on this
regulation to https://www.regulations.gov. Follow the ``Submit a
comment'' instructions.
2. By regular mail. You may mail written comments to the following
address ONLY: Centers for Medicare & Medicaid Services, Department of
Health and Human Services, Attention: CMS-5528-IFC, P.O. Box 8013,
Baltimore, MD 21244-8013.
Please allow sufficient time for mailed comments to be received
before the close of the comment period.
3. By express or overnight mail. You may send written comments to
the following address ONLY: Centers for Medicare & Medicaid Services,
Department of Health and Human Services, Attention: CMS-5528-IFC, Mail
Stop C4-26-05, 7500 Security Boulevard, Baltimore, MD 21244-1850.
For information on viewing public comments, see the beginning of
the SUPPLEMENTARY INFORMATION section.
FOR FURTHER INFORMATION CONTACT: Andrew York, 410-786-7400.
SUPPLEMENTARY INFORMATION:
Inspection of Public Comments: All comments received before the
close of the comment period are available for viewing by the public,
including any personally identifiable or confidential business
information that is included in a comment. We post all comments
received before the close of the comment period on the following
website as soon as possible after they have been received: https://www.regulations.gov. Follow the search instructions on that website to
view public comments.
I. Executive Summary
A. Purpose
High drug prices are impacting the wallets of Medicare
beneficiaries, especially during the Coronavirus disease 2019 Public
Health Emergency (PHE). Increases in drug prices are accelerating at a
rate that significantly outpaces the growth in spending on other
Medicare Part B services, and prices in the United States (U.S.) for
most Medicare Part B drugs with the highest Medicare spending far
exceed prices in other countries. Specifically, drugs have consistently
been a major contributor to the overall Medicare Part B spending trend.
Medicare Part B Fee-For-Service (FFS) spending for separately payable
physician-administered drugs and drugs furnished in a hospital
outpatient department represented about 11 percent of Medicare Part B
FFS benefit spending in 2015, but accounted for about 37 percent of the
change in Medicare Part B FFS benefit spending from 2015 to 2020, and
spending on these Medicare Part B FFS drugs increased to represent
roughly 14 percent of Medicare Part B FFS benefit spending in 2019.\1\
In addition to the continued growth in spending, the U.S. already pays
almost twice as much on average as other developed countries pay. In
one analysis of 27 drugs, acquisition costs in the U.S. were 1.8 times
higher than in comparator countries.\2\ A more recent analysis using
the prescription drugs and countries in the MFN Model suggests Medicare
Part B paid at least 2.05 times as much as other higher-income
countries in 2018.\3\ The Centers for Medicare & Medicaid Services'
(CMS) Center for Medicare and Medicaid Innovation (Innovation Center)
is taking action on President Trump's goal to lower drug costs and
seeking to realign financial incentives by implementing the Most
Favored Nation (MFN) Model as described in this IFC.
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\1\ 2020 Annual Report of the Boards of Trustees of the Federal
Hospital Insurance and Federal Supplementary Medical Insurance Trust
Funds. Accessed via: https://www.cms.gov/files/document/2020-medicare-trustees-report.pdf.
\2\ ``Comparison of U.S. and International Prices for Top
Medicare Part B Drugs by Total Expenditures'' accessed via https://aspe.hhs.gov/pdf-report/comparison-us-and-international-prices-top-medicare-part-b-drugs-total-expenditures.
\3\ El-Kilani Z, Finegold K, Mulcahy A, and Bosworth A. Medicare
FFS Part B and International Drug Prices: A Comparison of the Top 50
Drugs. Washington, DC: Office of the Assistant Secretary for
Planning and Evaluation, U.S. Department of Health and Human
Services. November 20, 2020 (https://aspe.hhs.gov/pdf-report/medicare-ffs-part-b-and-international-drug-prices).
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Medicare pays substantially more than other countries for many of
the highest-cost Medicare Part B drugs that beneficiaries receive in an
outpatient setting for which Medicare Part B allows separate
payment.\4\ In many instances, Medicare pays more than twice as much
for certain drugs as other countries do.5, 6 This is because
Medicare generally establishes the payment for separately payable
Medicare Part B drugs using the methodology in section 1847A of the
Act. In most cases, this means payment is based on the Average Sales
Price (ASP) plus a statutorily mandated 6 percent add-on. Under this
methodology, the Medicare program does not get the benefit of the
substantial discounts provided in other
[[Page 76181]]
countries, because ASP is calculated using only the prices that
manufacturers charge to certain U.S.-based purchasers. ASP-based
payments may encourage the use of more expensive drugs because the
dollar amount of the 6 percent add-on portion is larger for drugs with
higher ASPs.\7\ As MedPAC noted in its June 2017 Report, ``Although, in
some cases, drugs with patent protection may face competition from
other brand drugs in the same therapeutic class, price competition
between such products may be limited because the [Medicare] Part B drug
payment system is not structured to facilitate competition among brand
products with similar health effects.'' \8\ Thus, the ASP-based payment
approach currently used in Medicare Part B may not promote price
competition or provide sufficient incentive to minimize avoidable
costs.
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\4\ ``Comparison of U.S. and International Prices for Top
Medicare Part B Drugs by Total Expenditures'' accessed via https://aspe.hhs.gov/pdf-report/comparison-us-and-international-prices-top-medicare-part-b-drugs-total-expenditures; El-Kilani Z, Finegold K,
Mulcahy A, and Bosworth A. Medicare FFS Part B and International
Drug Prices: A Comparison of the Top 50 Drugs. Washington, DC:
Office of the Assistant Secretary for Planning and Evaluation, U.S.
Department of Health and Human Services. November 20, 2020 (https://aspe.hhs.gov/pdf-report/medicare-ffs-part-b-and-international-drug-prices).
\5\ ``Comparison of U.S. and International Prices for Top
Medicare Part B Drugs by Total Expenditures'' accessed via https://aspe.hhs.gov/pdf-report/comparison-us-and-international-prices-top-medicare-part-b-drugs-total-expenditures; El-Kilani Z, Finegold K,
Mulcahy A, Bosworth A. Medicare FFS Part B and International Drug
Prices: A Comparison of the Top 50 Drugs. Washington, DC: Office of
the Assistant Secretary for Planning and Evaluation, U.S. Department
of Health and Human Services. November 20, 2020 (https://aspe.hhs.gov/pdf-report/medicare-ffs-part-b-and-international-drug-prices).
\6\ Individual countries differ in the regulatory processes and
standards governing approval of drugs and biologicals. Use of
international drug prices in the MFN Model should not be interpreted
to connote FDA approval or to otherwise describe any scientific or
regulatory relationship between U.S.-approved and non-U.S.-approved
products.
\7\ MedPAC, June 2017, ``Medicare Part B Drug Payment Policy
Issues,'' accessed via https://medpac.gov/docs/default-source/reports/jun17_ch2.pdf.
\8\ MedPAC, June 2017, ``Medicare Part B Drug Payment Policy
Issues,'' accessed via: https://medpac.gov/docs/default-source/reports/jun17_ch2.pdf.
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The MFN Model aims to take a global approach to calculating
Medicare Part B drug payment amounts, by testing a new payment
methodology that takes into account the discounts that other countries
enjoy, and pays providers and suppliers with a fixed add-on amount that
does not reward the use of higher-cost drugs. We expect that this model
will reduce Medicare program expenditures while preserving or enhancing
quality of care furnished to Medicare beneficiaries, and will lower
beneficiary cost-sharing through lower drug payment amounts. The MFN
Model will be tested in all states and U.S. territories by the CMS
Innovation Center for 7 performance years, from January 1, 2021 to
December 30, 2027.
B. Summary of the Major Provisions
The MFN Model will focus on a select cohort of separately payable
Medicare Part B drugs. This cohort will initially include 50 single
source drugs and biologicals (including biosimilar biological products)
that encompass a high percentage of Medicare Part B drug spending. The
MFN Model will require mandatory participation. Participants in the MFN
Model will include all providers and suppliers that participate in the
Medicare program and submit a separately payable claim for an MFN Model
drug with limited exceptions, such as providers and suppliers that are
paid for separately payable Medicare Part B drugs based on reasonable
costs. The vast majority of providers and suppliers that furnish
separately payable Medicare Part B drugs are physicians and non-
physician practitioners, supplier groups (such as a group of physicians
or other practitioners), hospital outpatient departments (HOPDs),
including on- or off-campus provider-based departments (PBDs), whether
paid under the outpatient prospective payment system (OPPS) or the
physician fee schedule (PFS), and ambulatory surgical centers (ASCs)
paid under the ASC Payment System. Claims from these providers and
suppliers will encompass approximately 88 percent of the annual
Medicare Part B spending on the drugs we selected for inclusion in the
MFN Model beginning in performance year 1. Other types of providers and
suppliers that furnish separately payable selected drugs will also be
required to participate in the MFN Model, but they may not often
furnish the selected drugs or may not typically receive separate
payment for Medicare Part B drugs.
The MFN Model will--
Calculate the payment amount for MFN Model drugs based on
a price that reflects the lowest per capita Gross Domestic Product-
adjusted (GDP-adjusted) price of any non-U.S. member country of the
Organisation for Economic Co-operation and Development (OECD) with a
GDP per capita \9\ that is at least sixty percent of the U.S. GDP per
capita, based on available data;
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\9\ For the purposes of this IFC, GDP means GDP based on
purchasing power parity (PPP), rather than nominal GDP. A nation's
GDP at purchasing power parity (PPP) exchange rate is the sum value
of all goods and services produced in the country valued at prices
prevailing in the U. S.
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Make an alternative add-on payment for MFN Model drugs
that will remove or reduce the financial incentive to prescribe higher-
cost drugs more frequently; and
Reduce beneficiary cost sharing on MFN Model drugs.
C. Summary of Costs and Benefits
We believe the MFN Model will substantially lower drug payment
amounts for the most costly Medicare Part B drugs, thereby lowering
program expenditures and out-of-pocket costs for beneficiaries. As
discussed in more detail in section VI. of this IFC, we estimate that
the MFN Model will result in substantial overall Medicare savings
during the 7-year model performance period (that is, 28 calendar
quarters). In the CMS Office of the Actuary (OACT) estimate, OACT
estimates savings of roughly $64.4 billion in Medicare FFS benefits,
$49.6 billion in Medicare Advantage (MA) payments, and $9.9 billion in
Medicaid \10\ spending ($5.7 billion in federal payments and $4.3
billion in state payments). Overall, OACT estimates that the MFN Model
will result in savings of $85.5 billion, net of the associated change
in the Part B premium, in Medicare Part B spending. In addition, OACT
estimates that all beneficiaries will save a total of $28.5 billion
from a reduction in the Medicare Part B premium as a result of the MFN
Model, and will also see their coinsurance reduced. In the HHS Office
of the Assistant Secretary for Planning and Evaluation (ASPE) estimate,
ASPE estimates roughly a net reduction of $87.8 billion in spending on
MFN Model drugs by the federal government, state governments, and
beneficiaries over the 7 years of the model. We note that there is much
uncertainty around the assumptions for both the OACT and ASPE estimates
and refer readers to section VI. of this IFC for a more complete
discussion of potential impacts of the MFN Model.
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\10\ Medicaid savings estimates do not include impacts of
changes in Average Manufacturer Price (AMP) and Best Price on
manufacturer rebates under the Medicaid Drug Rebate Program.
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II. Background on Need for Regulatory Action
On May 11, 2018, President Trump released his Blueprint to Lower
Drug Prices and Reduce Out-of-Pocket Costs,\11\ which outlined the
steps his administration is taking to combat high drug prices, end
foreign freeloading, and spur biomedical innovation.\12\
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\11\ American Patients First: The Trump Administration Blueprint
to Lower Drug Prices and Reduce Out-of-Pocket Costs, Available at:
https://www.hhs.gov/sites/default/files/AmericanPatientsFirst.pdf?language=es.
\12\ ``President Donald J. Trump's Blueprint To Lower Drug
Prices,'' accessed via: https://www.whitehouse.gov/briefings-statements/president-donald-j-trumps-blueprint-lower-drug-prices/.
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On October 25, 2018, CMS released an advance notice of proposed
rulemaking (ANPRM) (83 FR 54546) \13\ (hereafter called the October
2018 ANPRM) describing a potential model, referred to in the October
2018 ANPRM as the International Pricing Index Model (IPI), that would
test whether changing the payment amount for selected Medicare Part B
drugs would reduce Medicare expenditures and preserve or enhance
quality of care. In the October 2018 ANPRM, we sought comment on a
model test that would--
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\13\ International Pricing Index Model for Medicare Part B
Drugs; Medicare Program, 83 Fed. Reg (210) 54246 (Oct 30, 2018)
available at: https://www.govinfo.gov/content/pkg/FR-2018-10-30/pdf/2018-23688.pdf.
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Calculate the Medicare payment amount for selected
Medicare Part B
[[Page 76182]]
drugs to be phased down to more closely align with international
prices;
Allow private-sector vendors to negotiate prices for
drugs, take title to drugs, and compete for physician and hospital
business;
Increase the drug add-on payment to reflect 6 percent of
historical drug costs; and
Pay physicians and hospitals the add-on based on a set
payment amount structure.
We considered the comments that we received in response to the
October 2018 ANPRM in developing the MFN Model described in this IFC.
In addition to considering these comments, we considered feedback and
suggestions from a broad set of stakeholders gathered through comments
on the President's Blueprint and through numerous meetings with
stakeholders.
President Trump discussed an Executive Order (E.O.) regarding an
MFN payment model for Medicare Part B drugs on July 24, 2020, and
subsequently published a superseding Executive Order on Lowering Drug
Prices by Putting America First on September 13, 2020.\14\ In response
to the September 13, 2020 Executive Order, we will implement the MFN
Model described in this IFC.
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\14\ Executive Order 13948, https://www.govinfo.gov/content/pkg/FR-2020-09-23/pdf/2020-21129.pdf.
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A. Medicare Part B Drug Benefit and ASP Payment Methodology
Medicare Part B includes a limited drug benefit for drugs and
biologicals described in section 1861(t) of the Act. The majority of
drugs paid under Medicare Part B generally fall into three categories:
Drugs furnished incident to a physician's service in the physician
office, HOPD, or other outpatient setting; drugs administered via a
covered item of durable medical equipment (DME); and other categories
of drugs specified by statute (generally in section 1861(s)(2) of the
Act).
Many drugs covered under Medicare Part B are administered via
injection or infusion in a physician's office, an HOPD, and certain
other outpatient settings, such as ASCs, and, when Medicare allows
separate payment for these drugs, the payment limit is typically based
on the methodology described in section 1847A of the Act. The payment
amount for these drugs does not include payment for administering the
drug to a beneficiary; payment for drug administration services is made
in accordance with the applicable payment policy for the setting in
which the drug was furnished, such as the Physician Fee Schedule (PFS)
(https://www.cms.gov/Medicare/Medicare-Fee-for-Service-Payment/PhysicianFeeSched/), the Hospital Outpatient Prospective
Payment System (OPPS) (https://www.cms.gov/Medicare/Medicare-Fee-for-Service-Payment/HospitalOutpatientPPS/index.html), or the Ambulatory
Surgical Center Payment System (https://www.cms.gov/Medicare/Medicare-Fee-for-Service-Payment/ASCPayment/). Medicare Part B also
allows separate payment for drugs in less common situations such as
osteoporosis drugs furnished by a home health agency, and when a
beneficiary does not have benefits available under the Part A program.
The payment methodology for drugs described in section 1847A of the
Act is generally based on the volume-weighted ASP for all National Drug
Codes (NDCs) that are assigned to a Healthcare Common Procedure Coding
System (HCPCS) code for the drug plus a 6 percent add-on. The volume-
weighted ASP for a HCPCS code is calculated quarterly using
manufacturer-submitted data \15\ on sales to all purchasers (with
limited exceptions as articulated in section 1847A(c)(2) of the Act,
such as sales at nominal charge and sales exempt from Medicaid best
price \16\) with manufacturers' rebates, discounts, and price
concessions included in the ASP calculation (that is, the sales price
is net of these rebates, discounts, and price concessions). The ASP+6
percent payment amount that Medicare pays for an individual Medicare
Part B drug claim generally does not vary based on the exact price an
individual provider or supplier pays to acquire the drug. In the case
of multiple source drugs, the price of a brand name drug and its
generic equivalent(s) included in the same billing code are averaged
together to determine the payment allowance.\17\ As noted earlier, this
payment methodology may create an incentive for the use of more
expensive drugs, but, as noted in the MedPAC report (and by sources
cited in the report; pages 68 and 79), an add-on may be needed to
account for handling and overhead costs and additional mark-up in
distribution channels that are not captured in the manufacturer-
reported ASP.
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\15\ OMB Control Number 0938-0921.
\16\ Best price is defined in section 1927(c)(1)(C) of the Act.
\17\ Under section 3139 of the Affordable Care Act (Pub. L. 111-
148) the add-on amount for a biosimilar is based on the ASP of the
reference product. Biosimilars are not grouped together with one
another or the reference product for payment purposes.
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Currently, under Medicare Part B, beneficiaries' cost-sharing \18\
is generally 20 percent of the Medicare-allowed amount. The term
``Medicare-allowed amount'' means the maximum amount that a provider or
supplier will be paid for a covered health care service or drug.
However, for items and services paid under the OPPS, beneficiaries are
only financially responsible for a copayment amount up to the amount of
the inpatient hospital deductible.\19\ Medicare pays for the remaining
portion of the Medicare-allowed amount.\20\
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\18\ Not including the annual deductible.
\19\ Section 1833(t)(8)(C)(i) of the Act limits the amount of
beneficiary copayment that may be collected for a procedure
performed in a year to the amount of the inpatient hospital
deductible for that year. This limit is $1,408 in 2020.
\20\ 2020 Medicare Parts A & B Premiums and Deductibles: Fact
Sheet, available at: https://www.cms.gov/newsroom/fact-sheets/2020-medicare-parts-b-premiums-and-deductibles.
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B. Medicare and Beneficiary Spending
Medicare Part B spending for separately payable physician-
administered drugs and drugs furnished in hospital outpatient
departments represented about 11 percent of Medicare Part B FFS
spending in 2015 but increased to represent roughly 14 percent of
Medicare Part B FFS spending in 2019; spending on these Medicare Part B
separately payable drugs accounted for about 37 percent of the change
in Medicare Part B FFS spending from 2015 to 2019. Furthermore,
Medicare Part B FFS spending per capita for separately payable drugs
has increased at an average annual rate of 11.5 percent over this same
period while Medicare Part B FFS spending per capita has increased by
3.8 percent. From 2015 to 2019, Medicare Part B spending for separately
payable drugs increased from $19.4 billion to $29.8 billion (a nearly
55-percent increase) with per capita spending increasing from $583 to
$900. This increase in Medicare Part B FFS spending for separately
payable drugs during this period reflects increases in the prices of
drugs, introduction of new drugs, changes in utilization of these
drugs, changes in Medicare Part B FFS enrollment, and changes in the
mix of drugs for those beneficiaries who received them.\21\ Since
beneficiaries
[[Page 76183]]
without supplemental insurance typically pay 20 percent of the
Medicare-allowed amount, as described in section II.A. of this IFC,
they have faced similar increases in spending on Medicare Part B drugs
as has Medicare.\22\
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\21\ The average annual growth in number of Medicare Part B FFS
beneficiaries was less than 0 percent from 2015 to 2019, so the
change in Medicare Part B beneficiaries does not fully account for
the average annual growth (11.4 percent) in Medicare Part B spending
for physician-administeredpayable drugs. Instead, the increase
during this period is more fully explained by increases in the
prices of drugs, introduction of new drugs, changes in drug
utilization, and changes in the mix of drugs than by increases in
Medicare enrollment.
\22\ In 2016, 8 in 10 beneficiaries in traditional Medicare (81
percent) had some type of supplemental insurance (which typically
covers some or all of Medicare Part A and Medicare Part B cost-
sharing), including employer-sponsored insurance (30 percent),
Medigap (29 percent), and Medicaid (22 percent). Nearly 1 in 5
beneficiaries in traditional Medicare (19 percent)--6.1 million
beneficiaries overall--had no source of supplemental coverage in
2016. https://www.kff.org/medicare/issue-brief/sources-of-supplemental-coverage-among-medicare-beneficiaries-in-2016/.
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A new Issue Brief from the Office of the Assistant Secretary for
Planning and Evaluation (ASPE) provides additional evidence of the need
for the rule. Between 2006 and 2017, Medicare Part B FFS drug spending
per enrollee grew at 8.1 percent, more than twice as high as per capita
spending on Medicare Part D (3.4 percent) and nearly three times as
high as overall retail prescription per capita drug spending (2.9
percent). Spending and enrollment projections by OACT for the 2021
President's Budget suggest that per capita spending on Medicare Part B
physician-administered drugs and separately payable hospital outpatient
drugs will grow at a very similar annual rate of 8 percent between 2020
and 2027, before consideration of any COVID-19 pandemic impacts.\23\
Because biologics account for about 77 percent of Medicare Part B FFS
prescription drug spending, there has been little opportunity to reduce
Medicare Part B spending growth through generic substitution, as has
occurred in Medicare Part D and in retail pharmacy overall.\24\
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\23\ ASPE analysis of OACT spending and enrollment projections.
\24\ Nguyen X. Nguyen and Steve Sheingold. Medicare Part B
Drugs: Trends in Spending and Utilization, 2006-2017. Washington,
DC: Office of the Assistant Secretary for Planning and Evaluation,
U.S. Department of Health and Human Services. November 20, 2020
(https://aspe.hhs.gov/pdf-report/medicare-part-b-drugs-spending-and-utilization).
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C. Relative High Price of Medicare Part B Drugs
Drug acquisition costs in the U.S. exceed those in Europe, Canada,
and Japan, according to an October 2018 ASPE analysis \25\ of Medicare
Part B physician-administered drugs. This finding was generally
consistent with the existing evidence base as described in the HHS
analysis's background section, which found peer-reviewed literature on
this topic to be relatively limited and dated, but with similar
findings of higher drug prices in the U.S. compared to other
countries.\26\ The HHS analysis compared U.S. drug acquisition costs
for a set of Medicare Part B physician-administered drugs to
acquisition costs in 16 other developed economies--Austria, Belgium,
Canada, Czechia, Finland, France, Germany, Greece, Ireland, Italy,
Japan, Portugal, Slovakia, Spain, Sweden, and the United Kingdom
(UK).\27\ The main analysis in the HHS report focused on 27 drugs
accounting for 64 percent of total Medicare Part B drug spending in
2016.\28\ Among the 27 drugs included in the analysis, acquisition
costs in the U.S. were 1.8 times higher than in comparator countries.
Acquisition cost ratios ranged from U.S. prices being on par with
international prices for one of the 27 drugs, to U.S. prices being up
to 7 times higher than the international prices for others. There was
variability across the 16 countries in the study as well, with no one
country consistently acquiring drugs at the lowest prices. The U.S. had
the highest drug prices for 19 of the 27 products.\29\
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\25\ Comparison of U.S. and International Prices for Top
Medicare Part B Drugs by Total Expenditures'' accessed via https://aspe.hhs.gov/pdf-report/comparison-us-and-international-prices-top-medicare-part-b-drugs-total-expenditures.
\26\ ``Comparison of U.S. and International Prices for Top
Medicare Part B Drugs by Total Expenditures'' accessed via https://aspe.hhs.gov/pdf-report/comparison-us-and-international-prices-top-medicare-part-b-drugs-total-expenditures.
\27\ Please refer to the HHS report (``Comparison of U.S. and
International Prices for Top Medicare Part B Drugs by Total
Expenditures'' accessed via https://aspe.hhs.gov/pdf-report/comparison-us-and-international-prices-top-medicare-part-b-drugs-total-expenditures) for more information on the countries selected
for analysis.
\28\ ``Comparison of U.S. and International Prices for Top
Medicare Part B Drugs by Total Expenditures'' accessed via https://aspe.hhs.gov/pdf-report/comparison-us-and-international-prices-top-medicare-part-b-drugs-total-expenditures.
\29\ The ASPE report utilized ex-manufacturer prices (sometimes
called the ex-factory price) stated in U.S. currency on the
transaction date. The report defines ex-manufacturer prices as the
price received by manufacturers of a product, including discounts
applied at the point of sale.
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A new ASPE Issue Brief updates the earlier analysis for the set of
Medicare Part B drugs and the set of countries in the MFN Model. In
2018, based on available data, ASP rates were at least 2.05 times the
value-weighted average price for these drugs in OECD countries with per
capita GDP at least 60 percent of that in the U.S.\30\
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\30\ El-Kilani Z, Finegold K, Mulcahy A, and Bosworth A.
Medicare FFS Part B and International Drug Prices: A Comparison of
the Top 50 Drugs. Washington, DC: Office of the Assistant Secretary
for Planning and Evaluation, U.S. Department of Health and Human
Services. November 20, 2020 (https://aspe.hhs.gov/pdf-report/medicare-ffs-part-b-and-international-drug-prices).
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The results of these reports demonstrate that, save for a few
outlier cases, the U.S. prices used to calculate ASP rates are
significantly higher than the prices in international comparator
countries.\31\ Based on this significant difference, which aligns with
the analysis we present in this IFC, we will test the impact of more
closely aligning payment for Medicare Part B drugs and biologicals with
international prices in the MFN Model.
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\31\ ASP is defined in statute, and based on sales in the U.S.
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III. Provisions of the Interim Final Rule With Comment Period
A. Model Performance Period
In part 513, we codify the MFN Model that will be tested for 7
performance years. We define ``model performance period'' to mean
January 1, 2021, the date the model will begin, through December 31,
2027. We are testing a 7-year performance period because it will allow
a smooth transition to the MFN Price (described in section III.E.5. of
this IFC) by performance year 4 and adequate duration to understand the
impact of the MFN Model. As discussed in section III.N. of this IFC, we
will assess for potential impacts of the MFN Model across quarterly
time periods throughout the performance period. Further, we will assess
initial impacts of the MFN Model on quality of care, including access
to drugs, prior to beginning performance year 5.
B. Defined Population
Our goal is to include all beneficiaries who are furnished an MFN
Model drug by an MFN participant and who, on the date of service, are
enrolled in Medicare Part B, have Medicare as the primary payer, and
are not covered under Medicare Advantage or any other group health
plan, including a United Mine Workers of America health plan, hereafter
called MFN beneficiaries. Thus, the defined population for the MFN
Model will be Medicare FFS beneficiaries who receive an MFN Model drug
from an MFN participant where payment for such drug is allowed under
the MFN Model. We define the term ``MFN beneficiary'' in Sec. 513.2.
Testing the model in the population of beneficiaries who receive
drugs with high annual Medicare Part B spending allows the MFN Model
payment to apply to a broad set of conditions, drugs, medical
specialties, clinical settings, and localities rather than having MFN
Model payment focused on a particular clinical presentation, course of
treatment or single type of care setting. Defining the population in
this
[[Page 76184]]
manner allows CMS to observe the implications of a global approach to
calculating Medicare Part B drug payment amounts and an alternative
add-on approach across a broad set of providers and suppliers and
beneficiaries, as well as a large set of manufacturers. Learnings from
the MFN Model will inform CMS and other stakeholders about the effect
of applying the innovative payment model to a broad set of drugs on a
diverse set of beneficiaries and to the Medicare program.
C. MFN Participants
1. Eligible Providers and Suppliers
A majority of Medicare spending on separately payable Medicare Part
B drugs is for drugs that are furnished incident to a physician's
service (see section 1861(s)(2)(A) of the Act), in a HOPD (see section
1861(s)(2)(B) of the Act), including in an on- or off-campus PBD
(regardless of whether those PBDs are excepted or nonexcepted),\32\ or
in an ASC (see section 1832(a)(2)(F)(i) of the Act). Depending upon the
circumstances, Medicare Part B allows separate payment for drugs to
other providers and suppliers, such as pharmacies, home health
agencies, hospices, radiation therapy centers, independent diagnostic
testing facilities, ambulance suppliers, durable medical equipment
(DME) suppliers, mass immunization suppliers, inpatient hospitals (when
Part A payment is not permitted), and other types of providers and
suppliers. Our goal is to broadly include providers and suppliers that
receive separate payment for MFN Model drugs as MFN participants, with
limited exceptions. MFN participants will consist of Medicare
participating providers and suppliers that submit a claim for a
separately payable drug that is an MFN Model drug furnished to an MFN
beneficiary, unless otherwise excluded.\33\ Because separately payable
Medicare Part B drugs (that is, potential MFN Model drugs) are most
often furnished by physicians, non-physician practitioners, supplier
groups (such as group practices), hospitals that are paid under the
OPPS as defined in 42 CFR 419.20 (including off-campus PBDs paid under
the PFS), and ASCs, these providers and suppliers will represent the
vast majority of MFN participants. Other types of providers and
suppliers (that are not excluded) also will be MFN participants to the
extent that they submit a claim for an MFN Model drug furnished to an
MFN beneficiary. For example, a home health agency that receives
separate payment for an osteoporosis drug (defined in section 1861(kk)
of the Act) will be an MFN participant if such drug is an MFN Model
drug and the home health agency furnishes such drug to an included
beneficiary and a claim is submitted.
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\32\ That is, regardless of whether those PBDs are excepted or
nonexcepted under section 1833(t)(21)(B)(ii) of the Act, as added by
section 603 of the Bipartisan Budget Act of 2015 (Pub. L. 114-74).
\33\ These providers and suppliers will be included as
participants in the MFN Model only if they participate in Medicare;
this means that nonparticipating physicians and non-physician
practitioners will not be MFN participants and will continue to be
paid in accordance with current program policies.
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We will exclude certain types of providers and suppliers that are
ultimately not paid for drugs based on ASP as well as those who are
subject to the hold harmless provision in section 1833(t)(7)(D)(ii) of
the Act. Thus, in Sec. 513.100(c), we exclude from the MFN Model the
following providers and suppliers: Children's hospitals (defined under
section 1886(d)(1)(B)(iii) of the Act); PPS-exempt cancer hospitals
(defined under section 1886(d)(1)(B)(v) of the Act); critical access
hospitals (CAHs) (defined under section 1820 of the Act); Indian Health
Service (IHS) facilities (described in section 1880 of the Act), except
when MFN Model drugs are furnished and such service is described in
section 1880(e)(2)(B) of the Act; Rural Health Clinics (RHCs) (defined
under section 1861(aa)(2) of the Act); Federally Qualified Health
Centers (FQHCs) (defined under section 1861(aa)(4) of the Act);
hospitals that are not subsection (d) hospitals (as defined in section
1886(d)(1)(B) of the Act) and are paid on the basis of reasonable costs
subject to a ceiling under section 1886(b) of the Act; and extended
neoplastic disease care hospitals (defined in section 1886(d)(1)(B)(vi)
of the Act). In addition, for the first quarter and second quarter of
performance year 1, we will exclude acute care hospitals that
participate in a CMS Innovation Center model under which they are paid
for outpatient hospital services furnished to Medicare FFS
beneficiaries, including MFN Model drugs, on a fully capitated or
global budget basis in accordance with a waiver under such model of
section 1833(t) of the Act. This exclusion, codified at Sec.
513.100(c)(9), will apply during the first quarter and second quarter
of performance year 1, and only if the hospital participates in a CMS
Innovation Center model under which it is paid on a fully capitated or
global budget basis. As codified at Sec. 513.100(c)(10), for the third
quarter of performance year 1 (that is, beginning July 1, 2021) and
beyond, acute care hospitals that participate in a CMS Innovation
Center model under which they are paid for outpatient hospital services
furnished to Medicare FFS beneficiaries, including MFN Model drugs, on
a fully capitated or global budget basis in accordance with a waiver
under such model of section 1833(t) of the Act will be excluded from
the MFN Model if the parameters of the other CMS Innovation Center
model adjust for the difference in payment for MFN Model drugs between
the MFN Model and non-MFN Model drug payments such that savings under
the MFN Model are incorporated into the other CMS Innovation Center
model's parameters (for example, the annual global budget) for the
duration of the MFN Model. Thus, acute care hospitals that are
participating in the Maryland Total Cost of Care Model will not be MFN
participants during the first two calendar quarters of 2021 while they
are paid on a fully capitated or global budget basis. Further, if the
parameters of the Maryland Total Cost of Care Model have been updated
to adjust for the difference in payment for MFN Model drugs between the
MFN Model and non-MFN Model drug payments such that savings under the
MFN Model are incorporated into the parameters for the Maryland Total
Cost of Care Model (for example, the annual global budget) for the
duration of the MFN Model, then these acute care hospitals will remain
excluded from the MFN Model beginning with the third quarter of
performance year 1 and beyond. However, if the parameters of the
Maryland Total Cost of Care Model change such that the participating
acute care hospitals are no longer paid on a fully capitated or global
budget basis or if a participating acute care hospital leaves the
Maryland Total Cost of Care Model such that they are paid under section
1833(t) of the Act, then such hospitals would no longer fall under this
exclusion. This exclusion also applies on the same terms to acute care
hospitals participating in the Pennsylvania Rural Health Model that
otherwise meet the definition of MFN participant, unless the parameters
of the Pennsylvania Rural Health Model change such that the
participating acute care hospitals are no longer paid on a fully
capitated or global budget basis or if a participating acute care
hospital leaves the Pennsylvania Rural Health Model such that they are
paid under section 1833(t) of the Act. We expect that the CMS
Innovation Center will adjust the parameters of the Maryland Total Cost
of Care Model and the Pennsylvania Rural Health Model such
[[Page 76185]]
that the participants in these CMS Innovation Center models will remain
excluded from the MFN Model for the duration of the MFN Model. Further,
as discussed in section III.J.1. of this IFC, the CMS Innovation Center
intends to address model overlaps with other CMS Innovation Center
models whether or not the participants in other models are MFN
participants, for example we will account for changes in Medicare Part
B drug payments that impact other models' financial calculations.
We note that community mental health centers, comprehensive
outpatient rehabilitation facilities (CORF), outpatient rehabilitation
facilities (ORF), and certain other providers and suppliers do not
submit claims for Medicare Part B drugs or are not paid separately for
Medicare Part B drugs; thus, an express exclusion for these providers
and suppliers is not necessary. We also note that including these
providers and suppliers in the MFN Model would complicate the model
design and make it challenging to test the impact of the MFN Model on
these types of providers and suppliers because of the varied payment
structures among these providers and suppliers.
Table 1 shows the distribution of 2019 Medicare Part B allowed
charges for separately payable Medicare Part B drugs by provider and
supplier type using available final action claims where Medicare was
the primary payer, with limited exclusions as noted. This table shows
the distribution of Part B drug claims among provider and supplier
types. To assign claims to a provider or supplier type, we considered
the type of Medicare Administrative Contractor (MAC) that processed the
claim, type of bill, provider number, revenue center, line place of
service code, and specialty of the health care practitioner associated
with the drug claim line.
BILLING CODE 4120-01-P
[[Page 76186]]
[GRAPHIC] [TIFF OMITTED] TR27NO20.000
BILLING CODE 4120-01-C
To minimize the complexity of the MFN Model, we are not including
in the MFN Model Medicare Part B drugs that are furnished in the
inpatient setting,
[[Page 76187]]
administered through covered DME, orally administered, or paid under
the End-Stage Renal Disease Prospective Payment System (ESRD PPS).
Therefore, in Sec. 513.100(d), we provide an exception for claims
submitted by acute care hospitals for separately payable Medicare Part
B drugs that were administered during an inpatient stay or included on
an inpatient claim, such as when a beneficiary has exhausted their Part
A benefit days, claims administered by the Durable Medical Equipment
Medicare Administrative Contractors (DME MACs) as described in 42 CFR
421.404(c)(2), and claims paid under the ESRD PPS, including claims for
drugs that are paid using the transitional drug add-on payment
adjustment.
Under the approach set forth in Sec. 513.100(b), all Medicare
participating providers and suppliers that submit a claim for an MFN
Model drug (excluding claims specified in Sec. 513.100(d)) furnished
to an MFN beneficiary will be included as MFN participants unless
otherwise excluded (as specified in Sec. 513.100(c)), regardless of
the volume of MFN Model drugs for which they submit claims. As Table 1
shows, a significant proportion of suppliers bill for a relatively
lower volume of MFN Model drugs, such as less than $2,000 in total
annual allowed charges, and will likely have limited claims paid under
the MFN Model. We considered whether to make specific payment
adjustments under the MFN Model for MFN participants that bill for a
low volume of MFN Model drugs during a historical period or whether
low-volume providers and suppliers could have the option to opt into or
out of the MFN Model. However, we believe that requiring participation
in the model only of providers and suppliers that bill for a higher
volume of MFN Model drugs would not allow us to observe the impact of
the MFN Model on a full range of providers and suppliers and would
create opportunities for shifting sites of care and gaming. As such, we
are including a broad set of providers and suppliers as MFN
participants, regardless of their volume of billing for MFN Model
drugs. As described in section III.I.2. of this IFC, the MFN Model
includes a financial hardship exemption in the form of a potential
reconciliation amount for MFN participants that are significantly
affected by their participation in the MFN Model.
We note that MFN Model drugs could be furnished to a beneficiary in
an HOPD who is subsequently admitted to an inpatient hospital stay.
When a beneficiary receives outpatient hospital services, including MFN
Model drugs, during the 3 days immediately preceding admission to a
hospital defined under section 1886(d) of the Act, the outpatient
hospital services are treated as inpatient services if the beneficiary
has Medicare Part A coverage and such services are not separately
payable under Medicare Part B. We will apply this policy consistently
under the MFN Model such that if a beneficiary receives an MFN Model
drug in an HOPD that is an MFN participant and is admitted to this
hospital within 3 days, then those services, including drugs, will be
treated as inpatient services (in accordance with Medicare inpatient
payment policies) and will not be separately payable under the MFN
Model. We note that when a beneficiary receives outpatient hospital
services during the day immediately preceding a hospital admission to a
hospital not paid under the Inpatient Prospective Payment System
(IPPS), such as psychiatric hospitals and units, inpatient
rehabilitation hospitals and units, long-term care hospitals,
children's hospitals, and cancer hospitals, the statutory payment
window is one day preceding the date of the patient's admission; but
because these categories of hospitals will be excluded from the MFN
Model, as discussed previously, the payment window policy will not be
applicable for this model.
We are codifying these provisions in Sec. Sec. 513.100(a) through
(d).
We note that we include a limitation on the MFN Drug Payment Amount
in Sec. 513.210(d)(5) that will apply to certain claims submitted by
340B covered entities as described in section III.E.10. of this IFC to
ensure that beneficiaries who are furnished MFN Model drugs by a 340B
covered entity do not face increased cost-sharing under the MFN Model
than would otherwise apply.
2. Mandatory Participation and Requirements
Model participation will be mandatory for Medicare participating
providers and suppliers that satisfy the MFN participant definition.
There will be no specific enrollment activities for MFN participants;
rather, their participation will be effectuated by the submission of a
claim for an MFN Model drug furnished to an MFN beneficiary, and we
will apply the MFN Model payment to such a claim.
As we have described in previous rules implementing models with
required provider or supplier participation, such as the Comprehensive
Care for Joint Replacement (CJR) Model, mandatory participation can
enhance the generalizability of model results, as mandatory model
participants may be more broadly representative of all entity types
that could be affected by a model. Requiring participation in the MFN
Model will allow us to observe the experiences of providers and
suppliers with diverse characteristics, such as geographies, patient
populations, and specialty mixes. Mandatory participation (with
specified exceptions) by providers and suppliers submitting claims for
MFN Model drugs in a nationwide model, as further discussed in section
III.C.3. of this IFC, will minimize administrative complexity and risk
to the integrity of the MFN Model.
In Sec. 513.100(e) and Sec. 513.100(f), we are codifying MFN
participant requirements during and after the MFN Model. During the MFN
Model performance period described in Sec. 513.1(c), MFN participants
must--
Adhere to the beneficiary protections requirements in
Sec. 513.410 to ensure beneficiaries' access to care is not adversely
impacted;
Adhere to the MFN Model-specific billing instructions
established by CMS and the MAC responsible for processing the MFN
participant's claims, including without limitation those described in
Sec. 513.200, to ensure appropriate and accurate Medicare payments;
and
Participate in MFN Model monitoring and evaluation
activities in accordance with 42 CFR 403.1110(b), including collecting
and reporting of information as the Secretary of Health and Human
Services (the Secretary) determines is necessary to monitor and
evaluate the MFN Model, including without limitation ``protected health
information'' as that term is defined at 45 CFR 160.103.
For 2 years after termination of the MFN Model, MFN participants
must participate in MFN monitoring activities as described in Sec.
513.420.
MFN participants will continue to bill Medicare for separately
payable MFN Model drugs furnished to MFN beneficiaries and be
responsible for collecting beneficiary cost sharing amounts for MFN
Drug Payment Amounts. As such, we anticipate MFN participants will have
the same administrative requirements for collection of beneficiary
cost-sharing amounts under the MFN Model as apply to collection of
beneficiary cost-sharing outside the MFN Model.
As discussed in section III.L. of this IFC, manufacturers will
exclude from their calculation of ASP all units of MFN Model drugs that
are furnished to MFN beneficiaries and for which payment under Sec.
513.210 is allowed.
[[Page 76188]]
Manufacturers will need to determine the number of units to exclude and
may adjust purchasing arrangements with MFN participants in order to
obtain information about such units. While MFN participants are not
required to provide data to manufacturers related to the number of
units of MFN Model drugs that were furnished to MFN beneficiaries and
for which payment under Sec. 513.210 was allowed, we anticipate that
manufacturers may establish mechanisms to obtain such information,
which also may create administrative burden for MFN participants
related to the MFN Model. For example, manufacturers could require use
of separate purchasing accounts, or reporting of information about
units of MFN Model drugs that were furnished to MFN beneficiaries and
for which payment under Sec. 513.210 was allowed in order to receive a
more favorable purchase price.
3. Model Geographic Area
In the October 2018 ANPRM, CMS anticipated the geographic area
included in a potential IPI Model would encompass 50 percent of
Medicare Part B drug spending. Several commenters expressed concern
that having model participants subjected to multiple payment
methodologies for included drugs based on having some but not all of
their locations within the model's geographic area would be
administratively burdensome. Additionally, some commenters expressed
concern at the idea of requiring participation in some geographic areas
but not others, noting that this approach would disproportionately
affect some providers and suppliers and not others. Multiple commenters
noted that reduced cost-sharing for patients in the model compared to
those outside of the model would create potential differences in access
for beneficiaries. One commenter noted that there would be a risk of
patient steering if the model created a financial incentive for
providers and suppliers to provide care at sites outside of the model
geographic area rather than at sites in the model geographic area.
Due to the administrative complexity and risk to model integrity
associated with a limited scope, CMS believes that the MFN Model cannot
realize its full potential in spending reductions for Medicare and its
beneficiaries and improvement in quality of care without broad
participation of Medicare participating providers and suppliers through
a nationwide scope. Section 1115A(b) of the Act gives the Secretary
discretion in the design of models, including the scope of models.
Section 1115A(a)(5) of the Act states that the Secretary may elect to
limit testing of a model to certain geographic areas. It follows that
the Secretary could similarly elect not to limit testing to certain
geographic areas, and instead test a nationwide model.
The MFN Model requires mandatory, nationwide participation of
Medicare participating providers and suppliers (with limited
exclusions) to be able to successfully test the model for the reasons
described later in this section. First, a nationwide scope avoids
additional administrative burden on MFN participants with some service
locations inside the MFN Model geographic area and others outside of
the MFN Model geographic area, which could lead to such MFN
participants needing to track and follow separate requirements for how
drugs are acquired, furnished, and billed, depending on the service
location. Second, a nationwide model geographic area eliminates the
potential for MFN participants with service locations both inside and
outside the MFN Model's geographic area to seek to influence
beneficiaries' choice of treatment location in response to the
differences between non-model payments and the MFN Model payments. This
potential issue is of particular concern for the MFN Model given the
broad use of MFN Model drugs and the ambulatory settings in which these
drugs may be furnished, which can be geographically distributed over
wide areas. Third, CMS also believes that a nationwide model geographic
area maintains continuity with current treatment patterns by limiting
disruption to beneficiary and health care provider treatment plans that
may arise due to potential changes in the site of care. Fourth, a
nationwide model geographic area allows all eligible beneficiaries who
receive an MFN Model drug from an MFN participant where separate
payment is allowed to benefit from the cost-sharing reductions under
the MFN Model. Finally, CMS believes that a nationwide model geographic
area along with mandatory participation creates the necessary market
participation to increase the likelihood of MFN participants being able
to acquire MFN Model drugs at lower prices as discussed in section VI.
of this IFC. CMS notes that several of these points were commented on
by several respondents to the October 2018 ANPRM. These points
highlight the challenges that accompany a limited scope (non-
nationwide) model geographic area. CMS therefore believes a nationwide
scope is the most appropriate for the MFN Model. Thus, we are codifying
in Sec. 513.120 that the MFN Model geographic area includes all states
and U.S. territories.
As described in section VI. of this IFC, we anticipate that there
could be potential challenges associated with a mandatory, nationwide
model, namely greater impacts on manufacturers, a greater number of MFN
participants that potentially receive lower payments for drugs under
the model, and fewer non-participants who potentially increase their
patient volume should beneficiaries need to locate alternative sites of
care. We have designed the model to mitigate these potential challenges
where possible.
D. MFN Model Drugs
We will begin the MFN Model with 50 Medicare Part B drugs,
identified by Healthcare Common Procedure Coding System (HCPCS) codes
with high annual spending during 2019 (based on dates of service and
after applying certain exclusions), that will be included on the MFN
Model Drug HCPCS Codes List (described later in this section), and
maintain approximately 50 Medicare Part B drugs on the MFN Model Drug
HCPCS Codes List during the 7-year model performance period. We will
focus the model on the separately payable, physician-administered
Medicare Part B drugs with the highest annual spending which make up a
portion of the roughly 550 HCPCS codes listed on the quarterly ASP
pricing files, but encompass approximately three-quarters of annual
Medicare Part B drug spending, \34\ and are furnished by the types of
providers and suppliers that frequently bill under Medicare Part B. The
MFN Model payments will apply only to MFN Model drugs when these drugs
are administered by MFN participants to MFN beneficiaries and Medicare
Part B allows separate payment as the primary payer.
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\34\ CMS publishes a Medicare Part B Drug Dashboard which can be
used to view annual spending on drugs by HCPCS code. The
downloadable file can be used to examine the proportion of annual
spending for the included drugs. See: https://www.cms.gov/Research-Statistics-Data-and-Systems/Statistics-Trends-and-Reports/Information-on-Prescription-Drugs/MedicarePartB.
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In Sec. 513.130(b), we exclude some categories of Medicare Part B
drugs from the model, such as certain vaccines, radiopharmaceuticals,
oral drugs, compounded drugs, and intravenous immune globulin products.
We also exclude drugs that are billed with HCPCS codes to which any
generic drugs are assigned, including in applicable instances where
single
[[Page 76189]]
source drugs or biologicals were within the same billing and payment
code as of October 1, 2003. For purposes of the MFN Model, we consider
a drug to be a generic drug if it is approved under an abbreviated new
drug application (ANDA) under section 505(j) of the Federal Food, Drug,
and Cosmetic Act. In accordance with President Trump's Blueprint to
Lower Drug Prices, we are excluding such drugs because these drugs are
already subject to competitive market forces and because the Medicare
Part B payment allowances for these drugs already reflect price
competition from generic products. In addition, we are excluding drugs
for which there is an Emergency Use Authorization (EUA) or approval by
the Food and Drug Administration (FDA) to treat patients with suspected
or confirmed coronavirus disease 2019 (COVID-19). Since there may
likely be urgent, high demand for such drugs and available supply may
be targeted to certain populations, this exclusion allows maximum
flexibility for potential changes in drug distribution for such drugs.
To encourage introduction and use of biosimilars, the Trump
Administration has taken several actions, including establishing
separate HCPCS codes for Medicare Part B biosimilar biological
products. We are not excluding biosimilar biological products from the
MFN Model, however, given the relative lower annual Medicare Part B
spending for HCPCS codes for separately payable biosimilar biological
products through 2019, only one biosimilar biological product is
included among the performance year 1 MFN Model Drug HCPCS Codes List
in Table 2.
We further discuss the drugs that will be included in or excluded
from the MFN Model in the following four subsections.
1. MFN Model Drug HCPCS Codes List
We will use an approach for including drugs in the MFN Model that
is similar to what we described in the October 2018 ANPRM. However,
rather than beginning with approximately 27 drugs, as discussed in the
October 2018 ANPRM, and adding drugs annually, we will include
approximately 50 Medicare Part B drugs in the MFN Model for each
performance year. We will identify the top 50 Medicare Part B
separately payable drugs with the highest aggregated Medicare Part B
total allowed charges in the baseline period, after excluding certain
claims, to result in an initial set of drugs that will be included in
the model beginning in performance year 1. Thereafter, annual additions
will follow a similar process using claims data for the subsequent
year.
Compared to beginning with a smaller number of drugs and phasing in
additional drugs in each subsequent performance year, beginning with 50
Medicare Part B drugs simplifies the model design and reduces
complexity for MFN participants. Based on spending patterns over time
for high spend Medicare Part B drugs,\35\ we expect the set of included
Medicare Part B drugs to remain relatively stable over the model's 7-
year performance period, and we believe that a generally stable set of
MFN Model drugs will help MFN participants plan their drug acquisition
strategies. We believe the benefits of this stability outweigh the
incremental challenge of beginning the MFN Model with a longer drug
list than envisioned in the October 2018 ANPRM, and allows Medicare and
its beneficiaries to benefit from the model payment methodology sooner
for more of the highest spend Medicare Part B drugs, if anticipated
savings are realized.
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\35\ CMS publishes a Medicare Part B Drug Dashboard, which can
be used to view annual spending on drugs by HCPCS code. See: https://www.cms.gov/Research-Statistics-Data-and-Systems/Statistics-Trends-and-Reports/Information-on-Prescription-Drugs/MedicarePartB.html.
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By focusing the MFN Model on separately payable Medicare Part B
drugs, payments for products that are bundled or otherwise included in
payment for a procedure or other services will not be affected by the
MFN Model and payments for such bundled services will not have to be
separated or adjusted. This approach does not exclude drugs that are
packaged under a Medicare payment system in certain settings and
separately payable in other settings. However, the MFN Model payment
only applies to such drugs in settings where separate payment is
allowed.
In Sec. 513.130, we describe the creation and periodic updates of
an MFN Model Drug HCPCS Codes List, which designates the MFN Model
drugs that are subject to the MFN Model payments specified in Sec. 513
subpart C. Specifically, to select the list of drugs included in the
MFN Model for the beginning of performance year 1 (that is, beginning
January 1, 2021), the regulation text at Sec. 513.130(a)(1) codifies
that, after making the exclusions specified in Sec. 513.130(b)(1) and
(b)(2), CMS identifies the top 50 drugs by HCPCS code with the highest
aggregate 2019 Medicare Part B total allowed charges, and adds those
HCPCS codes to the MFN Model Drug HCPCS Codes List, after updating such
HCPCS codes for any applicable changes. We will use HCPCS codes to
identify drugs because they are an established way to identify, bill,
and pay for separately payable Medicare Part B drugs in the Medicare
claims processing system, and they are commonly used in other Medicare
Part B drug payment resources like the ASP drug pricing files. For this
process, we will use final action Medicare Part B claims for separately
paid drugs with dates of service within calendar year 2019 and allowed
charges greater than $0 where Medicare was the primary payer from all
Medicare providers and suppliers as the baseline period. This period is
the most recent full calendar year of claims data that was sufficiently
available prior to the model performance period start on January 1,
2021. Accordingly, we arrayed drugs, using HCPCS codes, in descending
order based on the aggregate Medicare Part B total allowed charges in
the 2019 baseline period, after making the exclusions specified in
Sec. 513.130(b)(1) and (b)(2), and identified the 50 Medicare Part B
drugs (identified by HCPCS codes) with the highest total Medicare Part
B allowed charges. These HCPCS codes are included on the MFN Model Drug
HCPCS Codes List for the beginning of performance year 1 as shown in
Table 2 of this IFC.
The MFN Model uses an annual calendar year baseline period for
purposes of identifying the drugs that will be added to the MFN Model
Drug HCPCS Codes List for performance year 1 (and annually thereafter,
using the next subsequent calendar year as the baseline) because: The
vast majority of HCPCS Code updates occur annually in the January HCPCS
update; the model will use an annual baseline period to calculate the
alternative add-on payment amount described in section III.F. of this
IFC; and these baseline periods will be aligned for consistency in the
model design.
This approach for identifying the drugs that are included in the
MFN Model at the beginning of performance year 1 captures most of the
drugs listed in the October 2018 ASPE report,\36\ which used the
Medicare Part B National Summary Drug file from 2016 to identify
approximately 27 HCPCS codes associated with high amounts of spending,
and nearly all the drugs listed in the November 20, 2020 ASPE report,
which applied the criteria in the MFN Model to Medicare Part B claims
data
[[Page 76190]]
for 2018.\37\ This approach also results in the inclusion of a variety
of drugs and biologicals (including biosimilar biological products)
that are used to treat common conditions in the Medicare Part B
beneficiary population. These drugs and biologicals with high annual
Medicare allowed charges are frequently prescribed and administered by
various physician specialties to beneficiaries with various medical
conditions. Examples of uses of the drugs included in the MFN Model
are: Drugs and biologicals used to treat cancer and related conditions,
biologicals used for the treatment of rheumatoid arthritis and other
immune mediated conditions, and biologicals used to treat macular
degeneration. Beneficiaries who receive such drugs, often on a
recurring basis, face substantial cost-sharing liability directly or
through their supplemental insurance, and such costs may be partly
avoidable (that is, reduced) if Medicare payment for these drugs were
not based on the current ASP methodology.
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\36\ ``Comparison of U.S. and International Prices for Top
Medicare Part B Drugs by Total Expenditures'' https://aspe.hhs.gov/pdf-report/comparison-us-and-international-prices-top-medicare-part-b-drugs-total-expenditures.
\37\ El-Kilani Z, Finegold K, Mulcahy A, and Bosworth A.
Medicare FFS Part B and International Drug Prices: A Comparison of
the Top 50 Drugs. Washington, DC: Office of the Assistant Secretary
for Planning and Evaluation, U.S. Department of Health and Human
Services. November 20, 2020 (https://aspe.hhs.gov/pdf-report/medicare-ffs-part-b-and-international-drug-prices).
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Beginning with 50 of the highest spend HCPCS codes based on annual
Medicare Part B allowed charges during 2019, after taking into account
certain exclusions, focuses the MFN Model on a wide variety of
frequently utilized Medicare Part B drugs and specialties that
administer such drugs to Medicare FFS beneficiaries, and allows CMS to
test the MFN Model payment on a broad set of drugs and biologicals that
are furnished to many beneficiaries. We believe that including single
source drugs and biologicals (including biosimilar biological products)
that move into the top 50 HCPCS codes on an annual basis will capture
potential shifts in utilization to drugs that had not yet been included
in the MFN Model, if such shifting were to occur, and will mitigate the
potential for medically unnecessary shifts in utilization.
In developing this approach, we also considered comments we
received in response to the October 2018 ANPRM on using drug classes to
help inform which drugs to include in the MFN Model, as well as
requests to consider how access to Medicare Part B drugs (as a whole
and for specific subsets of drugs) might be affected by inclusion in
the model. We considered these suggestions and believe that using
annual Medicare Part B allowed charges as a primary factor is a more
transparent, consistent, and clear approach because attempting to
identify drugs for inclusion in the MFN Model based on groups or
classes of drugs could become complicated and confusing for MFN
participants. There are numerous drug classification approaches
available; for example, drug classification can be based on a chemical
class, site of action, mechanism of action, as well as other factors.
These approaches can become difficult to apply consistently when drugs
from different chemical classes are used to treat the same condition,
when a drug has more than one mechanism of action, or when conditions
are treated with drugs having more than one mechanism of action. For
example, the Medicare Part B biological products commonly used to treat
rheumatoid arthritis include a variety of monoclonal antibodies. Using
broad terms such as monoclonal antibodies to identify a ``group'' of
MFN Model drugs would include a variety of biologicals that are
commonly also used in treating other conditions, such as Crohn's
disease, ulcerative colitis, cancer, and multiple sclerosis. Attempting
to select MFN Model drugs using more narrow terms, for example by
specifying agents that exert effects on more specific inflammatory
pathways, such as tumor necrosis factor and interleukins, would miss
biologicals that affect other pathways, like T cell stimulation. These
approaches may also miss products that are primarily used to treat
other diseases, but may be used less frequently in rheumatoid
arthritis, and these approaches may not be readily adaptable for novel
products that may be introduced over the 7-year performance period of
the model.
In Sec. 513.130(a)(2), we are codifying the process for annual
updates of the MFN Model Drug HCPCS Codes List to update the list of
drugs that will be included in the MFN Model for the subsequent
performance year, as further described in section III.D.3. of this IFC.
2. Exclusion of Certain HCPCS Codes and Claims
In the October 2018 ANPRM, we discussed the potential exclusion of
several groups of drugs from the potential IPI Model (83 FR 54555).
Commenters generally agreed that these drugs should be excluded. As
codified in Sec. 513.130(b)(1), the MFN Model excludes the following
types of drugs, by excluding claims at the HCPCS code level, before
identifying the top 50 drugs with the highest aggregate annual Medicare
Part B total allowed charges:
Medicare Part B vaccines specified in section 1861(s)(10)
of the Act (that is, influenza, pneumococcal pneumonia, and Hepatitis B
vaccines, and any future vaccine for COVID-19). These preventive
products are paid under section 1842(o)(1)(A)(iv) based on average
wholesale price (AWP), a price that does not include discounts or
rebates. Including such drugs in the MFN Model also would not comport
with our test of an alternative add-on payment amount (described in
section III.F. of this IFC) because the statutory add-on percentage
under section 1847A of the Act does not apply to these drugs.
Radiopharmaceuticals. Many radiopharmaceuticals are
typically acquired outside of the traditional drug supply chain.
Nuclear pharmacies are frequently involved in the preparation of
patient-ready doses of these drugs, and Medicare Part B payment is
frequently based on contractor pricing. We are excluding
radiopharmaceuticals from the MFN Model because it is unlikely that we
will be able to obtain reliable international drug pricing information
for radiopharmaceuticals.
Oral Medicare Part B drugs, including oral anticancer
drugs described in section 1861(s)(2)(Q) of the Act, oral antiemetic
drugs described in section 1861(s)(2)(T) of the Act and
immunosuppressive drugs described in section 1861(s)(2)(J) of the Act.
Oral anticancer, antiemetic, and many immunosuppressive drugs are often
used outside of the provider and supplier settings (for example, these
drugs are often used at home); therefore, we are excluding these oral
drugs from the MFN Model.
Compounded drugs including products prepared by
outsourcing facilities.\38\ Although subject to certain FDA
requirements, these products are not approved by FDA per se, and with
one exception under the OPPS \39\ are not billed under drug-specific
HCPCS codes; they are typically billed using under ``not otherwise
classified'' (NOC) codes. Also, compounded drugs are typically acquired
outside of the traditional drug supply chain, and Medicare Part B
payment for compounded drugs is generally based on contractor pricing,
such as invoice pricing. We are excluding these drugs because it is
unlikely that we will be able to obtain reliable international drug
pricing information for compounded drugs.
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\38\ See section 503B of the Federal Food, Drug, and Cosmetic
Act (21 U.S.C. 353b) with respect to the definition of outsourcing
facilities and their regulation by FDA.
\39\ C9257 Injection, bevacizumab, 0.25 mg.
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[[Page 76191]]
Intravenous immune globulin products. In response to the
October 2018 ANPRM, a commenter suggested that CMS exclude plasma-
derived products and stated such products have potential unique
sourcing and distribution, and past supply shortages. We note that FDA
has identified a current shortage related to one of the HCPCS codes
that is among the top drugs with high aggregate 2019 Medicare Part B
total allowed charges (J1569, Gammagard liquid infusion). Three other
immune globulin products are also among the top drugs in 2019, J1459
(Inj ivig privigen 500 mg), J1561 (Gamunex-c/gammaked), and J1568
(Octagam injection). After considering this concern, we are excluding
intravenous immune globulin products from the MFN Model because these
products are at higher risk of shortage based on their complex sourcing
and production, and we are aware of the ongoing exploration of the
potential benefit of plasma in the treatment of patients with COVID-19.
Drugs that are subject to an EUA or receive FDA approval
to treat patients with suspected or confirmed COVID-19. The exclusion
of these drugs will minimize any potential for the MFN Model to impact
rapid, widespread availability of such drugs in the U.S. to treat
patients with suspected or confirmed COVID-19.
Drugs without drug-specific HCPCS codes, that is, those
billed under ``not otherwise classified'' (NOC) codes, such as J3490.
NOC codes are used to bill for drugs not assigned to a particular HCPCS
code. NOC codes typically include a variety of unrelated drugs that
cannot be easily separated for the purpose of ranking allowed charges
of the individual drugs. Also, significantly greater claims processing
complexity for Medicare and MFN participants would result if we had to
identify whether an MFN Model drug was billed under a NOC code during
MFN Model operations. By excluding HCPCS codes for these types of
drugs, these drugs will be fully excluded from the MFN Model.
While we intend that the MFN Model drugs will encompass a wide
variety of frequently utilized Medicare Part B drugs, we also intend
that drugs will not be included on the basis of substantial use at
home. Thus, in Sec. 513.130(b)(2), we codify the exclusion of claims
that were processed and paid by the DME MACs as described in 42 CFR
421.404(c)(2), and professional claims with a place of service code
that indicates the drug was used in a home, including home-like
settings, prior to identifying the top 50 drugs (by HCPCS code).\40\
The place of service exclusion applies only to professional claims
because place of service codes are not used on institutional claims to
identify home use. Specifically, professional claims with place of
service codes 04--homeless shelter, 12--home, 13--assisted living
facility, 14--group home, 16--temporary lodging, and 33--custodial care
facility will be excluded prior to identifying the top 50 drugs (by
HCPCS code).
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\40\ The DME MACs process Medicare Durable Medical Equipment,
Orthotics, and Prosthetics (DMEPOS) claims for a defined geographic
area or ``jurisdiction,'' servicing suppliers of DMEPOS.
Professional claims must comply with the ASC X12 837 Professional
guide (005010X222A1).
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For future years of model implementation, we seek comment on
whether all blood related, plasma derived, and human tissue products
should be included in or excluded from the MFN Model. We also seek
comment on how CMS should define such products and what would be the
supporting rationale for such an exclusion and how to address such
considerations in the future. We note that we are also considering as a
potential addition to the model design whether certain drugs, such as
certain gene and cell therapies (for example, chimeric antigen receptor
T-cell (CAR-T) products) and drugs approved by FDA after the start of
the MFN Model that are indicated for and used to treat rare diseases or
conditions, should be excluded from the MFN Model for all performance
years, or for several years after the drug is first sold in the U.S. We
note that under the MFN Model, annual Medicare Part B allowed charges
would have to exceed tens of millions of dollars for such drugs to
reach the top 50 and be added to the MFN Model. We also note that many
of the top 50 drugs in 2019 are used to treat conditions with limited
populations and were first approved within the last 5 years. In
addition, we note that while drugs may initially be approved for one or
a few very narrow indications, subsequently approved indications can
quickly expand the use of the drug to a much larger patient population.
We are considering whether we should exclude certain gene and cell
therapies based on supply chain criteria, similar to our policy to
exclude vaccines and compounded drugs. For future years, we seek
comment on whether we should exclude certain gene and cell therapies or
new drugs for the treatment of rare diseases and conditions from the
MFN Model, and how CMS would identify such drugs for exclusion,
particularly how we would define such drugs, identify rare diseases and
conditions for purposes of the MFN Model, and determine the appropriate
length of such exclusion (for example, all performance years or several
years after the drug is first sold in the U.S.).
Some commenters have suggested that drugs in short supply (based on
inclusion on the FDA drug shortages list) should be excluded from drug
payment models. As discussed previously, we are excluding intravenous
immune globulin products from inclusion on the MFN Model Drug HCPCS
Codes List, because these products are at higher risk of shortage based
on their complex sourcing and production. Otherwise, based on our
experience with ASP pricing, shortages of high cost single source drugs
and biologicals are uncommon, of short duration, and generally apply to
some but not all package sizes of a drug. As described in section
III.E.12. of this IFC and codified in Sec. 513.210(d)(2), we include a
quarterly payment exception for MFN drugs that are in short supply
(based on inclusion on the FDA drug shortages list). We believe it will
be less disruptive to the MFN Model to include a quarterly payment
exception for MFN Model drugs during the time they are in short supply
than to exclude such drugs from the MFN Model altogether because a
quarterly payment exception approach will avoid changing the inclusion
status of drugs should a shortage occur and again when the shortage is
resolved, eliminate the need to consider developing a process to add
and remove replacement drugs to maintain the number of MFN Model drugs,
and avoid manufacturers having to change processes for capturing sales
of such drugs in their ASP calculations as discussed in section III.L.
of this IFC (under this policy, manufacturers will not include in their
calculation of the manufacturer's ASP any units of MFN Model drugs
billed by MFN participants where the MFN Drug Payment Amount is paid by
Medicare as the primary payer).
Finally, we considered whether an exception to inclusion on the MFN
Model Drug HCPCS Codes List might be appropriate for MFN Model drugs in
cases where pharmaceutical manufacturers that distribute the drug in
the U.S. do not own the rights to the drug product for distribution
outside the U.S. and therefore do not control ex-U.S. pricing for the
drug product. To avoid a gaming opportunity whereby manufacturers' new
or recent business arrangements create such cases, this type of
exception could be defined such that only ownership rights that were
transferred prior to the October 2018 ANPRM, when CMS announced a new
[[Page 76192]]
Medicare Part B drug payment model was being developed, would qualify.
To avoid an exception being too broad, we are concerned that additional
criteria should be required to qualify for it, such as whether the
increase in the MFN Model drug's applicable ASP (a measure of U.S.
prices) based on sales since October 2018 has been slower than
inflation (that is, the change in the CPI-U from the end of October
2018 through the ASP calendar quarter for the first calendar quarter of
the model), and whether the U.S. manufacturer makes a legally
enforceable commitment to future U.S. price increases being slower than
inflation moving forward, if such an exception were to be granted. In
addition, to maintain the exception for the remainder of the model, the
increase in the MFN Model drug's applicable ASP since October 2018
would need to be assessed quarterly to determine whether it continues
to be slower than inflation. Given the complex and numerous
relationships that manufacturers may have across U.S. and international
markets, we are not including such an exception for the MFN Model.
We seek comments for future years on our approach to identifying
and maintaining the MFN Model Drug HCPCS Codes List and whether there
is a need for an exception relating to manufacturers' ownership of drug
products internationally, and if so, how such an exception might be
defined and operated transparently.
3. Annual Updates to the MFN Model Drug HCPCS Codes List
As discussed in section III.D.1. of this IFC, the MFN Model will
begin with 50 drugs and biologicals by HCPCS code on the MFN Model Drug
HCPCS Codes List for performance year 1. We will keep approximately 50
drugs by HCPCS code in the MFN Model during the 7-year performance
period so that drugs that continue to account for a large portion of
Medicare Part B drug spending will continue to be included in the
model. However, we believe that some adjustments to the MFN Model Drug
HCPCS Codes List will likely be required from time to time as drugs
enter and exit the market and as utilization of Medicare Part B drugs
(measured by annual total allowed charges) changes. Thus, we will
update the MFN Model Drug HCPCS Codes List annually. The annual update
process will occur prior to the beginning of each performance year
rather than more frequently, such as a quarterly process, because less
frequent changes to the MFN Model Drug HCPCS Codes List will decrease
the burden associated with participating in the model. We believe that
making fewer changes to the MFN Model Drug HCPCS Codes List will result
in MFN participants having to make fewer changes to acquisition
arrangements, and this in turn will lessen any potential for disruption
in workflow and care delivery compared to a quarterly update process.
Additionally, as specified in Sec. 513.130(a)(4), some quarterly
changes may be necessary to comport with HCPCS coding updates that are
applicable to the HCPCS codes on the MFN Model Drug HCPCS Codes List,
such as when a code is terminated and a successor code is established.
For each annual update for performance years 2 through 7, as
described in Sec. 513.130(a)(2), we will array in descending order all
separately payable Medicare Part B drugs, using HCPCS codes, based on
total allowed charges after applying the exclusions codified in Sec.
513.130(b)(1) and (b)(2), using the most recent full calendar year's
Medicare Part B claims from all providers and suppliers. Those drugs
(as identified by HCPCS codes) that have total allowed charges that
fall in the top 50 drugs by spending for that calendar year that are
not already on the MFN Model Drug HCPCS Codes List will be added to the
MFN Model Drug HCPCS Codes List to take effect on the first day of the
next performance year and the MFN Drug Payment Amount that will apply
will be based on the applicable MFN Price phase-in for that performance
year and will follow the annual payment updates thereafter. This
process will be used only to add HCPCS codes that are new to the top
50--to maintain consistency, we will not remove any codes from the MFN
Model Drug HCPCS Codes List on the grounds that the HCPCS code dropped
out of the top 50. We will keep all HCPCS codes that were included on
the MFN Model Drug HCPCS Codes List for the prior performance year on
the MFN Model Drug HCPCS Codes List, except in certain circumstances as
noted in section III.D.4. of this IFC, in order to have greater
stability in the set of drugs that are included in the MFN Model across
the performance years. As a result, in performance years 2 through 7,
the number of HCPCS codes on the MFN Model Drug HCPCS Codes List may be
greater than 50. We believe this approach has the potential to identify
drugs that are alternative therapies to MFN Model drugs, such as
competitor products, where MFN participants may shift utilization to
avoid using drugs subject to the MFN Model payment, and will provide a
mechanism for adding such drugs to the MFN Model. In addition, this
approach will serve as a mechanism to identify newer drugs with high
annual Medicare Part B spending for inclusion in the MFN Model.
To maintain transparency, when we add HCPCS codes that are new to
the top 50 or are replacement codes for HCPCS codes that are listed on
the MFN Model Drug HCPCS Codes List, we will list the code's start date
for inclusion in the MFN Model. In addition, we will revise HCPCS codes
on the MFN Model Drug HCPCS Codes List as necessary to reflect
quarterly HCPCS code updates that are applicable to the HCPCS codes on
the MFN Model Drug HCPCS Codes List, for example when a permanent code
replaces a temporary code, a HCPCS code is terminated and a replacement
code is established, or a HCPCS code is established for Medicare use.
In such case, we will include an end date on the MFN Model Drug HCPCS
Codes List for the terminated code. We will notify MFN participants of
updates to the MFN Model Drug HCPCS Codes List no less frequently than
quarterly by adding the updated MFN Model Drug HCPCS Codes List to the
MFN Model website (https://innovation.cms.gov/initiatives/most-favored-nation-model).
4. Approach for Removing Drugs From the MFN Model Drug HCPCS Codes List
We do not anticipate that drugs will be removed from the MFN Model
frequently. In accordance with Sec. 513.130(a)(3), we will remove
drugs from the MFN Model Drug HCPCS Codes List only under the following
limited circumstances, but no more frequent than quarterly, to align
with quarterly MFN Model payment updates:
If they are permanently withdrawn from the U.S. market;
If a specific HCPCS code included on the MFN Model Drug
HCPCS Codes List is terminated with no replacement code available or
planned; or
The drug is excluded from the MFN Model pursuant to the
exclusions in Sec. 513.130(b)(1), for example a HCPCS code describes a
generic drug approved under an ANDA or a drug with an EUA or FDA
approval to treat patients with suspected or confirmed COVID-19.
To maintain transparency, we will remove HCPCS codes by setting an
end date on the MFN Model Drug HCPCS Codes List at the next quarterly
update after CMS becomes aware, through environmental scanning
activities, that all of the NDCs assigned to a HCPCS code have been
withdrawn from the U.S. market and the drug is permanently withdrawn
from the U.S. market, or the HCPCS code has been terminated with
[[Page 76193]]
no replacement code available or planned, or the exclusion in Sec.
513.130(b) applies. HCPCS codes that are removed from the MFN Model
Drug HCPCS Codes List will no longer be subject to the MFN Model
payment, but rather will be subject to current Medicare payment
policies. If the conditions for removal no longer exist, the HCPCS code
could again qualify for inclusion on the MFN Model Drug HCPCS Codes
List at the next annual update.
5. Performance Year 1 MFN Model Drug HCPCS Codes List
To create the MFN Model Drug HCPCS Codes List for performance year
1, we arrayed drug HCPCS codes by aggregate 2019 Medicare Part B total
allowed charges \41\ after applying the exclusions in Sec.
513.130(b)(1) and (b)(2). We then identified the top 50 drugs by HCPCS
code with the highest aggregate 2019 Medicare Part B total allowed
charges. This process excluded HCPCS codes for two influenza vaccines
(90662 (Iiv no prsv increased ag im) and 90653 (Iiv adjuvant vaccine
im)), two pneumococcal pneumonia vaccines (90732 (Ppsv23 vacc 2 yrs+
subq/im) and 90670 (Pcv13 vaccine im)), and a radiopharmaceutical
(A9606 (Radium ra223 dichloride ther)) from the MFN Model Drug HCPCS
Codes List. The exclusion of intravenous immune globulin products
excluded four HCPCS codes: J1459, Inj ivig privigen 500 mg; J1561,
Gamunex-c/gammake; J1568, Octagam injection; and J1569, Gammagard
liquid injection. Additionally, one HCPCS code that describes a generic
drug (J9395, Injection, fulvestrant) was excluded. Excluding claims
that were processed and paid by the DME MACs resulted in the following
HCPCS codes no longer falling within the top 50 drugs in 2019: J7605
(Arformoterol non-comp unit); J7686 (Treprostinil, non-comp unit); and
J3285 (Treprostinil injection). Excluding claims based on the place of
service exclusion resulted in one HCPCS code, J7192 (Factor viii
recombinant nos), no longer falling within the top 50 drugs in 2019.
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\41\ We used 2019 final action claims data that were available
in the CMS Chronic Conditions Data Warehouse in September 2020 where
Medicare was the primary payer.
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Using this approach for selecting MFN Model drugs, the resulting
performance year 1 MFN Model Drug HCPCS Codes List includes single
source drugs and biologicals that accounted for approximately 75
percent of annual Medicare Part B drug allowed charges for separately
payable drugs during 2019. Table 2 displays the list of MFN Model drugs
(by HCPCS code) that are included on the MFN Model Drug HCPCS Codes
List for the beginning of performance year 1, along with the top
billing specialties.
CMS will publish the MFN Model Drug HCPCS Codes List quarterly on
the MFN Model website (https://innovation.cms.gov/initiatives/most-favored-nation-model), in advance of the calendar quarter, along with
MFN Model Payment amounts and other MFN Model information and
materials.
BILLING CODE 4120-01-P
[[Page 76194]]
[GRAPHIC] [TIFF OMITTED] TR27NO20.001
[[Page 76195]]
[GRAPHIC] [TIFF OMITTED] TR27NO20.002
[[Page 76196]]
BILLING CODE 4120-01-C
E. Model Payment Methodology for MFN Model Drugs
The MFN Model will test an innovative approach to calculating drug
payment through use of a more comprehensive set of drug pricing data to
calculate an alternative payment amount for MFN Model drugs, along with
an alternative add-on payment, which is described in section III.F. of
this IFC. Payment for drug administration services, when applicable,
will continue to be separately billed by model participants to
Medicare; there will be no change in the payment for drug
administration services under the MFN Model. Providers and suppliers
will continue to purchase MFN Model drugs, furnish such drugs to
beneficiaries, submit claims to Medicare, and collect applicable
beneficiary cost-sharing. Under the MFN Model, payments for separately
payable Medicare Part B drugs will include the alternative drug payment
amount and the alternative add-on payment amount, both subject to
sequestration, as applicable.
Similar to the current approach under section 1847A of the Act, the
MFN Model alternative payment limit for the ``drug portion'' of payment
for MFN Model drugs (that is, not including the add-on amount) will be
calculated by CMS quarterly. This amount is called the MFN Drug Payment
Amount. The calculation of the MFN Drug Payment Amounts is codified in
Sec. 513.210(b). Beneficiary cost-sharing will apply to the MFN Drug
Payment Amount for included drugs.
We will calculate an MFN Drug Payment Amount for each drug on the
MFN Model Drug HCPCS Codes List based on an MFN Price, which will be
derived from the lowest GDP-adjusted country-level price, based on non-
U.S. OECD member countries with a GDP per capita that is at least 60
percent of the U.S. GDP per capita.\42\ We will use GDP per capita
information that is based on purchasing power parity. We are also
establishing limits such that the MFN Drug Payment Amount will not
exceed non-model payment for the drug (excluding any non-model add-on
payment amount), will not apply to drugs that are not separately
payable, and certain other limitations discussed later in this section.
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\42\ Individual countries differ in the regulatory processes and
standards governing approval of drugs and biologicals. Use of
international drug pricing information in the MFN Model should not
be interpreted to connote FDA approval or to otherwise describe any
scientific or regulatory relationship between U.S.-approved and non-
U.S.-approved products.
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Section III.E.1. of this IFC identifies the data sources for the
MFN Model drugs' international drug pricing information that we will
use to calculate the MFN Price for each drug. Section III.E.2. of this
IFC outlines the international drug pricing information we will include
in these calculations and the included countries. Section III.E.3. of
this IFC defines the MFN Drug Payment Amount. Section III.E.4. of this
IFC outlines our approach to calculating each drug's MFN Drug Payment
Amount. Section III.E.5. of this IFC describes the phase-in of the MFN
Price. Section III.E.6. of this IFC describes the alternative
calculation for the MFN Drug Payment Amount for situations where no
international drug pricing information is available for an MFN Model
drug. Section III.E.7. of this IFC provides illustrative MFN Drug
Payment Amounts for each drug on the performance year 1 MFN Model Drug
HCPCS Codes List in Table 2 using historical data. Section III.E.8. of
this IFC describes the timing of data and MFN Drug Payment Amount
updates. Section III.E.9. of this IFC describes adjustments to the
phase-in formula and incentives for manufacturers to address rising
U.S. drug prices. Section III.E.10. of this IFC describes the
limitation on the MFN Drug Payment Amount. Section III.E.11. of this
IFC describes the method for establishing MFN Drug Payment Amounts for
MFN Model drugs added to the model for performance year 2 and
subsequent performance years. Section III.E.12. of this IFC describes
the quarterly payment exception for MFN Model drugs in short supply.
Section III.E.13. of this IFC describes continued payment of the blood
clotting factor furnishing fee under the MFN Model.
1. Data Sources on International Drug Pricing Information
We will rely on existing data sources to obtain data that we will
use to calculate and update the MFN Drug Payment Amounts. We will use
existing data sources that contain international drug pricing
information, including list prices, sales and/or volume data (for
example, package size and number of packages sold), as available, in
order to optimize operational efficiency. Sales may be based on ex-
manufacturer prices (sometimes called the ex-factory price), that
represent actual or calculated prices paid to the manufacturer by
wholesalers and other distributors, retail prices, prices for other
distribution channels, or a combination thereof. Confidential
manufacturer rebates will not likely be accounted for within these
data; therefore, existing sources for international drug sales data may
overstate actual prices realized by manufacturers.
In the October 2018 ANPRM, we considered establishing a data
collection system for manufacturers to report to CMS their
international drug sales data for prices and units sold to support the
calculation of the model payment for each drug. In response to the
October 2018 ANPRM, we received comments stating that CMS should use
existing data sources for international drug pricing information in
order not to place burden on manufacturers. Some commenters expressed
concerns that new data reporting would greatly increase burdens and
costs for manufacturers, further limiting their ability to invest in
research and development for innovative therapies, and would be
impractical because defining price reporting for foreign markets would
be too complex and could not adequately capture fluid pricing policy
changes. We appreciate these concerns, and as such, we will rely on
existing data sources for purposes of calculating MFN Drug Payment
Amounts. We believe that existing data sources are adequate for
purposes of calculating country-level prices, GDP-adjusted country-
level prices, and the MFN Prices, as described in this IFC, that will
be used to calculate the MFN Drug Payment Amount.
Commenters also noted that one potential adverse reaction to the
model described in the October 2018 ANPRM may be a shift
internationally to a high price and high rebate pricing strategy.
Specifically, commenters expressed concern that if the international
drug pricing information used to establish payment under a model relied
on the list prices in the included countries, then manufacturers would
restructure their pricing arrangements to increase the list prices of
the model's drugs in those countries, and offer higher rebates to
offset the increased list price. CMS appreciates this concern, and we
will prioritize use of available international drug pricing information
that incorporate discounts and rebates to the extent possible, rather
than just the list prices.
We have assessed several existing data sources to determine the
availability and sufficiency of international drug pricing information.
In Sec. 513.140(c), we are codifying the use of one or more
international drug pricing data sources. Specifically, we will use one
or more data sources, available to CMS at least 20 business days prior
to the start of a calendar
[[Page 76197]]
quarter, that utilize a standardized method for identifying drugs
across countries within that data source, such as using an
internationally recognized method for identifying scientific and
nonproprietary names (for example, active ingredient name) and a
standard method for identifying drug forms that at a minimum
distinguishes among injectable, oral, and other forms of a drug. For
example, the data source might use the International Nonproprietary
Names (INN), as applicable.\43\ This process requires mapping between
the data source's standardized method for identifying scientific and
nonproprietary names and HCPCS codes, as discussed and illustrated in
section III.E.7. of this IFC. Further, we will use one or more data
sources that contain international drug pricing information stated in
U.S. currency, such as list prices, ex-manufacturer prices (sometimes
called the ex-factory price) that represents actual or calculated
prices paid to the manufacturer by wholesalers and other distributors,
actual or calculated sales for retail and other distribution channels,
or volume data (for example, number of units sold).
---------------------------------------------------------------------------
\43\ World Health Organization, International Nonproprietary
Names accessed via https://www.who.int/medicines/services/inn/en/.
---------------------------------------------------------------------------
If more than one data source is available for an MFN Model drug, as
noted previously, we will prioritize the data sources using a hierarchy
that we describe later in this section. Thus, for each MFN Model drug,
we will identify and use the most comprehensive data source available,
using the hierarchy codified in Sec. 513.140(c)(3). We will use only
one data source for an MFN Model drug for a quarter, meaning we will
not combine data from different data sources or time periods to
calculate the MFN Drug Payment Amount for an MFN Model drug for a
quarter.
Whenever possible, we will use international drug pricing
information from two calendar quarters prior to the calendar quarter to
which the MFN Drug Payment Amount will apply since the ASP payment
limits that apply to that calendar quarter are based on manufacturers'
U.S. sales from two calendar quarters prior such that the U.S. and
international drug pricing data will be based on information from the
same calendar quarter. We use the term applicable ASP calendar quarter
to mean the period that is two calendar quarters prior to the calendar
quarter to which the MFN Drug Payment Amount will apply.
The hierarchy of data sources we will use is as follows:
A data source with sales and volume data for the
applicable ASP calendar quarter from at least one included country,
that is, a non-U.S. OECD member country at the end of the applicable
ASP calendar quarter with a GDP per capita that is at least 60 percent
of the U.S. GDP per capita.
A data source that does not have sales and volume data for
the applicable ASP calendar quarter, but contains sales and volume data
for any prior calendar quarter beginning on or after October 1, 2019
from at least one included country.
The extracted data used by CMS to determine the most
recent MFN Price used to calculate an MFN Drug Payment Amount posted on
the MFN Model website.
A data source with ex-manufacturer price data for the
applicable ASP calendar quarter from at least one included country.
A data source with list price data for the applicable ASP
calendar from at least one included country.
In each of these cases, if there is more than one data source
meeting the requirements in Sec. 510.140(c), we will use the data
source at the highest level of the hierarchy that contains information
from the highest number of included countries, and, if available,
incorporates discounts and rebates into its drug pricing information.
It is possible that we will use different data sources for different
drugs over different quarters. We will use the data as available from
the data source, and we will not make adjustments to account for
differences between the data sources or for confidential rebates. We
note that, based on the performance year 1 MFN Model Drug HCPCS Codes
List shown in Table 2, levels 4 and 5 of the hierarchy will only apply
to MFN Model drugs that are added to the MFN Model Drug HCPCS Codes
List after performance year 1 and perhaps for Q2043 (Sipuleucel-t auto
cd54+) \44\ and J2507 (Pegloticase injection), because for other MFN
Model drugs in performance year 1, the first three levels of the
hierarchy will always result in an available data source as we consider
the data used by CMS to create the illustrative MFN Prices and MFN Drug
Payment Amounts in Table 6 of this IFC to satisfy level 3 of our
hierarchy. To illustrate: Suppose we identified four data sources
meeting the requirements of Sec. 510.140(c), where Data Source 1
contains sales and volume data for MFN Model drug X for the applicable
ASP calendar quarter from 10 included countries, Data Source 2 contains
sales and volume data for MFN Model drug X for the applicable ASP
calendar quarter from 15 included countries, Data Source 3 contains
sales and volume data from the third calendar quarter of 2020 for MFN
Model drug X from 16 included countries, and Data Source 4 contains
list price information for the applicable ASP calendar quarter from all
included countries. In this scenario, we would use information solely
from Data Source 2 to determine the MFN Price for MFN Model drug X by
calculating unadjusted country-level prices for each of the 15
countries for which Data Source 2 contains information, and we would
not use Data Sources 1, 3, or 4 to calculate the MFN Price for MFN
Model drug X for that quarter. For further illustration of how we will
apply the hierarchy in calculating MFN Drug Payment Amounts, see
section III.E.4.a. of this IFC.
---------------------------------------------------------------------------
\44\ No data on international pricing or sales of Sipuleucel-t
auto cd54+ were available in the data source used for Table 6, but
international drug pricing information for this drug could be
available in other sources.
---------------------------------------------------------------------------
We will use international sales and volume information from as
early as the third calendar quarter in 2020 to minimize the possibility
of having no international sales and volume information with which to
calculate the MFN Price and to mitigate the potential effect of
manufacturers' limiting the reporting of international drug pricing
information during the model performance period.
In addition, the one or more data sources we will use will have
mechanisms in place to maintain, update, and correct, if necessary, the
data source on at least a quarterly basis. Further, the data sources we
will use will be maintained by organizations that seek to limit the lag
inherent in data to no more than 180 days from the end of the calendar
quarter for which drug pricing information is compiled to the time that
the organization makes such updates available to users of the data
source.
We plan to monitor the implementation of a World Health Assembly
(WHA) resolution to ``improve the transparency of markets for
medicines, vaccines, and other health products.'' This resolution aims
to help Member States make more informed decisions when purchasing
health products, negotiate more affordable prices, and ultimately
expand access to health products for their populations. In particular,
the WHA resolution \45\--
---------------------------------------------------------------------------
\45\ World Health Assembly Update, 28 May 2019, accessed via:
https://apps.who.int/gb/ebwha/pdf_files/WHA72/A72_R8-en.pdf.
---------------------------------------------------------------------------
Urges Member States to publicly share information on net
prices paid for
[[Page 76198]]
health products, to promote greater transparency on pharmaceutical
patents and clinical trial results and to improve suppliers' reporting
of information such as sales revenues and units sold; and,
Requests the WHO secretariat to support the development
and implementation of national policies relevant to transparency and to
monitor the impact of transparency on affordability and availability of
health products, including the effect of differential pricing.
We will monitor developments related to this WHA resolution and
assess its impact on the availability of data we will use to calculate
and update MFN Drug Payment Amounts.
As discussed previously, we will use a hierarchy when selecting
from available data sources and start by using data sources that
incorporate discounts and rebates to the extent possible in order to
address commenters' concerns about a shift internationally to a high
price and high rebate pricing strategy. We believe that using one or
more data sources will help to ensure that we will capture sufficient
information to monitor the international drug pricing landscape and to
calculate and update MFN Drug Payment Amounts. Data sources that
include the information described previously, as determined by CMS,
will be considered sufficient, and as such, we will calculate MFN Drug
Payment Amounts for MFN Model drugs using information extracted from
such data sources. Specifically, as necessary, for each MFN Model drug,
we will extract and use data that align with the data sources'
standardized method for identifying scientific and nonproprietary names
and dosage forms (for example, injectable forms), and with the HCPCS
code's long descriptor, including dosage form, for the HCPCS codes on
the MFN Model Drug HCPCS Codes List, as applicable. Further, we will
only use the extracted data for dosage formulations that could be
described by the MFN Model drug's HCPCS code descriptor as determined
by CMS when such limitation is not feasible prior to extracting the
data. For example, for a drug, one HCPCS code may include drug products
that are a certain type of formulation, such as short-acting,
intravenously administered drug products, and another HCPCS code may
include drug products with the same scientific and nonproprietary name
but a different formulation (such as a long-acting suspension for
intramuscular injection), and the extracted data contains international
drug pricing information for both formulations. In such case, we will
align the extracted data in accordance with the HCPCS code descriptor
for the MFN Model drug. In order to align with our existing policies
for how we utilize manufacturer-reported ASP data to calculate payment
limits, we may find it necessary to make adjustments to the data that
we extract from international drug pricing information data sources.
For example, in calculating payment amounts based on ASP we do not
adjust the volume or units of a drug (that is, the amount of a drug in
a package) for intentional overfill (see 75 FR 73466). If we find that
a data source from which we obtain international drug pricing
information makes adjustments for overfill, we will make adjustments to
the data that we extract from such source so that the extracted data is
comparable to ASP data. There could be other cases where we will have
to examine the extracted data and make adjustments to align the data
with a HCPCS code descriptor for an MFN Model drug. Specifically, we
will adjust the extracted international drug pricing information for
MFN Model drugs when the data source shows the package size of a drug
product that is inconsistent with the manufacturer's information about
that product as determined by CMS. In such cases where we confirm a
difference, we will make adjustments to the pricing, sales and volume
data as necessary before calculating the unadjusted country-level price
for the drug at the HCPCS code level. We believe that such cases will
be rare. However, we identified the need to make such adjustment to the
international drug pricing information we used to illustrate the MFN
Drug Payment Amounts for J9311 (Inj rituximab, hyaluronidase) shown in
Table 6 to align the package size volume with manufacturer labeling and
the HCPCS code dosage descriptor. We note that there could be
additional cases if international drug pricing data sources that we
will select show prices, sales or volume data that are adjusted for
intentional overfill, include multiple ingredients for a single drug
product, or are in error (for example, the package size represents the
maximum volume of a vial instead of the volume of drug in a package).
We will only use the extracted data that have complete package size
information. As discussed previously, we will use a hierarchy to
determine which data source to use for each MFN Model drug for a
quarter, in which we will select a data source that includes sales and
volume data first. Data without both sales and volume data will not be
able to be combined with other data, therefore we will exclude such
observations. For data sources with international sales and volume data
for a given MFN Model drug, we will exclude from the calculation of the
unadjusted country-level price data that fall below a minimum threshold
or are incomplete, that is, international pricing data with less than
$1,000 in quarterly sales, with less than 1,000 units in quarterly
volume, or where both sales and volume data are not present. We believe
that $1,000 in quarterly sales and 1,000 units in quarterly volume for
a package size is an appropriate minimum necessary to establish
sufficient sales and volume for data to be included in the calculation
of a meaningful and reliable unadjusted country-level price for an MFN
Model drug and will minimize inclusion of potential outlier data. We
will exclude presentations with low volume or low sales to prevent
outlier presentations from exerting undue influence.
In developing the illustrative MFN Prices shown in Table 6, we
applied these exclusions. Minimal sales and volume across all countries
were excluded because of the low volume or sales exclusion criteria. We
explored the impact of different volume and expenditure thresholds, and
determined that $1,000 in quarterly sales and 1,000 units are a
reasonable threshold to reduce risk associated with extremely low
values. We found that data with potential outlier sales remained
relatively common with lower thresholds (that is, below $1,000 in
quarterly sales). While using higher thresholds may further reduce
potential inclusion of outlier sales data, doing so would result in
having less data to calculate unadjusted country-level prices.
The exclusion of international pricing data with less than $1,000
in quarterly sales or with less than 1,000 units in quarterly volume
from the calculation of the unadjusted country-level price will greatly
minimize the potential risk for including possible outlier or errant
data. To better understand this potential issue, we considered the
impact of including or excluding data with less than $1,000 in
quarterly sales or less than 1,000 units in quarterly volume in the
calculation of the unadjusted country-level price. There was little
impact from including these data but, as a potential safeguard to
prevent inclusion of inappropriately low or high international drug
pricing information in our calculations for the MFN Model, we will
exclude such data from the calculation of the unadjusted country-level
price. Overall, where this approach had more than a 1 percent
[[Page 76199]]
impact, there tended to be an increase in the MFN Prices.
We also considered whether pricing information that is greater than
or less than 95 percent of the mean across all data for the drug at the
equivalent of the HCPCS code billing unit level should be considered a
possible outlier or error and whether trimming such data or removing
such data would be warranted. In our experience with international drug
pricing information data sources, outlier or potentially erroneous data
appear only in isolated instances and are often suggestive of
unintended differences in the unit at which data is shown. For example,
the pricing data for a product with a standard unit of one gram in one
country could appear to be 1,000 times lower than the pricing data for
that same product from other countries in the data source; in such a
case, it seems likely that the data for the one country with a very low
relative price represents the price per milligram not per gram and such
data would likely be corrected over time by the data source. We believe
international drug pricing data sources have mechanisms to correct such
discrepancies based on market research of currently available
international drug pricing information data sources. Further, as
codified in Sec. 513.140(c), the international drug pricing
information data sources that we will obtain will have mechanisms in
place to maintain, update, and correct, if necessary, the information
on international drug pricing in the database on at least a quarterly
basis. As such, because we will revise the MFN Drug Payment Amounts
quarterly, we will recalculate the MFN Drug Payment Amounts for up to
four prior quarters when revised international drug pricing information
is available in the data source that we used to calculate the MFN Model
drug's MFN Price for the relevant quarter or ASP updates for the
relevant quarter are available.\46\ In cases where an MFN Drug Payment
Amount for a prior quarter is recalculated by CMS, CMS will
prospectively apply the recalculations in the quarterly update
following the availability of revised international drug pricing
information and ASP updates, and will not automatically reprocess
claims to apply the recalculation, but reserves the right to do so. To
the extent that MFN Model claims are reprocessed due to revisions to
the international drug pricing information, the Medicare payment amount
and beneficiary cost sharing will be recalculated to reflect the
revised prices. If prior to calculating the unadjusted-country level
prices for a quarter, the data source confirms that there is an error
that they plan to correct in a future version of the dataset and we
have the corrected information, we will make the correction to avoid
the need to reprocess claims later. Therefore, we do not believe it is
necessary to take further steps to trim or remove potential outlier or
erroneous international drug pricing information before calculating the
unadjusted country-level prices. We note that CMS does not make outlier
adjustments to ASP data.
---------------------------------------------------------------------------
\46\ We will apply the recalculations in the quarterly update
following the availability of revised international drug pricing
information and ASP updates.
---------------------------------------------------------------------------
In addition, for future years, we seek comment on whether a
threshold should be applied to determine whether the MFN Drug Payment
Amount should be recalculated for a prior quarter. Specifically, we are
interested in comments on whether recalculations should only occur when
the international drug pricing information data source used corrects
its data and the impact on the MFN Price is more than a nominal amount.
We seek comment on the appropriate amount of such threshold and how a
nominal amount should be defined. Finally, in the event that the
international drug pricing information data source that we used to
calculate the MFN Drug Payment Amount for an MFN Model drug for a
quarter identifies an error in their data and does not correct such
error within 180 days after the applicable ASP calendar quarter, we
seek comment on whether CMS should recalculate the MFN Drug Payment
Amount for such MFN Model drug and quarter using international drug
pricing information in accordance with the hierarchy in Sec.
513.140(c)(3) after excluding the data source we initially used. We
also seek comment on whether CMS should adopt an alternative approach
to remediating such data errors.
2. International Data Included in the MFN Model
In the October 2018 ANPRM, for purposes of a potential IPI Model,
we stated that we were considering using pricing data from the
following countries: Austria, Belgium, Canada, Czechia, Denmark,
Finland, France, Germany, Greece, Ireland, Italy, Japan, Netherlands,
and the United Kingdom. We considered including these countries' data
as they are either economies comparable to the U.S. or they are
included in Germany's market basket for reference pricing for their
drug prices, and existing data sources contain pricing information for
these countries. We received wide-ranging and helpful feedback in
response to the October 2018 ANPRM regarding which countries' data to
include in a model. In addition to comments received to the October
2018 ANPRM, we also conducted significant outreach to stakeholders,
such as stakeholder meetings and conference calls, to gather targeted
feedback. There was also a substantial number of media and press
reports surrounding which countries' data to include in the MFN Model.
Generally, we received a significant number of comments that
expressed opposition to including data from countries that have health
care systems that are substantially dissimilar to the U.S.'s health
care system. Specifically, many commenters stated that data from
countries utilizing government-run health care systems or imposing
strict drug price controls should be excluded. Alternatively, other
commenters noted that CMS should consider broadening the scope to
include more countries, because the more countries that are included in
the index, the harder it would be for pharmaceutical companies to
manipulate or game the pricing changes. Commenters also recommended
utilizing various criteria for selecting the countries that would be
included, such as the launching speed of new drugs, the presence of
rigorous health technology assessment, the proportions of public and
private markets, the economies of those countries, and Human
Development Index (HDI).\47\
---------------------------------------------------------------------------
\47\ The Human Development Index is utilized by the United
Nations and is ``is a summary measure of average achievement in key
dimensions of human development: a long and healthy life, being
knowledgeable and have a decent standard of living. The HDI is the
geometric mean of normalized indices for each of the three
dimensions.'' Please see the United Nations Development Programme's
Human Development Reports for more information: https://hdr.undp.org/en/content/human-development-index-hdi.
---------------------------------------------------------------------------
Based on the comments received, we believe the most appropriate
criteria for considering a country for MFN pricing is membership in the
OECD and GDP per capita relative to the U.S. The current list of OECD
countries includes all countries included in the October 2018 ANPRM as
well as Australia, Chile, Colombia, Estonia, Hungary, Iceland, Israel,
Latvia, Lithuania, Luxembourg, New Zealand, Norway, Poland, Portugal,
Republic of Korea, Slovakia, Slovenia, Spain, Switzerland, and Turkey.
OECD countries comprise a set of countries that share with the U.S.
democratic principles and commitment to market-based economies, and
these countries' GDP per capita (based on purchasing power parity)
range from
[[Page 76200]]
approximately 25 percent of the U.S. GDP per capita to over 175 percent
of the U.S. GDP per capita. Based on this wide range of GDP per capita
data, we believe it is most appropriate to include available
international drug pricing information for countries with a GDP per
capita of at least 60 percent of the U.S. GDP per capita, as codified
in Sec. 513.140(b). We believe that applying a minimum of 60 percent
of the U.S. GDP per capita strikes a balance between--(1) having too
low a GDP per capita threshold and including data from countries with
economies that are substantially different from the U.S., while; (2)
also not having such a high GDP per capita threshold that the list of
countries would be very short, which commenters suggested we should
avoid. To avoid creating a potential incentive for countries to
discontinue their membership in the OECD, we will include available
international drug pricing information for countries that were OECD
members as of October 1, 2020, regardless of whether they remain OECD
members after October 1, 2020, unless the country's GDP per capita, as
determined by CMS quarterly, falls below the threshold of 60 percent of
the U.S. GDP per capita. Based on available data, this means that we
will calculate the MFN Price for the first quarter of performance year
1 based on available international drug pricing information from
Australia, Austria, Belgium, Canada, Denmark, Finland, France, Germany,
Iceland, Ireland, Israel, Italy, Japan, Republic of Korea, Luxembourg,
Netherlands, New Zealand, Norway, Spain, Sweden, Switzerland, and the
United Kingdom.\48\ These 22 OECD countries are among the countries
with the highest GDP per capita worldwide.\49\
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\48\ The non-U.S. OECD countries that will not be an included
country for purposes of calculating the MFN Price for MFN Model
drugs for the first quarter of performance year 1 will be Chile,
Colombia, Czechia, Estonia, Greece, Hungary, Latvia, Lithuania,
Mexico, Poland, Portugal, Slovakia, Slovenia, and Turkey.
\49\ https://www.cia.gov/library/publications/the-world-factbook/fields/211rank.html.
---------------------------------------------------------------------------
We considered alternative approaches to including data from
countries for the MFN Model. Specifically, we considered including all
non-U.S. OECD countries or selecting countries based on factors such as
World Health Organization (WHO) recognition as a Stringent Regulatory
Authority (SRA) and intellectual property protections. We also
considered including data from only countries that may represent large
markets for drug manufacturers such as the European Union, Canada,
Japan, and United Kingdom. Additionally, the Foundation for Research on
Equal Opportunity (FREOPP) recommended an alternative approach called
the Market-Based International Index (MBII) as a benchmark for
evaluating other countries' prescription drug pricing systems; \50\
this approach would include data from the following countries that
FREOPP identified as having market-based health care systems: Austria,
Belgium, Czechia, Denmark, France, Germany, Ireland, Japan,
Netherlands, Portugal, Singapore, Slovakia, and Switzerland.
---------------------------------------------------------------------------
\50\ Roy, A. (2018) The Foundation for Research on Equal
Opportunity, ``What Medicare Can Learn From Other Countries on Drug
Pricing,'' accessed via https://freopp.org/what-medicare-can-learn-from-other-countries-on-drug-pricing-bf298d390bc5.
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Based on analyses examining potential alternatives, we believe that
none of these alternative approaches would be as objective and
predictable for purposes of calculating MFN Prices as our approach. Our
approach will result in a large set of countries that are economically
similar, have reasonably comparable purchasing power to the U.S., and
generally have existing international drug pricing information that is
available. We considered an alternative that would phase-in countries
over time based on a defined set of characteristics, such GDP per
capita or average drug prices. We believe that phasing in countries
over time would create instability in the MFN Price. Thus we are
adopting a set of included countries that meet the requirements in
Sec. 513.140(b), which allows for the inclusion of data from countries
that were non-U.S. OECD member countries as of October 1, 2020, when
CMS calculates the MFN Drug Payment Amounts for a calendar quarter.
That means that at the end of each applicable ASP calendar quarter, CMS
will assess the non-U.S. OECD member countries as of October 1, 2020,
that have a GDP per capita that is at least 60 percent of the U.S. GDP
per capita. Because available GDP data are updated infrequently, we
believe this approach will result in a highly stable process for
developing the MFN Prices.
We will include available international drug pricing information
from the included countries when such data are contained in the data
sources that we have described in Sec. 513.140(c), as described in
section III.E.1. of this IFC.
There are several existing sources for GDP data, including the
Central Intelligence Agency (CIA) World Factbook,\51\ the World
Bank,\52\ and the International Monetary Fund.\53\ Upon examining these
sources, we noted that the GDP data across these sources are highly
associated with one another. We will use the CIA World Factbook as our
source for GDP data as it is issued by a U.S. government agency and
includes estimates for all OECD member countries. We will use the
following process to determine the countries that were non-U.S. OECD
member countries as of October 1, 2020, with a GDP per capita that is
at least 60 percent of the U.S. GDP per capita. For each country, we
will assess the GDP per capita based on purchasing power parity that is
available in the CIA World Factbook at the end of the applicable ASP
calendar quarter. The CIA World Factbook contains the most recent
estimate of GDP per capita based on purchasing power parity for a
country as well as historical data. We will identify whether a country
has a GDP per capita that is at least 60 percent of the U.S. GDP per
capita by dividing the most recent estimate of GDP per capita based on
purchasing power parity for a country by the U.S. GDP per capita, using
data for the same year, and assessing the results. We will use the GDP
per capita from the same year as the international drug pricing
information that is used to calculate the unadjusted country-level
price, if available, or the most recent prior year.
---------------------------------------------------------------------------
\51\ https://www.cia.gov/library/publications/the-world-factbook/fields/211rank.html.
\52\ https://data.worldbank.org/indicator/ny.gdp.mktp.cd.
\53\ https://www.imf.org/external/pubs/ft/weo/2019/01/weodata/weoselgr.aspx.
---------------------------------------------------------------------------
3. Definition of the MFN Drug Payment Amount
As described later in this section, we will calculate the MFN Drug
Payment Amount for a calendar quarter for the MFN Model drug based on a
phased-in blend of the applicable ASP and the MFN Price, which we will
determine by selecting the lowest GDP-adjusted country-level price from
the included countries for the applicable ASP calendar quarter.
4. Calculation of the MFN Drug Payment Amounts
We will calculate an MFN Drug Payment Amount for each MFN Model
drug for which there is international drug pricing information from at
least one data source that meets our criteria for at least one included
country. Section III.E.6. of this IFC describes an alternative approach
for calculating the MFN Drug Payment Amount for situations where no
international drug
[[Page 76201]]
pricing information is available for an MFN Model drug, for example,
because the MFN Model drug is not approved for marketing by any
included country.
When using international drug pricing information to calculate the
MFN Drug Payment Amounts, we want to account for the relative economic
resources of non-U.S. countries to be able to fairly compare country-
level prices. We will address relative economic resources in two ways:
(1) We will only use available international drug pricing information
from non-U.S. OECD member countries with a GDP per capita that is at
least 60 percent of the U.S. GDP per capita; and (2) we will adjust the
extracted country-level prices using a GDP adjuster that adjusts for a
country's GDP per capita if it is lower than that of the U.S.
Specifically, to calculate the MFN Drug Payment Amounts for a
calendar quarter in a performance year, we will follow a multi-step
process using the corresponding quarterly ASP pricing file, as well as
the available international drug pricing information for included
countries for the applicable ASP calendar quarter, where available. The
key steps to calculate the MFN Drug Payment Amount for each MFN Model
drug will be--
Identify the available international drug pricing
information for the MFN Model drug (by applying the hierarchy of data
sources obtained by CMS and extracting the relevant data); \54\
---------------------------------------------------------------------------
\54\ Applicable subsequent steps depend upon the level of the
hierarchy for the selected data source. For example, when there are
no international sales and volume data available for the drug for an
applicable ASP calendar quarter or from any quarter beginning on or
after October 1, 2019, in accordance with level 3 of the hierarchy,
we will use the extracted data used by CMS to determine the most
recent MFN Price used to calculate an MFN Drug Payment Amount posted
on the MFN Model website, including the data used by CMS to create
the illustrative MFN Prices and MFN Drug Payment Amounts in Table 6
of this IFC. In such case, it will not be necessary to redo steps to
extract data from the data source; however, CMS will follow the
remaining steps in the MFN Drug Payment Amount calculation.
---------------------------------------------------------------------------
Remove incomplete and low sales and volume data, as
applicable;
Convert extracted volume data to the HCPCS code unit level
and adjust for volume issues such as intentional overfill, as
applicable;
Calculate \55\ the unadjusted country-level price
(representing the average price per unit of drug where the unit of drug
is the same as the HCPCS code billing unit) for the MFN Model drug for
each included country with available data in the selected data source
for that drug;
---------------------------------------------------------------------------
\55\ The calculation used depends upon whether volume data is
available.
---------------------------------------------------------------------------
Calculate the GDP adjuster for each included country;
Apply the GDP adjuster to the unadjusted country-level
price;
Select the lowest GDP-adjusted country-level price for
each MFN Model drug, which, if available, will be the MFN Price;
Identify the applicable ASP (which we define as the
payment amount determined in accordance with 1847A of the Act, less the
applicable add-on percentage, for the MFN Model drug's HCPCS code);
\56\
---------------------------------------------------------------------------
\56\ In general, the ASP Pricing File contains payment limits
based on 106 percent of the volume weighted average of
manufacturers' ASP for a given HCPCS code. To identify the
applicable ASP, we will divide the payment limit by 1.06 after
removing the blood clotting factor furnishing fee, if applicable.
For a biosimilar, we will remove the amount that represents 6
percent of the reference biological product's ASP.
---------------------------------------------------------------------------
Compare the MFN Price to the applicable ASP (to apply
limit, if applicable);
Identify the applicable phase-in formula and adjustments;
and
Apply the applicable phase-in formula and adjustments, if
applicable, to calculate the MFN Drug Payment Amount.
The following paragraphs further describe how we will calculate the
MFN Model Drug Payment Amounts for each MFN Model drug for each
calendar quarter during the model:
a. Identify the Available International Drug Pricing Information for
the MFN Model Drug
Using the data sources that we obtain and applying the hierarchy
described previously in this IFC, we will extract the available
international drug pricing information for an MFN Model drug for the
applicable time period (that is, the applicable ASP calendar quarter)
by aligning the MFN Model drug's HCPCS code long description (in terms
of name and dosage form) with the data sources' standard method for
identifying scientific names or nonproprietary names (such as the
International Nonproprietary Names). That is, for an MFN Model drug, we
will identify the data sources' standardized scientific name or
nonproprietary name for that drug, and then use that naming to identify
data for all products within that data source with an applicable
formulation. We will extract the applicable data (for example, data for
all package sizes for injectable forms of the drug aligned with the
identified scientific or nonproprietary name and formulations, for the
included countries) from the data source for the applicable ASP
calendar quarter, and in accordance with our hierarchy, select the data
source for the MFN Model drug for that quarter.
As previously discussed in this IFC, we will only use extracted
data from the selected data source that appears complete and represent
dosage formulations that could be described by the MFN Model drug's
HCPCS code descriptor, as determined by CMS. For example, J0178,
Aflibercept injection, represents injectable ophthalmic formulations
whereas a data source may contain data for aflibercept for both
ophthalmic and systemic formulations; only data for ophthalmic
formulations will be used to calculate the MFN Price for such drug. The
international drug pricing data used to calculate the MFN Price will
not be limited to distinguish between products with different inactive
ingredients (for example, different excipients) or whether or not the
product is protein bound. However, we will limit the international drug
pricing data for combination drugs that contain multiple active
ingredients or biological products to the extent feasible, as
determined by CMS. This approach is particularly relevant for four of
the MFN Model drugs for performance year 1, aflibercept injection
(J0178), which represents ophthalmic formulations compared to systemic
formulations; paclitaxel protein bound (J9264), which represents
protein bound formulations compared to formulations of paclitaxel that
are not protein bound; ferric carboxymaltos (J1439), which represents
injected formulations compared to oral formulations; and rituximab,
hyaluronidase (J9311), which represents formulations for subcutaneous
administration compared to formulations of rituximab for intravenous
administration.
In accordance with the hierarchy for selecting international drug
pricing information data sources, we will prioritize use of
international drug pricing information that includes sales and volume
data for the applicable ASP calendar quarter if such information is
available for a drug for one or more included countries. If more than
one such data source is available, we will select the data source with
international drug pricing information for the applicable ASP calendar
quarter, even if another data source includes a higher number of
included countries. For example, if the applicable ASP calendar quarter
is the third quarter of 2021 and an available data source has sales and
volume data for a drug for 20 of the included countries for the second
quarter of 2021 and for 15 included countries for the third quarter of
2021, we would extract and then calculate unadjusted country-level
prices for that drug based on sales and volume data
[[Page 76202]]
from the third quarter of 2021 only for the 15 included countries for
which data from that quarter are available.
If there are available data from a data source at the second level
of our hierarchy (that is, no international sales and volume data for
the applicable ASP calendar quarter, but sales and volume data from any
quarter beginning on or after October 1, 2019), for a drug, we will use
available international sales and volume data from that data source for
the most recent prior quarter that begins on or after October 1, 2019
for that drug for included countries.
If there are no international sales and volume data available for
the drug, we will use the extracted data used by CMS to determine the
most recent MFN Price used to calculate an MFN Drug Payment Amount
posted on the MFN Model website, in accordance with the third level of
the hierarchy.
If no MFN Drug Payment Amount has been publicly posted for the
drug, we will use a data source at the fourth level of our hierarchy if
available (the data source contains ex-manufacturer price data but does
not include volume data for the applicable ASP calendar quarter).
If ex-manufacturer price data for the applicable ASP calendar
quarter are not available, we will use a data source at the fifth level
of our hierarchy (the data source contains list price data for the
applicable ASP calendar quarter).
b. Remove Incomplete Low Sales and Volume Data, as Applicable
If the data source we select has sales and volume data at the
package level for an included country, we will apply the exclusions for
data with incomplete data and low sales and volume. That is, we will
exclude data without both sales and volume data, with less than $1,000
in quarterly sales (expressed as U.S. currency), or with less than
1,000 units in quarterly volume.
c. Convert the Extracted Volume Data to the HCPCS Code Unit Level and
Adjust for Volume Issues, Such as Intentional Overfill, as Applicable
We will adjust the remaining volume data to the same level as the
HCPCS billing unit, as applicable. For example, if the data for a
package size shows the volume is 1,000 units and each unit represents a
1 MG vial package and for another package size the volume is 500 units
and each unit represents a 10 MG vial package, and both of these data
are for a drug assigned to the same HCPCS code with a HCPCS billing
unit of 1 MG, the adjusted volume data for these packages would be
1,000 units and 5,000 units, respectively, for a total adjusted volume
of 6,000 units. The volume for the 1 MG vial package is unchanged
because the amount of drug in one package (that is, 1 MG) equals the
amount of drug in one HCPCS billing unit. The volume for the 10 MG vial
package is changed to be 10 times higher because the amount of drug in
one vial (that is, 10 MG) equals 10 times the amount of drug in one
HCPCS billing unit.
Before this step is performed, as applicable, we will adjust the
extracted volume information before converting it to the HCPCS billing
unit level when the data source shows the package size of a drug
product that is inconsistent with the manufacturer's information about
that product based on the available product information, such as
package labeling, compared to the data extracted from the data source.
In addition, we will limit the number of billing units in a package
when the available package labeling specifies use of a limited amount
of drug is to be used from the package. For example, we will limit the
number of billing units in a package for an aflibercept vial to one 2
mg dose in accordance with available package labeling, which specifies
that each vial, regardless of the labeled volume, has one 2 mg dose.
For injectable formulations for HCPCS codes with dosage specified as
per dose, we will limit the number of billing units in a package to no
more than one per vial. This approach was applied to illustrate the MFN
Prices for J7324 (Orthovisc inj per dose) in Table 6.
d. Calculate the Unadjusted Country-Level Price for the MFN Model
Drug's HCPCS Code for Each Included Country With Available Data in the
Selected Data Source for That Drug
Using the data available after completing the prior steps, we will
calculate the unadjusted country-level price for each included country
with available data. The unadjusted country-level price represents the
average price per unit of drug where the unit of drug is the same as
the HCPCS code billing unit.
We will use a calculation that is applicable to the data available
at this step. If volume data are available, we will use a calculation
that includes volume-weighting across the different data (which often
represent different package sizes) of the drug included in the data
source for the country to calculate the unadjusted country-level price.
If volume data are not available, we will use a calculation that treats
all packages of the drug included in the data source for the country
equally, after converting the pricing data to the HCPCS code unit
level, in calculating the unadjusted country-level price.
If sales and volume data are available, we will first sum the
adjusted volume data for all package sizes for the drug. We will then
sum the total sales for all package sizes for the drug, and divide that
sum by the sum the adjusted volume data for all package sizes for the
drug, resulting in an average price per unit of drug where the unit of
drug is the same as the HCPCS code billing unit. If the data source we
select has ex-manufacturer or list prices and does not have volume
data, we will calculate the number of HCPCS billing units in a package
and divide the ex-manufacturer price or list price for a package by the
number of HCPCS billing units in the package, resulting in a price per
unit of drug for each package listed in the data source. We will then
sum the price per unit of drug for each package listed in the data
source for the drug and divide the sum by the number of packages listed
in the data source for the drug, resulting in an average price per unit
of drug where the unit of drug is the same as the HCPCS code billing
unit.
We will repeat this process for each country specified in Sec.
513.140(b), to the extent international drug pricing information for
the drug for the country is available from the selected data source. As
explained previously and specified in Sec. 513.140(c)(3)(i), we will
use the highest tier data source, in accordance with the hierarchy,
which includes data for the drug in at least one included country. If
the selected data source for a drug for a calendar quarter does not
include data from a particular included country, we will still
calculate the MFN Price for that drug using the data from the selected
data source based on the included countries from which there are data
for the drug. We will not include any information from countries that
did not have data in the selected data source for that drug. In cases
where there is no data source that meets our criteria for using
international drug pricing information (that is, there are no
international sales, volume, or other pricing data available from any
of the included countries in our international drug pricing information
data sources, including data used by CMS to determine the most recent
MFN Price used to calculate an MFN Drug Payment Amount posted on the
MFN Model website, for an MFN Model drug for any quarter beginning on
or after October 1, 2019 up to and including the model performance
period, we will not calculate an unadjusted country-level price (or
GDP-adjusted country-level price) and will instead use the applicable
ASP (which we will define as
[[Page 76203]]
the payment amount determined in accordance with section 1847A of the
Act minus the applicable add-on percentage, for the MFN Model drug's
HCPCS code) as the MFN Model Drug Payment Amount, as described in
section III.E.6. of this IFC.
e. Calculate the GDP Adjuster for Each Included Country
As discussed previously, we want the MFN Price to account for the
relative economic resources and purchasing power for each included
country to be able to fairly compare country-level prices. As such, we
will calculate a GDP adjuster, using a country's GDP per capita based
on purchasing power parity, that will be used to adjust the unadjusted
country-level price for each drug (whether based on international sales
and volume data or international ex-manufacturer or list prices) to
reflect the country's economic resources relative to the U.S. We
believe that GDP per capita based on purchasing power parity represents
a broadly used and reliable measure of a country's economic resources
to ensure a meaningful comparison of country-level prices.
As previously mentioned, there are several existing sources for GDP
data, including the CIA World Factbook,\57\ the World Bank,\58\ and the
International Monetary Fund.\59\ Our analyses suggest that the GDP data
across these sources are highly associated with one another. We will
use the CIA World Factbook as our source for GDP data as it is issued
by a U.S. government agency and includes estimates for all current OECD
member countries. The GDP adjuster will be based on the GDP per capita
available from the CIA World Factbook at the end of the applicable ASP
calendar quarter. We will use the most recent GDP per capita data
available for each included country and the U.S. GDP per capita from
the same year as the GDP per capita data that is available from the
included country. For example, if the most recent GDP per capita from
the comparison OECD country is from 2016 and the most recent U.S. GDP
per capita is 2017, then we will use the GDP per capita from 2016 for
both countries when comparing. In cases where we use international drug
pricing information from a quarter other than the applicable ASP
calendar quarter (that is, an earlier time period) to determine the
unadjusted country-level price, we will use the GDP per capita data for
that time period, if available, or the most recent earlier data
available. That is, CMS will use the GDP per capita for the same year
as the data used to calculate the unadjusted country-level price, if
available, or the most recent earlier year available.
---------------------------------------------------------------------------
\57\ https://www.cia.gov/library/publications/the-world-factbook/fields/211rank.html.
\58\ https://data.worldbank.org/indicator/ny.gdp.mktp.cd.
\59\ https://www.imf.org/external/pubs/ft/weo/2019/01/weodata/weoselgr.aspx.
---------------------------------------------------------------------------
To create a simple, easily understandable GDP adjuster, each
country's GDP adjuster will be a straight ratio of its GDP per capita
based on purchasing power parity divided by U.S. GDP per capita,
subject to the limitation described later in this section. The U.S. GDP
per capita for 2017, the most current data available, was $59,800.
Table 4 presents GDP per capita for 2017 and the GDP adjusters for each
non-U.S. OECD member country, based on the U.S. GDP per capita of
$59,800 for 2017, that we will use to calculate the MFN Drug Payment
Amounts for performance year 1, quarter 1. In cases when an included
country's GDP per capita and the U.S. GDP per capita are not updated in
the CIA World Factbook at the same time, we will use the most recent
GDP per capita for the included country and the U.S. GDP per capita
from the same year to ensure that the GDP adjuster for an included
country is calculated using GDP data from both countries from the same
time period. For example, if at the end of an applicable calendar
quarter a 2018 estimate of a country's GDP per capita based on
purchasing power parity becomes available in the CIA World Factbook but
the most recent U.S. GDP per capita available in the CIA World Factbook
continues to be for 2017, we will continue to use data from 2017 for
both countries to calculate the GDP adjuster for that country.
The GDP adjuster will be capped at 1 such that the adjuster will
only increase the unadjusted country-level price for a drug; it will
not decrease it. We will cap the GDP adjuster at 1 because its purpose
is to adjust for countries' economic resources when lower than those of
the U.S. Capping the GDP adjuster at 1 will ensure that we do not make
an adjustment that would result in an amount that would be lower than
the unadjusted country-level price. For example, if Country X with a
higher GDP per capita based on purchasing power parity than the U.S.,
such as a GDP per capita ratio of 2, has an unadjusted country-level
price of $100 for an MFN Model drug, we would use a GDP adjuster of 1.0
and calculate a GDP-adjusted country-level price of $100 rather than
using a GDP adjuster of 2.0 and calculating a GDP-adjusted country-
level price of $50.
Table 4--Non-U.S. OECD Member Country GDP per Capita (Based on
Purchasing Power Parity) and GDP Adjusters for Performance Year 1,
Quarter 1
------------------------------------------------------------------------
CIA GDP per
capita, based GDP adjuster for
OECD countries on purchasing performance year
power parity 1, quarter 1
(2017)
------------------------------------------------------------------------
The following countries have a GDP
per capita of at least 60 percent
of U.S. GDP per capita:[dagger]
------------------------------------------------------------------------
Australia....................... $50,400 0.843
Austria *....................... 50,000 0.836
Belgium *....................... 46,600 0.779
Canada *........................ 48,400 0.809
Denmark *....................... 50,100 0.838
Finland *....................... 44,500 0.744
France *........................ 44,100 0.737
Germany *....................... 50,800 0.849
Iceland......................... 52,200 0.873
Ireland *....................... 73,200 ** 1.000
Israel.......................... 36,400 0.609
[[Page 76204]]
Italy *......................... 38,200 0.639
Japan *......................... 42,900 0.717
Republic of Korea............... 39,500 0.661
Luxembourg...................... 105,100 ** 1.000
Netherlands *................... 53,900 0.901
New Zealand..................... 39,000 0.652
Norway.......................... 72,100 ** 1.000
Spain........................... 38,400 0.642
Sweden.......................... 51,200 0.856
Switzerland..................... 62,100 ** 1.000
United Kingdom *................ 44,300 0.741
------------------------------------------------------------------------
The following countries have a GDP per capita below 60 percent of U.S.
GDP per capita:
------------------------------------------------------------------------
Chile........................... 24,600 0.411
Colombia........................ 14,400 0.241
Czechia *....................... 35,500 0.594
Estonia......................... 31,700 0.530
Greece *........................ 27,800 0.465
Hungary......................... 29,600 0.495
Latvia.......................... 27,700 0.463
Lithuania....................... 32,400 0.542
Mexico.......................... 19,900 0.333
Poland.......................... 29,600 0.495
Portugal........................ 30,500 0.510
Slovakia........................ 33,100 0.554
Slovenia........................ 34,500 0.577
Turkey.......................... 27,000 0.452
------------------------------------------------------------------------
* Indicates countries that were listed as potential included countries
in the October 2018 ANPRM (83 FR 54557).
** Indicates that the GDP adjuster is capped at 1.000.
[dagger] The 2017 U.S. GDP per capita is $59,800.
f. Apply the Applicable GDP Adjuster To Calculate the GDP-Adjusted
Country-Level Price for the MFN Model Drug
Next, we will apply the country-specific GDP adjuster to the
unadjusted country-level price for that country by dividing the
unadjusted country-level price by the country's GDP adjuster. The
result will be the GDP-adjusted country-level price for the MFN Model
drug for that country. We will repeat this calculation to produce a
GDP-Adjusted Price for every country for which we have calculated an
unadjusted country-level price for the MFN Model drug.
g. Identify the Lowest GDP-Adjusted Country-Level Price for the MFN
Model Drug
We will examine the GDP-adjusted country-level prices for the MFN
Model drug, and identify the lowest GDP-adjusted country-level price
for the MFN Model drug. The lowest GDP-adjusted country-level price
will be the MFN Price for the MFN Model drug.
h. Compare the MFN Price to the Applicable ASP
As a safeguard for beneficiaries, we will compare the MFN Price to
the applicable ASP in order to ensure that beneficiaries are always
paying the lowest amount of coinsurance available. If the applicable
ASP is less than the MFN Price, we will establish the MFN Price as
equal to the applicable ASP.
i. Identify the Applicable Phase-In Formula and Adjustments
As described in section III.E.5. of this IFC, we will phase-in the
use of the MFN Price over the course of the MFN Model. As discussed in
section III.E.9. of this IFC, we will also accelerate the applicable
phase-in formula when the applicable ASP for an MFN Model drug rises
faster than both a designated inflation factor and the change in MFN
Price, and lower the MFN Drug Payment Amount below the MFN Price by a
certain percentage if the applicable ASP for an MFN Model drug
continues to increase faster than the inflation factor and the MFN
Price after the full phase-in of the MFN Price. In this step of the
process to calculate the MFN Drug Payment Amount, we will determine the
applicable phase-in formula and whether any of these adjustments will
apply.
j. Calculate the MFN Drug Payment Amount
As the last step, we will calculate the MFN Drug Payment Amount for
the MFN Model drug using the applicable phase-in formula, which blends
the applicable ASP and the MFN Price as described in section III.E.5.
of this IFC. This calculation, including any adjustments that apply,
will result in the MFN Drug Payment Amount for the MFN Model drug
(except as otherwise specified).
5. Phase-In of the MFN Price
We will use a phase-in approach that will blend the MFN Price with
the applicable ASP to allow MFN participants time to adjust to the
model payment amounts and processes. The phase-in formula will be
stable for a given performance year, whereas the MFN Price and
applicable ASP will vary quarterly based on fluctuations in drug
[[Page 76205]]
prices in the U.S. and in included countries. We will phase-in the MFN
Price by 25 percent per year for performance years 1 to 3 of the model,
reaching 100 percent of the MFN Price for performance years 4 through 7
of the model. The phase-in formula uses a blend of the applicable ASP
and MFN Price for an MFN Model drug as shown in Table 5. The MFN Drug
Payment Amount will be based on 100 percent of the MFN Price starting
in performance year 4, unless an adjustment that accelerates the phase-
in applies as described in section III.E.9. of this IFC. Thus, the
phase-in represents the outer bound in terms of the amount of time it
will take for the MFN Drug Payment Amount to transition to 100 percent
of the MFN Price.
We believe that a phase-in approach during the initial years of the
model will enable MFN participants and the markets to adjust to the
model's payment methodology, while enabling CMS to test the full phase-
in of the MFN Price over a 7-year model performance period. As noted in
section III.E.11. of this IFC, when MFN Model drugs get added to the
MFN Model Drug HCPCS Codes List during the model performance period,
their MFN Drug Payment Amount gets determined as set forth for the
corresponding performance year, meaning that if an MFN Model drug were
to be added during performance year 4, the MFN Drug Payment Amount will
equal 100 percent of the MFN Price.
Table 5--Phase-In of MFN Prices by Performance Year
------------------------------------------------------------------------
Blend of the ASP and MFN price for an MFN
Performance year model drug at the HCPCS code level
------------------------------------------------------------------------
Year 1....................... 75 percent applicable ASP and 25 percent
MFN Price.
Year 2....................... 50 percent applicable ASP and 50 percent
MFN Price.
Year 3....................... 25 percent applicable ASP and 75 percent
MFN Price.
Year 4....................... 100 percent MFN Price.
Year 5....................... 100 percent MFN Price.
Year 6....................... 100 percent MFN Price.
Year 7....................... 100 percent MFN Price.
------------------------------------------------------------------------
We are codifying the phase-in formula in Sec. 513.210(b)(8).
6. Alternative Calculation for the MFN Drug Payment Amount
Over the course of the MFN Model, we may determine that the
international drug pricing information data sources that we obtain do
not contain any international drug pricing information (meaning no
sales, volume, ex-manufacturer price, or list price data from any
included country from any quarter beginning in the fourth calendar
quarter of 2018 through the applicable quarter in the model performance
period) for an MFN Model drug, for example, because the MFN Model drug
is not approved for marketing in the included countries. For such
cases, we will establish the MFN Drug Payment Amount at the applicable
ASP for the applicable calendar quarter, subject to any adjustment in
Sec. 513.210(d) that applies, until international drug pricing
information is available.
Because international drug pricing information may become available
for a subsequent calendar quarter, we will use this method to establish
the MFN Drug Payment Amount instead of excluding or removing drugs
without any international drug pricing information from the model until
international drug pricing information becomes available. We believe
having a stable list of MFN Model drugs will be more predictable for
MFN participants, lessening MFN participants' need to monitor changes
to the MFN Model Drug HCPCS Codes List, and will avoid creating an
opportunity for manufacturers to get their products out of the model by
stopping the reporting of international drug pricing information. Based
on our experience with international drug pricing information data
sources, we expect the potential of no international drug pricing
information for an MFN Model drug across all included countries will be
limited. We note that our approach may increase model payments compared
to non-model payments for MFN Model drugs with no international drug
pricing information because the alternative add-on payment, a single
flat add-on amount per dose (see section III.F. of this IFC), could be
greater than the add-on payment outside of the model.
7. Illustrative MFN Drug Payment Amounts
To illustrate how CMS will calculate the MFN Drug Payment Amounts
under the MFN Model in accordance with Sec. Sec. 513.130 and 513.140,
we applied the methodology for determining the applicable ASPs, MFN
Prices, and MFN Drug Payment Amounts using historical ASP-based payment
limits,\60\ available international drug pricing information from 2019
for the included countries, and the MFN Model performance year 1 phase-
in formula. Table 6 shows illustrative data for applicable ASPs, MFN
Prices, and MFN Drug Payment Amounts for one billing unit for the HCPCS
codes that are included on the performance year 1 MFN Model Drug HCPCS
Codes List in Table 2. Actual MFN Drug Payment Amounts per billing unit
for performance year 1, quarter 1, and thereafter will be calculated as
specified in Sec. 513.210. We will publish the quarterly MFN Drug
Payment Amounts on a CMS website (such as the MFN Model website),
similar to how the ASP Drug Pricing Files are posted online prior to
the start of the calendar quarter. The performance year 1, quarter 1
MFN Drug Payment Amounts will be published on a CMS website before the
start of the MFN Model.
---------------------------------------------------------------------------
\60\ We used the 2019 Quarter 3 and Quarter 4 and 2020 Quarter 1
and Quarter 2 ASP data that align with manufacturer-reported data
based on sales during 2019 to identify the applicable ASPs. The ASP
pricing files are posted at links available here: https://www.cms.gov/Medicare/Medicare-Fee-for-Service-Part-B-Drugs/McrPartBDrugAvgSalesPrice/.
---------------------------------------------------------------------------
Illustrative MFN Drug Payment Amounts per billing unit are listed
in Table 6 by HCPCS code. For this illustration, we partnered with
ASPE, which purchases licenses to data products maintained by IQVIA\TM\
(formerly known as Quintiles-IMS). IQVIA's proprietary MIDAS data set
\61\ is a widely used source of drug sales and volume data.
---------------------------------------------------------------------------
\61\ https://www.iqvia.com/solutions/commercialization/brand-strategy-and-management/market-measurement/Midas.
---------------------------------------------------------------------------
[[Page 76206]]
MIDAS data contain estimates of drug sales (called ``Monetary Value ''
within the MIDAS data set) and volume (called ``Quantity'' within the
MIDAS data set) that are based on audits of drug transactions in
different countries and distribution channels (for example, retail
pharmacies and hospitals). The audits underlying the MIDAS data collect
sales and volume information at the ex-manufacturer (that is, prices as
drugs are sold by manufacturers), ex-wholesaler, and/or retail levels.
IQVIA applies a set of country- and channel-specific assumptions on
markups between manufacturer, wholesale, and retail prices to estimate
ex-manufacturer and retail sales. Sales information within the database
is stated in local and U.S. currency, as of the transaction date or
current date, and are expressed as ex-manufacturer, trade, and public
(retail) sales.\62\ MIDAS uses a variable called ``Molecule List''
(also called ``Moleculelist'') which identifies scientific and
nonproprietary names for drug and biological products. Users extract
data from the MIDAS database by selecting report filters, which are
values for various data fields included in the database, such as
``Molecule List'' and ``NFC123'' (or ``New Form Code,'' a 3-digit code
which identifies the dosage form \63\). The database has a standard
method for identifying drugs within the U.S. and across countries, and
a standard method for identifying drug forms. MIDAS data is updated
monthly and retains up to 12 years of history.
---------------------------------------------------------------------------
\62\ Ex-manufacturer sales are: Manufacturer Selling Price or
Wholesaler Purchasing Price or Price to Wholesaler (PTW). Trade
sales are: Wholesaler Selling Price or Pharmacy Purchase Price or
Price to Chemist (PTC). Public (retail) sales are: Pharmacy Selling
Price or Consumer Purchase Price or Price to the Public (PTP).
\63\ For more information on the New Form Codes see: https://www.ephmra.org/classification/new-form-codes/.
---------------------------------------------------------------------------
CMS obtained a MIDAS data extract of available 2019 international
drug pricing information for the included countries for the MFN Model
drugs for performance year 1 from ASPE. After identifying the MFN Price
for each drug, we applied the phase-in formula for performance year 1
(75 percent of the applicable ASP and 25 percent of the MFN Price) and
applied the exceptions in Sec. 513.210(d) when no international drug
pricing information was available in the MIDAS data. In Table 6, the
illustrative MFN Prices, calculated using available international drug
pricing sales and volume information at the ex-manufacturer level,
represent the lowest of the GDP-adjusted country-level prices available
in the single data source we used. For a complete discussion of how CMS
used international drug pricing information available through IQVIA and
CMS data to calculate the illustrative applicable ASPs, MFN Prices, and
MFN Drug Payment Amounts displayed in Table 6, we refer readers to the
supplemental documentation available on the MFN Model website.\64\ We
also refer readers to the Medicare Part B Drug Spending Dash board \65\
that can be used to search for brand name or generic name; search
results present certain manufacturer information when available.
---------------------------------------------------------------------------
\64\ See: https://innovation.cms.gov/initiatives/most-favored-nation-model/.
\65\ See: https://www.cms.gov/Research-Statistics-Data-and-Systems/Statistics-Trends-and-Reports/Information-on-Prescription-Drugs/MedicarePartB.
---------------------------------------------------------------------------
BILLING CODE 4120-01-P
[[Page 76207]]
[GRAPHIC] [TIFF OMITTED] TR27NO20.003
[[Page 76208]]
[GRAPHIC] [TIFF OMITTED] TR27NO20.004
[[Page 76209]]
[GRAPHIC] [TIFF OMITTED] TR27NO20.005
[[Page 76210]]
[GRAPHIC] [TIFF OMITTED] TR27NO20.006
[[Page 76211]]
[GRAPHIC] [TIFF OMITTED] TR27NO20.007
[[Page 76212]]
[GRAPHIC] [TIFF OMITTED] TR27NO20.008
BILLING CODE 4120-01-C
[[Page 76213]]
We note that, as codified in Sec. 513.210(d)(5), and described in
section III.E.10. of this IFC, the MFN Drug Payment Amount will not
exceed the non-model drug payment amount for line items submitted with
the JG modifier (or any successor modifier used to identify drugs
purchased under the 340B program) after removing any add-on amount, if
applicable.
8. Timing of Data and MFN Drug Payment Amount Calculations
As discussed in section III.E.4. of this IFC, we will calculate the
MFN Drug Payment Amounts on a calendar quarter basis using the most
recent ASP and correlated international drug pricing information (that
is, data from the highest level of hierarchy available). Under the
reporting requirements outlined in section 1927(b)(3)(A)(iii),
manufacturers that report ASPs are required to submit them to CMS no
later than 30 days after the last day of the previous quarter. CMS uses
these data to calculate the ASP-based Medicare payment amounts for the
next calendar quarter. As a result, there is a two-quarter lag between
the time when sales reflected in the ASP occur and the time when these
sales become the basis for Medicare payment amounts.
We will use international drug pricing information from the same
time period (that is, the same calendar quarter), if available in
accordance with the hierarchy specified in Sec. 513.140(c)(3), in
order to align information across the ASP Drug Pricing files and the
data sources for international drug pricing information that we will
use. This approach will consistently correspond to the two-quarter lag
used for the ASP pricing files when an international drug pricing
information data source at the highest level of the hierarchy specified
in Sec. 513.140(c)(3) is available. Table 7 illustrates how the
information we will use to calculate the MFN Drug Payment Amounts for
each calendar quarter during performance year 1 using data from the
applicable ASP calendar quarter will align when an international drug
pricing information data source at the highest level of the hierarchy
specified in Sec. 513.140(c)(3) is available. We will use the same
approach for each performance year.
Table 7--Alignment of Performance Year Calendar Quarters for ASP and MFN Price Data Based on January 2021 Model
Start
----------------------------------------------------------------------------------------------------------------
ASP pricing file
Performance year Performance year for calendar Applicable ASP MFN price for
calendar quarter quarter calendar quarter calendar quarter*
----------------------------------------------------------------------------------------------------------------
1............................. 2021, Quarter 1.... 2021, Quarter 1.... 2020, Quarter 3... 2020, Quarter 3
1............................. 2021, Quarter 2.... 2021, Quarter 2.... 2020, Quarter 4... 2020, Quarter 4
1............................. 2021, Quarter 3.... 2021, Quarter 3.... 2021, Quarter 1... 2021, Quarter 1
1............................. 2021, Quarter 4.... 2021, Quarter 4.... 2021, Quarter 2... 2021, Quarter 2
----------------------------------------------------------------------------------------------------------------
*When an international drug pricing information data source at the highest level of the hierarchy specified in
Sec. 513.140(c)(3) is available.
For example, for the initial calculations to calculate payment
amounts for the start of the MFN Model on January 1, 2021, the
beginning of the first calendar quarter in 2021, we will use the
January 2021 ASP Pricing File (which will be based on manufacturers'
ASP for the third quarter of 2020, from July 1, 2020, to September 30,
2020) and international drug pricing information for the third quarter
of 2020, from July 1, 2020, to September 30, 2020. For each subsequent
calendar quarter for a performance year, the MFN Drug Payment Amount
will be established by calculating the MFN Price based on more recent
international drug pricing information, using data for the applicable
ASP calendar quarter, if available, as illustrated in Table 7, and
calculating the MFN Drug Payment Amount.
9. Adjustments to Phase-In Formula and Incentives for Manufacturers To
Address Rising U.S. Drug Prices
In response to the October 2018 ANPRM, we received several comments
asking that we consider including model design features to address
potential spillover effects and cost-shifting to the commercial market
and Medicare payment outside of the model geographic area. The
commenters requested that CMS carefully consider the potential impacts
of a potential model on other markets--including the potential for
cost-shifting to other segments of the Medicare program, the Medicaid
program, and the commercial market. The commenters recommended that in
order to avoid unintended consequences and cost-shifting, CMS should
closely monitor prices for included drugs and consider additional
policies or actions if drug prices in other markets rise above certain
pricing thresholds (for example, above the Consumer Price Index (CPI)
or inflation).
We appreciate these concerns, as it is possible that, in response
to the MFN Model, manufacturers may take steps to increase U.S. prices
outside of the MFN Model, such as in the commercial and Medicare
Advantage markets, which may be seen in increases in manufacturers'
ASPs. In response to the concerns expressed in the October 2018 ANPRM
comments and to minimize the possibility of a spillover impact on
beneficiaries outside of the MFN Model, we will make adjustments to the
phase-in formula in order to mitigate cost-shifting in the market and
incentivize manufacturers of MFN Model drugs to maintain stable ASPs of
MFN Model drugs to minimize the potential for spillover impacts. In
addition to creating spillover impacts, rapid increases in ASP that
outstrip not only U.S. inflation but also changes in international
prices over time would reduce our ability to test the phase-in of the
MFN Price over time, as the MFN Price's contribution to the MFN Drug
Payment Amount could be obscured by a significant increase in the MFN
Model drug's ASP.
As discussed in section III.E.5. of this IFC, we will phase-in the
MFN Prices to allow MFN participants time to adjust to the MFN Model
payment amounts and processes. Calculating the MFN Prices and MFN Drug
Payment Amounts each calendar quarter will allow manufacturers to
address the large difference between prices in the U.S. and in other
countries for MFN Model drugs during the course of the MFN Model and
serves as an incentive for manufacturers to refrain from raising U.S.
prices faster than a reasonable inflation allowance. Furthermore, as
discussed in section III.M. of this IFC, we are waiving requirements of
section 1847A in order to exclude units of MFN Model drugs from the
calculation of the manufacturer's ASP. However, if these incentives
prove to be insufficient to deter manufacturers from raising U.S.
prices for MFN Model drugs faster than a reasonable inflation
allowance, we will adjust the calculation of the MFN Drug Payment
Amount by adjusting the
[[Page 76214]]
phase-in formula for MFN Model drugs where such concerns are observed.
Specifically, to preserve the integrity of the model test as
described previously, we will make an adjustment to the phase-in
formula for an MFN Model drug if the applicable ASP or monthly U.S.
list price (defined as Wholesale Acquisition Cost (WAC) available in a
U.S. drug pricing compendium or if WAC is not available, other
available list prices, such as Average Wholesale Price (AWP) available
in a U.S. drug pricing compendium) increases faster than both inflation
and the MFN Price. CMS will accelerate the phase-in of the MFN Price by
5 percentage points at the next quarterly update for each MFN Model
drug with: (1) A greater cumulative percentage increase in either the
applicable ASP \66\ or any monthly U.S. list price for any of the NDCs
assigned to the MFN Model drug's HCPCS code compared to the cumulative
percentage increase in the Consumer Price Index for All Urban Consumers
(CPI-U) \67\ based on all items in U.S. city average and not seasonally
adjusted; and (2) a greater cumulative percentage increase in either
the applicable ASP or any monthly U.S. list price for any of the NDCs
assigned to the MFN Drug's HCPCS code compared to the cumulative
percentage increase in the MFN Price. To apply these conditions for an
MFN Model drug, we will identify the cumulative percentage increase
from a baseline to the applicable ASP calendar quarter. For all MFN
Model drugs with an applicable ASP for the first quarter of performance
year 1, we will set the baseline as the ASP calendar quarter for the
applicable ASP for the first quarter of performance year 1 (that is,
the third calendar quarter of 2020 (July 2020 through September 2020)).
For all MFN Model drugs that do not have an applicable ASP for the
first quarter of performance year 1 (for example, a drug that is first
marketed in the U.S. after the start of the model), the baseline will
be the ASP calendar quarter for the first applicable ASP based on the
manufacturer's average sales price for that MFN Model drug that occurs
after the third quarter of 2020. For example, the baseline for an MFN
Model drug with its first applicable ASP based on the manufacturer's
average sales price occurring in the second quarter of performance year
1 (that is, April 2021 through June 2021) will have a baseline of the
fourth calendar quarter of 2020 (October 2020 through December 2020).
---------------------------------------------------------------------------
\66\ We note that the manufacturers' ASPs will be based on non-
model sales only as codified in Sec. 513.600(b) and as discussed in
section III.M. of this IFC.
\67\ All references to CPI-U are based on all items in U.S. city
average and not seasonally adjusted.
---------------------------------------------------------------------------
The cumulative percentage change will be calculated from the end of
the baseline to the end of the applicable ASP calendar quarter. We will
apply the adjustment to the phase-in formula similarly for all MFN
Model drugs regardless of when the MFN Model drug is added to the MFN
Model Drug HCPCS Codes List.
Further, if both conditions are not met, such as the cumulative
percentage increase in any monthly U.S. list prices for the NDCs
assigned to the MFN Drug's HCPCS code outpaces the cumulative
percentage increase in CPI-U but is less than the cumulative percentage
increase in the MFN Price, then the trigger conditions will not be met
and the phase-in formula will not be accelerated. If the cumulative
percentage change in the CPI-U or MFN Price is negative, we will use
zero as the cumulative percentage increase in the CPI-U or MFN Price,
as applicable, for the relevant quarter.
We will accelerate the phase-in formula by 5 percentage points as
we believe this amount strikes a balance between moving the MFN Drug
Payment Amount more quickly toward the MFN Price while still retaining
the stepwise nature of the phase-in. As an example, in the case that
both trigger conditions are met for an MFN Model drug during the
applicable ASP calendar quarter for the second quarter of performance
year 1, the phase-in formula would be 70 percent applicable ASP and 30
percent MFN Price for that quarter and remaining quarters in
performance year 1, assuming both trigger conditions are not met in the
ASP calendar quarters for the third and fourth quarter of performance
year 1.
We will apply the acceleration of the phase-in formula for each
calendar quarter of the MFN Model where both trigger conditions are
met. That is, for an MFN Model drug that is subject to the accelerated
phase-in of the MFN Price, we will further accelerate the phase-in of
the MFN Price by an additional 5 percentage points at the next
quarterly update if the cumulative percentage increase in the
applicable ASP or any of the monthly U.S. list prices for the NDCs
assigned to the MFN Model drug's HCPCS code continues to be greater
than the cumulative percentage increase in the CPI-U and MFN Price. In
the previous example, if both of the trigger conditions were met for
the same MFN Model drug during the applicable ASP calendar quarter for
quarters 3 and 4 of performance year 1, the phase-in formula would be
65 percent applicable ASP and 35 percent MFN Price for quarter 3 of
performance year 1, and 60 percent applicable ASP and 40 percent MFN
Price for quarter 4 of performance year 1. The accelerated phase-in of
the MFN Price will not be reversed, but will remain in place for the
duration of the model performance period for that drug, even if the
manufacturer lowers its ASP and U.S. list prices after the accelerated
phase-in is in effect.
Further, after the full phase-in of the MFN Price is reached, if
both of the trigger conditions are met, there will be a decrease in MFN
Model Drug Payment Amount equal to the largest difference in the
cumulative percentage increase in the applicable ASP or any of the
monthly U.S. list prices for the NDCs assigned to the MFN Model drug's
HCPCS code compared to the cumulative percentage increase in the CPI-U
and in the MFN Price. This additional adjustment will lead to the
affected drug's MFN Drug Payment Amount falling below the MFN Price for
that drug. For example, for an MFN Model drug, if 100 percent of the
MFN Price was already applied in the calculation of the MFN Model Drug
Payment Amount for a quarter and its applicable ASP cumulatively
increased by 14 percent, the largest cumulative percentage increase of
any of the monthly U.S. list prices for the NDCs assigned to the HCPCS
code was 13 percent, the CPI-U cumulatively increased by 12 percent,
and the MFN Price cumulatively increased by 11 percent, we would reduce
the MFN Drug Payment Amount for the quarter (in this case, previously
established as to equal the MFN Price) by 3 percent (that is, the
difference between 14 and 11) of the MFN Price.
Any such additional adjustment will apply for the duration of the
model performance period, unless a larger additional adjustment is
triggered. As with the adjustment before the full phase-in is reached,
we will update the calculation for the additional adjustment for each
additional calendar quarter of the model. That is, for an MFN Model
drug that is subject to the additional adjustment of the MFN Price,
each calendar quarter thereafter, we will calculate the largest
difference between the cumulative percentage increase in the applicable
ASP or any of the monthly U.S. list prices for the NDCs assigned to the
MFN Model drug's HCPCS code and the cumulative percentage increase in
CPI-U and in MFN Price and increase the additional adjustment if the
result of the updated calculation results in a larger additional
adjustment. CMS will not reduce the
[[Page 76215]]
additional adjustment based on the results of the updated calculation.
We believe this policy will serve as a strong incentive for
manufacturers to avoid taking steps that could cause spillover impacts
and will help to address commenters' concerns.
10. Limitation on MFN Drug Payment Amount To Protect Beneficiaries
To avoid potentially increasing beneficiary cost-sharing or
coinsurance, we are codifying in Sec. 513.210(b)(6) to compare the MFN
Price to the applicable ASP in order to ensure that beneficiaries are
always paying the lowest amount of coinsurance available. If the
applicable ASP is less than the MFN Price, we will establish the MFN
Price as equal to the applicable ASP. In addition, in Sec. 513.210(a),
we are codifying that the allowed MFN Drug Payment Amount will not
exceed the billed amount on the claim for the MFN Model drug. In
addition, to maintain beneficiary protections for all claims paid under
the OPPS, we are codifying in Sec. 513.210(d)(4) that the MFN Drug
Payment Amount cannot exceed the non-model drug payment amount for line
items submitted with the JG modifier (or any successor modifier used to
identify drugs purchased under the 340B program) after removing any
add-on amount, if applicable. We will apply this limitation to line
items submitted with the JG modifier. We refer readers to the Calendar
Year (CY) 2021 OPPS/ASC Notice of Proposed Rulemaking (CMS-1736-P) \68\
(85 FR 48880) for a discussion of CMS's proposal for CY 2021 and
subsequent years to pay for drugs acquired under the 340B program at
ASP minus 34.7 percent, plus an add-on of 6 percent of the product's
ASP, for a net payment rate of ASP minus 28.7 percent based on the
results of the Hospital Acquisition Cost Survey for 340B--Acquired
Specified Covered Drugs. If CMS finalizes the proposed OPPS payment
policy to pay for drugs acquired under the 340B program at ASP minus
34.7 percent, plus an add-on of 6 percent of the product's ASP, the MFN
Drug Payment Amount for an MFN Model drug furnished by an MFN
participant and billed with the JG modifier will be capped at ASP minus
34.7 percent. In such cases, the MFN participant will also receive the
per-dose add-on payment amount described in section III.F. of this IFC.
---------------------------------------------------------------------------
\68\ https://www.govinfo.gov/content/pkg/FR-2020-08-12/pdf/2020-17086.pdf.
---------------------------------------------------------------------------
In the CY 2021 OPPS/ASC Notice of Proposed Rulemaking, CMS proposed
in the alternative to continue its current policy of paying ASP minus
22.5 percent for 340B-acquired drugs. If CMS finalizes this alternative
proposal, the MFN Drug Payment Amount for an MFN Model drug furnished
by an MFN participant and billed with the JG modifier will be capped at
ASP minus 22.5 percent (85 FR 48890). In such cases, the MFN
participant will also receive the per-dose add-on payment amount
described in section III.F. of this IFC.
11. Method for Establishing MFN Drug Payment Amounts for Drugs Added to
the MFN Model
We will add annually any top 50 drugs that are not already included
on the MFN Model Drug HCPCS Codes List, after taking the exclusions in
Sec. 513.130(b) into account. In accordance withSec. 513.210, we will
calculate the MFN Price that will apply to drugs that are added to the
list of MFN Model drugs and the applicable phase-in formula for a given
performance year and adjustments will apply. We will apply the
applicable phase-in formula for drugs that are added to the MFN Model
Drug HCPCS Codes List, in order to simplify and maintain consistent
payment policies for all MFN participants and MFN Model drugs. For
example, for a drug added as an MFN Model drug for performance year 2,
the phase-in formula will be a blend of 50 percent of the ASP and 50
percent of the MFN Price for the drug. Thus, Medicare Part B drugs that
will be added to the MFN Model Drug HCPCS Codes List for performance
year 2 and beyond will have an MFN Drug Payment Amount that will start
more heavily based on the MFN Price than drugs that were included in
earlier performance years. We believe this approach is appropriate
because the MFN Model seeks to test a new payment methodology that
takes into account the discounts that other countries enjoy and
delaying the phase-in of the MFN Price for drugs that will be added to
the MFN Model Drug HCPCS Codes List for performance year 2 and beyond
will not allow CMS to fully evaluate the model payment test for such
drugs during the model performance period.
For drugs added to the MFN Model Drug HCPCS Codes List in a later
performance year, this approach could result in a more significant
change in payment for the drug upon entry to the model compared to
drugs that are included from the beginning of the model. Although there
is the potential for a larger change in payment for drugs that are
added later in the model, we believe that it is necessary to maintain
the same phase-in for all included drugs to enable us to test the full
phase-in of the MFN Price by performance year 4. We also believe that
MFN participants are aware of which separately payable Medicare Part B
drugs have high annual spending and therefore will have a basis for
assessing which drugs that are not on the MFN Model Drug HCPCS Codes
List in performance year 1 are more likely be added to the MFN Model
Drug HCPCS Codes List in a later performance year. For future years, we
seek comment on whether additional information that CMS could provide
would be helpful to MFN participants for their planning purposes, for
example drug utilization reports developed through the model monitoring
activities that CMS could make available on the model website.
12. Payment Exceptions for MFN Model Drugs in Short Supply
Rather than broadly excluding drugs that are in short supply from
the model, we will keep MFN Model drugs in the model while they are in
short supply, but revert the MFN Drug Payment Amount to the applicable
ASP, which could be the amount determined under section 1847A(e) of the
Act if the conditions set forth in that provision are met, beginning
with the first day of the next calendar quarter after the date on which
the MFN Model drug is reported as ``Currently in Shortage'' by FDA, as
available on these websites: https://www.accessdata.fda.gov/scripts/drugshortages/ and https://www.fda.gov/vaccines-blood-biologics/safety-availability-biologics/cber-regulated-products-current-shortages, and
continuing for subsequent calendar quarters as warranted. Once the MFN
Model drug is no longer reported as ``Currently in Shortage'' by FDA,
the MFN Model payment will resume the first day of the next quarter
after the date on which it is no longer reported in shortage. For
example, as noted in section III.D.2. of this IFC, one of the HCPCS
codes with high aggregate 2019 Medicare Part B total allowed charges
(J1569, Gammagard liquid infusion) represents a drug that is currently
on the FDA shortages list. If this HCPCS code were to be included on
the MFN Model Drug HCPCS Codes List and remain on the FDA shortages
list, the MFN Drug Payment Amount will be the applicable ASP until the
first day of the next quarter of the model performance period after it
is no longer reported as ``Currently in Shortage'' by FDA. However, we
note that we are excluding HCPCS codes that describe intravenous immune
globulin from the MFN Model Drug HCPCS Codes List as discussed in
section III.D.2 of this IFC.
[[Page 76216]]
13. Payment of Blood Clotting Factor Furnishing Fee Under the MFN Model
Currently, payment for the blood clotting factor furnishing fee
under 42 CFR 410.63(c) is made along with payment for the blood
clotting factor. Under the MFN Model, a HCPCS code that is used to bill
for a blood clotting factor may be an MFN Model drug if such HCPCS code
is included on the MFN Model Drug HCPCS Codes List. To maintain the
current payment approach for the blood clotting factor furnishing fee
during the MFN Model, we are codifying in Sec. 513.210(e), that when
applicable, the blood clotting furnishing fee under Sec. 410.63(c)
will be payable along with the MFN Drug Payment Amount. We believe this
approach will eliminate the need to establish different billing
instructions for MFN Model drugs that are blood clotting factors.
F. MFN Model Alternative Add-On Payment
1. Overview of the Alternative Add-On Payment
In the October 2018 ANPRM, we sought public comment on testing an
alternative add-on payment to the current system, required by section
1847A of the Act, under which Medicare Part B pays a fee based on 6
percent of the ASP of the drug so that the dollar amount of the add-on
increases with the price of the drug rather than reflecting the service
being performed. In general, the amount of add-on realized by providers
and suppliers has been described by commenters as 4.3 percent as a
result of sequestration.\69\ In the October 2018 ANPRM, we described
our belief regarding how a potential model could pay a drug add-on
amount that would be different from the current drug add-on amount. We
sought public comment on potential ways to structure the alternative
add-on, including but not limited to: An amount based on drug class,
the physician's specialty, or the practice's historical billing
patterns, with a possible bonus pool tied to clinically appropriate
utilization. We requested feedback on several design topics, such as
how we could best define and determine the alternative add-on payment
amount, whether CMS should develop an encounter-based or monthly add-on
payment approach, and potential inclusion of a quality bonus pool to
incentivize evidence-based care. We stated that our goal was to
maintain relative stability in provider and supplier revenue through an
alternative drug add-on payment for furnishing drugs that removes the
current percentage-based drug add-on payments.
---------------------------------------------------------------------------
\69\ Stakeholders have reported that the add-on percentage is
slightly further reduced when the OPPS beneficiary cost-sharing
limitation applies. Further, we note that current payments under the
OPPS for certain drugs when the drug is acquired under the 340B
program are made based on ASP-22.5 percent and are not considered to
include a drug add-on payment amount. We refer readers to to the
Calendar Year (CY) 2021 OPPS/ASC Notice of Proposed Rulemaking (CMS-
1736-P) (85 FR 48880) for a discussion of CMS's proposal for CY 2021
and subsequent years to pay for drugs acquired under the 340B
program at ASP minus 34.7 percent, plus an add-on of 6 percent of
the product's ASP, for a net payment rate of ASP minus 28.7 percent
based on the results of the Hospital Acquisition Cost Survey for
340B-Acquired Specified Covered Drugs. We also refer readers to the
alternative proposal in the CY 2021 OPPS/ASC Notice of Proposed
Rulemaking (85 FR 48890) to continue the current policy of paying
ASP-22.5 percent for 340B drugs and biologicals under the OPPS.
---------------------------------------------------------------------------
In response to the October 2018 ANPRM, we received feedback from a
number of stakeholder groups on the structuring of an alternative add-
on payment. Overall, there was no consensus on the best approach to
designing an alternative add-on payment, though several commenters
supported calculating the alternative add-on payment in such a way that
model participants would be held harmless. Some commenters supported
the idea of testing an alternative add-on payment that is not tied to
increases in drug prices over time, with one commenter noting that this
could promote revenue stability. One commenter noted an approach that
varies the alternative add-on payment between different drugs would
risk creating perverse incentives in prescribing decisions between
alternative treatment options. Several commenters supported a flat fee
with more than one tier. Several commenters expressed concern about
linking a bonus pool to prescribing lower cost drugs. One commenter
opposed reducing the add-on amount to allow for a bonus pool.
After considering the comments we received, we were persuaded that
potential model requirements to qualify for a modest quality bonus
would be challenging and may be burdensome for MFN participants to
implement and adhere to consistently for all MFN beneficiaries, and
would add potential financial risk for MFN participants, which is not
necessary for purposes of testing an alternative add-on payment
approach under the MFN Model. Thus, we are not including a quality
bonus in the MFN Model. We were also persuaded that the alternative
add-on should be designed in as straightforward a manner as possible to
minimize administrative burden for MFN participants and potential
confusion for beneficiaries.
We will pay MFN participants a single add-on payment amount per
dose of an MFN Model drug; this payment will not vary based on the
amount of drug furnished in a dose, billing units billed on the claim
line, or by MFN participant or specialty. The goals for the model's
approach to the alternative add-on payment are to test an innovative
way to pay the add-on portion of the drug payment, boost add-on revenue
for MFN participants on average based on historical overall add-on
revenue, create an incentive to encourage appropriate drug utilization
by breaking the link between the manufacturer's drug price and the
calculation of the Medicare Part B payment for the add-on amount, and
remove or reduce the incentive to furnish higher-cost drugs inherent in
the current methodology.
With the MFN alternative add-on payment, we will test a single add-
on payment amount that will paid per dose, where ``dose'' for the
purposes of the MFN alternative add-on payment is defined as the number
of HCPCS billing units reported on a claim line \70\ (also called
service line or line item). We are codifying this alternative add-on
payment at Sec. 513.220. We will waive beneficiary cost-sharing for
the add-on payment. As such, the add-on approach will test a separate
standardized add-on payment amount per dose that is not tied to the
Medicare Part B payment amount for a drug. We will start with an amount
that is calculated based on 6.1224 percent of historical applicable
ASPs for 2019 final action claim lines for the selected MFN Model drugs
for the beginning of performance year 1 as further described in Sec.
513.220, trended forward using an inflationary adjustment for the start
of performance year 1. With this approach, the per-dose add-on payment
amount will be calculated once at the beginning of the model and will
not be recalculated as the MFN Model Drug HCPCS Codes List changes. For
each calendar quarter thereafter, beginning with performance year 1,
quarter 2, we will update the per-dose add-on payment amount using an
inflation factor.
---------------------------------------------------------------------------
\70\ An exception is when a claim line is billed with the
modifier JW, indicating discarded drug.
---------------------------------------------------------------------------
For the MFN Model drugs for the beginning of performance year 1
that are biosimilar biological products, we will use 6.1224 percent of
the historical applicable ASPs for the reference biological product in
the calculation of the per-dose add-on amount rather than 6.1224
percent of the historical
[[Page 76217]]
applicable ASPs for the biosimilar biological product to align with the
determination of the add-on amount to such products under section
1847A. Based on the performance year 1 MFN Model Drug HCPCS Codes List
in Table 2, this applies to Q5111 (Injection, udenyca 0.5 mg).
We selected 6.1224 percent because that amount results in an add-on
pool that will allow MFN participants to realize, on average, a 6
percent add-on per dose after sequestration, which generally
applies.\71\ In the absence of actual drug acquisition costs for
eligible providers and suppliers, we believe it is appropriate to use
an amount for the add-on pool that represents, on average, a 40 percent
increase compared to 4.3 percent of ASP in use in the baseline period
to achieve a goal of the model to provide increased add-on revenue for
MFN participants on average.
---------------------------------------------------------------------------
\71\ Note that Section 3709 of the Coronavirus Aid, Relief, and
Economic Security (CARES) Act temporarily suspends Medicare
sequestration from May 1, 2020 to December 31, 2020. Available at:
https://www.govinfo.gov/content/pkg/BILLS-116hr748enr/pdf/BILLS-116hr748enr.pdf.
---------------------------------------------------------------------------
2. Per-Dose Add-On Payment Amount Methodology
a. Calculation of the Single Per-Dose Add-On Payment Amount
In Sec. 513.220(b), we specify how we calculated a single per-dose
add-on payment amount for the start of the MFN Model. Using 2019
historical claims data, we calculated a per-dose add-on payment amount
by applying the applicable ASP (that is, the payment amount determined
in accordance with section 1847A of the Act for a quarter minus the
applicable add-on percentage) to the identified 2019 claims lines,
based on the calendar quarter in which the claim's date of service
falls, which corresponds to the manufacturer-reported ASPs from two
calendar quarters prior, with an exception for biosimilar biological
products as described previously. We used all 2019 Medicare Part B FFS
claims lines for separately paid drugs (by HCPCS code) included on the
MFN Model HCPCS Codes List for the beginning of performance year 1 that
were furnished by eligible Medicare-participating providers and
suppliers (that is, entities that are eligible to be an MFN
participant). We excluded claims submitted by excluded providers and
suppliers described in Sec. 513.100(c) (such as CAHs, and cancer
hospitals) as well as certain claims described in Sec. 513.100(d)
(such as claims processed by the DME MAC), as applicable in 2019, as
well as claims where Medicare was not the primary payer. We included
all relevant claim lines for an MFN Model drug with an allowed charge
greater than zero dollars in the calculation. As we used nearly all
2019 claims for drugs included on the MFN Model HCPCS Codes List for
the beginning of performance year 1 furnished from any eligible
Medicare-participating provider or supplier, we believe that one
calendar year provided sufficient data for purposes of calculating a
single per-dose add-on payment amount. Calendar year 2019 represents
the same baseline year that we used to select the MFN Model drugs for
the beginning of performance year 1, as identified in Table 2.
Once all relevant 2019 claim lines were identified for each drug
(by HCPCS code) on the MFN Model HCPCS Codes List for the beginning of
performance year 1, we multiplied the number of HCPCS units billed on
each claim line by 6.1224 percent of the 2019 applicable ASP (which we
define as the payment amount determined in accordance with 1847A of the
Act less the applicable add-on percentage for the MFN Model drug's
HCPCS code) for the calendar quarter that matches the claim line's date
of service and then summed across all claim lines for that drug to
yield a total add-on spending amount for that drug. For biosimilar
biological products, we used the applicable ASP for the reference
biological product.
Then we pooled together the total add-on spending amounts for all
drugs on the MFN Model HCPCS Codes List for performance year 1 and the
total number of claim lines for those drugs (excluding claim lines
billed with the JW modifier). Lastly, we calculated the per-dose add-on
payment amount as the total pooled add-on spending amount divided by
the total pooled number of claim lines.
Using the drugs (by HCPCS code) included on the performance year 1
MFN Model Drug HCPCS Codes List in Table 2, available 2019 claims data
subject to the exclusions and exception previously noted, and
applicable ASPs from 2019, we calculated a single per-dose add-on
payment amount in the amount of $146.55. This amount represents the
single per-dose add-on payment amount for a dose of any MFN Model drug
prior to application of the inflationary factor as described in section
III.F.2.b. of this IFC.
b. Trending the Single Per-Dose Add-On Payment Amount Forward Each
Calendar Quarter During the MFN Model
We will trend forward the single per-dose add-on payment amount
each calendar quarter during the MFN Model to account for inflation
over time by using a cumulative inflationary factor as described in
this section of this IFC. We will not use changes in ASP or MFN Drug
Payment Amount to trend forward the single per-dose add-on payment
amount to align with our intention to test the removal of the link
between a drug's add-on payment and its price.
As specified in Sec. 513.220(b)(7), after calculating the single
per-dose add-on payment amount, we multiplied the single per-dose add-
on payment amount ($146.55) by an inflationary factor, which equals the
percentage increase in the CPI-U from the midpoint of the baseline year
(2019) through the first month of the calendar quarter prior to the
start of the model (that is, the percentage increase in CPI-U from July
2019 through October 2020). The resulting per-dose alternative add-on
payment amount for the first calendar quarter of performance year 1
(January 1, 2021 through March 31, 2021) is $148.73.
To calculate the per-dose alternative add-on payment amount for
each subsequent calendar quarter during the model performance period,
as specified in Sec. 513.220(c), we will multiply the performance year
1, quarter 1 alternative add-on payment amount by a cumulative
inflation factor that will ensure the amount will remain equal to or
greater than the alternative add-on payment amount calculated for
performance year 1, quarter 1. We will calculate a cumulative inflation
factor as equal to the percentage increase in the CPI-U from October
2020 through the first month after the end of the applicable ASP
calendar quarter. If the cumulative percentage change in the CPI-U is
negative, we will use an inflation factor of 1. For example, the
cumulative inflation factor for performance year 1, quarter 2 (that is,
April 1, 2021 through June 30, 2021) will be the percentage increase in
the CPI-U from October 2020 through January 2021. Similarly, the
cumulative inflation factor for performance year 1, quarter 3 will be
the percentage increase in the CPI-U from October 2020 through April
2021.
As discussed in section III.G. of this IFC, MFN participants will
use a new HCPCS code (M1145, MFN drug add-on, per dose) to bill for and
receive the alternative add-on payment amount for each dose of an MFN
Model drug that is billed on the claim.
3. Discussion of the Per-Dose Add-On Payment Approach
The per-dose add-on payment amount approach will test an
alternative way to
[[Page 76218]]
calculate the add-on payment that is not tied to the sales price of the
drug that is furnished. This approach also aims to boost add-on
revenue, on average, for MFN participants by setting the per-dose add-
on payment amount based on 6.1224 percent of historical ASP payment
allowances trended forward for inflation. However, the impact on MFN
participants will vary based on the MFN participant's prescribing
patterns, including the amount and types of MFN Model drugs they
furnish to Medicare FFS beneficiaries.
Compared with the current add-on payment policy, on an average per
dose basis based on 2019 historical claims, the single per-dose add-on
approach will initially decrease add-on payments for MFN Model drugs
with relatively higher historical applicable ASP-based payment amounts
per dose and increase add-on payments for MFN Model drugs with
relatively lower historical applicable ASP-based payment amounts per
dose. Average 2019 historical add-on payment amounts per dose for the
MFN Model drugs for performance year 1 ranged from $10.44 to $2,575.47
per average dose for a drug. Based on 2019 claims, on average, a single
per-dose add-on payment amount, calculated as described in this IFC and
after sequestration is applied, will represent an increase in the add-
on payment amount for 70 percent of doses on average compared to the
effective historical add-on amount of 4.3 percent of the applicable ASP
after sequestration.
To examine the potential impact of the single per-dose add-on
approach on MFN participants using 2019 claims data, we considered the
overall potential change in the add-on payment amount at the eligible
entity level, specialty level, and type of provider and supplier. That
is, for this entity level analysis, we grouped 2019 claim lines for the
drugs (by HCPCS code) identified in Table 2 based on the provider's or
supplier's CMS Certification Number (``CCN'') or Taxpayer
Identification Number (``TIN''). To examine the potential impact of the
single per-dose add-on payment amount at the specialty level, we
assigned claims to a specialty category based on the primary specialty
of the National Provider Identifier (NPI) associated with the
furnishing of the drug as listed in the Medicare Provider Enrollment,
Chain, and Ownership System (PECOS). Eligible providers were assigned
to the specialty that was most frequently associated with their 2019
claims for the drugs (by HCPCS code) identified in Table 2. We also
used the type of bill to examine the potential impacts on various types
of providers and suppliers.
These analyses highlight that different subsets of providers and
suppliers will potentially gain (or lose) under the single per-dose
add-on approach. For 340B covered entities that were paid under the
OPPS during calendar year 2019, the entirety of the alternative add-on
payment amount represent an increase in payment when drugs are acquired
under the 340B program. Thus, we removed these entities from the
following analyses.
To explore the potential entity level change in the add-on amount
for the single per-dose add-on payment approach, we assigned each CCN
or TIN to only one specialty based on the specialty code with the
highest total allowed spending for the entity's claim lines, regardless
of setting (for example, hospitals, ASCs, and physician office). We
also assigned each specialty a value of ``low,'' ``medium,'' or
``high,'' based on the percentage of its Medicare revenue that is
related to Part B drugs, such that ``high'' means the specialty's drug
revenue is more than 50 percent of its total Medicare revenue,
``medium'' means the specialty's drug revenue is 25 to 50 percent of
its total Medicare revenue, and ``low'' means the specialty's drug
revenue is less than 25 percent of its total Medicare revenue.
Based on the single per-dose add-on payment amount of $146.55
(prior to the application of the inflationary factor that applies
during the model) and using 2019 drug utilization, MFN participants
will fare, on average, 40 percent better overall across all specialties
with the per-dose add-on payment amount than they did historically
based on 4.3 percent of ASP after sequestration. Some MFN participants
will see more than a 40 percent increase in revenue related to the MFN
add-on payment amount compared to their 2019 historical Part B drug
claims, and others will see less than a 40 percent increase, including
some who will see a reduction in add-on revenue. Based on our analysis,
in general, physician practices will be better off under the per-dose
add-on payment approach than hospital outpatient departments, and
single specialty practices will be better off than multi-specialty
practices. Table 8 shows the estimated variation in impacts for the top
specialties by comparing 2019 baseline add-on payments based on 4.3
percent of the applicable ASP with a post-sequestration single per-dose
add-on payment amount (that is, for this comparison, we used the per-
dose add-on payment amount prior to the application of the inflationary
factor ($146.55) and applied the effects of sequestration for this
comparison). The Entity-Level Percentage Change By Percentile portion
of Table 8 shows the distribution of entities based on size of the
difference between their 2019 baseline add-on payments (based on 4.3
percent of the applicable ASP) and the single per-dose add-on amount
(post-sequestration). Each row shows the size of the impact for the
given specialty. The 5th percentile will experience the largest
negative impact whereas the 95th percentile will experience the largest
positive impact.
BILLING CODE 4120-01-P
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[GRAPHIC] [TIFF OMITTED] TR27NO20.009
BILLING CODE 4120-01-C
Based on these data, as shown in Table 8, all but 9 of the top 35
specialties (in terms of overall 2019 allowed dollars) impacted by the
MFN
[[Page 76220]]
Model will on average see increases in add-on revenue compared to 4.3
percent of the applicable ASP with a single payment amount (the
exceptions are hematology/oncology, medical oncology, neurology,
hematology, gastroenterology, gynecological/oncology, infectious
disease, hematopoietic cell transplantation & cellular therapy, and
dermatology). At the 25th percentile, 57 percent of the entities will
see increased add-on revenue for the top 35 specialties with the single
per-dose add-on payment amount; whereas at the 50th percentile, 83
percent of the entities will see increased add-on revenue for the top
35 specialties with the single per-dose add-on payment amount. Please
note that some of the large percentage increases seen shown in the 95th
percentile column are likely driven by the small volume of drugs
furnished by entities in this percentile.
We observed that volume is not consistently associated with whether
an entity will be better or worse off under the per-dose add-on payment
approach when we look at the single per-dose add-on amount approach for
the top five specialties in terms of total aggregate Medicare spending
on MFN Model drugs in 2019: internal medicine, hematology/oncology,
ophthalmology, rheumatology, and medical oncology. When we specifically
looked at the top, middle, and bottom of a distribution of all entities
based on how much better or worse off each entity will be under the
per-dose add-on payment amount compared to their add-on revenue (based
on their 2019 claims), we found that entities in the top 5 percent
(that is, those that will do the best) had very low volume (that is,
few claims for these drugs in 2019 claims). Entities in the bottom 5
percent (that is, those that will do the worst) tended to have lower
volume than the middle 10 percent, though volume was highest in the
bottom 5 percent of entities in the internal medicine and ophthalmology
specialties. Overall, entities that will be worse off compared to their
add-on revenue (based on their 2019 claims) under the per-dose add-on
payment approach tended to furnish more drugs with higher drug add-on
payment amounts per dose more frequently than the entities that will be
better off. We estimate that similar impacts will be experienced across
the performance years unless ASPs for MFN Model drugs rise faster than
inflation, in which case the overall increase in add-on revenue
compared to non-model add-on revenue will diminish over time.
4. Beneficiary Cost-Sharing Responsibilities
In response to the October 2018 ANPRM, which suggested continuing
beneficiary cost-sharing for the alternative add-on payment, some
commenters suggested that CMS should ensure any alternative add-on
payment does not increase out-of-pocket costs for beneficiaries. Other
commenters noted that an alternative add-on payment could be confusing
to beneficiaries since currently they pay cost-sharing based on a
single amount, versus separate amounts, such as the MFN Model Drug
Payment Amount and alternative add-on that we are including in the MFN
Model. We appreciate these commenters' feedback.
To support reducing out-of-pocket drug costs and minimizing
potential confusion for MFN beneficiaries related to the alternative
add-on payment amount, and decreasing administrative burden for MFN
participants, we will waive beneficiary cost-sharing (coinsurance and
deductible amounts) on the portion of the allowed MFN Model Payment
amount that is based on the alternative add-on payment. Under the MFN
Model, the MFN Drug Payment Amount will be subject to beneficiary
coinsurance and the annual deductible amount. MFN participants will
continue to collect beneficiary cost-sharing applicable to the portion
of the allowed payment amount that is based on the MFN Drug Payment
Amount. For the alternative add-on, Medicare will pay the entire
allowed payment amount that is based on the alternative add-on payment
to ensure that beneficiaries do not experience an increase in cost-
sharing under the MFN Model as a result of testing an alternative add-
on amount. That is, beneficiaries will not owe any coinsurance or
amount for the annual deductible for the per-dose add-on payment
amount.
G. Billing and Claims Processing Approach
We intend to issue model-specific claims submission instructions
that MFN participants will be required to follow. Currently, for
separately payable Part B drugs, providers and suppliers submit
separate claim lines for each drug. Among the information included in
each claim line for the applicable bill type, providers and suppliers
specify the appropriate HCPCS code to indicate the drug that was
furnished, the number of billing units to indicate the total amount of
the drug that was furnished, billing code modifiers as necessary, and a
billing amount (or charge). In general, providers and suppliers
routinely use one claim line to bill for a furnished drug dose, and
using billing modifiers when doing so may be necessary to comply with
billing instructions. In certain situations, a second claim line may be
necessary to report the amount of drug that was furnished, for example,
when the number of billing units necessary to indicate the dosage given
exceeds the character size of the units field or when appropriately
discarded drug is billed. When applicable, a separate line item is
billed with the modifier JW to identify the amount of unused drugs (or
biologicals) from single use vials or single use packages that was
appropriately discarded. The Medicare claims processing system
calculates payment for the amount of discarded drug when the modifier
JW is present. MFN participants will be required to submit a separate
claim line using a new model-specific HCPCS code (M1145, MFN drug add-
on, per dose) to bill for and receive the alternative add-on payment
amount for each dose of an MFN Model drug that is billed on the claim.
The MFN participant will indicate in the units field of the claim line
with HCPCS code M1145 the number of doses of a separately payable MFN
Model drug that are billed on the claim. To do so, the MFN participant
will count the number of claim lines with a HCPCS code that is included
on the applicable MFN Model Drug HCPCS Codes List (based on the date of
service), including all claim lines when the number of billing units
necessary to indicate the dosage given exceeds the character size of
the units field and the claim has more than one claim line for such MFN
Model drug (we note that this is expected to be a rare situation), and
excluding the number of claim lines billed with the JW modifier. This
approach will allow the Medicare claims processing system to apply the
alternative add-on payment amount for each dose, and not apply
beneficiary cost-sharing to the alternative add-on payment amount. MFN
participants will still bill for wastage as they otherwise would, using
a separate claim line and the JW modifier, and the payment for such
claim lines will be based on the MFN Drug Payment Amount (the
alternative add-on payment amount is not applicable to such claim
lines).
This billing and claims processing approach will initiate from the
MFN participant's billing system and will establish a clear mechanism
for MFN participants to track when the alternative add-on amount was
billed and paid. This approach will simplify Medicare claims processing
changes for the MFN Model. However, this
[[Page 76221]]
approach may increase administrative burden for MFN participants and
requires MFN participants to count the number of claim lines for MFN
Model drugs included on a claim, indicate this number in the units
field of the claim line for the alternative add-on (using HCPCS code
M1145), and submit a billing amount (or charge) on the claim line for
the alternative add-on. In addition, the alternative add-on payment
amount will be updated quarterly. Because Medicare allows the lesser of
the applicable payment amount or the billed amount, MFN participants
will have to ensure that they submit an appropriate billing amount (or
charge) for the alternative add-on for the applicable quarter. Because
the same HCPCS code will be used to bill for the alternative add-on for
all MFN Model drugs, we believe this approach minimizes, but does not
eliminate, the additional administrative burden for MFN participants.
We are waiving program requirements in section 1833(a)(1)(S),
section 1833(a)(1)(G) and section 1833(t) of the Act, respectively to
allow flexibility in the way in which claims subject to the MFN Model
payment will be processed. Section 1833(a)(1)(S) of the Act specifies
that the Medicare payment for drugs and biologicals not paid on a cost
or prospective payment basis is 80 percent of the lesser of actual
charge or the amount established in section 1842(o) of the Act.
Similarly, section 1833(a)(1)(G) of the Act specifies that the amounts
paid with respect to facility services furnished in connection with
certain surgical procedures and with respect to services furnished to
an individual in an ASC shall be 80 percent of the lesser of the actual
charge for the services or the amount determined by the Secretary under
such revised payment system. Section 1833(t) of the Act specifies how
payment under the OPPS is calculated including beneficiary copayment.
Specifically, we are waiving these program requirements to the extent
necessary to allow the total allowable model payment for the service as
specified in Sec. 513.210 and Sec. 513.220 (that is, the sum of the
allowed MFN Drug Payment Amount and the allowed alternative add-on
payment amount) and to not apply beneficiary cost-sharing to the
alternative add-on payment amount.
H. Quality Measures
The October 2018 ANPRM stated our intention to include quality
measures as part of the potential IPI Model, and our interest in
several categories of potential measures, specifically: patient
experience measures, medication management measures, medication
adherence measures, and measures related to patient access and
utilization. We sought public input on ways to assess quality of care
for purposes of real-time monitoring of utilization, hospitalization,
mortality, shifts in site-of-service and other important indicators of
patient access and outcomes, without requiring providers or suppliers
to report additional data. We received numerous comments in response to
the October 2018 ANPRM on this topic. Several commenters expressed
concern that testing alternative payments for Part B drugs in general
may impact beneficiaries' access to care and may impact the overall
patient experience of care. Some commenters requested that any quality
measurement not add burden to model participants. Some commenters also
discussed the importance of adherence to nationally recognized clinical
guidelines in treatment decisions, stating that adherence to nationally
recognized clinical guidelines would reduce drug spending while also
maintaining and possibly increasing quality of care.
We appreciate the public feedback on ways we could structure a
model to enhance and monitor quality of care. In the MFN Model, we will
implement robust monitoring activities, such as analyzing claims data,
using patient survey data, and site visits, to identify any unintended
consequences and ensure that MFN beneficiaries' access to medications
is not impeded and that quality of care is preserved or enhanced.
Further, we believe the following principles are appropriate for a
quality measurement approach for the MFN Model: (1) Use quality
measures for the purpose of monitoring quality of care and beneficiary
access to treatment and experience with care; (2) avoid unnecessary
participant reporting burden as many providers and suppliers are
currently reporting quality measures to other programs and payers, for
example, the MFN Model should use claims-based measures where
appropriate; and (3) establish standards for adding quality measures,
if necessary, during the model. We believe that this approach will
allow CMS to test the MFN Model's alternative drug payment methodology,
while creating a safeguard for beneficiary access and quality of care,
as well as a means to monitor patient access and quality of care. We
are also sensitive to concerns regarding adding administrative burden
to MFN participants and beneficiaries and, thus, seek to minimize
burden on them. As such, in Sec. 513.400(b)(1) we will collect only
one quality measure, focused on patient experience, to help better
understand the impact of the MFN Model on beneficiary access and
quality of care. This survey will be fielded by CMS to avoid any
quality measure reporting burden for MFN participants, although there
will be reporting burden on beneficiaries. CMS will also monitor for
quality as outlined in section III.I.4. of this IFC, including
monitoring access to medications through rapid analysis of claims data,
using monthly claims extracts that will provide frequent assessments of
beneficiary access to MFN Model drugs and that complement existing
methods to receive, assess, and respond to beneficiary and health care
provider feedback on the MFN Model.
For the patient experience focused quality measure, we will use a
patient experience survey, which we will field periodically to a sample
of Medicare beneficiaries, beginning in performance year 1. The patient
experience survey will be administered to these beneficiaries by a
third party contractor throughout the model performance period. A
sample of beneficiaries will be surveyed regarding their experience of
care, access, or other issues they experienced under the MFN Model, and
we may also sample beneficiaries who are not in the MFN Model.
Beneficiaries will not be required to complete the survey.
Survey results will be used to monitor the impact of the MFN Model
on MFN beneficiaries' care experience and potentially to inform
educational materials for MFN participants. As is outlined in section
III.I.4. of this IFC, claims data will also be monitored to assess
patient access and outcomes.
If during the model the patient experience of care quality measure
and claims-based monitoring strategies are found to be insufficient to
adequately measure the quality of care that MFN beneficiaries are
receiving or MFN participants are providing, CMS may specify additional
measures to monitor quality. If additional quality measures are added,
they will meet the following criteria: (1) Additional measures would be
among one or more of the following categories: Patient experience of
care, patient activation, shared decision making, adherence,
utilization, and process measures; (2) Additional measures would not
add significant burden to MFN participants or beneficiaries; and (3)
Additional measures would utilize an instrument that CMS has used
previously in a model to adjust payment or for monitoring or
evaluation. We are codifying the inclusion of the patient
[[Page 76222]]
experience quality measure and its use as well as the criteria for
adding measures during the MFN Model in Sec. 513.400.
I. Beneficiary Protections and Monitoring Actions
We are interested in enhancing protections for beneficiaries
included in the MFN Model. In addition to existing beneficiary
protections, we will actively monitor the MFN Model to ensure it is
operating effectively and meeting the needs of beneficiaries, providers
and suppliers, and the Medicare program. We will coordinate with the
Medicare Beneficiary Ombudsman and other customer facing components to
ensure that any MFN Model-related beneficiary complaints, grievances,
or requests for information submitted are responded to in an
appropriate and timely manner, per CMS protocol.
We believe it will also be necessary to have additional protections
in place in the MFN Model to ensure that beneficiaries retain their
existing rights and are not harmed by the model test. Further, we
believe it is important for beneficiaries to know and understand their
rights as beneficiaries who are receiving care from MFN participants.
We therefore believe it is necessary to include certain policies
regarding beneficiary choice, appeals, and the availability of
services.
1. Beneficiary Freedom of Choice
A beneficiary's ability to choose his or her provider or supplier
is an important principle of Medicare fee-for-service and is reflected
in section 1802 of the Act. We are codifying in Sec. 513.410(a) that
any MFN participant must not commit any act or omission, nor adopt any
policy that inhibits a beneficiary from exercising his or her freedom
to choose to receive care from any Medicare participating provider or
supplier or any provider or supplier who has opted out of Medicare. We
believe these provisions are necessary to ensure the MFN Model does not
prevent beneficiaries from the general rights and guarantees provided
under Medicare.
2. Appeals Processes and Financial Hardship Exemption
a. Appeals Processes
In Sec. 513.410(b), we are codifying that MFN beneficiaries and
their assignees will have access to the existing formal claims appeals
process under 42 CFR part 405, subpart I. In other words, once an MFN
Model drug is furnished by an MFN participant to a beneficiary and a
claim is submitted and processed for payment, that claim will be
eligible for the current Medicare claims appeals processes. If a
beneficiary receives an MFN Model drug from an MFN participant it does
not mean that he or she should lose this right, but instead this right
should necessarily be applicable to included beneficiaries as it would
be if they were not a part of the MFN Model.
b. Financial Hardship Exemption
To include financial protection for physicians and other MFN
participants, specifically those who furnish substantial amounts of MFN
Model drugs as part of the services they furnish to Medicare FFS
beneficiaries, especially MFN Model drugs with the greatest difference
between the MFN Price and the applicable ASP, we are including a
financial hardship exemption codified in Sec. 513.230. The financial
hardship exemption process for MFN participants will be available in
the event unintended consequences arise to ensure access to MFN Model
drugs for MFN beneficiaries and financial protections for MFN
participants who are unable to obtain MFN Model drugs at or below the
MFN Model Payment for such drugs and are significantly affected by
their participation in the MFN Model.
The financial hardship exemption process will occur independently
of existing Medicare claims processing and appeals processes. In Sec.
513.230(a), we codify that a financial hardship exemption for a
performance year may be granted to an MFN participant by CMS, in its
sole discretion and will not be subject to appeal, when the provisions
in Sec. 513.230 are met. This means that a financial hardship
exemption, if granted, will be applied at the MFN participant level (as
defined in Sec. 513.2). As further described in this section of this
IFC, a financial hardship exemption will be limited to cases where the
MFN participant experienced a financial loss.
Specifically, to be eligible for a financial hardship exemption,
the MFN participant must submit its request for a financial hardship
exemption to CMS in accordance with the submission process that CMS
will post on the MFN Model website prior to October 1, 2021, and in the
form and manner and with the content that will be specified by CMS,
including without limitation the requirements specified in Sec.
513.230(b). Such requests must be submitted to CMS within 60 calendar
days following the end of the performance year for which the MFN
participant seeks a financial hardship exemption. The MFN participant
must include the following in its request for a financial hardship
exemption:
Evidence of methods used to obtain each MFN Model drug
that was furnished by the MFN participant during the performance year
to any patient;
Average net acquisition cost for each MFN Model drug
(inclusive of all on-invoice prices and price reductions, off-invoice
discounts, any adjustments thereto, and any other price concessions
related to the purchase of the MFN Model drug) that was furnished by
the MFN participant during the performance year to MFN beneficiaries;
Average net acquisition cost for each MFN Model drug
(inclusive of all on-invoice prices and price reductions, off-invoice
discounts, any adjustments thereto, and any other price concessions
related to the purchase of the MFN Model drug) that was furnished by
the MFN participant during the performance year to patients who were
not MFN beneficiaries;
Statement of any remuneration received by the MFN
participant from manufacturers of MFN Model drugs, wholesalers, and
distributors that is not reflected in the MFN participant's average net
acquisition costs with a justification of why such remuneration should
not be treated as a price concession related to the purchase of an MFN
Model drug;
Administrative information, including: MFN participant's
name, TIN or CCN (as applicable), contact name, phone number, and email
address; and
The MFN participant's attestation that--
++ It experienced a reduction in Medicare Part B FFS payments for
separately payable drugs on a per beneficiary basis during the
performance year as compared to the prior year (that is, the four
calendar quarters immediately preceding the performance year) due to
its inability to obtain one or more of the MFN Model drugs at or below
the MFN Model Payments for such drugs during the performance year;
++ It has not received and will not receive any remuneration from
manufacturers of MFN Model drugs, wholesalers, and distributors related
to the purchase of an MFN Model drug that was furnished by the MFN
participant during the performance year that is not reflected in the
MFN participant's submission; and
++ Its submission is true, accurate, and complete.
In addition, MFN participants must use a template that CMS will
post on the MFN Model website for submission of their net acquisition
costs for MFN Model drugs and administrative information. This template
will be
[[Page 76223]]
similar to the template CMS provided for the 2020 Hospital Survey for
Specified Covered Outpatient Drugs (SCODs) Average Acquisition
Cost.\72\ The MFN participant will submit the other required materials
to CMS along with the template.
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\72\ The template for the 2020 Hospital Survey for Specified
Covered Outpatient Drugs (SCODs) (CMS-10709; OMB 0938-1374)
available at: https://www.cms.gov/Medicare/Medicare-Fee-for-Service-Payment/HospitalOutpatientPPS/index.
---------------------------------------------------------------------------
In Sec. 513.230(c), we codify the standards that CMS will use to
determine if an MFN participant is granted a financial hardship
exemption. Specifically, to be eligible for the financial hardship
exemption, we codify in Sec. 513.230(c)(2)(i) that the MFN participant
must submit a timely, complete request for a financial hardship
exemption in accordance with the requirements specified in Sec.
513.230(b) that in the sole discretion of CMS demonstrates all of the
following:
The MFN Participant exhausted all reasonable methods to
obtain the MFN Model drugs at or below the MFN Model Payments for such
drugs during the performance year.
The MFN participant's average net acquisition cost for
each MFN Model drug (including on- and off-invoice discounts or
adjustments) that was furnished by the MFN participant during the
performance year to patients who were not MFN beneficiaries was not
less than the MFN participant's average net acquisition costs for such
MFN Model drug (including on- and off-invoice discounts or adjustments)
that was furnished by the MFN participant during the performance year
to MFN beneficiaries.
Any remuneration the MFN participant received from
manufacturers of MFN Model drugs, wholesalers, and distributors that
was not reflected in the MFN participant's average net acquisition
costs was not a price concession related to the purchase of an MFN
Model drug.
In addition, in Sec. 513.230(c)(2)(ii), we are codifying that the
agency in its sole discretion must also determine that the MFN
participant's excess reduction amount per beneficiary (as determined by
CMS in accordance with Sec. 513.230(d)(6)) is greater than zero. That
is, the MFN participant must have experienced a reduction in Medicare
FFS allowed charges for separately payable Medicare Part B drugs on a
per beneficiary basis during the performance year as compared to the
prior year (that is, the four calendar quarters immediately preceding
the performance year) that is greater than 25 percent of the MFN
participant's total Medicare Part A and Medicare Part B FFS allowed
charges on a per beneficiary basis during the prior year. We are
establishing a threshold of 25 percent of the MFN participant's total
Medicare Part A and Medicare Part B FFS allowed charges on a per
beneficiary basis as a criterion to qualify for the financial hardship
exemption because the exemption is designed to be limited to MFN
participants that experience a significant year-to-year reduction in
total allowed charges as a result of the MFN Model. We believe this
threshold will protect MFN participants from significant financial
hardship under the MFN Model while also preserving the model test of
aligning payment for Medicare Part B drugs with the lowest
international prices using a phase-in approach.
Incomplete financial hardship exemption requests will not be
considered by CMS.
In Sec. 513.230(d), we are codifying how CMS will calculate the
MFN participant's excess reduction amount per beneficiary. CMS will
calculate the MFN participant's excess reduction amount per beneficiary
using available final action claims data that are estimated to be more
than 90 percent complete (claims are generally complete within 2 months
after the service month) where Medicare was the primary payer, as
determined by CMS. This approach will not include non-claims based
payments or other transactions, for example, performance-based payment
or repayments. CMS will calculate, for dates of service within the
performance year, the MFN participant's total allowed charges for
separately payable Medicare Part B drugs, and the total number of
beneficiaries that had at least one claim for a service furnished by
the MFN participant with a Medicare Part A or Medicare Part B allowed
charge greater than $0. Then, CMS will divide the MFN participant's
total allowed charges for separately payable Medicare Part B drugs for
dates of service within the performance year by the total number of
beneficiaries that had at least one claim for a service furnished by
the MFN participant with a Medicare Part A or Medicare Part B allowed
charge greater than $0 with a service date within the performance year.
CMS will repeat this calculation using the available claims data for
the prior year, to calculate the MFN participant's average per
beneficiary total allowed charges for separately payable Medicare Part
B drugs for the prior year. Then, CMS will subtract the MFN
participant's average per beneficiary total allowed charges for
separately payable Medicare Part B drugs for the performance year from
the MFN participant's average per beneficiary total allowed charges for
separately payable Medicare Part B drugs for the prior year. This
difference will then be compared to 25 percent of the MFN participant's
average per beneficiary total allowed charges for all Medicare Part A
and Part B claims with dates of service within the prior year, using
subtraction as described in Sec. 513.230(d)(6). The latter quantity
will be calculated by identifying 25 percent of the MFN participant's
total allowed charges for all Medicare Part A and Part B claims with
dates of service within the prior year, then dividing this amount by
the total number of beneficiaries that had at least one claim for a
service furnished by the MFN participant with a Medicare Part A or
Medicare Part B allowed charge greater than $0 with a date of service
within the prior year. If the resulting amount, called the excess
reduction amount per beneficiary, is greater than zero, then the MFN
participant will meet this eligibility criterion for the financial
hardship exemption.
In Sec. 513.230(e)(1), we are codifying that if CMS in its sole
discretion grants a financial hardship exemption to an MFN participant
for a performance year, CMS shall provide to such MFN participant, a
reconciliation payment for the performance year. To calculate the
reconciliation amount for the MFN participant, CMS will multiply the
excess reduction amount per beneficiary by the total number of
beneficiaries that had at least one claim for a service furnished by
the MFN participant with a Medicare Part A or Medicare Part B allowed
charge greater than $0 with a service date within the performance year.
The reconciliation payment amount will be paid by a CMS contractor
using Medicare Part B funds as soon as practical after CMS notifies the
MFN participant of CMS's decision regarding the MFN participant's
financial hardship exemption request and the amount of the
reconciliation payment, if any, to be made to the MFN participant. In
Sec. 513.230(e)(2), we are codifying that there will be no appeal of
the amount of the reconciliation payment, if any, to be made to the MFN
participant. In addition, the reconciliation payment amount will not be
subject to beneficiary cost sharing (including any deductible or
coinsurance) because the reconciliation payment will not be tied to
specific beneficiary claims, beneficiaries will have been responsible
for 20 percent cost-sharing on the allowed payment amounts for the
[[Page 76224]]
Medicare Part B drugs they received during the performance year, and
steps to seek additional cost-sharing from beneficiaries would likely
cause significant confusion and burden for beneficiaries and MFN
participants.
We do not foresee that many MFN participants will qualify for a
reconciliation payment for performance year 1, because the estimated
overall reduction in Medicare Part B drug payment during performance
year 1 is 7 percent on average. This reflects the MFN Price phase-in
formula in section III.E.5. of this IFC which will begin with the MFN
Price making up 25 percent of the MFN Drug Payment Amount and the
alternative add-on payments in section III.F. of this IFC will
represent a 40 percent increase on average for MFN participants
relative to historical Medicare add-on payments. Given the financial
hardship execption threshold of 25 percent of the MFN participant's
total Medicare Part A and Medicare Part B FFS allowed charges on a per
beneficiary basis in the prior year will be determined at the entity
level, MFN participants with a high proportion of their overall
Medicare payments related to MFN Model drugs will be more likely to
qualify for the hardship exemption if their Medicare Part B drug
allowed charges on a per beneficiary basis during a performance year
were to decrease significantly compared to the prior year. MFN
participants that are hospitals will likely have significant Medicare
Part A revenues and purchasing abilities that will lessen the
likelihood that they will qualify for a financial hardship exemption
based on their experience in the MFN Model during performance year 1.
Non-hospital MFN participants will be more likely to potentially
qualify in later performance years.
For future years, we seek comment on whether an alternative
threshold might better protect beneficiary access to MFN Model drugs or
mitigate impacts on physicians and other MFN participants under the MFN
Model. For example, we are interested in whether a uniform threshold
should be applied for all MFN participants, and whether certain
physician specialties or types of MFN participants would find the
threshold insufficient in protecting beneficiary access to MFN Model
drugs. For future rulemaking, we also seek comment on how CMS could
refine the design of the financial hardship exception to advance the
model goals to reduce program expenditures and maintain or improve
quality of care.
CMS pledges to maintain confidentiality of individual financial
hardship exemption requests to the extent provided by law. However, CMS
may make public descriptive information about MFN participants that are
granted a financial hardship exemption and the extent to which they
were unable to obtain MFN Model drugs at or below the MFN Model Payment
for such drugs. We do not intend to make such information available in
an individually identifiable manner.
3. Availability of Services
The MFN Model is designed to test potential improvements to the
delivery of and payment for healthcare to reduce Medicare expenditures
while preserving or enhancing the quality of care for beneficiaries. As
such, an important aspect of testing models is that beneficiaries must
continue to have access to and receive needed care.
In Sec. 513.410(c), we are codifying that MFN participants must
not take any action to select or avoid treating beneficiaries based on
their diagnoses, care needs, income levels, or other factors that would
render them ``at-risk beneficiaries'' as that term is defined at 42 CFR
425.20 (``lemon dropping''). We will use monitoring to ensure that MFN
participants are complying with this requirement. We believe that this
is a necessary precaution to protect beneficiaries against potential
beneficiary selection bias from MFN participants and ensure that MFN
beneficiaries retain access to medically necessary treatment.
4. Monitoring and Compliance Activities
Consistent with other CMS Innovation Center models, CMS will
implement a monitoring program for the MFN Model to ensure that the MFN
Model is implemented safely and appropriately. Given that MFN
participants will receive model-specific payments and access to payment
rule waivers while participating in the MFN Model, we believe that
enhanced compliance review and monitoring of MFN participants is
necessary and appropriate to ensure the integrity of the MFN Model. In
addition, as part of the CMS Innovation Center's assessment of the
impact of new models such as the MFN Model, we have a special interest
in ensuring that model tests do not interfere with ensuring the
integrity of the Medicare program. Our interests include ensuring the
integrity and sustainability of the MFN Model and the underlying
Medicare program from both a financial and policy perspective, as well
as protecting the rights and interests of Medicare beneficiaries. For
these reasons, as a part of the models currently being tested by the
CMS Innovation Center, CMS or its designee(s) monitors model
participants to assess compliance with model terms and with other
applicable program laws and policies. We believe our monitoring efforts
help ensure that model participants are furnishing medically necessary
covered services and are not falsifying data, increasing program costs,
or taking other actions that compromise the integrity of the model or
are not in the best interests of the model, the Medicare program, or
Medicare beneficiaries.
In Sec. 513.420, we are codifying a framework for conducting
compliance monitoring activities for the MFN Model that is consistent
with the standard practices in other CMS Innovation Center models.
Under the monitoring policy at Sec. 513.420(b), MFN participants will
be monitored to assess compliance with the MFN Model requirements, to
determine the effects of the MFN Model on MFN beneficiaries, providers,
suppliers, and on the Medicare program and to facilitate real time
identification and response to potential issues. Further, under Sec.
513.420(a)(2), an MFN participant will be required to notify CMS within
15 calendar days after becoming aware that the MFN participant is under
investigation or has been sanctioned by the federal, state, or local
government, or any licensing authority (including, without limitation,
the imposition of program exclusion, debarment, civil monetary
penalties, corrective action plans, and revocation of Medicare billing
rights).
In Sec. 513.420(b)(2), we are codifying that when we are
conducting compliance monitoring and oversight activities, CMS or our
designees will be authorized to use any relevant data or information,
including without limitation Medicare claims submitted for items or
services furnished to MFN beneficiaries. In Sec. 513.420(b)(3), we are
codifying that MFN participants will be required to cooperate with the
model monitoring and evaluation activities, comply with the
government's right to audit, inspect, investigate, and evaluate any
documents or other evidence regarding implementation of the MFN Model,
and to retain and provide the government with access to records.
In Sec. 513.420(b)(1), we are codifying that monitoring activities
will include, but will not be limited to: (1) Documentation requests
sent to the MFN participant, including surveys and questionnaires; (2)
audits of claims data, medical records, and other data from the MFN
participant; (3) interviews with any individual or entity participating
in the MFN Model, including members of the MFN participant's
leadership,
[[Page 76225]]
management, and staff; (4) interviews with beneficiaries and their
caregivers; (5) site visits to the MFN participant; and (6) tracking
complaints and appeals. We believe these specific monitoring
activities, which align with those currently used in other models being
tested by the CMS Innovation Center, are necessary in order to ensure
compliance with the terms and conditions of the MFN Model and to
protect beneficiaries from potential harms that may result from
activities of an MFN participant, such as attempts to reduce access to
medically necessary covered services or appropriate drugs.
We anticipate that monitoring of the MFN Model activities will
include gathering and analyzing data captured through the Ombudsman's
service, the evaluation of the MFN Model, the patient experience
survey, and audits of charts, claims data, medical records, among other
data as available. As previously noted in this IFC, one purpose of
monitoring and analyzing these data sources will be to provide timely
information about the effects of the MFN Model on MFN beneficiaries,
providers, suppliers, and on the Medicare program, and to facilitate
real time identification and response to potential issues. We
anticipate that these findings will inform model oversight and the
potential need for action to address identified issues.
In Sec. 513.420(c), we outline parameters for site visits. We will
require that MFN participants cooperate in periodic site visits
conducted by CMS or its designee. Such site visits will be conducted to
facilitate the model implementation.
In order to operationalize this model, CMS or its designee will
provide the MFN participant with no less than 15 calendar days advance
notice of a site visit, to the extent practicable. Furthermore, to the
extent practicable, CMS will attempt to accommodate a request that a
site visit be conducted on a particular date, but that the MFN
participant will be prohibited from requesting a date that was more
than 60 calendar days after the date of the initial site visit notice
from CMS. We believe the 60-calendar day period will reasonably
accommodate MFN Model participants' schedules while not interfering
with the operation of the MFN Model. Further, we will require MFN
participants to ensure that personnel with the appropriate
responsibilities and knowledge pertaining to the purpose of the site
visit be available during any and all site visits. We believe this is
necessary to ensure an effective site visit and prevent the need for
unnecessary follow-up site visits.
Finally, CMS or its designee can perform unannounced site visits to
all physical locations of MFN participants at any time to investigate
concerns related to the health or safety of beneficiaries or other
patients or other program integrity issues, notwithstanding these
provisions. Further, nothing in part 513 will limit CMS from performing
other site visits as allowed or required by applicable law. We believe
that, regardless of the model being tested, CMS must always have the
ability to timely investigate concerns related to the health or safety
of beneficiaries or other patients, or program integrity issues, and to
perform functions required or authorized by law. In particular, we
believe that it will be necessary for us to monitor, and for MFN
participants to be compliant with our monitoring efforts, to ensure
that they are not denying or limiting the coverage or provision of
medically necessary covered services to beneficiaries in an attempt to
change the MFN Model results or their MFN Model payments, including
discrimination in the provision of services to at-risk beneficiaries
(for example, due to eligibility for Medicaid based on disability).
We intend to monitor MFN participants through any of the previously
described monitoring activities (such as documentation requests, audits
of claims data, audits of medical records, etc.) to ensure that MFN
Model drugs are not being inappropriately billed (for example,
excessive doses or units). We anticipate that this monitoring activity
will discourage MFN participants from furnishing smaller and more
frequent doses of MFN Model drugs to beneficiaries in order to maximize
the alternative add-on payments. If it is found that an MFN participant
has been engaged in inappropriate billing, then we will use applicable
remedial actions set forth in Sec. 513.440(a)(2).
We may employ longer-term analytic strategies to confirm our
ongoing analyses and detect more subtle or hard-to-determine changes in
care delivery and beneficiary outcomes. Some determinations of
beneficiary outcomes or changes in treatment delivery patterns may not
be able to be built into ongoing claims analytic efforts and may
require longer-term study.
a. Reduced Access
We will monitor claims data from MFN participants--for example, to
compare MFN participants' case mix relative to a pre-model historical
baseline to determine whether complex patients are being systematically
excluded. To the extent that the use of a patient experience survey
includes items focused on access, we will analyze these data as well to
determine whether MFN beneficiaries continue to be able to access the
right drug at the right time. We will use these data to promote
transparency and develop an understanding of the MFN Model's effects.
We intend to review and audit MFN participants if we have reason to
believe that they are compromising beneficiary access to care.
We intend to conduct analyses of claims data, such as monthly
updates and historic comparisons of trends including drug utilization,
program spending, and prescribing patterns (including observing for any
shift to compounded or other categories of drugs that are not included
in the MFN Model) as well as changes in site of service delivery,
mortality, hospital admissions, and other indicators present in claims
data. We will monitor physician visits, days in a hospital, and other
services as part of the thorough look at how MFN beneficiaries are
receiving care to determine whether any treatment patterns are changing
systematically. We will use the monitoring results to detect potential
issues with beneficiary access to care or potential provider and
supplier payment issues.
b. Quality of Care Monitoring
We anticipate that quality monitoring activities may include claims
and survey data analytics, site visits, medical record review, and
tracking patient complaints and appeals. We will also use the most
recent claims data available to track utilization and beneficiary
outcomes under the MFN Model. We believe this type of monitoring is
important as we want to ensure to the greatest extent possible that
patients continue to receive high-quality care.
We believe that this set of monitoring activities will allow us to
promptly identify any unintended consequences of the MFN Model. We
anticipate that by identifying unintended potential consequences of the
MFN Model, that we will then be able to determine methods to address or
alleviate those potential consequences.
c. Remedying Improper Payment
We anticipate that our monitoring activities may identify instances
of incorrect MFN Model payments. As such, we are codifying that CMS is
authorized to correct model-specific payments under Sec. 513.420(d).
Specifically, under this section if CMS discovers that it has made or
received
[[Page 76226]]
an incorrect model-specific payment under the terms of the MFN Model,
then CMS may make payment to, or demand payment from, the MFN
participant. Should these monitoring activities identify a need for
additional protections, we will consider appropriate action.
d. Compliance With Laws
MFN participants will remain subject to all existing requirements
and conditions for Medicare participation as set out in Federal
statutes and regulations and provider and supplier agreements, unless
waived under the authority of section 1115A(d)(1) of the Act solely for
purposes of testing the MFN Model. In Sec. 513.420(a)(1), we therefore
require that MFN participants must comply with all applicable laws and
regulations. We note that a law or regulation is not ``applicable'' to
the extent that its requirements have been waived under section
1115A(d)(1) of the Act solely for purposes of testing the MFN Model.
5. Enforcement Authority and Remedial Action
We are codifying at Sec. 513.440(b) that nothing contained in the
terms of the MFN Model or part 513 will limit or restrict the authority
of the HHS Office of Inspector General (OIG) or any other Federal
Government authority, including its authority to audit, evaluate,
investigate, or inspect the MFN participant.
It is necessary for CMS to have the ability to impose remedial
actions to address non-compliance with the requirements of the MFN
Model and to ensure that the MFN Model does not interfere with the
program integrity interests of the Medicare Program. Thus, in Sec.
513.440(a)(1), CMS may take remedial action against an MFN participant
if CMS determines, in CMS' sole discretion, that the MFN participant--
Has failed to comply with any applicable Medicare program
requirement, rule, or regulation;
Has failed to comply with any of the terms of the MFN
Model, including applicable requirements of part 513;
Systematically engaged in the under delivery or over
delivery of an MFN Model drug;
Has taken any action that threatens the health or safety
of an MFN beneficiary or other patient;
Has undergone a change of control that presents a program
integrity risk;
Has submitted false data or made false representations,
warranties, certifications or attestations in connection with any
aspect of the MFN Model;
Has avoided at-risk beneficiaries, as this term is defined
in Sec. 425.20;
Has avoided patients on the basis of payer status;
Is subject to any sanctions or final actions of an
accrediting organization or a Federal, State, or local government
agency;
Takes any action that CMS determines for program integrity
reasons is not in the best interests of the MFN Model, or the Medicare
program, or fails to take any action that CMS determines for program
integrity reasons should have been taken to further the best interests
of the MFN Model or Medicare program;
Is subject to investigation or action by HHS (including
the HHS Office of the Inspector General (OIG)) or the Department of
Justice due to an allegation of fraud or significant misconduct,
including being subject to the filing of a complaint, filing of a
criminal charge, being subject to an indictment, being named as a
defendant in a False Claims Act qui tam matter in which the Federal
Government has intervened, or similar action;
Is the subject of administrative enforcement action
imposed by CMS; or
Has failed to demonstrate improved performance following
any remedial action imposed by CMS.
In Sec. 513.440(a)(2), we are codifying that if CMS determines
that one or more grounds for remedial action exists, CMS may take one
or more of the following remedial actions:
Notify the MFN participant of the violation.
Require the MFN participant to provide additional
information to CMS or its designees.
Require the MFN participant to develop and implement a
corrective action plan in a form and manner and by a deadline specified
by CMS.
Subject the MFN participant to additional monitoring,
auditing, or both.
Remove the MFN participant from the MFN Model;
Recoup model-specific payments.
Such other action as may be permitted under the terms of
Sec. 513.420.
6. Audits and Record Retention
By virtue of participation in the MFN Model, MFN participants will
receive model-specific payments and access to payment rule waivers. We
therefore believe that CMS' ability to audit, inspect, investigate, and
evaluate records and other materials related to participation in the
MFN Model is necessary and appropriate. In order to expand a phase 1
model tested by the CMS Innovation Center, among other things, the
Secretary must first determine that such expansion would not deny or
limit the coverage or provision of benefits under the applicable title
for applicable individuals. Thus, there is a particular need for CMS to
be able to audit, inspect, investigate, and evaluate records and
materials related to participation in CMS Innovation Center models to
allow us to ensure that the model is not denying or limiting the
coverage or provision of benefits for beneficiaries.
We note that there are audit and record retention requirements
under the Medicare Shared Savings Program (42 CFR 425.314) and in
current models being tested under section 1115A (such as under 42 CFR
510.110 for the CMS Innovation Center's Comprehensive Care for Joint
Replacement Model). Building off those existing requirements, in Sec.
513.430(a), the Federal Government, including, but not limited to, CMS,
HHS, and the Comptroller General, or their designees, have a right to
audit, inspect, investigate, and evaluate any documents and other
evidence regarding implementation of the MFN Model. Additionally, in
order to align with the policy of current models being tested by the
CMS Innovation Center, we are codifying in Sec. Sec. 513.430(b) and
(c) that MFN participants must--
Maintain and give the Federal Government, including, but
not limited to, CMS, HHS, and the Comptroller General, or their
designees, access to all documents (including books, contracts, and
records) and other evidence sufficient to enable the audit, evaluation,
inspection, or investigation of the MFN Model, including without
limitation, documents and other evidence regarding all of the
following:
++ The MFN participant's compliance with the terms of the MFN
Model, including new subpart E of part 513.
++ Quality measure information and the quality of services
performed under the terms of the MFN Model, including new subpart E of
part 513.
++ Patient safety.
++ The accuracy of model-specific payments under the MFN Model.
++ Utilization of items and services furnished under the MFN Model.
++ Any other program integrity issues.
Maintain the documents and other evidence for a period of
6 years from the last payment received by the MFN participant under the
MFN Model or from the date of completion of any audit, evaluation,
inspection, or
[[Page 76227]]
investigation, whichever is later, unless--
++ CMS determines there is a special need to retain a particular
record or group of records for a longer period and notifies the MFN
participant at least 30 calendar days before the normal disposition
date; or
++ There has been a termination, dispute, or allegation of fraud or
similar fault against the MFN participant in which case the records
must be maintained for an addition 6 years from the date of any
resulting final resolution of the termination, dispute, or allegation
of fraud or similar fault.
If CMS notifies the MFN participant of the special need to retain
records or group of records at least 30 calendar days before the normal
disposition date, the records must be maintained for such period of
time determined by CMS.
J. Interaction With Other Models and Programs
1. Approach for Overlap With Other Models
In designing each CMS Innovation Center model, CMS considers
potential overlap between a new model and other ongoing and potential
models and programs. Based on the type of overlap, such as health care
provider or beneficiary, operating rules may be established for whether
or not health care providers and beneficiaries can be part of both
models as well as how to handle overlap when it occurs. These policies
help to ensure that the evaluation of model impact is not compromised
by issues of model overlap and that double counting of beneficiaries
and dollars across different models does not occur.
In response to the October 2018 ANPRM, several commenters expressed
concern regarding model overlap, specifically with the Oncology Care
Model (OCM) and initiatives involving accountable care organizations
(ACOs). Some commenters noted that OCM participants should be excluded
from the potential IPI Model or excluded from mandatory participation.
Some commenters also requested that ACO initiatives take precedence in
terms of calculating shared savings as well as for clarity on how
overlap between ACO initiatives and the potential IPI Model would work.
We appreciate commenters' request for detailed information about
model overlap policies. In developing the MFN Model, CMS conducted an
internal review of which models will have potential overlap with the
MFN Model. As a result of our review, we expect there will be
situations where a Medicare beneficiary who receives an MFN Model drug
will also be assigned, aligned, or attributed to another CMS Innovation
Center model or CMS program. Overlap could also occur among providers
and suppliers at the individual or organization level, for example, a
health care practitioner or a physician group practice could
participate in multiple CMS Innovation Center models and CMS programs
concurrently. Of note, some existing models and programs will not have
overlap at the health care practitioner or participant level due to the
way in which the model or program operates and makes payments.
We believe that the MFN Model is operationally compatible with
existing models and programs that provide opportunities to improve care
and reduce spending, especially total cost of care-focused CMS programs
and Innovation Center models. The MFN Model will test an innovative way
to pay for Medicare Part B drugs that seeks to address any existing
incentives for prescribing higher cost drugs and ways to lower costs
for beneficiaries and the Medicare program; total cost of care-focused
CMS programs and Innovation Center models incentivize more appropriate
provision of care across multiple clinical areas, including use of
Medicare Part B drugs; the MFN Model addresses only use of certain
Medicare Part B drugs. To some degree, incentives for inappropriate use
of higher cost drugs are reduced, and intended effects of the MFN Model
are already built into total cost of care-focused models, so the
addition of the MFN Model should not have further effects in those
programs. We do not plan to make adjustments to the MFN Drug Payment
Amount or MFN alternative add-on payment due to overlap between the MFN
Model and another model or program, unless such model tests an
alternative approach to the add-on portion of payment for Medicare Part
B drugs as specified in Sec. 513.220(d)(2). However, for certain
models and programs, adjustments to those models and programs may be
necessary to account for payment changes under the MFN Model.
Because the MFN Model will focus on approximately 50 separately
payable Medicare Part B drugs, when claims are considered from all
beneficiaries aligned with or assigned to some other Innovation Center
models or CMS programs that focus on total cost of care, such as the
Medicare Shared Savings Program, we do not expect that the MFN Model
will have a significant impact on shared savings, total cost of care,
or other benchmarks and measures. Therefore, changes to benchmarks,
targets, and reconciliation methodologies may not be necessary, and
will be determined by each other model, program, or initiative as
appropriate.
However, we recognize that the design of some other models,
programs, and initiatives could create unique challenges at the
organization, clinician, or beneficiary level. As a result, we will
work with such models, programs, or initiatives to resolve any
potential overlaps that could result in overpayment of savings due to
double counting of the impact of a result that could be attributed to
the interventions from two different models. For example, OCM focuses
on improved care management and coordination for Medicare beneficiaries
with cancer who receive chemotherapy during 6-month episodes of care.
An OCM practice has the opportunity to receive a performance-based
payment if it reduces the total cost of care in its OCM episodes
compared to a target. Based on the performance year 1 MFN Model Drug
HCPCS Codes List, we anticipate substantial overlap between MFN
participants and MFN beneficiaries with OCM practices and OCM
beneficiaries. To avoid paying performance-based payments in OCM that
are due simply to the drug payment change that will occur under the MFN
Model and not to changes in care delivery, for OCM, we will adjust
reconciliation calculations such that the drug payments included in OCM
episode expenditures will be calculated as if the MFN Model were not
occurring. OCM participants will be notified and provided with further
information through OCM's typical channels of communication.
As discussed in the section III.C.1. of this IFC, CMMI has already
waived section 1833(t) of the Act for certain acute care hospitals due
to their participation in models under section 1115A of the Act for
which payment for outpatient hospital services furnished to Medicare
FFS beneficiaries, including MFN Model drugs, is made under such model
on a fully capitated or global budget basis. For the first and second
quarters of performance year 1, we will exclude these entities from the
MFN Model with limitation. That is, the acute care hospitals that
participate in another CMS Innovation Center model under which they are
paid for outpatient hospital services furnished to Medicare FFS
beneficiaries, including MFN Model drugs, on a fully capitated or
global budget basis under a waiver under such model of section 1833(t)
of the Act, such as the Maryland Total Cost of Care Model and the
Pennsylvania Rural Health Model, will be excluded
[[Page 76228]]
from the MFN Model. For the third quarter of performance year 1 and
beyond, acute care hospitals that participate in a CMS Innovation
Center model under which they are paid for outpatient hospital services
furnished to Medicare FFS beneficiaries, including MFN Model drugs, on
a fully capitated or global budget basis under a waiver under such
model of section 1833(t) of the Act will be excluded from the MFN Model
if the parameters of the other CMS Innovation Center model adjust for
the difference in payment for MFN Model drugs between the MFN Model and
non-MFN Model drug payments such that savings under the MFN Model are
incorporated into the other CMS Innovation Center model's parameters
(for example, the annual global budget) for the duration of the MFN
Model. These exclusions will apply only during the period of the
hospital's participation in such model under which it is paid on a
fully capitated or global budget basis. Upon termination of such
participation for any reason or if the model is revised such that the
waiver of section 1833(t) of the Act no longer applies under such
model, the hospital--if it otherwise meets the definition of MFN
participant--will be required to participate in the MFN Model.
We anticipate model overlap may occur between the MFN Model and
future CMS models or programs not yet implemented. As discussed in
section III.F.5. of this IFC, if there are MFN participants that
concurrently participate in a future CMS model that also tests an
alternative approach to the add-on portion of payment for Part B drugs,
we will not make the MFN alternative add-on payment to those MFN
participants for those MFN Model drugs that overlap with the other
model. Instead, we will follow the other model's approach to making an
alternative add-on payment. We expect this overlap policy will maintain
the intended financial effects of the MFN Model, while allowing
operational compatibility with other models that test alternative
approaches to Medicare Part B drug payment.
2. Quality Payment Program
The MFN Model will not qualify as an Advanced APM under the Quality
Payment Program. Specifically, the MFN Model does not require
participant health care providers to use CEHRT, does not base payment
to participant health care providers on quality measures, and does not
satisfy the financial risk criteria because it does not involve
requiring participating APM Entities to bear risk for monetary losses
of more than nominal amounts under the APM and is not a Medical Home
Model expanded under section 1115A(c) of the Act. The MFN Model also
will not qualify as a MIPS APM, because it does not hold participant
health care providers financially accountable for both the cost and
quality of care provided to Medicare beneficiaries.
K. Interaction With Other Federal Programs
The MFN Model may have impacts on other federal programs, such as
Medicaid, the 340B Program, the Veterans Health Administration, the
Department of Defense, the Public Health Service, the Coast Guard, and
Medicare.
1. Impact on Medicaid
a. Impact on Medicaid ``Best Price''
With respect to single source or innovator multiple source drugs
(which Medicaid recognizes to include biologicals), the term ``Medicaid
Best Price'' is the lowest price available from the manufacturer during
the rebate period to any wholesaler, retailer, provider, health
maintenance organization, non-profit entity or governmental entity
within the U.S. with certain exclusions. That is, a manufacturer's best
price determination represents the lowest price available from the
manufacturer during a rebate period (a quarter) to best price eligible
entities or purchasers in the U.S. only.
Since the MFN Drug Payment Amount will be paid to MFN participants
for each MFN Model drug as a Medicare payment, and it will not be a
``price available from the manufacturer,'' the MFN Drug Payment Amounts
themselves will not be included in the manufacturer's determination of
best price. However, in order for MFN participants to purchase MFN
Model drugs at prices that does not lead to financial loss, the
manufacturer will need to make available prices that are competitive
with the MFN Drug Payment Amounts. We expect that the MFN Drug Payment
Amounts will likely drive manufacturer drug prices available to MFN
participants down over the course of the model, and the model may
indirectly impact a manufacturer's best price to the extent that a
manufacturers' U.S. best price will be lower than what it would be
otherwise. In other words, if during the course of the MFN Model,
market forces result in manufacturers reducing prices available to MFN
participants, such available prices to MFN participants will be
considered in a manufacturer's determination of best price and could
potentially lower best price and possibly increase Medicaid rebates.
Specifically, if the manufacturer lowers prices available to an MFN
participant at or below the MFN Drug Payment Amount, such prices will
be considered in the manufacturer's determination of best price and may
reset the manufacturer's best price if the reduced price is lower than
the manufacturer's best price that would otherwise apply. This is
particularly possible because the MFN Drug Payment Amount, which is
expected to be lower than the payment amounts for the same drugs
outside of the model, will include the impact of pricing outside of the
U.S., which is typically lower than prices in the U.S., and will likely
impact the prices made available by the manufacturer in the U.S.
b. Impact on Average Manufacturer Price (AMP)
AMP is defined at section 1927(k)(1) of the Act. Generally, AMP is
determined based on the average price paid to the manufacturer for a
covered outpatient drug in the U.S. by wholesalers for drugs
distributed to retail community pharmacies and retail community
pharmacies that purchase drugs directly from the manufacturer with
certain exclusions. Because the MFN Model will focus on certain Part B
drugs that are furnished in the outpatient setting and these drugs are
most likely injected or infused, the AMP for an MFN Model drug is
likely determined using the AMP computation for 5i drugs,\73\ which
includes sales that are not generally dispensed through retail
community pharmacies (see section 1927(k)(1)(B)(i)(IV) of the Act, 42
CFR 447.504(d)), such as sales to physicians, pharmacy benefit managers
(PBMs) and hospitals. Thus, a manufacturer's sales of MFN Model drugs
to MFN participants (or price paid by MFN participants) will be
included in the AMP or 5i AMP. If, as described in section III.K.1.a.
of this IFC, the manufacturer lowers prices available to an MFN
participant at or below the MFN Drug Payment Amount, the manufacturer's
AMP for an MFN Model drug may be lower. If a drug's AMP decreases, it
may result in potentially lowering the applicable Medicaid drug rebate
paid (the rebate, in part, is based on a percentage of AMP). However,
the MFN Model may also lower a manufacturer's best price for an MFN
Model drug as previously discussed. The resulting effect on the
Medicaid
[[Page 76229]]
drug rebate will depend upon the relationship of any AMP change and any
best price change.
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\73\ Inhalation, infusion, instilled, implanted or injectable
drugs.
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We also note that if the AMP for an MFN Model drug is lowered it
may be more likely that, in accordance with section 1847A of the Act,
the Inspector General may find that the ASP for an MFN Model drug
exceeds the AMP for such drug, and that the circumstances in which 103
percent of AMP is substituted for ASP in CMS's determination of the
non-model payment allowance for such drug would occur. We refer readers
to section III.L. of this IFC for a discussion of excluding units of
MFN Model drugs from manufacturers' ASP, which may also increase the
likelihood that the ASP for an MFN Model drug will be greater than the
AMP for such drug.
2. Interaction With 340B Program
The Health Resources and Services Administration (HRSA) administers
the 340B Drug Pricing Program that allows certain hospitals and other
health care providers (``covered entities'') to obtain discounted
prices on ``covered outpatient drugs'' (as defined at 1927(k)(2) of the
Act) from drug manufacturers. HRSA calculates a 340B ceiling price for
each covered outpatient drug, which represents the maximum price a
manufacturer can charge a covered entity for the drug that is provided
to an eligible patient. Several types of hospitals as well as clinics
that receive certain federal grants from the HHS may enroll in the 340B
program as covered entities. Such entities will be included in the MFN
Model and will be subject to the MFN Model payment test. That is, these
340B covered entities will be MFN participants and receive the MFN Drug
Payment Amount and alternative add-on payment. To the extent these
entities receive payment under the model that is lower than their
current Medicare payment, there may be fewer resources available for
their 340B program activities.
Under the MFN Model, MFN participants will be paid for MFN Model
drugs according to the payment approach discussed in section III.E. of
this IFC. If the MFN participant is a 340B covered entity, the drug
portion of the model payment will be the lower of the MFN Drug Payment
Amount or the non-model payment amount paid to 340B covered entities
for 340B drugs under the OPPS for the MFN Model drug for that
corresponding calendar quarter. The MFN alternative add-on payment will
be paid to MFN participants that are 340B covered entities in the same
way as MFN participants that are non-340B covered entities.
We are including certain 340B covered entities in the MFN Model in
order to test the innovative payment approach, including the
alternative (per-dose) add-on payment amount, broadly. MFN participants
that are 340B covered entities may need to enhance their direct
contracting with manufacturers in order to obtain MFN Model drugs
within the MFN Drug Payment Amount. Our analyses estimate that 340B
covered entities will realize a total add-on percentage amount of 4.5
percent in the first year of the model due to the mix of MFN Model
drugs they historically furnish. The amount of the alternative add-on
that 340B entities realize will be an increase in revenue compared to
their historical baseline. However, these entities will face the same
or increased burden from model participation. Thus, we believe the
modest increase in add-on revenue that will be paid to these entities
through the alternative add-on payment approach will potentially be
offset through higher facility costs for acquiring included drugs (for
example, higher costs for direct contracting). Programs that support
vulnerable Americans are a vital safety net. We refer readers to
section III.C. of this IFC where we discuss providers and suppliers
that will be MFN participants. We discuss potential impacts on 340B
covered entities in more detail in section VI. of this IFC.
a. Impact on 340B Ceiling Price
Covered entities that enroll in the 340B Program can purchase
covered outpatient drugs at no more than a ``ceiling price,'' which is
calculated as AMP minus Medicaid unit rebate amount. We note that a
ceiling price is just a ceiling; some 340B hospitals can obtain covered
outpatient drugs at less than the ceiling price. Since the Medicaid
unit rebate amount is based partly on AMP minus best price, to the
extent the MFN Model affects a drug's AMP and best price, the 340B
prices will be affected. We discuss the potential impacts on a drug's
AMP and best price in section III.K.1. of this IFC.
3. Interaction With Medicare
a. Medicare Part B
As discussed in section VI. of this IFC, we believe the MFN Model
will result in lower Medicare spending for MFN Model drugs, including
lower program spending and lower beneficiary cost-sharing, and in
overall reduced Medicare Part B Trust Fund expenditures, which in turn
will lower Medicare FFS expenditures and beneficiaries' Part B
premiums.
As discussed in section III.K. of this IFC, manufacturers' ASPs for
MFN Model drugs may be higher or lower than they otherwise would be
absent the MFN Model. In turn, non-model Medicare Part B FFS payment
for MFN Model drugs could be higher or lower. We are excluding from the
calculation of the manufacturer's ASP any units of an MFN Model drugs
furnished to MFN beneficiaries and billed by MFN participants. Thus,
during the MFN Model, manufacturers' ASPs for MFN Model drugs could be
higher or lower than they might be absent the model, resulting in
Medicare payments to providers and suppliers that are not MFN
participants that would be higher or lower than what the payments would
have been absent the model.
We note that if the AMP for an MFN Model drug is lowered it may be
more likely that, in accordance with section 1847A of the Act, the
Inspector General may find that the ASP for an MFN Model drug exceeds
the AMP for such drug, and that the circumstances in which 103 percent
of AMP is substituted for ASP in CMS's determination of the non-model
payment allowance for such drug would occur.
b. Medicare Advantage
Medicare Advantage (MA) plans will not be MFN participants. We note
that when MA plans pay non-contracted, out of network providers who
have administered an MFN model drug to an enrollee, the amount paid
will be based on the non-model Medicare FFS payment amount (that is,
the amount that MA plans pay to these providers will not be the MFN
Model payment amounts).
As discussed in section VI. of this IFC, we expect the MFN Model
will lower overall Medicare FFS expenditures; that is, Medicare Part B
MFN Drug Payment Amounts will be lower than such payment would be
absent the model, the Medicare Part B alternative add-on payments will
be greater than such payment would be absent the model, there could be
increases in Medicare Part A spending, and taken together the model
will result in an overall reduction in Medicare expenditures. The
overall decrease in Medicare FFS expenditures will be considered in
determining the historical FFS claims experience for calculating the
rates for plan service areas. Payments to Medicare Advantage
Organization plans are anticipated to be lower than they would be
absent the model. At a high level, the FFS
[[Page 76230]]
component of the non-ESRD MA rates is based on the product of the
projected national per-capita spending and a county-level relative cost
index. Thus, the MA ratebook calculations will reflect changes in
actual FFS spending due to the impact of the MFN Model. We note that
this approach is consistent with treatment of payments made under other
CMS Innovation Center models and the Medicare Shared Savings Program.
As discussed in more detail in section VI. of this IFC, we estimate
that total payments to MA plans over the 7-year course of the model
will be substantially lower as a result of reduced FFS spending under
the MFN Model, that is, total payments to MA plans may be approximately
$49.6 billion lower in the OACT estimate and $28.5 billion lower in the
ASPE estimate. We note that there is much uncertainty around the
assumptions for these estimates.
L. Exclusion of Certain MFN Model Sales From Manufacturers' Calculation
of ASP for MFN Model Drugs
In accordance with sections 1847A and 1927(b)(3)(A)(iii) of the
Act, manufacturers 74 75 submit ASP data for their products
to CMS on a quarterly basis. The manufacturer's ASP is based on sales
to all purchasers in the U.S. with limited exceptions (that is,
exclusions are limited to sales exempt from best price (as defined in
section 1927(c)(1)(C)(i) of the Act), sales at a nominal charge, and
units sold to a CAP vendor), and is net of discounts such as volume
discounts, prompt pay discounts, cash discounts, free goods that are
contingent on any purchase requirement, chargebacks, and rebates (other
than certain rebates specified in section 1927 of the Act). Specific
ASP reporting requirements are set forth in section 1927(b)(3) of the
Act. In accordance with sections 1847A and 1927(b)(3) of the Act,
manufacturers report most ASP data by National Drug Code (NDC), which
identifies products in terms of the labeler, product, and package size
and type. The reported ASP data are used to establish the Medicare
payment amounts. In general, Medicare's payment limit for most
separately payable Part B drugs is based on the methodology in section
1847A of the Act, that is, 106 percent of the volume-weighted average
of manufacturers' ASP for a drug (at the billing and payment code
level), and is updated quarterly. The payment requirements in section
1847A of the Act will be waived for purposes of testing the MFN Model
as discussed in section III.M.1. of this IFC, but will continue to
apply outside of the model as discussed in this section.
---------------------------------------------------------------------------
\74\ For the purposes of reporting under section 1847A of the
Act, the term ``manufacturer'' is defined in section 1927(k)(5) of
the Act and means any entity engaged in the production, preparation,
propagation, compounding, conversion or processing of prescription
drug products; either directly or indirectly by extraction from
substances of natural origin, or independently by means of chemical
synthesis, or by a combination of extraction and chemical synthesis;
or in the packaging, repackaging, labeling, relabeling, or
distribution of prescription drug products. The term manufacturer
does not include a wholesale distributor of drugs or a retail
pharmacy licensed under State law. However, manufacturers that also
engage in certain wholesaler activities are required to report ASP
data for those drugs that they manufacture. Note that the definition
of manufacturers for the purposes of ASP data reporting includes
repackagers.
\75\ Manufacturer is also defined in 42 CFR 447.502.
---------------------------------------------------------------------------
Section 1115A of the Act authorizes the CMS Innovation Center to
test innovative payment and service delivery models to reduce program
expenditures, while preserving or enhancing the quality of care
furnished to beneficiaries. The MFN Model will test an alternative
approach for determining Medicare's payment limit for MFN Model drugs,
which will phase down the Medicare payment amount for selected Part B
drugs to more closely align with available international prices, and
test an alternative add-on payment. Under the MFN Model, the model's
payment test will apply when Medicare makes separate payment for an MFN
Model drug that was furnished on an outpatient basis by an MFN
participant to an MFN beneficiary within the model's nationwide
geographic area.
In designing the MFN Model, we considered ways to mitigate
potential impacts on manufacturers' ASPs stemming from price
concessions given to MFN participants for purchases related to the MFN
Model and on Medicare payment for units of MFN Model drugs that are not
subject to the MFN Model payment test. For example, sales to MFN
participants may include larger price concessions than are typical
today, resulting in lower net sales prices as compared to what net
sales prices would be absent the MFN Model. As such, the manufacturer's
ASP for an MFN Model drug, which will reflect the average price for all
non-excluded sales--including sales to MFN participants to the extent
applicable--may be lower than the manufacturer's ASP would be absent
the MFN Model. Because CMS will base the non-model Medicare payment
limit for an MFN Model drug on 106 percent of the manufacturer's ASP,
payment to providers and suppliers for such drug outside of the model
may be lower than it otherwise would be absent the MFN Model. To
conduct the MFN Model test it is necessary to minimize this potential
spillover effect for providers and supplier that are not MFN
participants to best observe the impacts of the payment change. Thus,
we will exclude from the calculation of the manufacturer's ASP any
units of MFN Model drugs billed by MFN participants where the MFN Drug
Payment Amount is based on available international drug pricing
information and Medicare Part B is the primary payer. policy will only
apply when the MFN Price is based on available international drug
pricing information. That is, the policy will not apply when there is
no available international drug pricing information and the MFN Price
is equal to the applicable ASP because there will be no concern for
spillover impacts in such cases. We are waiving requirements of section
1847A of the Act as necessary to exclude such units of MFN Model drugs
from the calculation of the manufacturer's ASP. We will also indicate
the MFN Drug Payment Amounts that are (and are not, when applicable)
based on available international drug pricing information within the
quarterly MFN Model drug pricing files posted on a CMS website.
This approach is responsive to comments we received in response to
the October 2018 ANPRM. Several commenters requested clarification
about how sales for purposes of the model would be taken into account
in computing the ASP under section 1847A of the Act. Some commenters
who expressed concern about potential spillover effects of the
potential model payment test recommended that purchases made for use
under the potential model be excluded from the ASP calculation. Based
on our interactions with stakeholders, particularly those with
experience operating chargebacks related to the 340B program, we
believe our exclusion of units of MFN Model drugs that are billed by
MFN participants and have the MFN Drug Payment Amount paid by Medicare
from manufacturers' ASPs will be feasible. Manufacturers have existing
processes and tools to exclude various prices from the calculation of
their ASPs, and excluding certain MFN Model related units of MFN Model
drugs could be similar.
Distribution management systems are employed throughout the drug
distribution system to order drugs, track sales and shipments, trace
custody, manage price and customer lists, record financial
transactions, and support other industry processes. Separate purchasing
accounts are often used to align with purchasing arrangement terms, and
[[Page 76231]]
through a process called the ``chargeback process,'' manufacturers
reduce the final drug prices to wholesalers and other distributors to
reflect the purchasing terms and contract prices that apply to the end
purchaser. End purchasers of drugs who purchase under more than one
contract use virtual inventory or replenishment purchasing tools or
business processes to manage their purchases under their various
contract arrangements. For example, a provider or supplier that belongs
to more than one group purchasing organization could use such tools or
business processes to track drug purchasing, maintain records toward
volume targets and, should the need to return a product occur, conduct
returns. However, based on stakeholder feedback, we understand that all
MFN participants are unlikely to have such tools in place. Hospitals,
particularly those that participate in the 340B program, are more
likely to currently have these tools compared to other hospitals,
physician offices and ASCs. Thus, manufacturers may establish
mechanisms to obtain information from MFN participants about the number
of units of MFN Model drugs that were furnished to MFN beneficiaries
and for which payment under Sec. 513.210 was allowed, which would
increase MFN participants' activities related to the model.
CMS also seeks to minimize the potential for excessive increases in
non-model Medicare drug payment amounts during the MFN Model. For
example, during the model, manufacturers' ASPs may increase causing a
concomitant increase in non-model Medicare drug payment amounts outside
of the model if: (1) The policy that manufacturers not include units of
an MFN Model drug billed by MFN participants where the MFN Drug Payment
Amount is paid by Medicare and Medicare Part B is the primary payer in
the manufacturer's ASP for the MFN Model drug results in higher ASPs;
or (2) manufacturers raise drug prices or lower existing discounts for
U.S. sales that are not subject to the model's payment test. Because
manufacturers will continue to have the ability to set their own drug
prices, as a behavioral response to the MFN Model, manufacturers could
raise prices for MFN Model drugs in the United States in part to make
up for price concessions that may be given to model participants.
We believe the policy for manufacturers not to include in the
manufacturer's ASP units of an MFN Model drug administered to an MFN
beneficiary and billed by MFN participants where the MFN Drug Payment
Amount applied by Medicare is based on available international drug
pricing information and Medicare is the primary payer will minimize the
potential for manufacturers to choose to increase purchase prices for
non-model participants and for MFN participants' purchases of MFN Model
drugs for use outside of the MFN Model. Additionally, we believe that
the adjustments to the MFN Price phase-in, as described in section
III.E. of this IFC, will also minimize the potential for manufacturers
to increase prices for non-model participants and non-model purchases.
We also believe this policy is necessary for a rigorous test of the
model payment for MFN drugs because price concessions tied to the model
will not lower Medicare payment when MFN Model drugs are purchased for
use outside the model, which would limit our ability to observe the
impacts of the payment change.
We will not collect the number of units that manufacturers exclude
from ASP as part of their ASP submission to CMS to avoid establishing a
new data collection effort and to minimize administrative burden for
manufacturers.
As an alternative approach, we considered whether manufacturers
should exclude from the manufacturer's ASP for the MFN Model drug price
concessions on units of an MFN Model drug billed by MFN participants
where the MFN Drug Payment Amount applied by Medicare is based on
available international drug pricing information and Medicare is the
primary payer. We believe that excluding from the manufacturer's ASP
price concessions on units of an MFN Model drug billed by MFN
participants where the MFN Drug Payment Amount applied by Medicare is
based on available international drug pricing information and Medicare
is the primary payer, and not excluding the manufacturer's ASP the
units of an MFN Model drug billed by MFN participants where the MFN
Drug Payment Amount is applied by Medicare is based on available
international drug pricing information and Medicare is the primary
payer would inappropriately raise the ASP. We believe this is the case
because those units would likely be factored into the manufacturer's
ASP calculation as undiscounted sales. Thus, this approach, while it
may be less complex, would likely lead to inappropriately higher
Medicare payment outside of the model.
We are waiving requirements in section 1847A(c) to the extent
necessary to exclude from the calculation of the manufacturer's ASP any
units of an MFN Model drug administered to an MFN beneficiary and
billed by MFN participants where the MFN Drug Payment Amount applied by
Medicare is based on available international drug pricing information
and Medicare is the primary payer. Consistent with section 1847A(c)(5)
of the Act, we will issue program instructions to further describe how
the waiver will impact manufacturers' calculation of the manufacturer's
ASP. For example, we envision that manufacturers will take reasonable
steps and make reasonable assumptions to exclude applicable units. We
note that all other existing statutory requirements and regulations
will continue to apply. For example, manufacturers who misrepresent or
fail to report manufacturer ASP data will remain subject to civil
monetary penalties, as applicable and described in sections 1847A and
1927(b) of the Act and codified in regulations at Sec. 414.806.
M. Program Waivers and Model Termination
1. Waivers of Medicare Program Requirements for Purposes of Testing the
Model
We will test the MFN Model under the authority of section 1115A of
the Act and waive certain Medicare program requirements as necessary
solely for purposes of testing the model. Under section 1115A(d)(1) of
the Act, the Secretary may waive the requirements of Titles XI and
XVIII and of sections 1902(a)(1), 1902(a)(13), 1903(m)(2)(A)(iii), and
1934 of the Act (other than subsections (b)(1)(A) and (c)(5) of such
section) as may be necessary solely for purposes of carrying out
section 1115A of the Act with respect to testing models described in
section 1115A(b) of the Act. The purpose of these waivers will be to
allow Medicare to test the MFN Model described in this IFC, with the
goal of reducing Medicare expenditures while improving or maintaining
the quality of beneficiaries' care.
In Sec. 513.500, we waive program requirements that are necessary
solely for purposes of testing the MFN Model--
Sections 1833(t)(6) and 1833(t)(14) of the Act and 42 CFR
419.62 and 419.64 related to Medicare payment amounts for drugs and
biologicals under the OPPS as necessary to permit testing of an
adjusted payment amount for MFN Model drugs using the pricing
approaches described in this IFC;
Section 1833(i)(2)(D) of the Act related to Medicare
payment to ASCs for drugs and biologicals as necessary to permit
testing of an adjusted payment
[[Page 76232]]
amount for MFN Model drugs using the pricing approaches described in
this IFC;
Sections 1847A(b) and 1847A(c) of the Act and 42 CFR
414.904 and 414.802 related to use of the ASP-based, WAC-based, or
other applicable payment methodology and calculation of manufacturers'
ASP as necessary to permit testing of an adjusted payment for MFN Model
drugs and to exclude certain units of MFN Model drugs from
manufacturers' ASPs;
Section 1833(a)(1) of the Act related to Medicare payment
portion of the allowed payment amount for an included MFN Model drug
that is determined under Sec. 513.220 as necessary to permit testing
of an innovative payment approach for the alternative add-on payment
amount;
Section 1833(a)(1)(S) related to Medicare payment for
drugs and biologicals at 80 percent of the lesser of actual charge or
the amount established in section 1842(o) of the Act as necessary to
allow CMS to not apply beneficiary cost-sharing to the alternative add-
on payment amount;
Section 1833(a)(1)(G) of the Act related to the amounts
paid with respect to facility services furnished in connection with
certain surgical procedures and with respect to services furnished to
an individual in an ASC shall be 80 percent of the lesser of the actual
charge for the services or the amount determined by the Secretary under
such revised payment system as necessary to allow CMS to not apply
beneficiary cost-sharing to the alternative add-on payment amount;
Section 1833(t) of the Act related to how Medicare payment
under the OPPS is calculated including beneficiary copayment to allow
CMS to not apply beneficiary cost-sharing to the alternative add-on
payment amount; and
Section 1833(t)(9)(B) of the Act related to the
requirement that Medicare account for adjustments to ensure that the
amount of expenditures under the OPPS for the year does not increase or
decrease from the estimated amount of expenditures under the OPPS that
would have been made if the adjustments had not been made (that is,
OPPS budget neutrality). CMS intends to continue to maintain budget
neutrality under the OPPS as it currently does, including as described
in 42 CFR 419.32(d)(1). This includes continuing to use the applicable
payment amount for each separately payable drug under that payment
system, rather than the MFN Drug Payment Amount and alternative add-on
payment amount. CMS may consider using volume for drugs included in the
MFN Model for purposes of the budget neutrality calculations under the
OPPS beginning in 2022, but would utilize the applicable OPPS payment
amount for the drug or biological, rather than the MFN Drug Payment
Amount. We believe a waiver of the OPPS budget neutrality requirements
for Part B drugs furnished under the MFN Model is necessary solely for
purposes of testing the MFN Model because if reductions in Medicare
Part B drug expenditures were redistributed through the OPPS budget
neutrality process to non-drug Part B services under the OPPS, the
model would change pricing for numerous other services that are not
related to Part B drugs. This would make it difficult to determine the
independent impact of a change in Part B drug payment levels to MFN
Model pricing if there is also a corresponding change in the payment
amount for all non-drug hospital outpatient items and services as a
result of the OPPS budget neutrality requirements.
Our intent is to include a waiver for all program requirements in
title XVIII of the Act as may be necessary solely to test separate
payment for MFN Model drugs furnished to MFN beneficiaries by MFN
participants. To the extent that MFN participants receive separate
payment for MFN Model drugs under program requirements that we have not
listed in Sec. 513.500, we waive such requirements as necessary to
effectuate part 513.
2. Model Termination
CMS may terminate the MFN Model for reasons including, but not
limited to, the following: CMS determines that it no longer has the
funds to support the model; or CMS terminates the model in accordance
with section 1115A(b)(3)(B) of the Act. As provided by section
1115A(d)(2) of the Act, termination of the model under section
1115A(b)(3)(B) of the Act is not subject to administrative or judicial
review. We are codifying these policies in Sec. 513.1000.
N. Evaluation
We will conduct an evaluation of the MFN Model, as required under
section 1115A(b)(4) of the Act. The evaluation of the MFN Model will
include an analysis of the quality of care furnished under the model
and the changes in spending under Medicare by reason of the model.
There will be several populations of interest for the MFN Model
evaluation. A population of interest for the evaluation will be
Medicare beneficiaries who are likely to receive one of the MFN Model
drugs based on recent diagnoses and/or prior treatment. One possible
prescriber behavior change due to the MFN Model could be shifts from
prescribing MFN Model drugs to other alternative Part B or Part D drugs
or vice versa. A population defined by recent diagnoses and/or prior
treatment will capture the model's impact on beneficiaries affected by
these prescribing behavioral changes due to the model. Other
populations such as, but not limited to, MFN Model drug users and
subgroups of particular patient populations (for example, cancer,
rheumatoid arthritis, ophthalmologic conditions) will be considered in
the evaluation.
For each of the populations of interest, we will create separate
impact estimates for two types of outcomes: Medicare spending and drug/
other health care utilization. Medicare spending will be examined in
terms of total Part B drug spending for MFN Model drugs, total Part B
drug spending for any Part B drugs, total Parts A and B spending, and
potentially other spending measures for specific types of health care
services (for example, inpatient hospital spending). The evaluation of
the model's impact on quality of care will examine drug access,
measured by utilization (for example, rates of any use and duration of
use) of both Part B (both MFN Model drug and non-MFN Model drugs) and
Part D drugs. We will also examine non-drug health care utilization
that may change as a result of the MFN Model to estimate any impacts on
access to care. Examples of other non-drug health care utilization
include hospitalizations, emergency department visits, and condition-
specific utilization related to a given subgroup of beneficiaries. The
impact estimates will reflect the collective effect of the MFN Model's
changes to Medicare payments and beneficiary cost-sharing for MFN Model
drugs.
Because the MFN Model will be a nationwide, mandatory model, we
must employ an evaluation design that does not require an independent
comparison group to establish the counterfactual (what would have
happened in the absence of the model). The term ``interrupted time
series'' (ITS) refers to the situation in which multiple observations
for the treatment group are available both before and after the
intervention is implemented.\76\ ITS models can be employed both with
and
[[Page 76233]]
without comparison groups, and be used to imply causality without
comparison groups.\77\ The design is used when data are available both
for the pre-intervention period and the post-intervention period, and
the intervention takes place at a specific, identifiable point in
time.\78\ The time-relationship between the data points can then be
used to estimate treatment effects. The trends from the pre-
intervention period establish a baseline that is used to project what
would be expected in the absence of the intervention. The typical ITS
approach assumes linear trends before and after the intervention, but
ITS models can be made more general to address potential non-linear
trends.79 80 Intervention effects are demonstrated when
observations gathered after the intervention start period deviate from
the baseline projections.
---------------------------------------------------------------------------
\76\ Wagner, A.K., Soumerai, S.B., Zhang, F. and Ross-Degnan, D.
(2002), Segmented regression analysis of interrupted time series
studies in medication use research. Journal of Clinical Pharmacy and
Therapeutics, 27: 299-309. doi: 10.1046/j.1365-2710.2002.00430.x.
\77\ Sheingold, S., Bir, A, (2019), Evaluation for Health Policy
and Health Care: A Contemporary Data Driven Approach, Sage
Publications.
\78\ Bernal, J.L., Cummins, S., Gasparrin, A., (2017)
Interrupted time series regression for the evaluation of public
health interventions: A tutorial, International Journal of
Epidemiology, 2017, Vol. 46, No. 1: 348-355, doi: 10.1093/ije/
dyw098.
\79\ Kontopantelis, E., Doran, T., Springate, D.A., Buchan, I
Reeves, D, (2015), Regression based quasi-experimental approach when
randomisation is not an option: Interrupted time series analysis,
BMJ 2015;350:h2750, doi: 10.1136/bmj.h2750.
\80\ Valsamis, E.M., Ricketts, D., Husband, H., and Rogers, B.A.
(2019), Segmented linear regression models for assessing change in
retrospective studies in healthcare. Computational and Mathematical
Methods in Medicine. doi: 10.1155/2019/9810675.
---------------------------------------------------------------------------
Using this design for evaluating the effects of an intervention--
that is, implying a causal relationship between the intervention and
its target outcomes--relies on a strict set of conditions. As
previously described, when there is no comparison group, the
counterfactual is established as the continuation of the pre-
intervention trend for the treated group. The intervention impact is
estimated as the difference between the actual post-intervention trend
and the pre-intervention trend extended.
The most common statistical method for analyzing ITS data is called
segmented regression.81 82 Segmented regression focuses on
two parameters, the level (intercept) and the trend (slope). For
observations before the model, we will have a level (intercept) and
trend (slope). After the model begins, the data may exhibit changes in
any one of these features. The fundamental idea behind segmented
regression is to estimate a regression specification with a linear
trend for the data points before the model and estimate a regression
specification with a linear trend for the data points after the model
start. The level and trend before and after the model start will then
be compared. We will use quarterly observations for the pre- and post-
model start time periods ending with the most recent data that will be
currently available. Given the MFN Model design, we provide our
specification in this section of this IFC for the longitudinal
regression using a more general specification of the trends to capture
the non-linear nature of the data.
---------------------------------------------------------------------------
\81\ Wagner, A.K., Soumerai, S.B., Zhang, F. and Ross-Degnan, D.
(2002), Segmented regression analysis of interrupted time series
studies in medication use research. Journal of Clinical Pharmacy and
Therapeutics, 27: 299-309. doi: 10.1046/j.1365-2710.2002.00430.x.
\82\ Valsamis, E.M., Ricketts, D., Husband, H., and Rogers, B.A.
(2019), Segmented linear regression models for assessing change in
retrospective studies in healthcare. Computational and Mathematical
Methods in Medicine. doi: 10.1155/2019/9810675.
---------------------------------------------------------------------------
In the longitudinal regression equation provided in this section of
this IFC, the vector Xit consists of factors that will
change from the pre-model time period to the model performance period
and may include, but is not necessarily limited to, the medical care
component of the Consumer Price Index (CPI-U), national unrelated
policy changes, economic factors (for example, unemployment rate). The
unit of analysis (for example, a hospital referral region (HRR) as
defined by the Dartmouth Atlas \83\ or beneficiary) on which the
quarterly observations are measured will be allowed to vary in order to
estimate the model's impact at these different levels of aggregation.
The anticipated statistical model specification includes a polynomial
time trend variable f(t) to account for trends in spending and
utilization over time. In addition, the statistical model includes
separate indicator variables (It=k) for each of the model
performance period quarters, which will allow for estimates of the
model's impact in each performance period quarter relative to the
entire pre-period after adjusting for the time trend and other factors.
---------------------------------------------------------------------------
\83\ https://www.dartmouthatlas.org/faq/#research-methods-faq.
Yit = b0 + b1 [middot] Xit
+ b2 [middot] f(t) + a1 [middot] It=1
+ a2 [middot] It=2 + a3 [middot]
It=3 + a4 [middot] It=4 + . . . +
---------------------------------------------------------------------------
uit
Where:
Yit = outcome (see the previous section for cost and
utilization measures), for a particular unit of analysis in a
specific quarter
Xit = vector of adjustment factors
f(t) = polynomial function to account for time trend
It=k = denotes an indicator for time period k (all after
model implementation)
uit = unaccounted variation
i = unit of analysis (for example, beneficiary, HRR)
t = time quarter (-12, -11 . . . 0, 1, 2, 3 . . .) using a 3 year
pre-model time period, with 0 indicating the start of the model
b0, b1, b2, a1 . . . .
an are the statistical model coefficients
b0 = the statistical model intercept
b1 = vector of estimates for the adjustment factors
b2 = estimate of the time trend f(t) across the pre-
period and model performance period
a1 thru an = estimate of change per model
performance period quarter (t) relative to entire pre-period
With the statistical model specification as previously described,
in an initial, exploratory data assessment, the null hypothesis
(Ho: a1 = a2 = a3 =
a4 = . . . = an = 0) will be that there is no
change in each of the model performance period quarters when compared
to the pre-period after adjusting for the time trend and the other
factors. The corresponding alternate hypothesis (Ha:
a1 or a2 or a3 or a4 or . .
. an [ne] 0) will be that any of the model performance
period quarters is statistically significantly different than the pre-
model time period, suggesting that the model either positively or
negatively impacted Medicare spending and quality of care in at least
one model performance period quarter. These null and alternate
hypotheses will apply to each outcome and population of interest.
The assessment just described will not directly indicate success or
failure of the model. CMS will need to observe a consistent
statistically significant directional pattern over multiple consecutive
time periods for the outcome and population of interest in order to
draw sound conclusions about the model's impact. Based on a combination
of results from exploratory data assessment and policy goals, CMS will
set a hypothesis that encompasses the chosen outcome and population of
interest. This hypothesis will be tested using data that is different
from what was used in the exploratory assessment--for instance, due to
being gathered later in time or consisting of a different randomly
assigned subset of contemporaneous data.
Statistical inference will be conducted using cluster-robust
standard errors.\84\ Cluster-robust standard errors account for serial
correlation as well as spatial correlation within geographies (such as
an HRR). We will conduct hypothesis testing using an alpha-level of 5
percent
[[Page 76234]]
and CMS will report the p-value and standard error to allow for
inferences at other alpha-levels.
---------------------------------------------------------------------------
\84\ Cameron, A.C., & Miller, D.L. (2015). A practitioner's
guide to cluster-robust inference. Journal of Human Resources,
50(2), 317-372.
---------------------------------------------------------------------------
As an illustration of a potential subgroup analysis and the
expected changes that could be detected in the MFN Model evaluation,
CMS identified two groups of Medicare cancer patients using 2018 data.
CMS defined the first narrower group as Medicare cancer patients who
received an MFN Model drug. CMS defined the second broader group as
Medicare cancer patients who either received an MFN Model drug or would
have been considered eligible to receive an MFN Model drug.
Specifically, CMS estimated that in 2018 approximately 400,000 Medicare
beneficiaries were being treated for the most prevalent cancer types
(that is, colorectal, endometrial, breast, lung, prostate, and certain
forms of leukemia and lymphoma) and received an MFN Model drug. These
400,000 Medicare beneficiaries were identified using the inclusion and
exclusion criteria for the model, including the use of an MFN Model
drug. Cancer treatment was determined by the utilization of Part B and/
or Part D cancer drugs and the presence of cancer diagnosis codes on
Parts A and B claims. A subgroup analysis that requires MFN Model drug
use, as in the narrower definition that identified 400,000 Medicare
beneficiaries being treated for cancer and who received an MFN Model
drug, would exclude cancer patients using an alternative non-MFN Model
drug cancer therapy. A broader cancer population definition based on
any Part B and/or Part D cancer drug use or just an incident cancer
diagnosis based on new evidence of diagnosis codes on Parts A and B
claims in the current year would capture the model's impact on
beneficiaries affected by prescribing behavioral changes due to the
model. This second broader cancer subgroup population definition
applied to approximately 1.1 million Medicare beneficiaries in 2018.
CMS believes that looking for unintended consequences will be
critical for the monitoring and evaluation of the MFN Model. In the
narrower definition of the cancer subgroup, CMS expects that
approximately 100,000 Medicare cancer patients who receive a MFN Model
drug will be eligible for inclusion in the quarterly evaluation
analysis. In the broader cancer subgroup population, CMS expects that
approximately 280,000 Medicare cancer patients will be included in the
quarterly evaluation analysis. With a nationwide MFN Model (and the
assumptions of an alpha-level of 5 percent and power of 80 percent),
CMS will have the sample sizes needed in these two populations to
detect small changes in Medicare total cost of care (approximately a 1
percent change), drug access, and other important measures of quality
of care. With multiple quarterly assessments of the impact of the model
on subgroup populations, CMS will be able to intervene early in the
model's performance period should any potential unintended consequences
be detected in the potential subgroups of interest. Although CMS uses
the cancer subgroup patient population in the previously discussed
example, we recognize that other patient populations (for example,
patients diagnosed with rheumatoid arthritis and wet macular
degeneration) and certain types of providers could be differentially
impacted by the MFN Model. These other patient and provider subgroups
will be of interest in the evaluation. The model's impact on the
Medicaid program and commercial insurance (including Medicare
Advantage) population is also of interest.
The evaluation will explore the experiences of MFN participants
(beneficiaries and providers) and other stakeholders affected by the
changes in payment and conditions included in the model. In particular,
CMS will interview MFN participants and beneficiaries, either by focus
groups, surveys, or one-on-one stakeholder interviews, to assess the
model's influence on access to and quality of care, and administrative
burden from their perspectives. Further, CMS intends to ask
beneficiaries about their total out of pocket costs under the MFN Model
to determine if those costs were reduced. MFN participants will be
asked for their opinions about the MFN Model's payment changes to the
drug and add-on payment amounts separately. The evaluation will also
include qualitative analyses of primary data collected from MFN
participants and beneficiaries. The results of the qualitative analyses
will be used to provide additional context for the results of the
quantitative analyses on health care spending and to help further
explain the observed changes.
Evaluation reports detailing the results and findings will be
developed and publicly posted on the CMS website. The evaluation
reports will include the results of the quantitative and qualitative
analyses of the MFN Model's impact on spending and quality of care and
the model's implementation as described in this section. The evaluation
reports covering the earlier performance years of the MFN Model will be
used in the decision making process on whether or not to continue the
MFN Model into performance years 5 to 7.
The evaluation may require that MFN participants collect and submit
additional data specifically for the evaluation (please see Sec.
513.100(e) and Sec. 513.100(f)). Such requirements for additional data
to carry out model evaluation will be in compliance with 42 CFR
403.1110(b), which requires entities participating in the testing of a
model under section 1115A to collect and report such information,
including protected health information (as defined at 45 CFR 160.103),
as the Secretary determines is necessary to monitor and evaluate the
model.
O. Limitations on Review
In Sec. 513.450, we are codifying the preclusion of administrative
and judicial review under section 1115A(d)(2) of the Act. Section
1115A(d)(2) of the Act states that there is no administrative or
judicial review under section 1869 or 1878 of the Act or otherwise for
the all of the following:
The selection of models for testing or expansion under
section 1115A of the Act.
The selection of organizations, sites, or participants to
test models selected.
The elements, parameters, scope, and duration of such
models for testing or dissemination.
Determinations regarding budget neutrality under section
1115A(b)(3) of the Act.
The termination or modification of the design and
implementation of a model under section 1115A(b)(3)(B) of the Act.
Determinations about expansion of the duration and scope
of a model under section 1115A(c) of the Act, including the
determination that a model is not expected to meet criteria described
in paragraph (1) or (2) of such section.
We interpret the preclusion from administrative and judicial review
regarding the CMS Innovation Center's selection of organizations,
sites, or participants to test models selected to preclude from
administrative and judicial review CMS' selection of an MFN
participant, as well as CMS' decision to terminate an MFN participant,
as these determinations are part of CMS' selection of participants for
CMS Innovation Center model tests.
We interpret the preclusion from administration and judicial review
regarding the elements, parameters, scope, and duration of models for
testing or dissemination to preclude from administrative and judicial
review the following CMS determinations made in connection with the MFN
Model:
[[Page 76235]]
The selection of the model geographic area for the MFN
Model by CMS;
The selection of MFN Model drugs by CMS; and
The selection of included international data, including
selection of countries, international drug pricing databases, and
international drug pricing information.
In addition, we interpret the preclusion from administrative and
judicial review regarding the elements of the MFN Model to preclude
from administrative and judicial review the methodology for determining
MFN Prices, MFN Drug Payment Amounts, Alternative Add-on Amounts, and
reconciliation payments related to financial hardship exemptions.
V. Collection of Information Requirements
As stated in section 1115A(d)(3) of the Act, Chapter 35 of title
44, United States Code, shall not apply to the testing and evaluation
of CMS Innovation Center Models. As a result, the information
collection requirements contained in this IFC need not be reviewed by
the Office of Management and Budget. However, costs incurred through
information collections are included in section VI.C.5. of this IFC.
V. Response to Comments
Because of the large number of public comments we normally receive
on documents, we are not able to acknowledge or respond to them
individually. We will consider all comments we receive by the date and
time specified in the DATES section of this preamble, and, when we
proceed with a subsequent document, we will respond to the comments in
the preamble to that document.
VI. Regulatory Impact Analysis
A. Statement of Need
This IFC is necessary to address the current Medicare Part B
payment system for separately payable Medicare Part B drugs, which has
several features that may be incentivizing avoidable costs and causing
greater utilization of higher priced drugs. By testing ways to address
these payment issues, the MFN Model seeks to improve quality of care,
address features of the current payment system that may be
incentivizing unnecessary Medicare Part B drug spending and utilization
of high cost drugs, and ensure that the Medicare program and its
beneficiaries pay generally comparable prices for Medicare Part B drugs
relative to certain other countries.
As detailed in section III of this IFC, this IFC will establish a
7-year nationwide MFN Model alternative payment test for approximately
50 separately payable Medicare Part B drugs furnished by certain
providers and suppliers. As discussed in section III.C. of this IFC,
MFN participants will include Medicare-participating providers and
suppliers that furnish MFN Model drugs, with certain exclusions. Most
of the MFN participants will be: Physicians; non-physician
practitioners; supplier groups; HOPDs (including on- and off-campus
outpatient provider-based departments, but excluding cancer hospitals,
children's hospitals, CAHs, and other hospitals exempt from the OPPS);
and ASCs. When other providers and suppliers that are not excluded bill
for separately payable MFN Model drugs (for example, pharmacies and
independent diagnostic testing facilities), they will be included in
the MFN Model as MFN participants; based on 2018 Medicare Part B claims
data, their aggregate annual volume of separately payable Part B drugs
was less than $3.6 million. MFN participants will be subject to the
participation requirements described in section III. of this IFC.
B. Overall Impact
We have examined the impacts of this IFC, as required by Executive
Order 12866 on Regulatory Planning and Review (September 30, 1993),
Executive Order 13563 on Improving Regulation and Regulatory Review
(February 2, 2013), the Regulatory Flexibility Act (RFA) (September 19,
1980, Pub. L. 96-354), section 1102(b) of the Act, section 202 of the
Unfunded Mandates Reform Act of 1995 (UMRA) (March 22, 1995, Pub. L.
104-4), Executive Order 13132 on Federalism (August 4, 1999), and the
Congressional Review Act (5 U.S.C. 804(2)), and Executive Order 13771
on Reducing Regulation and Controlling Regulatory Costs (January 30,
2017).
Executive Orders 12866 and 13563 direct agencies to assess all
costs and benefits of available regulatory alternatives and, if
regulation is necessary, to select regulatory approaches that maximize
net benefits (including potential economic, environmental, public
health and safety effects, distributive impacts, and equity). Section
3(f) of Executive Order 12866 defines a ``significant regulatory
action'' as an action that is likely to result in a rule: (1) Having an
annual effect on the economy of $100 million or more in any 1 year, or
adversely and materially affecting a sector of the economy,
productivity, competition, jobs, the environment, public health or
safety, or state, local or tribal governments or communities (also
referred to as ``economically significant''); (2) creating a serious
inconsistency or otherwise interfering with an action taken or planned
by another agency; (3) materially altering the budgetary impacts of
entitlement grants, user fees, or loan programs or the rights and
obligations of recipients thereof; or (4) raising novel legal or policy
issues arising out of legal mandates, the President's priorities, or
the principles set forth in the Executive Order. This IFC triggers
these criteria.
A regulatory impact analysis (RIA) must be prepared for major rules
with economically significant effects ($100 million or more in any 1
year). We estimate that this rulemaking is ``economically significant''
as measured by the $100 million threshold and hence also a major rule
under the Congressional Review Act. Accordingly, we have prepared a RIA
that, to the best of our ability, reflects the economic impact of the
policies contained in this IFC.
C. Detailed Economic Analysis
The MFN Model will test different payment rates for certain
separately payable Medicare Part B drugs and their associated drug add-
on payment. The payment rates for these Medicare Part B drugs will be
phased in over 4 years, ultimately arriving at the lowest price for a
particular drug from a selected group of countries. Eligible providers
and suppliers participating in the 340B program will be paid the lesser
of this amount or the payment outside the model for MFN Model drugs
they purchase under the 340B program. This IFC includes a single
alternative add-on payment, with MFN participants receiving an amount
that represents 6 percent (after sequestration) of the average sales
price (ASP) baseline for the initial set of included drugs trended
forward. The phased-in MFN Price discount relative to applicable ASP is
shown in Table 9, assuming the relationship remains constant.
[[Page 76236]]
Table 9--Most Favored Nation Discount From ASP by Calendar Year
----------------------------------------------------------------------------------------------------------------
Calendar year 2021 2022 2023 2024 2025 2026 2027
----------------------------------------------------------------------------------------------------------------
MFN Price impact............ -16% -33% -49% -65% -65% -65% -65%
----------------------------------------------------------------------------------------------------------------
The model will require participation by eligible providers and
suppliers for the selected separately payable Medicare Part B drugs
included in the model. Certain provider types, defined previously in
this IFC, will be excluded from the model. We assume that acute care
hospitals that are paid for outpatient hospital services on a fully
capitated or global budget basis under a waiver under such model of
section 1833(t) of the Act will be excluded from the MFN Model.
Because current payment rates for 340B covered entities that are
paid under the OPPS (hereafter called 340B providers) are different
from those for other providers and suppliers (hereafter called non-340B
providers), the impact of the MFN Model varies between the two provider
types, and therefore OACT and ASPE estimated the financial impacts
separately. Similarly, both analyses calculated the impact of the drug
add-on payment separately from the MFN Price impact. Since the drug
add-on payment inside the model will not be subject to beneficiary cost
sharing, and will be an additional payment to 340B covered entities,
the associated Medicare expenditures are higher.
The baseline for these analyses is shown in Table 10, separately
for OPPS 340B providers, OPPS non-340B providers, and physician
settings. These values include all drugs, exclude providers and
suppliers that are exempt from the model, and assume that 53% of the
hospital outpatient claims will be from 340B providers. These payments
were then adjusted for beneficiary responsibility, add-on payments, and
federal payments relative to ASP. These values are on a pre-COVID-19
basis, and the baseline is not are adjusted for the effects of the
pandemic. Similarly, the impact analysis does not include the effects
of the COVID-19 pandemic. Many assumptions such as utilization,
mortality, and morbidity are more uncertain than usual due to the
pandemic. The direction and magnitude of the financial impact of the
pandemic on Part B drug spending is uncertain. For example, higher
mortality due to COVID-19 could lead to lower drug utilization. A
COVID-19-related drug discovery could lead to higher drug utilization.
Beneficiaries seeking treatment for quality of life improvement may
defer care during the pandemic.
Table 10--Baseline Expenditures for Claims Included in the MFN Model
----------------------------------------------------------------------------------------------------------------
(In billions)
----------------------------------------------------------------------------------
2020 2021 2022 2023 2024 2025 2026 2027 2020-27
----------------------------------------------------------------------------------------------------------------
OPPS Non-340B Providers...... $6.1 $6.7 $7.5 $8.3 $9.2 $10.1 $11.2 $12.3 $71.4
OPPS 340B Providers.......... 6.9 7.6 8.4 9.4 10.4 11.4 12.6 13.9 80.5
Other Providers and Suppliers 19.4 21.2 23.3 25.7 28.1 30.8 33.8 37.0 219.3
----------------------------------------------------------------------------------
Total.................... 32.4 35.5 39.2 43.4 47.6 52.4 57.5 63.2 371.3
----------------------------------------------------------------------------------------------------------------
As the model does not dictate the price that a drug manufacturer
must charge an MFN participant, there are many possible behavioral
responses by manufacturers, providers, suppliers, and beneficiaries.
Because the estimates are highly sensitive to these behavioral
assumptions, OACT provided three scenarios: (i) An OACT estimate; (ii)
an illustrative estimate based on pricing-effects only; and (iii) an
additional illustration under the assumption that manufacturers will
refuse to change prices and MFN participants will be unwilling to
administer drugs for which model payment will be below their
acquisition cost. ASPE also developed a bottom-up estimate built from
analysis of the IFC's likely potential effects on different types of
separately payable Part B drugs.
To better understand the values shown in the three OACT scenarios,
the ASPE estimate, and the policy of the model, consider the following
example. Suppose the current ASP for a given drug is $100. The total
payment to the provider for this drug under the current system is
$104.30, inclusive of the federal payment for the drug and the add-on,
beneficiary cost-sharing, and net of sequestration. Now suppose the MFN
Price of this drug is also $100. The total payment to the provider
under the model would be $104.40. Under the model, the drug payment
after sequestration is unchanged ($98.40) but the add-on increases from
$5.90 to $6.00.
1. OACT Estimate
Manufacturers could adopt several strategies in response to the
model, such as (i) charging a lower price to providers and suppliers
inside the model; (ii) refusing to adjust their price from the non-
model amounts; or (iii) altering the availability and terms of their
international prices. Given that the international price data represent
a challenge to their U.S. market revenues, manufacturers are expected
to devote considerable resources to the third option. This assumption
is included in the OACT estimate as a different discount relative to
ASP compared with the values in Table 9. For drugs with significant use
outside of Medicare, manufacturers may be willing to sacrifice
utilization and revenue within the model. For drugs that are used
primarily in the Medicare program, manufacturers may believe that
offering some pricing relief is necessary to preserve a significant
portion of their revenue.
Eligible providers and suppliers will need to decide if the
difference between the amount that Medicare will pay and the price that
they must pay to purchase the drugs would allow them to continue
offering the drugs. For 340B providers, the payment rates in the first
year will match their payments outside the model. Accordingly, no
change to utilization or costs is expected under the model in the first
year for 340B providers. In later years, the impact varies depending on
the assumed change to international price data. For non-340B providers,
some may be
[[Page 76237]]
willing to provide the drugs under a lower payment rate to retain
utilization on other associated services.
Should an eligible provider or supplier be unable to offer access
to the included drugs, beneficiaries will be left with several options.
They could seek access to the drugs by traveling to an excluded
provider or supplier, access the drugs through a 340B provider in the
model, or forgo access.
It should be noted that this model does not have a reliable
precedent in the U.S. market; consequently, there is an unusually high
degree of uncertainty in these assumptions, particularly with respect
to the behavioral responses. To illustrate this uncertainty, three
potential financial effects are included in this analysis; a full range
of potential behavioral effects are presented under an Extreme
Disruption scenario where non-340B utilization of affected drugs drops
to zero percent and under a Pricing-Effects Only scenario where all
currently projected utilization is assumed to be retained. The OACT
estimate reflects one reasonable set of assumptions for potential
changes in manufacturer, provider, and supplier behavior. Other
estimates outside the range of the three scenarios could be reasonable
as well, due to the wide range of potential responses.
The OACT assumptions consider that the separately payable Medicare
Part B drugs make up approximately 5 percent of the overall U.S.
prescription drug market. Drug manufacturers could see this model as an
obstacle to their pricing throughout the market, which could cause
strong resistance to the model. The OACT assumptions reflect that some
manufacturers will adhere to their current pricing instead of lowering
sales prices in response to the model. This behavior may persist in
spite of pricing in other sectors of the market or other countries that
demonstrates an ability to offer the drug at the model payment rates,
and would result in unmet demand for these Medicare Part B drugs. After
considering the relative size of the Medicare Part B market, the
current price control of drug manufacturers, the size of the model
price reductions, the nature of the Medicare Part B drug providers and
suppliers, the flexibility that manufacturers may have in adjusting
pricing and arrangements in other countries, and many other factors,
actuarial judgment was applied to determine the assumptions that are
reflected in the OACT estimate, as shown in Table 11.
Beneficiaries lacking continued availability of their drugs through
their current provider or supplier are assumed to seek access outside
the model, to obtain their drugs through 340B providers, or to forgo
access. The schedule of the phase-in to the MFN price gives
manufacturers incentive to adjust or reduce access to international
price data quickly. Accordingly, manufacturers are assumed to raise the
published international prices beginning in 2022 and to retain a 25-
percent MFN Price discount relative to applicable ASP.
As a result of this expected behavior from manufacturers, 340B
provider payments will see a 3-percent reduction compared to the
current Medicare payment in 2022 and subsequent years. This 3-percent
reduction represents the impact of the 25-percent MFN Price discount
relative to the OPPS payment to 340B providers of ASP less 22.5
percent, as that is the current payment formula for 340B providers.
This represents a relatively small price change and is assumed to occur
later in the model, so will be more predictable than the payment
changes for non-340B providers. As a result, manufacturers and 340B
providers are assumed to come to an agreement to continue to provide
for all of their utilization.
Because all regions are covered under the model, beneficiaries
seeking a provider outside of the model will be limited to an excluded
provider or supplier, such as a critical access hospital. Based on the
historical trend of drug spending by excluded providers and suppliers
as a percentage of total Medicare Part B drugs, the OACT estimate
reflects only 1 percent of use shifting to non-model providers.
Furthermore, because the OPPS payment to 340B providers will be reduced
year two through year seven of the model, and because their capacity is
limited, 10 percent of use is assumed to shift to 340B providers. Other
utilization not covered by providers and suppliers continuing to
provide access in the model or by excluded providers and suppliers is
assumed to be utilization not covered by the Medicare benefit.
Table 11--Assumptions Reflected in OACT Estimate
----------------------------------------------------------------------------------------------------------------
2021 2022 2023 2024 2025 2026 2027
(%) (%) (%) (%) (%) (%) (%)
----------------------------------------------------------------------------------------------------------------
Non-340B providers:
Behavior:
Continued Availability................... 80 75 70 70 70 70 70
Altered Availability:
Move to non-MFN...................... 1 1 1 1 1 1 1
Move to 340B......................... 10 10 10 10 10 10 10
No Access............................ 9 14 19 19 19 19 19
Total............................ 100 100 100 100 100 100 100
MFN Price impact................................. -16 -25 -25 -25 -25 -25 -25
340B providers:
Behavior:
Continued Availability................... 100 100 100 100 100 100 100
MFN Price impact................................. 0 -3 -3 -3 -3 -3 -3
----------------------------------------------------------------------------------------------------------------
Table 12 shows the estimated financial impacts under the model
based on the assumptions in Table 11. Medicare savings are estimated to
be $85.5 billion, net of the premium offset. While there are
significant savings as a result of this model, a portion of the savings
is attributable to beneficiaries not accessing their drugs through the
Medicare benefit, along with the associated lost utilization. This
estimate does not capture any impacts to other program costs as a
result of lower utilization. This estimate is on a pre-COVID-19 basis,
and is not adjusted for the effects of the pandemic.
To the extent that manufacturers discount their products for
Medicare sales, there may be a reduction in Medicaid Best Price or AMP.
Reductions in Best Price could result in increased Medicaid rebates and
thus lower Medicaid costs. However, reductions in AMP generally result
in
[[Page 76238]]
lower statutory and inflationary rebates under the Medicaid program.
Therefore, if the manufacturer discounts a drug so that it is closer to
the Medicaid best price, there is a possibility of increased Medicaid
costs as a result of the model. Furthermore, the effects on AMP may be
reduced or eliminated, if manufacturers respond by increasing prices in
the private health insurance market. These estimates do not include
secondary impacts to other sectors of the market as a result of the
changes in Medicare payments under the model in part due to the
significant uncertainty around manufacturer pricing behavior in
response to this model.
Table 12--Estimated Financial Impact of MFN Model
----------------------------------------------------------------------------------------------------------------
(In billion dollars)
-------------------------------------------------------------------------
2021 2022 2023 2024 2025 2026 2027 2021-27
----------------------------------------------------------------------------------------------------------------
Drug price reduction:
FFS impact *...................... -4.7 -7.5 -9.3 -10.2 -11.2 -12.3 -13.5 -68.7
Gross impact (FFS+MA) **.......... -4.7 -7.5 -17.6 -19.5 -21.6 -24.0 -26.5 -121.4
Net of premium offset ***......... -3.5 -5.6 -13.2 -14.6 -16.2 -18.0 -19.9 -91.1
Medicaid impact................... -0.4 -0.6 -1.3 -1.5 -1.6 -1.8 -2.0 -9.1
Federal....................... -0.2 -0.3 -0.8 -0.8 -0.9 -1.0 -1.1 -5.2
State......................... -0.2 -0.2 -0.6 -0.6 -0.7 -0.8 -0.9 -3.9
Drug add-on payment:
FFS impact........................ 0.6 0.6 0.5 0.6 0.6 0.7 0.8 4.4
Gross impact (FFS+MA)............. 0.6 0.6 1.0 1.1 1.2 1.4 1.5 7.4
Net of premium offset............. 0.4 0.4 0.7 0.8 0.9 1.0 1.2 5.6
Medicaid impact................... -0.1 -0.1 -0.1 -0.1 -0.1 -0.1 -0.2 -0.8
Federal....................... -0.1 -0.1 -0.1 -0.1 -0.1 -0.1 -0.1 -0.5
State......................... 0.0 0.0 0.0 -0.1 -0.1 -0.1 -0.1 -0.4
Total impact:
FFS impact........................ -4.1 -7.0 -8.8 -9.6 -10.6 -11.6 -12.7 -64.4
Gross impact (FFS+MA)............. -4.1 -7.0 -16.6 -18.4 -20.4 -22.6 -25.0 -114.0
Net of premium offset............. -3.1 -5.2 -12.4 -13.8 -15.3 -16.9 -18.7 -85.5
Medicaid impact................... -0.4 -0.7 -1.4 -1.6 -1.8 -1.9 -2.1 -9.9
Federal....................... -0.3 -0.4 -0.8 -0.9 -1.0 -1.1 -1.2 -5.7
State......................... -0.2 -0.3 -0.6 -0.7 -0.8 -0.8 -0.9 -4.3
----------------------------------------------------------------------------------------------------------------
* Projected spending impact in the traditional Medicare FFS program under the model.
** Projected spending impact in both Medicare FFS and Medicare Advantage (MA).
*** Premium offset represents the change in the Part B premium income that would result from the change in Part
B drug expenditures.
These impacts are based on the President's Fiscal Year 2021 Budget
baseline for Medicare Part B drugs, including those dispensed by 340B
providers. Due to rounding, the sum of values in the table may differ
slightly from the total results in the table. In addition to the
behavioral assumptions in Table 11, these estimates reflect a number of
other technical assumptions, including the following:
Amounts illustrate the potential impact on Medicare Part B
drug spending, assuming the reductions are achievable and realized.
Amounts are presented by calendar year and are based on
the date the service is incurred and have therefore not been adjusted
to reflect when payment is made.
The model runs from January 1, 2021 through December 31,
2027. If any of the provisions of this rule are not effective on
January 1, 2021, the impacts will differ.
The model will include the top 50 Medicare Part B drugs
with the highest spending each year and will account for roughly 73
percent of Medicare Part B drug spending in each affected year.
All included providers and suppliers receive an add-on
payment of 6 percent (after sequestration) of the average sales price
(ASP) and this add-on payment is not subject to beneficiary cost
sharing.
The impacts reflect changes to payments to Medicare
Advantage plans starting in 2023.
The premium offset is 25 percent of the gross impact.
The Medicaid impact represents the portion of beneficiary
cost sharing paid on behalf of dual-eligible beneficiaries (split 57
percent/43 percent between Federal and State).
The Medicaid impact does not account for the potential
impacts to AMP or Best Price in the Medicaid program.
a. Pricing Effects Only Illustration
As mentioned previously, there is much uncertainty around the
behavioral assumptions underlying the estimated financial impacts. To
show the effects of the model absent any provider or beneficiary
behavioral responses, OACT calculated the impacts of the payment
changes alone. These values reflect the pricing changes inside the
model, as shown in Table 9, and the assumption that manufacturers and
MFN participants are able to continue to provide access to all drugs.
Again, because 340B providers will receive the lesser of the model
payment amount or the amount outside the model for the drug, no impact
to their costs is expected for the first year. Results for this
illustration are shown in Table 13, and they reflect the same technical
assumptions as the OACT estimate. The net impact on Medicare after the
premium offset is a savings of $155.6 billion over the 7-year period,
and none of the impact would be due to lost utilization.
[[Page 76239]]
Table 13--Estimated Impact of Pricing Effects Only Illustration
----------------------------------------------------------------------------------------------------------------
(In billion dollars)
-------------------------------------------------------------------------
2021 2022 2023 2024 2025 2026 2027 2021-27
----------------------------------------------------------------------------------------------------------------
Drug price reduction:
FFS impact *...................... -3.1 -7.3 -13.1 -20.1 -23.0 -25.3 -27.7 -119.7
Gross impact (FFS+MA) **.......... -3.1 -7.3 -24.7 -38.5 -44.4 -49.2 -54.5 -221.8
Net of premium offset ***......... -2.4 -5.5 -18.5 -28.9 -33.3 -36.9 -40.9 -166.4
Medicaid impact................... -0.2 -0.5 -1.9 -2.9 -3.3 -3.7 -4.1 -16.6
Federal....................... -0.1 -0.3 -1.1 -1.6 -1.9 -2.1 -2.3 -9.5
State......................... -0.1 -0.2 -0.8 -1.2 -1.4 -1.6 -1.8 -7.2
Drug add-on payment:
FFS impact........................ 0.9 1.0 1.1 1.2 1.3 1.4 1.6 8.3
Gross impact (FFS+MA)............. 0.9 1.0 2.0 2.2 2.5 2.8 3.1 14.4
Net of premium offset............. 0.7 0.7 1.5 1.7 1.9 2.1 2.3 10.8
Medicaid impact................... -0.1 -0.1 -0.1 -0.1 -0.1 -0.1 -0.1 -0.8
Federal....................... 0.0 -0.1 -0.1 -0.1 -0.1 -0.1 -0.1 -0.5
State......................... 0.0 0.0 0.0 0.0 -0.1 -0.1 -0.1 -0.3
Total impact:
FFS impact........................ -2.3 -6.4 -12.0 -19.0 -21.7 -23.9 -26.2 -111.4
Gross impact (FFS+MA)............. -2.3 -6.4 -22.7 -36.3 -41.9 -46.5 -51.4 -207.4
Net of premium offset............. -1.7 -4.8 -17.0 -27.2 -31.5 -34.9 -38.6 -155.6
Medicaid impact................... -0.3 -0.6 -2.0 -3.0 -3.5 -3.8 -4.2 -17.4
Federal....................... -0.2 -0.4 -1.1 -1.7 -2.0 -2.2 -2.4 -9.9
State......................... -0.1 -0.3 -0.8 -1.3 -1.5 -1.6 -1.8 -7.5
----------------------------------------------------------------------------------------------------------------
* Projected spending impact in the traditional Medicare FFS program under the model.
** Projected spending impact in both Medicare FFS and Medicare Advantage (MA).
*** Premium offset represents the change in the Medicare Part B premium income that would result from the change
in Medicare Part B expenditures.
b. Extreme Disruption Illustration
To cover the spectrum of possible outcomes, the impact of a greater
behavioral response from manufacturers and MFN participants was also
considered. Under this scenario, it is assumed that non-340B providers
and suppliers will not be able to obtain any of the current drugs
inside the model. All non-340B utilization will then be divided among
the three beneficiary choices of traveling to an excluded provider or
supplier, using a 340B provider, or forgoing access. Because there are
a small number of excluded providers and suppliers, OACT assumed they
only have capacity for a 25 percent increase in utilization.
Additionally, manufacturers are assumed to not change the international
prices; as a result, 340B providers will have reduced reimbursement
beginning in 2022, when the MFN Price dips below the baseline payment
of ASP less 22.5 percent--leading to reduced beneficiary access through
340B providers as well. The financial hardship exemption could possibly
apply under this scenario, but as this payment is retrospective and the
losses prior to the payment would be severe, it is unclear whether
providers will be in a position to request the exemption.
The illustrative results under these assumptions are shown in Table
14. They weredeveloped with the same technical assumptions listed under
the OACT estimate. The overall impact of the model would be a
substantial savings to Medicare of $286.3 billion, but nearly half of
that impact would be due to lost utilization.
Table 14--Estimated Impact of Extreme Disruption Illustration
----------------------------------------------------------------------------------------------------------------
(In billion dollars)
-------------------------------------------------------------------------
2021 2022 2023 2024 2025 2026 2027 2021-27
----------------------------------------------------------------------------------------------------------------
Drug price reduction:
FFS impact *...................... -17.6 -21.2 -26.9 -30.5 -33.7 -37.0 -40.6 -207.5
Gross impact (FFS+MA) **.......... -17.6 -21.2 -50.9 -58.4 -65.0 -72.0 -79.7 -364.8
Net of premium offset ***......... -13.2 -15.9 -38.2 -43.8 -48.7 -54.0 -59.8 -273.6
Medicaid impact................... -1.3 -1.6 -3.8 -4.4 -4.9 -5.4 -6.0 -27.4
Federal....................... -0.8 -0.9 -2.2 -2.5 -2.8 -3.1 -3.4 -15.6
State............................. -0.6 -0.7 -1.6 -1.9 -2.1 -2.3 -2.6 -11.8
Drug add-on payment:
FFS impact........................ -0.6 -0.8 -1.2 -1.5 -1.6 -1.8 -1.9 -9.4
Gross impact (FFS+MA)............. -0.6 -0.8 -2.3 -2.8 -3.1 -3.4 -3.8 -16.9
Net of premium offset............. -0.5 -0.6 -1.8 -2.1 -2.3 -2.6 -2.9 -12.7
Medicaid impact................... -0.1 -0.1 -0.1 -0.1 -0.1 -0.1 -0.2 -0.8
Federal....................... -0.1 -0.1 -0.1 -0.1 -0.1 -0.1 -0.1 -0.5
State......................... 0.0 0.0 0.0 -0.1 -0.1 -0.1 -0.1 -0.4
Total impact:
FFS impact........................ -18.2 -22.0 -28.2 -32.0 -35.3 -38.7 -42.5 -217.0
Gross impact (FFS+MA)............. -18.2 -22.0 -53.2 -61.2 -68.1 -75.5 -83.5 -381.7
Net of premium offset............. -13.7 -16.5 -39.9 -45.9 -51.1 -56.6 -62.6 -286.3
Medicaid impact................... -1.4 -1.7 -3.9 -4.5 -5.0 -5.5 -6.1 -28.2
Federal....................... -0.8 -1.0 -2.2 -2.6 -2.9 -3.2 -3.5 -16.1
[[Page 76240]]
State......................... -0.6 -0.7 -1.7 -1.9 -2.2 -2.4 -2.6 -12.1
----------------------------------------------------------------------------------------------------------------
* Projected spending impact in the traditional Medicare FFS program under the model.
** Projected spending impact in both Medicare FFS and Medicare Advantage (MA).
*** Premium offset represents the change in the Medicare Part B premium income that would result from the change
in Medicare Part B expenditures.
c. Additional Considerations
Because the model will make substantial changes to payment for
Medicare Part B drugs, there are many other potential responses not
considered in this analysis. It is possible that manufacturers could
increase prices for non-Part B drugs, which would affect both private
market and Part D expenditures, although that potential impact has not
been quantified for this estimate. It is also possible that moving to a
flat add-on payment from a percentage of drug cost will have additional
effects, which are not considered in the OACT analysis. The analysis is
on a pre-COVID-19 basis, and neither the baseline nor the impact
analysis are adjusted for the effects of the pandemic.
2. ASPE Estimate
The behavioral responses of manufacturers, providers, suppliers,
and beneficiaries to the MFN Model are critical to estimating its
impact on key outcomes. Lack of direct experience with policies such as
the MFN Model, however, results in great uncertainty for making these
behavioral assumptions. For a robust approach, ASPE made a number of
assumptions based on published literature and expert consensus, and
applied such assumptions on a drug-by-drug basis. Please note that ASPE
has not adjusted the assumptions and estimates based on the effects of
the COVID-19 pandemic.
The behavioral assumptions in this approach first address
manufacturers' responses in the international market that might
increase MFN Prices; and then the potential responses to the MFN Drug
Payment Amounts by the manufacturers and providers and suppliers that
purchase MFN Model drugs and submit a claim to Medicare after
administering such drugs to beneficiaries. In general, these
assumptions represent the proposition that manufacturers prefer to sell
their products, even at lower prices, as long as net revenues (net
sales prices minus production and distribution costs) remain positive;
and that providers and suppliers are committed to maintaining effective
treatments for beneficiaries either by negotiating lower prices,
accepting reduced revenue, or finding effective Medicare Part B or Part
D alternative treatments.
To assess the likelihood of each of the alternative manufacturer
responses to the MFN Model, ASPE reviewed published literature on the
impacts and interviewed a small cohort of experts regarding the
potential impacts. Published literature suggests that when a large
country establishes an international reference price, smaller reference
countries experience price increases and longer launch delays for new
products.\85\ ASPE's conversations with experts suggested that as a
result of the MFN Model, prices in other countries could increase at
the ex-manufacturer level, potentially up to current ASP levels, and
manufacturers could change formulations of MFN Model drugs to lessen
the impact of the model. The experts generally believe that
manufacturers will be able to price discriminate between the Medicare
Part B market and other markets within the U.S. Potential utilization
impacts will thus be limited to Medicare Part B beneficiaries, as
payments to providers and suppliers for drugs provided to other
patients will not be affected by the model.
---------------------------------------------------------------------------
\85\ Patricia M. Danzon, ``The Economics of the
Biopharmaceutical Industry'', in Sherry Glied and Peter C. Smith
(eds.), The Oxford Handbook of Health Economics, Oxford University
Press 2011, pp. 520-554.
---------------------------------------------------------------------------
Considering this information, ASPE made a series of assumptions for
a base analysis. First, ASPE considered a static group of 50 drugs for
this analysis. Based on the literature and interviews with experts,
ASPE assumed manufacturers of newly launched brand products that become
MFN Model drugs would adjust their international pricing strategies so
that the MFN Payment Amount will be equal to ASP absent of the MFN
Model. This assumption does not necessarily mean that net international
prices (ex-manufacturer sales prices minus the value of rebates or
other financial concessions) will be equal to the ASP. In addition,
ASPE assumed that manufacturers of currently marketed drugs outside but
near the top 50 Medicare Part B drugs based on annual allowed charges
(with certain exclusions and exemptions) will lower their U.S. prices
in an attempt to prevent them from becoming MFN Model drugs. To
compensate for this response, ASPE assumed that manufacturers will
increase prices for non-MFN Model drugs. Since companies often sell
many different drugs, ASPE assumed they will have some flexibility to
allocate discounts between different drugs to ensure no currently
marketed non-MFN Model drugs enter the top 50 while maintaining near
constant revenues. In some cases, there are relatively new drug
products that may not have launched or may be recently launched in the
included countries that may enter the top 50. In those cases, ASPE
assumed the manufacturers will re-evaluate their international pricing
strategies to ensure the MFN Price is comparable to ASP absent of the
MFN Model. ASPE assumed that these changes to U.S. prices of non-MFN
Model drugs will ultimately fully offset one another in terms of
Medicare Part B drug spending as well.
For the 50 MFN Model drugs, the MFN Price ultimately depends on the
prices for the drugs in the included countries. The exact mechanisms in
which prices are determined in included countries differ by country and
sometimes by product. These mechanisms include national (or sub-
national tendering \86\), therapeutic-level reference pricing,
international reference pricing, cost-effectiveness analysis, and
negotiation. These mechanisms generally result in lower observed prices
in other countries compared to the U.S., and these differences tend to
be larger for products that have more competition than in the U.S.
(such as more biosimilar competition) or have only a marginally better
clinical profile than a cheaper
[[Page 76241]]
therapy. Since the U.S. price under this model depends on the prices in
other countries, the model will likely result in increased observed
prices in other countries. This does not mean that net prices will
necessarily increase as countries will try to find ways to prevent
spending increases while limiting disruption in their drug markets. In
this analysis, ASPE considered the potential impact at the drug-level
because the context of each drug may determine the MFN Price.
---------------------------------------------------------------------------
\86\ Tendering is a formal procedure to purchase medications
using competitive bidding for a particular contract.https://
www.ncbi.nlm.nih.gov/pmc/articles/PMC5628685/.
---------------------------------------------------------------------------
ASPE modeled the pricing response to the change in direct drug
payment for each of the 50 MFN Model drugs shown in Table 6 of this
IFC. ASPE assumed that any changes in international sales prices for
included countries would not occur until the beginning of the second
performance year of the MFN Model. ASPE modeled the manufacturer
pricing response based on available 2019 international drug pricing
information, using the sales and volume data that CMS used to calculate
the MFN Prices shown in Table 6 of this IFC. ASPE did not model how
manufacturers and providers might take into account the changes to the
add-on.
If there was only one related brand for the included countries,\87\
then ASPE assumed the MFN Price for a drug will increase to the average
price of the drug for the included countries plus 10 percent (with the
cap of ASP). ASPE made this assumption because at this point the market
size of the included countries is roughly the size of the Medicare Part
B market for many of the MFN Model drugs. ASPE applied this approach to
34 of the 50 MFN Model drugs. ASPE assumed that the MFN Price will not
likely increase by more than this because, even if the net price is
constant for purchasers in the included countries, these countries may
seek to avoid larger increases in transaction prices. In the case of
drugs with no international spending in 2019, ASPE assumed that the
model would have no impact. ASPE applied this approach to 2 of the 50
MFN Model drugs. When the MFN Price was calculated based on
international drug pricing information for a country with access to
biosimilar products or a competitor brand product that is not one of
the MFN Model drugs, ASPE assumed smaller international price increases
because the MFN Model would reduce the incentive for the manufacturer
of an MFN Model drug to compete in those international markets. This
approach applied to 8 of the 50 MFN Model drugs. When the MFN Price was
calculated using international drug pricing information for a non-
innovator unbranded product, ASPE assumed that the MFN Price would not
increase. This assumption applied to 6 of the 50 MFN Model drugs.
---------------------------------------------------------------------------
\87\ For this analysis, we included available sales and volume
data for the brand drug manufacturer and any parallel importers of
the brand drug.
---------------------------------------------------------------------------
After analyzing price changes internationally, ASPE analyzed the
potential for beneficiaries to switch to other products with, for
example, the same active ingredient within the U.S. and billed with
HCPCS codes that are not among the MFN Model drugs. First, ASPE assumed
that when a manufacturer has multiple branded products with different
indications represented by the same HCPCS code, the manufacturer will
work to obtain a new HCPCS code for the product in which Medicare Part
B makes up a smaller portion of its overall market. In addition, the
manufacturer will restrict the amount of product sold that could be
billed under this new HCPCS code so that such products will not become
included in the MFN Model. This assumption applied to one of the MFN
Model drugs. ASPE also assumed that if an MFN Model drug is available
within the U.S. in a formulation that will be covered under Medicare
Part D, the manufacturer will work to shift 90 percent of the
utilization from Medicare Part B to Medicare Part D. This assumption
impacted 2 of the 50 MFN Model drugs.
In addition to these assumptions, ASPE made assumptions about
potential generic entry for some of the MFN Model drugs. ASPE assumed
that MFN Model drugs with generic drugs approved within the included
countries or currently subject to on-going Paragraph 4 patent
challenges would have generic competition by performance year 3. This
assumption impacted 6 of the 50 MFN Model drugs.
After examining the potential price impacts and other utilization
changes described previously, ASPE examined the potential for
utilization impacts. In general, economic theory and the experts ASPE
interviewed suggested that manufacturers will adjust U.S. prices to
maintain sales as long as price is greater than marginal costs of
producing and distributing the drug. ASPE also assumed that
manufacturers will have substantial ability to price discriminate--that
is, adjust pricing for Medicare-participating providers and suppliers
to reflect discounts for their Medicare Part B patient share as opposed
to all patients. Nonetheless, ASPE still considered the potential that
price discrimination will be less than perfect for some drugs. In these
cases, a manufacturer might refuse to negotiate lower prices for MFN
beneficiaries if doing so threatens its ability to sell in other
segments of the U.S. at a positive margin. That is, would the loss in
revenues from selling for all purchasers at a reduced price exceed the
loss in revenues from losing the MFN beneficiary share of business for
that drug? To examine this issue, ASPE estimated the Medicare Part B
share of each MFN Model drug compared with the estimated U.S. market.
If it seemed likely that a manufacturer will have higher revenues
selling to all purchasers at prices slightly above the MFN Drug Payment
Amount than not selling to MFN participants for MFN beneficiary use,
ASPE assumed the manufacturer will not restrict MFN beneficiaries'
access to an MFN Model drug under Medicare Part B. This included
examining if the MFN Model drugs had U.S. competitors. Since MFN
participants likely treat both Part B beneficiaries and non-Part B
beneficiaries (including individuals with employer, individual market,
or Medicaid coverage), an MFN participant may select an alternative
therapy marketed by a competitor that can be provided to both types of
patients. As a result, manufacturers will have an incentive to work to
maintain utilization so long as the MFN Payment Amount is not too low.
In cases where manufacturers might refuse to lower U.S. prices
sufficiently to make it financially feasible for MFN participants to
furnish the drug and receive the MFN Payment Amount, ASPE examined
whether there were products that had similar therapeutic effects to a
MFN Model drug. ASPE assumed that Medicare Part B beneficiaries will be
switched to the potential alternative products. ASPE made these
assessments for each performance year. ASPE assumed that half of
Medicare Part B beneficiaries will continue accessing their current
drugs through 340B providers. Such changes in drug utilization or
service providers will likely result in additional burdens for
patients. ASPE did not quantify these impacts.
Additionally, for biological drugs for which there are licensed
biosimilar products, ASPE assumed that there will be at least one
biosimilar manufacturer that is willing to provide its product at MFN
payment levels if the reference manufacturer would not supply this
drug. We note however that if reference manufacturers are willing to
sell at MFN payment levels, providers may not have any incentive to use
biosimilar products. The extent to which providers may use biosimilar
products will depend on whether they are easier to
[[Page 76242]]
access instead of a product subject to the model. The biosimilar
manufacturers will need to balance those considerations with the
possibility that sufficiently large sales may also result in that
product becoming an MFN Model drug. ASPE assumed any utilization
changes that occur will result in zero net changes in spending. ASPE
made no assumptions about the potential entry of biosimilar products
for reference products that currently do not have biosimilar
competition in the U.S. or referenced countries.
The overall utilization impact is the sum of the impacts for each
of the 50 MFN Model drugs. These impacts reflect, on a drug by drug
basis, the assumptions outlined previously. Specifically, where
estimates reduced utilization, it reflects assumptions that either
manufacturers will be unwilling to reduce prices to MFN participants,
viable substitute drugs are not available for all affected patients, or
both. In such cases, ASPE assumed that half of the impacted
beneficiaries will be able to still access the MFN Model drug through a
340B provider.
ASPE calculated the potential impacts of the MFN Model by calendar
year. ASPE assumed that at the end of the MFN Model, there will be no
continued impacts because Medicare Part B payments for MFN Model drugs
will immediately be based on non-model payment policies at the end of
the MFN Model. Given the predictable 7-year model performance period,
ASPE assumed manufacturers and MFN participants will have sufficient
time to structure their agreements to ensure a seamless transition
after the end of the MFN Model.
Table 15 summarizes the results of the ASPE analysis.
Table 15--Assumptions Reflected in ASPE Estimate
----------------------------------------------------------------------------------------------------------------
2021 2022 2023 2024 2025 2026 2027
(%) (%) (%) (%) (%) (%) (%)
----------------------------------------------------------------------------------------------------------------
Non-340B providers:
Behavior:
Continued Availability................... 100.0 100.0 97.7 95.9 96.2 96.5 96.7
Altered Availability:
Shift to other drugs................. 0.0 0.0 1.1 2.1 1.9 1.8 1.6
Move to 340B......................... 0.0 0.0 1.1 2.1 1.9 1.8 1.6
No Access............................ 0.0 0.0 0.0 0.0 0.0 0.0 0.0
Total............................ 100 100 100 100 100 100 100
MFN Price impact................................. -11.4 -14.3 -18.1 -20.5 -19.4 -17.9 -16.5
340B providers:
Behavior:
Continued Availability................... 100 100 100 100 100 100 100
MFN Price impact................................. 0 0 0 0 0 0 0
----------------------------------------------------------------------------------------------------------------
ASPE estimated the Medicare FFS program impacts of the change from
ASP-based payment to MFN-based payment.\88\ The Medicare FFS impact
includes changes in spending for Medicare Parts B and D.
---------------------------------------------------------------------------
\88\ An indirect benefit of this IFC may be reduced distortions
in the labor markets taxed to support the Medicare Trust Fund. Such
distortions are sometimes referred to as marginal excess tax burden
(METB), and Circular A-94--OMB's guidance on cost-benefit analysis
of federal programs, available at https://www.whitehouse.gov/sites/whitehouse.gov/files/omb/circulars/A94/a094.pdf-suggests that METB
may be valued at roughly 25 percent of the estimated transfer
attributed to a policy change; the Circular goes on to direct the
inclusion of estimated METB change in supplementary analyses. If
secondary benefits--such as reduced marginal excess tax burden is,
in the case of this IFC--are included in regulatory impact analyses,
then secondary costs must be as well, in order to avoid
inappropriately skewing the net benefits results, and including METB
only in supplementary analyses provides some acknowledgement of this
potential imbalance.
---------------------------------------------------------------------------
For patients that switch to 340B providers, ASPE estimated the
spending change based on the difference in the MFN Model payment for
drugs acquired under the 340B program and the current Medicare Part B
OPPS payment policy.
These impacts are generally considered transfer impacts of the
model. To estimate these impacts, ASPE took an approach similar to
OACT. ASPE used the direct reduction in Medicare Part B payments due to
lower MFN payment amounts and translated that into transfers from the
healthcare system to the government, beneficiaries, and Medicaid. In
addition to the direct effects of lower payments and associated cost-
sharing, the model results in downstream transfers associated with
changes in Part B premiums and government payments to Medicare
Advantage Plans. Like OACT, ASPE estimated Medicaid impacts based on
changes to federal and state shares of prescription drug costs for dual
eligibles but did not estimate impacts on Medicaid that may result from
changes in net payments under the Medicaid Drug Rebate Program.
Overall, the model results in changes to federal spending in
Medicare (including Part B, and Part D) from the model price and
utilization impacts, changes in federal and state spending on Medicaid
resulting from changes to the governmental obligation of Medicare cost-
sharing for dual eligible beneficiaries, and changes in federal
spending associated with add-on payment changes in the model. The model
also results in changes to beneficiary spending resulting from changes
in cost-sharing for drugs, changes in beneficiary premiums, and changes
to cost-sharing associated with the add-on payment. These transfers on
net balance out with reduced revenues for healthcare providers (which
may be completely or mostly offset by the reduced cost of acquiring
drugs), reduced revenues for pharmaceutical manufacturers, and reduced
revenues for MA plans.
Based on our estimates of annual impacts on prescription drug
pricing and annual add-on payments, ASPE did not model any impacts from
the provider hardship payments. Eligibility for the hardship exemption
will be based on year-over-year losses above 25 percent of total
Medicare Part A and Part B payments, including payments for Medicare
Part B drugs outside the model and payments for Medicare Part A and
Medicare Part B services other than prescription drugs. We expect that
few, if any, providers will have annual losses above this level, and
that those who do may be insolvent and therefore unable to obtain
retrospective hardship payments. We note in this regard that a
hypothetical provider could experience revenue losses of 24.9 percent
per year in each of the model's seven years, resulting in an 86.5
percent loss of revenue in Performance Year 7
[[Page 76243]]
compared with the pre-model base year and a 62.7 percent loss of
revenue over the seven-year demonstration period, without qualifying
for the hardship payments in any year.
Table 16 shows the net transfer impacts resulting from changes in
Medicare B, and D. According to the ASPE estimate, this model would
result in a net reduction of $87.8 billion in beneficiary, federal
government, and state government spending over the 7 years of the
model.
Table 16--Estimated Transfer Impact of MFN Model--ASPE Estimate
----------------------------------------------------------------------------------------------------------------
2021 2022 2023 2024 2025 2026 2027 2021-27
----------------------------------------------------------------------------------------------------------------
Part B Drug Price Reduction:
Federal Government Spending....... -2.4 -3.4 -8.4 -10.0 -10.3 -10.7 -10.8 -56.0
State Government Spending......... -0.1 -0.1 -0.4 -0.4 -0.4 -0.5 -0.5 -2.4
Beneficiary Spending *............ -1.4 -2.0 -5.0 -5.9 -6.2 -6.4 -6.4 -33.4
MA Plan Revenue................... 0.0 0.0 -4.8 -5.9 -6.1 -6.5 -6.5 -29.8
Health Care System Revenue **..... -4.0 -5.5 -8.9 -10.5 -10.9 -11.1 -11.1 -61.9
Part D Drug Switching:
Federal Government Spending....... 0.0 0.0 0.3 0.3 0.3 0.3 0.3 1.7
State Government Spending......... 0.0 0.0 0.0 0.0 0.0 0.0 0.0 0.1
Beneficiary Spending *............ 0.0 0.0 0.1 0.1 0.1 0.1 0.1 0.7
Health Care System Revenue **..... 0.0 0.0 0.5 0.5 0.5 0.5 0.5 2.5
Add-on Payment Impact:
Federal Government Spending....... 0.2 0.2 0.4 0.3 0.4 0.4 0.4 2.2
State Government Spending......... 0.0 0.0 0.0 0.0 0.0 0.0 0.0 -0.3
Beneficiary Spending *............ -0.1 -0.1 -0.1 -0.1 -0.1 -0.1 -0.1 -0.5
MA Plan Revenue................... 0.0 0.0 0.2 0.3 0.3 0.3 0.3 1.3
Health Care System Revenue **..... 0.0 0.0 0.0 0.0 0.0 0.0 0.0 0.1
Total Impact:
Federal Government Spending....... -2.2 -3.2 -7.7 -9.3 -9.7 -10.0 -10.0 -52.1
State Government Spending......... -0.1 -0.2 -0.4 -0.4 -0.5 -0.5 -0.5 -2.5
Beneficiary Spending *............ -1.6 -2.1 -4.9 -5.9 -6.1 -6.3 -6.3 -33.2
MA Plan Revenue................... 0.0 0.0 -4.6 -5.6 -5.8 -6.2 -6.2 -28.5
Health Care System Revenue **..... -3.9 -5.5 -8.4 -10.0 -10.3 -10.6 -10.6 -59.3
----------------------------------------------------------------------------------------------------------------
* Beneficiary spending includes spending by beneficiary Medigap plans.
** Health care system revenue includes revenue accrued by health care providers, hospitals, pharmacies, and
pharmaceutical manufacturers.
Based on this analysis, the model has the potential to generate
impacts internationally. In particular, this model may result in higher
prices or longer launch delays for new products in other OECD
countries. ASPE did not attempt to quantify the impact of higher prices
on utilization or the impact of these delays. The health effects of
such delays depend on which products experience these delays and the
potential alternative treatments. In addition, foreign governments may
seek to mitigate these impacts by accepting higher prices for the
products or pursuing alternative price arrangements that are less
transparent.
3. Aggregate Effects on the Market
There may be spillover effects in the non-Medicare market, or even
in the Medicare market outside Part B as a result of the MFN Model.
Testing changes in Medicare Part B drug payment policy may have
implications for non-Medicare payers. During the MFN Model,
manufacturers' ASPs may increase or decrease, which may cause the
payment limits in the quarterly Medicare ASP payment files to increase
or decrease. Other payers that align their payments for drugs included
in the MFN Model with the quarterly Medicare ASP payment files could
therefore be impacted. Because the extent to which other payers align
with Medicare Part B drug payments is unknown, we are not able to
quantify the potential impacts of the MFN Model in this regard.
Private secondary payers that pay for beneficiary cost-sharing,
such as Medigap plans and employer retiree coverage, will likely be
impacted by the MFN Model. For MFN beneficiaries, cost-sharing on MFN
Model drugs would be less than the amount that will apply outside of
the model. If manufacturers generally raise drug prices in response to
the MFN Model, the amount of cost-sharing paid by beneficiaries and
secondary payers may increase; the opposite will occur if manufacturers
decrease drug prices. Similarly, private primary insurers may be
impacted if manufacturers change drug pricing as a result of the MFN
Model. Market-wide changes in drug prices, including drugs not covered
by Medicare Part B, will impact any individual who receives such drugs.
In addition, to the extent manufacturers lower their overall prices for
drugs, manufacturers may realize lower revenue as a result of the MFN
Model. It is possible that manufacturers will increase international or
domestic drug prices, reduce marketing and other expenses, or implement
other efficiency measures to reduce their operating costs. Given the
uncertainty of manufacturers' potential behavioral responses to the MFN
Model, we are unable to quantify these potential spillover effects of
the MFN Model. We welcome comments on these potential impacts and
evidence on how this rule could affect other payers, patients, and drug
manufacturers.
Some of this final rule's important tradeoffs occur over the long
run. We request comment on whether the drug products affected by this
IFC are likely to be currently over- or under-incentivized, including
evidence from the research literature on optimal patent length, and on
the effects of the IFC on drug manufacturers' incentives.
4. Estimated Effect and Burden of MFN Model Changes on Medicare
Beneficiaries
We estimate that aggregate beneficiary Medicare Part B cost-sharing
within the context of the MFN Model will decrease as the MFN Drug
Payment Amount will not exceed 100 percent of the amount that applies
outside the MFN Model (that is, the applicable ASP or WAC or payment
limit that applies to drug acquired under the 340B program) and that
beneficiaries will not have a cost-sharing liability for the
alternative drug
[[Page 76244]]
add-on payment amount. Coinsurance for most separately payable drugs is
set at 20 percent of the payment rates, subject to limitation in the
hospital outpatient and ASC settings. To the extent that prescribing
patterns shift toward lower cost drugs under the MFN Model, in
aggregate, beneficiaries could benefit along with the Medicare program.
If prescribing patterns shift toward Part D drugs, beneficiary cost-
sharing may increase or decrease depending upon the drugs they take,
which phase of the Part D benefit such use occurs in, the beneficiary's
eligibility for help with drug costs, and their plan choice. In
addition, as a result of the MFN Model, we expect Medicare Part B
premiums to decrease. Beneficiaries will benefit from 25 percent of any
premium reduction that may result as this is the portion of annual
premiums that beneficiaries pay.
If MFN participants choose not to provide MFN Model drugs or
prescribe alternative therapies instead, beneficiaries may experience
access to care impacts by having to find alternative care providers
locally, having to travel to seek care from an excluded provider,
receiving an alternative therapy that may have lower efficacy or
greater risks, or postponing or forgoing treatment. There is
significant uncertainty with these potential effects of the MFN Model.
CMS will carefully monitor for evidence of these potential effects and
conduct beneficiary surveys to assess impacts of the MFN Model on
beneficiaries.
Given the uncertainty of these impacts, we are unable to quantify
these potential effects of the MFN Model.
In section III.H. of this IFC, we describe our intention to include
quality measures as part of the MFN Model, and our plan to collect one
quality measure, focused on patient experience, to help better
understand the impact of the MFN Model on beneficiary access and
quality of care. This information collection will be one part of robust
monitoring activities to ensure that MFN beneficiaries' access to
medications and quality of care is preserved or enhanced. We will use a
patient experience survey, which we will field to a sample of MFN
beneficiaries, beginning in performance year 1. We will include
additional items in the patient experience survey that focus on patient
access, to the extent that valid and reliable items are available. The
patient experience survey will be administered to these beneficiaries
by a third party contractor throughout the model performance period.
Beneficiaries will not be required to complete the survey.
The patient experience survey will be based on a standardized
instrument, designed to assess patients' experiences with health care
providers and staff in an ambulatory setting. We will use the most
current version of the instrument plus additional survey questions as
applicable to meet CMS's monitoring needs.
Based on drug claims analyses and the scope of the MFN Model, we
assume the patient experience survey will be administered to 75,000
beneficiaries and be completed by 30,000 beneficiaries per year. The
survey will take approximately 30 minutes to complete. Therefore, the
annual total number of hours for this information collection will be
15,000 hours (30,000 beneficiaries times 0.5 hours per beneficiary
responding).
To derive average costs for individuals we used data from the U.S.
Bureau of Labor Statistics' May 2019 National Occupational Employment
and Wage Estimates for our salary estimate (www.bls.gov/oes/current/oes_nat.htm). We believe that the burden will be addressed under All
Occupations (occupation code 00-0000) at $25.72 per hour since the
group of individual respondents varies widely from working and
nonworking individuals and by respondent age, location, years of
employment, and educational attainment, etc. We are not adjusting this
figure for fringe benefits and overhead since the individuals'
activities will occur outside the scope of their employment. Therefore,
the estimated cost for this information collection will be $385,800
(15,000 hours x $25.72). Beneficiaries will have annual costs
associated with responding to the patient experience survey, which we
estimate will be $385,800 annually during the model.
5. Estimated Effect and Burden on MFN Participants and Manufacturers
MFN participants and drug manufacturers will have administrative
costs related to adjusting to and complying with the regulations. These
costs may include adjusting purchasing arrangements, which for some
affected businesses may mean substantially changing their pricing
models and engaging in negotiations with other businesses; tracking
units of MFN Model drugs that are paid under the MFN Model and excluded
from manufacturers' ASPs; recordkeeping requirements, which may require
acquisition of new tools and information sharing; and adjusting to any
spillover effects. Additionally, MFN participants may be subject to
site visits for the purposes of monitoring the MFN Model.
During the model performance period, MFN participants must
participate in MFN Model monitoring and evaluation activities in
accordance with 42 CFR 403.1110(b), as the Secretary determines is
necessary to monitor and evaluate the MFN Model, including without
limitation collecting and reporting of information, including
``protected health information'' as that term is defined at 45 CFR
160.103. These monitoring activities may include a sample of site
visits to verify any monitoring concerns. We anticipate that these
monitoring and compliance requirements will not diverge from general
monitoring requirements for Medicare Part B providers. We believe that
these requirements do not add additional burden or impose regulatory
impact on participants. The MFN Model monitoring will likely include
beneficiaries and eligible providers and suppliers completing surveys.
Burden for the patient survey is described previously, and burden for
any provider and supplier survey will depend on the length, complexity,
and frequency of surveys administered as needed to ensure confidence in
the survey findings. We will make an effort to minimize the length,
complexity, and frequency of any provider and supplier surveys. A
typical survey on average requires about 20 minutes of the respondent's
time. In other evaluations of models where a survey is required, the
frequency of surveys varies from a minimum of one round of surveys to
annual surveys. We estimate the burden for annual surveys from
clinicians, assuming one per eligible provider and supplier, will be 7
surveys [annual] times \1/3\ hour [20 min.] times $200 [median
physician/surgeon hourly rate plus fringe benefits] times 22,888
[eligible providers and suppliers] = $10,702,429.
Finally, MFN participants may choose to apply for a financial
hardship exemption that requires the submission of a timely, complete
request for a financial hardship exemption. We think that approximately
900 MFN participants will submit a request for a financial hardship
exemption each performance year of the model. We expect that a medical
health service manager will need approximately 15 hours to compile the
necessary supporting documentation and submit a complete financial
hardship exemption request. We estimate the burden for applying for the
financial hardship exemption per year for all performance year of the
model will be 900 [number of MFN participants that submit
[[Page 76245]]
hardship exemption requests in each performance year] times 15 hours
times $111 [medical health service manager hourly rate plus fringe
benefits] = $1,498,500. Note, the financial hardship exemption requests
for performance year 1 (2021) will be submitted in 2022, and the
requests for performance year 7 will occur in 2028.
We expect that manufacturers will need to update their ASP
reporting. However, we expect the burden to be de minimis compared to
existing ASP reporting requirements and can likely be automated based
on existing processes.
6. Regulatory Review Cost Estimation
In order to comply with the regulatory changes in this IFC,
affected businesses will need to review the rule and MFN participants
will need to review MFN-specific billing guidance on how to bill for
the alternative add-on payment. We expect that a medical health service
manager reading 250 words per minutes could review the rule in
approximately 6 hours [(approximately 300 pages * 300 words/per page)/
250 words per minute)/60 minutes)]. We estimate 1 hour to review the
relevant MLN matters publication and 2 hours to read MFN Model billing
guidance for a total of 3 hours of billing specific training. Since all
MFN participants have experience billing HCPCS codes to Medicare, we do
not expect any additional specific burden related to the alternative
add-on payment M code during model implementation after the MFN-
specific billing guidance is reviewed. We estimate the salary of a
medical and health service manager is $111 per hour, using the wage
information from the 2019 BLS including overhead and fringe benefits
(BLS occupation code 11-9110). For each provider or supplier that
reviews the rule and MFN-specific billing guidance, the estimated cost
based on the expected time and salary of the person reviewing the rule
is $999 ($111 * 9 [6 hours for reviewing the rule and 3 hours for
billing training). We estimate that the cost for providers and
suppliers to review this IFC and MFN-specific billing guidance will be
approximately $117.9 million (118,101 entities times $999).
7. Regulatory Flexibility Act (RFA)
The RFA requires agencies to analyze options for regulatory relief
for small entities. For purposes of the RFA, small entities include
small businesses, nonprofit organizations, and small governmental
jurisdictions. Most hospitals, practitioners and most other providers
and suppliers are small entities, either by nonprofit status or by
having annual revenues that qualify for small business status under the
Small Business Administration standards. (For details, see the SBA's
website at https://www.sba.gov/content/table-smallbusiness-size-standards (refer to the 620000 series)). Individuals and states are not
included in the definition of a small entity. The RFA requires that CMS
analyze regulatory options for small businesses and other entities
unless CMS certifies that a rule will not have a significant economic
impact on a substantial number of small entities. The analysis must
include a justification concerning the reason action is being taken,
the kinds and number of small entities the rule affects, and an
explanation of any meaningful options that achieve the objectives with
less significant adverse economic impact on the small entities. The
vast majority of MFN participants are considered to be small entities,
based upon the SBA standards. There are over twenty thousand MFN model
participants that will be included or affected by the MFN Model.
Because many of the affected entities are small entities, the analysis
and discussion provided in this section, as well as elsewhere in this
IFC is intended to comply with the RFA requirements regarding
significant impact on a substantial number of small entities.
The RFA requires that a Regulatory Flexibility Analysis (RFA) be
prepared if an IFC will have a ``significant impact on a substantial
number'' of small entities. HHS interprets the statute as mandating
this analysis only if the impact is adverse, though there are differing
interpretations. For purposes of the RFA, most practitioners,
hospitals, and other providers and suppliers are small entities, either
by nonprofit status or by having annual revenues that qualify for small
business status under the Small Business Administration standards
(having revenues of less than $7.5 million to $38.5 million in any 1
year). For details, see the Small Business Administration's ``Table of
Small Business Size Standards'' at https://www.sba.gov/document/
support--table-size-standards. The rule of thumb used by HHS for
determining whether an impact is ``significant'' is an adverse effect
equal to 3 percent or more of total annual revenues. Because the
majority of providers/suppliers in the U.S. qualify as ``small,'' and
this model includes all eligible providers/suppliers that submit claims
for separately payable Medicare Part B drugs, we expect the majority of
MFN participants to be small entities. However, some of these small
entities may not administer Medicare Part B drugs and will not be MFN
participants.
There are a number of providers and suppliers, including various
physician specialties, that will see reduced drug component payments of
3 percent or more in performance year 1. Please refer to Table 3 to see
the number of entities impacted, as well as the types of providers and
suppliers that will be most likely impacted by the rule. Lower MFN
Model drug payments will likely be a fraction of these entities' total
revenues, taking into account non-Medicare patients and all other
services provided. Moreover, the alternative add-on payments could
offset such reductions to some extent, as described in section III.F.
of this IFC. We considered potential impacts on small entities; we
expect that the model's impact on an MFN participant's revenue will be
driven by the proportion of Medicare payments to the MFN participant
that is related to administering Medicare Part B drugs rather than its
size. Further, to provide financial protection for MFN participants, we
are including a financial hardship exemption for MFN participants
(regardless of size) that experience significant financial hardship as
a result of the model test, as described in section III.I.2. of this
IFC. It is likely that many, if not all, included providers and
suppliers will see an overall decrease in revenue for MFN Model drugs
of 3 percent or more over the course of the model. Accordingly, we have
determined that a Regulatory Flexibility Analysis (RFA) is required.
This RIA, together with the preamble, constitutes the required
analysis.
As a result of the model, we expect total allowed charges for
Medicare Part B drugs for small entities to go down commensurate with
the phase-in of the MFN Price in the calculation of the MFN Drug
Payment Amount (Year 1: 75 percent applicable ASP and 25 percent MFN
Price; Year 2: 50 percent applicable ASP and 50 percent MFN Price;
etc.). Although the alternative add-on payment was designed to hold MFN
participants harmless based on current revenue to the greatest extent
possible, as shown in Table 8, some specialties will benefit from a
higher aggregate add-on payment amount, while for other specialties
some portion of such specialties will have a decrease in aggregate add-
on payment. We estimate that MFN participants, on average, will see an
approximate 40 percent increase in historical revenue related to the
alternative add-on portion of the MFN Model payments, which will total
approximately $4.4 billion in
[[Page 76246]]
the OACT estimate and $2.2 billion in the ASPE estimate over the 7-year
model. In these estimates, the total Medicare FFS impact, as indicated
in Tables 12 and 16, would be a reduction of approximately $85.5
billion in Medicare FFS spending in the OACT estimate and a majority of
the $52.1 billion in reduced federal spending in the ASPE estimate over
the 7-year model, and will apply mainly to urban and non-340B MFN
participants. We note that there is much uncertainty around the
assumptions for these estimates. Finally, we have and will continue to
take steps to minimize the impact of this IFC on administrative and
reporting burdens for small businesses. We welcome comments on our
estimate of significantly affected providers and suppliers and the
magnitude of estimated effects. We also welcome comments on adjustments
to the MFN Model that could be considered for future rulemaking while
preserving the innovative approach to payment in the MFN Model.
8. Effects on Small Rural Hospitals
Section 1102(b) of the Act requires CMS to prepare a regulatory
impact analysis if a rule may have a significant impact on the
operations of a substantial number of small rural hospitals. This
analysis must conform to the provisions of section 604 of the RFA. For
purposes of section 1102(b) of the Act, we define a small rural
hospital as a hospital that is located outside of a metropolitan
statistical area and has 100 or fewer beds. We estimate that this IFC
will have a significant impact on small rural hospitals.
As described in section III.C. of this IFC, we will exclude CAHs
from the types of providers and suppliers that will be MFN
participants. Slightly less than 10 percent ($3.35 billion) of total
Medicare Part B drug allowed charges in 2019 are associated with rural
providers and suppliers (other than CAHs) based on claims with ZIP
codes associated with areas that are not assigned to metropolitan core
based statistical areas (CBSA) identified by the Office of Management
and Budget; of that amount, less than 0.015 percent ($4.87 million) is
for drugs furnished in the U.S. territories outside of the metropolitan
areas of Puerto Rico. These rural entities will experience drug payment
reductions and overall payment reductions similar to urban entities
under the MFN Model.
9. Unfunded Mandates Reform
Section 202 of the Unfunded Mandates Reform Act of 1995 (UMRA) also
requires that agencies assess anticipated costs and benefits before
issuing any rule whose mandates require spending in any 1 year of $100
million in 1995 dollars, updated annually for inflation. In 2020, that
threshold is approximately $156 million. This IFC does not mandate any
spending by State, local, or tribal governments, or by the private
sector, and hence an UMRA analysis is not required.
10. Federalism
Executive Order 13132 establishes certain requirements that an
agency must meet when it promulgates a final rule that imposes
substantial direct costs on State and local governments, preempts state
law, or otherwise has Federalism implications. We have examined the
provisions in the MFN Model included in this IFC in accordance with
Executive Order 13132, and have determined that they will not have a
direct effect on state, local or tribal governments, preempt state law,
or otherwise have a Federalism implication.
D. Reducing Regulation and Controlling Regulatory Costs
Executive Order 13771, titled Reducing Regulation and Controlling
Regulatory Costs, was issued on January 30, 2017, and requires that the
costs associated with significant new regulations ``shall, to the
extent permitted by law, be offset by the elimination of existing costs
associated with at least two prior regulations.'' This IFC is
considered an E.O. 13771 regulatory action. Details on the estimated
costs of this IFC can be found in the preceding and subsequent
analyses.
E. Alternatives Considered
This IFC contains a range of policies. It also provides
descriptions of the statutory provisions that are addressed, identifies
the final policies, and presents rationales for our policies and, where
relevant, alternatives that we considered in section III of this IFC.
Several alternatives we considered included: (1) The parameters
included in this IFC; (2) variations of certain parameters included in
this IFC, such as lengthening the phase-in of the MFN Price (described
in section III.E.8. of this IFC) to occur over 5-7 performance years,
limiting the model performance period to 5 performance years, expanding
or limiting the Medicare Part B drugs that would be eligible for
inclusion in the MFN Model and a different geographic area; (3) the
parameters in the October 2018 ANPRM for a potential IPI Model for
Medicare Part B Drugs; \89\ and (4) not implementing the model. In
addition, when developing the parameters for the October 2018 ANPRM and
this IFC, we noted that there are a range of methods to implement
external reference pricing, and these different approaches would affect
the impact of the model.90 91 In examining potential
variations of certain parameters included in this IFC, we considered
potential differences such variations would have on the impacts
presented in sections VI.C.1. and VI.C.2. of this IFC. We note that a
potential model design with a longer MFN Price phase-in would have a
lower estimate of overall Medicare savings; for example, a 7-year
phase-in of the MFN Price over a 7-year model performance period would
reduce estimates of Medicare savings in the OACT estimate by
approximately 25 percent. As noted in section III.E.5. of this IFC, our
policy is to phase-in the MFN Price more quickly during the initial
years to allow CMS to test the full phase-in of the MFN Price. In
considering the scope of the model, we actively assessed whether to
pursue a smaller geographic scope. As we discuss in section III.C.3. of
this IFC, we reviewed the comments that we received on the October 2018
ANPRM, where we considered 50 percent of the country in a model. We
weighed whether the ability to have a research design where we would
compare changes in drug spending and utilization relative to a
comparison group, a design that CMS uses frequently in its models,
would outweight the concerns we highlight in section III.C.3. of this
IFC. We ultimately concluded that operational concerns such as
administrative complexity as well as the risk to model integrity
associated with a limited geographic scope, as described in section
III.C.3. of this IFC, necessitate a test with a nationwide scope using
a different evaluation design.
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\89\ https://www.federalregister.gov/documents/2018/10/30/2018-23688/medicare-program-international-pricing-index-model-for-medicare-part-b-drugs.
\90\ https://jasmin.goeg.at/432/1/EURIPID_GuidanceDocument_V8.1_310718.pdf.
\91\ https://ec.europa.eu/health/sites/health/files/systems_performance_assessment/docs/pharmaproductpricing_frep_en.pdf.
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The estimates for the impact of this IFC show a substantial
reduction in Medicare Part B spending over a 7-year model.
[[Page 76247]]
In comparison, the parameters considered in the October 2018 ANPRM were
estimated to result in a less substantial reduction in Medicare Part B
spending over a 5-year model.\92\ The alternative of not implementing
the model would not have an impact compared to existing policy.
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\92\ https://www.federalregister.gov/documents/2018/10/30/2018-23688/medicare-program-international-pricing-index-model-for-medicare-part-b-drugs.
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F. Accounting Statements and Tables
As required by OMB Circular A-4 under Executive Order 12866
(available at https://obamawhitehouse.archives.gov/omb/circulars_a004_a-4/) in Tables 17 and 18 we have prepared two
accounting statements, based on the OACT and ASPE estimates
respectively, showing the classification of transfers, benefits, and
costs associated with the provisions in this IFC. The transfer from
beneficiaries to providers and MA plans represents the premium change
attributable to the drug price, i.e., the difference between the gross
impact and the net impact in the drug price section of Table 12. The
accounting statement in Table 17 is based on estimates provided in this
regulatory impact analysis in Table 12 and the accounting statement in
Table 18 is based on estimates in Table 16. Tables 17 and 18 include
the estimated effect and burden estimates on beneficiaries outlined in
section VI.C.4. of this IFC and on participants and manufacturers in
section VI.C.5. of this IFC. The costs shown in Table C18 reflect
additional medical expenses incurred as a result of the potential loss
of access to certain drugs for some beneficiaries in the ASPE estimate.
[GRAPHIC] [TIFF OMITTED] TR27NO20.010
[[Page 76248]]
[GRAPHIC] [TIFF OMITTED] TR27NO20.011
G. Conclusion
The changes in this IFC will affect providers and suppliers that
furnish separately payable Medicare Part B drugs in the outpatient
setting for which annual Medicare FFS spending is high. These providers
and suppliers are mostly physicians (including physician practices),
non-physician practitioners, supplier groups, HOPDs (including on- and
off-campus outpatient provider-based departments, but excluding cancer
hospitals, children's hospitals and CAHs), and ASCs. We estimate that
the effect of the MFN Model on providers and suppliers willvary,
depending on their type, location, what drugs they furnish, their
clinical patterns, and the alternative add-on payment for the MFN
Model. We estimate that eligible providers and suppliers will
experience a decrease in overall payment related to the MFN Model. We
estimate that beneficiaries who receive included drugs from MFN
participants will experience a decrease in cost-sharing, however, some
beneficiaries' providers and suppliers may choose not to offer access
to the MFN Model drugs, causing these beneficiaries to seek alternative
providers, treatment alternatives, or forgo access. The financial
hardship exemption is designed to mitigate this risk.
The changes in this IFC will also affect MA organizations, drug
manufacturers, primary and secondary payers, and potentially non-
Medicare patients. MA organizations will experience lower payments as a
result of the MFN Model because the MA ratebook calculations will
reflect changes in actual FFS spending due to the impact of the model.
Drug manufacturers may have lower revenue, depending upon their
behavioral response to the MFN Model. Other payers, including State
Medicaid Programs, and patients who take prescription drugs may
experience direct or indirect spillover effects that may increase or
decrease their costs. In addition, as shown in Tables 12 and 16, the
changes we are adopting in this IFC will reduce state and federal
Medicaid spending and beneficiary spending on Medicare premiums.
In accordance with the provisions of E.O. 12866, this IFC was
reviewed by the Office of Management and Budget.
VII. Waiver of Proposed Rulemaking and Delay in Effective Date
Under 5 U.S.C. 553(b) of the Administrative Procedure Act (APA),
the agency is required to publish a notice of the proposed rule in the
Federal Register before the provisions of a rule take effect.
Similarly, section 1871(b)(1) of the Act requires the Secretary to
provide for notice of the proposed rule in the Federal Register and
provide a period of not less than 60 days for public comment. Section
553(b)(B) of the APA provides for exceptions from the notice and
comment requirements; in cases in which these exceptions apply, section
1871(b)(2)(C) of the Act provides for exceptions from the notice and
60-day comment period requirements of the Act as well. Section
553(b)(B) of the APA and section 1871(b)(2)(C) of the Act authorize an
agency to dispense with
[[Page 76249]]
normal rulemaking requirements for good cause if the agency makes a
finding that the notice and comment process is impracticable,
unnecessary, or contrary to the public interest.
High drug prices in the U.S. have serious economic and health
consequences for beneficiaries in need of treatment. Increasing
premiums, out-of-pocket costs in both Part B and Part D, and increases
in drug prices are causing beneficiaries to divert scarce resources to
pharmaceutical treatments and away from other needs, or prompting them
to skip doses of their medications, take less than the recommended
doses, or abandon treatment altogether.93 94 In Medicare
Part B, drug spending increased by over 9 percent between 2009 and
2017. Over two thirds of that increase in spending was based on
increases in drug prices alone, and only one third due to increases in
utilization.\95\ Prices of certain drugs have increased by double-digit
percentages over time.\96\ These dramatic increases are on prices where
the U.S. already pays significantly more than other countries.\97\ When
CMS announced the 2020 Part B Premiums and Deductibles, we noted that
the increases in Part B premiums and deductibles was largely due to
rising spending on physician-administered drugs.\98\
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\93\ Kirzinger A, Neuman T, Cubanski J, Brodie M. Data Note:
Prescription Drugs and Older Adults, Aug 09, 2019, Kaiser Family
Foundation https://www.kff.org/health-reform/issue-brief/data-note-prescription-drugs-and-older-adults/.
\94\ Kirzinger A, Lopes L, Wu B, Brodie M. KFF Health Tracking
Poll--February 2019: Prescription Drugs, Kaiser Family Foundation,
Mar 01, 2019, https://www.kff.org/health-costs/poll-finding/kff-health-tracking-poll-february-2019-prescription-drugs/.
\95\ Medicare Payment Advisory Commission, Report to Congress
``Chapter 3: Medicare payment strategies to improve price
competition and value for Part B drugs,'' June 2019, https://www.medpac.gov/docs/default-source/reports/jun19_ch3_medpac_reporttocongress_sec.pdf?sfvrsn=0.
\96\ Hernandez I, San-Juan-Rodriguez A, Good CB, Gellad WF.
Changes in List Prices, Net Prices, and Discounts for Branded Drugs
in the US, 2007-2018. JAMA. 2020;323(9):854-862. doi:10.1001/
jama.2020.1012.
\97\ Comparison of U.S. and International Prices for Top
Medicare Part B Drugs by Total Expenditures'' https://aspe.hhs.gov/pdf-report/comparison-us-and-international-prices-top-medicare-part-b-drugs-total-expenditures.
\98\ CMS Newsroom. 2020 Medicare Parts A & B Premiums and
Deductibles. https://www.cms.gov/newsroom/fact-sheets/2020-medicare-parts-b-premiums-and-deductibles.
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With more than 25 million Medicare beneficiaries living at or below
200 percent of the Federal Poverty Line (FPL),\99\ high drug prices
could lead to improper medication adherence or skipped treatment. The
consequences of these behaviors can result in poor clinical outcomes
for chronic disease management.\100\ The COVID-19 pandemic has rapidly
exacerbated these problems. The risk of severe illness from COVID-19
increases with age and the presence of chronic illnesses, putting many
older adults at the highest risk levels.101 102 This is of
particular concern given that 84 percent of individuals over the age of
65 having at least one chronic health condition, and more than 53
million adults over the age of 65 are enrolled in
Medicare.103 104 With adults 65 and older comprising 8 out
of 10 COVID-19 deaths reported in the U.S., COVID-19 has
disproportionately impacted Americans 65 or older.\105\
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\99\ Schoen C, Davis K, Willink A, Medicare Beneficiaries' High
Out of Pocket Costs: Cost Burdens by Income and Health Status,
Commonwealth Fund, May 12, 2017, https://www.commonwealthfund.org/publications/issue-briefs/2017/may/medicare-beneficiaries-high-out-pocket-costs-cost-burdens-income?redirect_source=/publications/issue-briefs/2017/may/medicare-out-of-pocket-cost-burdens.
\100\ https://www.cdc.gov/mmwr/volumes/66/wr/mm6645a2.htm.
\101\ https://www.cdc.gov/coronavirus/2019-ncov/need-extra-
precautions/older-
adults.html#:~:text=Risk%20for%20Severe%20Illness%20Increases%20with%
20Age&text=The%20greatest%20risk%20for%20severe%2cas%20having%20under
lying%20medical%20conditions.
\102\ https://www.cdc.gov/coronavirus/2019-ncov/need-extra-precautions/people-with-medical-conditions.html.
\103\ National Council on Aging, https://www.ncoa.org/economic-security/money-management/debt/senior-debt-facts/.
\104\ MMCO Statistical & Analytic Reports, Managed Care
Enrollment Trends (2006-2018 Data), https://www.cms.gov/Medicare-Medicaid-Coordination/Medicare-and-Medicaid-Coordination/Medicare-Medicaid-Coordination-Office/Analytics.
\105\ https://www.cdc.gov/coronavirus/2019-ncov/need-extra-
precautions/older-
adults.html#:~:text=Risk%20for%20Severe%20Illness%20Increases%20with%
20Age&text=The%20greatest%20risk%20for%20severe%2cas%20having%20under
lying%20medical%20conditions.
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Furthermore, the COVID-19 pandemic has led to historic levels of
unemployment in the U. S., with both the unemployment rate and number
of unemployed persons remaining nearly twice their Feburary (pre-
pandemic) numbers.\106\ The COVID-19 pandemic has also led to an
increase in food prices, straining budgets for many of America's
seniors, particularly those who live on fixed incomes,\107\ such as the
6 million Medicare fee-for-service beneficiaries without supplemental
coverage and over 12 million beneficiaries dually eligible for Medicare
and Medicaid.108 109 110 Already facing increased financial
burden, this population is in need of urgent relief from high drug
prices in order to prevent stinting on care and alleviate general
financial instability worsened by the COVID-19 pandemic. This need is
exacerbated in communities of color and among women, wherein Black,
Latino, and Hispanic adults face higher economic insecurity than their
white counterparts.\111\ The economic disruptions caused by the COVID-
19 pandemic have increased the burdens placed on America's seniors and
other Medicare Part B beneficiaries and given rise to an urgent need
for swift action to reduce drug prices. Though we have seen some
positive economic and employment trends since the initial peak in
April,\112\ we are currently seeing a new surge in COVID-19 cases that
may lead to additional hardship and requires immediate action.\113\ As
such, we find that there is good cause to waive the notice and comment
requirements under sections 553(b)(B) of the APA and section
1871(b)(2)(C) because of the particularly acute need for affordable
Medicare Part B drugs now, in the midst of the COVID-19 pandemic.
Implementation of this model will provide immediate relief to Medicare
beneficiaries through reduced copays for MFN drugs due to lower drug
payments and no beneficiary cost-sharing on the alternative add-on
payment.
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\106\ U.S. Bureau of Labor Statistics. Economic News Release.The
Employment Situation--October 2020. November 06, 2020. https://www.bls.gov/news.release/empsit.nr0.htm.
\107\ 54 million people in America face food insecurity during
the pandemic. It could have dire consequences for their health.
AAMC. October 15, 2020. https://www.aamc.org/news-insights/54-million-people-america-face-food-insecurity-during-pandemic-it-could-have-dire-consequences-their.
\108\ MMCO Statistical & Analytic Reports, Managed Care
Enrollment Trends (2006-2018 Data), https://www.cms.gov/Medicare-Medicaid-Coordination/Medicare-and-Medicaid-Coordination/Medicare-Medicaid-Coordination-Office/Analytics.
\109\ An Overview of Medicare, Kaiser Family Foundation, Feb 12,
2019, https://www.kff.org/medicare/issue-brief/an-overview-of-medicare/.
\110\ Note: The number of Medicare beneficiaries without
supplemental insurance is from 2016 while the dual eligible numbers
are from 2018.
\111\ Center on Budget and Policy Priorities, Tracking the
COVID-19 Recession's Effects on Food, Housing, and Employment
Hardships. November 9, 2020. https://www.cbpp.org/research/poverty-and-inequality/tracking-the-covid-19-recessions-effects-on-food-housing-and.
\112\ U.S. Bureau of Labor Statistics. Economic News Release.The
Employment Situation- October 2020. November 06, 2020. https://www.bls.gov/news.release/empsit.nr0.htm.
\113\ Center for Disease Control. COVID-19 Forecasts: Cases.
https://www.cdc.gov/coronavirus/2019-ncov/cases-updates/forecasts-cases.html.
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We also usually provide for a delay in effective date under section
553(d) of the APA and section 1871(e)(1)(B) of the Act. However, such
delay in effective date may be waived for good cause,
[[Page 76250]]
when such delay is impracticable, unnecessary, or contrary to the
public interest, and the agency incorporates a statement of the finding
and a brief statement of the reasons therefore in the notice. We find
that delaying implementation of this IFC is contrary to the public
interest for the same reasons that we find good cause to waive prior
notice and comment.
List of Subjects in 42 CFR Part 513
Administrative practice and procedure, Health facilities, Medicare,
Reporting and recordkeeping requirements.
0
For the reasons set forth in the preamble and under the authority at 5
U.S.C. 301, the Centers for Medicare & Medicaid Services amends 42 CFR
Chapter IV by adding part 513 to read as follows:
SUBCHAPTER H--HEALTH CARE INFRASTRUCTURE AND MODEL PROGRAMS
PART 513--Most Favored Nation (MFN) MODEL
Sec.
Subpart A--General Provisions
513.1 Basis, scope, and duration.
513.2 Definitions.
Subpart B--Inclusion in the Model
513.100 MFN Model payments and MFN participants.
513.120 MFN Model geographic area.
513.130 MFN Model drugs, updates, categories and exclusions.
513.140 Included international data.
Subpart C--Payment Process and Methodology
513.200 Payment process and beneficiary cost-sharing.
513.210 Model payment methodology for MFN Model drugs.
513.220 Model alternative add-on payment.
513.230 Financial Hardship Exemptions, Request Process, and
Reconciliation Payment.
Subpart D--[Reserved]
Subpart E--Quality Strategy, Beneficiary Protections, and Compliance
Activities
513.400 Quality measures.
513.410 Beneficiary protections.
513.420 Monitoring and compliance activities.
513.430 Audits and record retention.
513.440 Enforcement authority.
513.450 Limitations on review.
Subpart F--Waivers
513.500 Waivers of Medicare program requirements for purposes of
testing the MFN Model.
Subparts G through J--[Reserved]
Subpart K--Model Termination
513.1000 Termination of the MFN Model.
Authority: 42 U.S.C. 1302, 1315(a), and 1395hh.
Subpart A--General Provisions
Sec. 513.1 Basis, scope, and duration.
(a) Basis. This part implements the test of the Most Favored Nation
(MFN) Model under section 1115A of the Act. Except as specifically
noted in this part, the regulations under this part do not affect
payment, coverage, program integrity, or any other requirements that
otherwise apply to providers of services and suppliers under this
chapter.
(b) Scope. This part sets forth the following:
(1) The types of providers and suppliers required to participate in
the MFN Model and applicable requirements.
(2) The beneficiaries included in the MFN Model.
(3) The drugs included in the MFN Model.
(4) The methodologies for establishing Medicare payment amounts for
and making payments for MFN Model drugs, including an alternative add-
on payment.
(5) Beneficiary protections.
(6) Beneficiary cost-sharing.
(c) Duration. The MFN Model has a performance period of 7
performance years. The first performance year (performance year 1)
begins on January 1, 2021, and the final performance year ends on
December 31, 2027, unless sooner terminated in accordance with Sec.
513.1000.
Sec. 513.2 Definitions.
For the purpose of this part the following definitions are
applicable unless otherwise stated:
Add-on percentage means the percentage above 100 percent.
Alternative add-on payment means the payment described in Sec.
513.220.
Applicable ASP means the payment amount determined in accordance
with section 1847A of the Act for a quarter minus the applicable add-on
percentage.
ASP stands for average sales price.
ASP calendar quarter means the period that is two calendar quarters
prior to the calendar quarter to which the MFN Drug Payment Amount will
apply.
CCN stands for CMS Certification Number.
Country-level price means the unadjusted country-level price for an
MFN Model drug at the HCPCS code level as calculated in accordance with
Sec. 513.210(b)(2).
CPI-U stands for Consumer Price Index for All Urban Consumers based
on all items in U.S. city average and not seasonally adjusted.
Days means calendar days.
DME stands for Durable Medical Equipment.
FDA stands for Food and Drug Administration.
GDP stands for gross domestic product.
GDP-adjusted country-level price means the country-level price
adjusted by the GDP adjuster as calculated in accordance with Sec.
513.210(b)(4).
GDP adjuster means the country-specific adjuster as calculated in
accordance with Sec. 513.210(b)(3).
HCPCS stands for Healthcare Common Procedure Coding System.
HCPCS code level means the specified drug and amount described in
the HCPCS code long descriptor.
MAC stands for Medicare Administrative Contractor.
Manufacturer's average sales price has the same meaning as under 42
CFR Subpart J.
MFN stands for most favored nation.
MFN beneficiary means an individual who is furnished an MFN Model
drug by an MFN participant and who, on the date of service, is enrolled
in Medicare Part B, has Medicare as his or her primary payer, and is
not covered under Medicare Advantage or any other group health plan,
including a United Mine Workers of America health plan.
MFN Drug Payment Amount means the portion of the total allowed
payment amount for an MFN Model drug determined in accordance with
Sec. 513.210.
MFN Model drug means a separately payable Medicare Part B drug or
biological described by a HCPCS code included on the MFN Model Drug
HCPCS Codes List.
MFN Model Drug HCPCS Codes List means the list of drugs included in
the MFN Model for a given calendar quarter of a performance year
established under Sec. 513.130.
MFN participant means a Medicare participating provider or
supplier, identified by its CCN or TIN, that is required to participate
in the MFN Model in accordance with Sec. 513.100(b).
MFN Model Payment means the total payment to an MFN participant for
an MFN Model drug in accordance with subpart C of this part, inclusive
of the MFN Drug Payment Amount and the Alternative Add-on Payment.
MFN Price means the lowest GDP-adjusted country-level price of the
countries specified in Sec. 513.140(b) for an MFN Model drug.
Model performance period means the 7-year period of time beginning
on January 1, 2021, through December 31, 2027.
NOC stands for not otherwise classified.
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OIG stands for the Department of Health and Human Services Office
of Inspector General.
Outpatient prospective payment system (OPPS) means the payment
system for designated hospital outpatient items and services and
certain Medicare Part B services furnished to hospital inpatients when
Part A payment cannot be made as defined by section 1833(t) of the Act.
Performance year means each 12-month period beginning on January 1
and ending on December 31 during the performance period for the MFN
Model specified in Sec. 513.1(c).
Provider means a ``provider of services'' as defined under section
1861(u) of the Act and codified at Sec. 400.202 of this chapter.
Supplier means a supplier as defined in section 1861(d) of the Act
and codified at Sec. 400.202 of this chapter.
TIN stands for taxpayer identification number.
WAC means wholesale acquisition cost as defined at section
1847A(c)(6)(B) of the Act.
Subpart B--Inclusion in the Model
Sec. 513.100 MFN Model payments and MFN participants.
(a) General. Subject to the exceptions specified in paragraph (d)
of this section, the MFN Model payments specified under this part apply
only to claims for an MFN Model drug furnished to an MFN beneficiary by
an MFN participant.
(b) MFN participants. Subject to the exclusions specified in
paragraph (c) of this section, the MFN Model requires participation by
each Medicare participating provider and supplier that submits a claim
(except for claims specified in paragraph (d) of this section) for a
separately payable drug that is an MFN Model drug furnished to an MFN
beneficiary.
(c) Excluded providers and suppliers. The following are excluded
from participation in the MFN Model:
(1) Children's hospitals (defined under section 1886(d)(1)(B)(iii)
of the Act).
(2) PPS-exempt cancer hospitals (defined under section
1886(d)(1)(B)(v) of the Act).
(3) Critical access hospitals (CAHs) (defined under section 1820 of
the Act).
(4) Indian Health Service (IHS) facilities (as described in section
1880 of the Act)), except when MFN Model drugs are furnished and such
service is described in section 1880(e)(2)(B) of the Act.
(5) Federally Qualified Health Centers (FQHCs) (defined under
section 1861(aa)(4) of the Act).
(6) Rural Health Clinics (RHCs) (defined under section 1861(aa)(2)
of the Act).
(7) Hospitals that are not subsection (d) hospitals (as defined in
section 1886(d)(1)(B) of the Act) and are paid on the basis of
reasonable costs subject to a ceiling under section 1886(b) of the Act.
(8) Extended neoplastic disease care hospitals (defined in section
1886(d)(1)(B)(vi) of the Act).
(9) For the first quarter and second quarter of performance year 1,
acute care hospitals that participate in any model authorized under
section 1115A of Act for which payment for outpatient hospital services
furnished to Medicare FFS beneficiaries, including MFN Model drugs, is
made under such model on a fully capitated or global budget basis under
a waiver of section 1833(t) of the Act.
(10) Beginning with the third quarter of performance year 1, acute
care hospitals that participate in any model authorized under section
1115A of Act for which payment for outpatient hospital services
furnished to Medicare FFS beneficiaries, including MFN Model drugs, is
made under such model on a fully capitated or global budget basis under
a waiver of section 1833(t) of the Act, where the parameters of such
model adjust for the difference in payment for MFN Model drugs between
the MFN Model and non-MFN Model drug payments such that savings under
the MFN Model are incorporated into the other CMS Innovation Center
model's parameters (for example, the annual global budget) for the
duration of the MFN Model.
(d) Exceptions. The MFN Model payments specified under this part do
not apply to any of the following:
(1) Claims for MFN Model drugs furnished in the inpatient hospital
setting under those circumstances where Part A would not pay for
hospital services.
(2) Claims for MFN Model drugs administered during an inpatient
hospital stay or included on an inpatient hospital claim.
(3) Claims administered by the DME MACs as described in Sec.
421.404(c)(2) of this chapter.
(4) Claims paid under the End-Stage Renal Disease Prospective
Payment System, including claims paid using the transitional drug add-
on payment adjustment.
(e) MFN participant requirements during the MFN Model. During the
model performance period described in Sec. 513.1(c), MFN participants
must do all of the following:
(1) Adhere to the beneficiary protections requirements under Sec.
513.410.
(2) Adhere to the MFN Model-specific billing instructions
requirements established by CMS and the MAC responsible for processing
the MFN participant's claims, including without limitation those
described in Sec. 513.200.
(3) Participate in MFN Model monitoring and evaluation activities
in accordance with Sec. 403.1110(b) of this chapter, including
collecting and reporting information as the Secretary determines is
necessary to monitor and evaluate the MFN Model, including without
limitation ``protected health information'' as that term is defined at
45 CFR 160.103.
(f) MFN participant requirements after the MFN Model. For 2 years
after termination of the MFN Model, MFN participants must participate
in MFN Model monitoring activities as described in Sec. 513.420.
Sec. 513.120 MFN Model geographic area.
The MFN Model geographic area is all states and U.S. territories.
Sec. 513.130 MFN Model drugs, updates, categories and excluded
drugs.
(a) MFN Model drugs. CMS creates and periodically updates the MFN
Model Drug HCPCS Codes List as described in this section. The MFN Model
Drug HCPCS Codes List designates the MFN Model drugs, which are subject
to the MFN Model payments specified in subpart C of this part.
(1) Initial MFN Model Drug HCPCS Codes List. For the beginning of
performance year 1, CMS identifies the top 50 drugs by HCPCS code with
the highest aggregate 2019 Medicare Part B total allowed charges after
making the exclusions specified in paragraphs (b)(1) and (b)(2) of this
section, and adds the remaining HCPCS codes, after updating such HCPCS
codes for any applicable changes, to the MFN Model Drug HCPCS Codes
List. Final action claims with dates of service within calendar year
2019 and allowed charges greater than $0 are used to determine
aggregate 2019 Medicare Part B total allowed charges.
(2) Annual Update of the MFN Model Drug HCPCS Codes List. For the
start of each subsequent performance year, using Medicare Part B total
allowed charge from the next subsequent calendar year, CMS identifies
the top 50 drugs by HCPCS code with the highest aggregate Medicare Part
B total allowed charges, after making the exclusions specified in
paragraphs (b)(1) and (b)(2) of this section, for the most recent full
calendar year, and adds any remaining
[[Page 76252]]
HCPCS codes not already on the MFN Model Drug HCPCS Codes List to the
MFN Model Drug HCPCS Codes List, after updating such HCPCS codes for
any applicable changes, effective on the first day of the performance
year.
(3) Removal. No more frequently than quarterly, CMS removes HCPCS
codes from the MFN Model Drug HCPCS Codes List when CMS becomes aware
that all of the National Drug Codes assigned to the HCPCS code have
been permanently withdrawn from the U.S. market and the drug has been
permanently withdrawn from the U.S. market, the specific HCPCS code
included on the MFN Model Drug HCPCS Codes List is terminated with no
replacement code available or planned, or an exclusion in paragraph
(b)(1) of this section applies.
(4) Maintenance. No more frequently than quarterly, CMS revises
HCPCS codes on the MFN Model Drug HCPCS Codes List as necessary to
reflect quarterly HCPCS code updates that are applicable to the HCPCS
codes on the MFN Model Drug HCPCS Codes List, including adding
replacement codes for HCPCS codes that were terminated.
(b) Exclusions. (1) The following are excluded from the MFN Model:
(i) Vaccines specified in section 1861(s)(10) of the Act
(influenza, pneumococcal pneumonia, coronavirus disease 2019 (COVID-
19), and Hepatitis B vaccines).
(ii) Radiopharmaceuticals.
(iii) Oral anticancer chemotherapeutic agents described in section
1861(s)(2)(Q) of the Act.
(iv) Oral anti-emetic drugs described in 1861(s)(2)(T) of the Act.
(v) Oral immunosuppressive drugs described in section 1861(s)(2)(J)
of the Act.
(vi) Compounded drugs.
(vii) Intravenous immune globulin products.
(viii) Drugs billed with HCPCS codes that describe a drug product
that was approved under an abbreviated new drug application under
section 505(j) of the Federal Food, Drug, and Cosmetic Act;
(ix) Drugs for which there is an Emergency Use Authorization (EUA)
from FDA, or FDA approval, to treat patients with suspected or
confirmed COVID-19; or
(x) Drugs billed using a not otherwise classified (NOC) or not
otherwise specified (NOS) billing and payment code.
(2) The following claims are excluded from the determination of
whether a drug is to be included on the MFN Model Drug HCPCS Codes
List:
(i) Professional claims with a place of service code indicating a
home setting, including home, homeless shelter, assisted living
facility, group home, temporary lodging, and custodial care facilities.
(ii) Claims administered by the DME MACs as described in Sec.
421.404(c)(2) of this chapter.
Sec. 513.140 Included international data.
(a) General. (1) CMS uses drug pricing information from
international data sources, available to CMS at least 20 business days
prior to the start of a calendar quarter, meeting the requirements in
paragraph (c) of this section for MFN Model drugs from countries
included in paragraph (b) of this section.
(2) For purposes of selecting a data source for each MFN Model drug
for a calendar quarter, CMS identifies available international drug
pricing information data sources for the MFN Model drug, by aligning
the MFN Model drug's HCPCS code long description (including dosage
form) with the data sources' standardized method for identifying
scientific names or nonproprietary names and dosage formulations, as
applicable.
(b) Non-U.S. member countries of the Organisation for Economic Co-
operation and Development (OECD). (1) CMS uses available international
sales, volume, and pricing data for countries that were non-U.S. OECD
member countries as of October 1, 2020 with a GDP per capita that is at
least 60 percent of the U.S. GDP per capita as determined by CMS in
accordance with this paragraph (b).
(2) Each country's GDP per capita is assessed using data available
at the end of the applicable ASP calendar quarter.
(3) Subject to the limitation specified in paragraph (b)(4) of this
section, the GDP per capita for a country is the the most recent
estimate of GDP per capita based on purchasing power parity for that
country available in the U.S. Central Intelligence Agency (CIA) World
Factbook.
(4) The country's GDP per capita and U.S. GDP per capita selected
from the CIA World Factbook must be for the same year.
(5) CMS identifies countries with a GDP per capita that is at least
60 percent of the U.S. GDP per capita by dividing the GDP per capita
for a country by the U.S. GDP per capita and assessing the results.
(c) Identification of international data sources. (1) CMS obtains
data from one or more international drug pricing information data
sources for purposes of identifying available international drug
pricing information for the countries specified in paragraph (b) of
this section.
(2) Such data sources must, as determined by CMS--
(i) Utilize a standardized method for identifying drugs across
countries within that data source, such as using internationally
recognized scientific and nonproprietary product names;
(ii) Utilize a standard method for identifying drug forms that at a
minimum distinguishes among injectable, oral, and other forms of a
drug; and
(iii) Be maintained by an organization that seeks to limit the lag
inherent in data to no more than 180 days from the end of the calendar
quarter for which drug pricing information is compiled to the time that
the organization makes such updates available to users of the database.
(iv) Contains international drug pricing information stated in U.S.
currency, such as the following:
(A) Sales data, which may be based on ex-manufacturer prices
(sometimes called ex-factory prices) that represent actual or
calculated prices paid to the manufacturer by wholesalers and other
distributors, or retail prices that represent actual or calculated
sales for retail purchasers, or prices paid by other purchasers in the
distribution channels.
(B) Volume data (for example, number of packages or units sold).
(C) List prices.
(v) Have mechanisms in place to maintain, update, and correct, if
necessary, the information on international drug pricing in the data
source on at least a quarterly basis.
(3) For each MFN Model drug for a calendar quarter, CMS selects a
data source using the following hierarchy.
(i) The data source contains sales and volume data for the
applicable ASP calendar quarter from at least one country described in
paragraph (b) of this section.
(ii) The data source does not have sales and volume data for the
applicable ASP calendar quarter, but contains sales and volume data for
any prior ASP calendar quarter beginning on or after October 1, 2019
from at least one country described in paragraph (b) of this section.
If sales and volume data from a prior ASP calendar quarter are used,
CMS uses sales and volume data from the most recent ASP calendar
quarter for which both sales and volume data are available.
(iii) The extracted data used by CMS to determine the most recent
MFN Price used to calculate an MFN Drug Payment Amount posted on the
MFN Model website.
[[Page 76253]]
(iv) The data source contains ex-manufacturer price data for the
applicable ASP calendar quarter from at least one country described in
paragraph (b) of this section.
(v) The data source contains list price data for the applicable ASP
calendar quarter from at least one country described in paragraph (b)
of this section.
(vi) If there is more than one data source for an ASP calendar
quarter, for each MFN Model drug, CMS selects the data source at the
highest level of the hierarchy that contains information from the
highest number of countries described in paragraph (b) of this section
and, if available, incorporates discounts and rebates into its drug
pricing information, and uses this data source to calculate the MFN
Price as described in Sec. 513.210(b).
Subpart C--Payment Process and Methodology
Sec. 513.200 Payment process and beneficiary cost-sharing.
(a) General. For purposes of the MFN Model, the allowed MFN Drug
Payment Amount does not exceed the billed amount on the claim for the
MFN Model drug.
(b) Model-specific billing instructions. MFN participants submit
claims for MFN Model drugs to the applicable MAC in the form and manner
specified by CMS in model-specific billing instructions.
(c) Beneficiary cost-sharing. Beneficiary coinsurance does not
apply to the portion of the allowed payment amount for an MFN Model
drug that is determined under Sec. 513.220.
Sec. 513.210 Model payment methodology for MFN Model drugs.
(a) Payment amount. The total allowed payment amount for an MFN
Model drug furnished to an MFN beneficiary by an MFN participant on a
given date of service within a calendar quarter is determined in
accordance with this section. The total allowed payment equals--
(1) For each billing unit in the HCPCS code descriptor of the MFN
Model drug, the MFN Drug Payment Amount determined in accordance with
paragraphs (b), (c) and (d) of this section, as applicable, where the
allowed MFN Drug Payment Amount does not exceed the billed amount on
the claim for the MFN Model drug as described in Sec. 513.200(a); and
(2) The alternative add-on payment determined under Sec. 513.220.
(b) Calculation of the MFN Drug Payment Amount with Available
International Drug Pricing Data. CMS selects an available international
drug pricing information data source described in Sec. 513.140(c) for
at least one country specified in Sec. 513.140(b) for an MFN Model
drug, and calculates, in advance of each calendar quarter for a
performance year, the applicable MFN Drug Payment Amount for one
billing unit of an MFN Model drug using the following steps:
(1) Available international drug pricing data. (i) For the MFN
Model drug, using the data source selected in accordance with Sec.
513.140(c)(3) (except for a data source described in Sec.
513.140(c)(3)(iii)), CMS identifies available international drug
pricing data for the MFN Model drug, by aligning the MFN Model drug's
HCPCS code long description (including dosage form) with the data
sources' standardized method for identifying scientific names or
nonproprietary names and dosage formulations, as applicable. CMS
extracts available drug pricing data for the countries specified in
Sec. 513.140(b) from the selected international drug pricing
information data source. CMS uses the extracted data that have complete
package size information and only for dosage formulations that could be
described by the MFN Model drug's HCPCS code descriptor, as determined
by CMS. If a data source described in Sec. 513.140(c)(3)(iii) is
selected, CMS uses such extracted data.
(ii) When international drug pricing data with sales and volume
data are available, CMS excludes from the calculation of the unadjusted
country-level price under paragraph (b)(2) of this section
international drug pricing data without both sales and volume data,
with less than $1,000 in quarterly sales (expressed as U.S. currency),
or with less than 1,000 units in quarterly volume.
(iii) CMS converts the extracted volume data to the MFN Model
drug's HCPCS code billing unit level, as applicable.
(iv) CMS adjusts the extracted volume data, as applicable, before
converting the extracted volume data to the MFN Model drug's HCPCS code
billing unit level when the data source shows the package size of a
drug product that is inconsistent with the manufacturer's information
about that product, as determined by CMS.
(v) CMS limits the number of HCPCS code billing units when--
(A) The package labeling indicates a limited amount of drug is to
be used from the package; and
(B) The HCPCS code dosage is per dose.
(2) Calculate the unadjusted country-level price for the MFN Model
drug by country.
(i) Using the drug pricing data extracted and adjusted in
accordance with paragraph (b)(1) of this section, CMS calculates the
unadjusted country-level price for the MFN Model drug by country, using
the calculation that is applicable.
(ii) If an international drug pricing information data source with
sales and volume data is used, the applicable calculation is as
follows:
(A) CMS sums the adjusted volume data (as specified in paragraph
(b)(1)(iii) of this section) for the drug.
(B) CMS sums the total sales for the drug (that remain after
performing the exclusions in paragraph (b)(1)(ii) of this section).
(C) CMS divides the sum determined in paragraph (b)(2)(ii)(B) of
the section by the sum determined in paragraph (b)(2)(ii)(A) of this
section, resulting in an average price per unit of drug, where the unit
of drug is the same as the HCPCS code billing unit.
(iii) If an international drug pricing information data source with
ex-manufacturer or list prices is used, the applicable calculation is
as follows:
(A) For each extracted ex-manufacturer or list price, CMS
calculates the number of HCPCS billing units in the package by dividing
the amount of drug in the package by the amount of drug represented in
one HCPCS billing unit.
(B) CMS divides the ex-manufacturer or list price, as applicable,
by the number of HCPCS billing units in the package, resulting in a
price per unit of drug where the unit of drug is the same as the HCPCS
code billing unit.
(C) CMS sums the price per unit of drug calculated in paragraph
(c)(3)(iii)(B) of this section.
(D) CMS divides the sum calculated in paragraph (c)(3)(iii)(C) of
this section by the number of ex-manufacturer or list prices that were
summed in paragraph (c)(3)(iii)(C) of this section, resulting in an
average price per unit of drug where the unit of drug is the same as
the HCPCS code billing unit.
(iv) CMS performs the applicable calculation for each country
specified in Sec. 513.140(b) for which international drug pricing
information is available in the selected data source.
(3) Calculate the GDP adjuster for each country. (i) CMS calculates
the GDP adjuster by dividing the country's GDP per capita by the U.S.
GDP per capita for the same year.
(ii) In cases where the resulting ratio exceeds 1.0, the GDP
adjuster is set to 1.0.
[[Page 76254]]
(iii) Subject to the limitations specified in paragraph (b)(3)(iv)
of this section, the GDP per capita for a country is the most recent
estimate of GDP per capita based on purchasing power parity for that
country available in the CIA World Factbook at the end of the
applicable ASP calendar quarter.
(iv) Limitations. (A) The country's GDP per capita and U.S. GDP per
capita must be for the same year.
(B) The GDP per capita used must be for the same year as the data
used to calculate the unadjusted country-level price, if available, or
the most recent earlier year available.
(4) Apply the GDP adjuster to calculate the GDP-adjusted country-
level price. CMS applies the applicable GDP adjuster identified in
paragraph (b)(3) of this section to each unadjusted country-level price
identified in paragraph (b)(2) of this section to calculate the GDP-
adjusted country-level price by dividing each unadjusted country-level
price by the applicable GDP adjuster.
(5) Identify the lowest GDP-adjusted country-level price. CMS
identifies the lowest GDP-adjusted country-level price for the MFN
Model drug. Except as provided in paragraph (b)(7) of this section, the
price identified is the MFN Model drug's MFN Price.
(6) Identify Applicable ASP. CMS identifies the applicable ASP for
the applicable quarter.
(7) Compare the MFN Price to the applicable ASP. CMS compares the
price determined in paragraph (b)(5) of this section to the applicable
ASP identified in paragraph (b)(6) of this section. The MFN Price
equals the applicable ASP if the applicable ASP is less than the price
determined in paragraph (b)(5) of this section.
(8) Phase-in. CMS identifies the applicable phase-in formula based
on the applicable performance year as follows:
(i) Performance year 1: 75 percent applicable ASP and 25 percent
MFN Price.
(ii) Performance year 2: 50 percent applicable ASP and 50 percent
MFN Price.
(iii) Performance year 3: 25 percent applicable ASP and 75 percent
MFN Price.
(iv) Performance year 4: 100 percent MFN Price.
(v) Performance year 5: 100 percent MFN Price.
(vi) Performance year 6: 100 percent MFN Price.
(vii) Performance year 7: 100 percent MFN Price.
(9) Final calculation steps. (i) CMS applies the applicable phase-
in formula to the applicable ASP and the MFN Price. Subject to any
applicable adjustments as provided in paragraph (d) of this section,
the amount determined in this paragraph is the MFN Drug Payment Amount.
(ii) Subject to the limitation in paragraph (b)(iii) in this
section, CMS recalculates the MFN Drug Payment Amounts for prior
quarters when revised international drug pricing information is
available in the data source that was used to calculate the MFN Price
and applicable ASP updates are available from CMS. CMS prospectively
applies the recalculations in the quarterly update following the
availability of revised international drug pricing information and ASP
updates.
(iii) MFN Drug Payment Amounts may be recalculated for the prior
four calendar quarters of the model.
(c) Frequency of MFN Drug Payment Amount updates. CMS updates the
MFN Drug Payment Amounts on a calendar quarter basis. CMS publishes the
quarterly MFN Drug Payment Amounts on the MFN Model website in advance
of the calendar quarter in which the MFN Drug Payment Amounts apply,
along with any recalculated MFN Drug Payment Amounts for prior
quarters.
(d) Exceptions. (1) Payment for MFN Model drugs for which no
international drug pricing data are available. If, as of the first
calendar quarter during which an MFN Model drug has been included in
the MFN Model Drug HCPCS Codes List in accordance with Sec. 513.130,
no international sales, volume or pricing information meeting the
requirements described in Sec. 513.140(c)--including data used by CMS
to determine the most recent MFN Price used to calculate an MFN Drug
Payment Amount posted on the MFN Model website--is available from any
country described in Sec. 513.120(b) for any calendar quarter
beginning on or after October 1, 2019 through the applicable quarter,
the MFN Drug Payment Amount is the applicable ASP.
(2) Payment for MFN Model drugs that are in short supply. If an MFN
Model drug is reported as ``Currently in Shortage'' by FDA, beginning
with the first day of the next calendar quarter after the date on which
it is reported in shortage, the MFN Drug Payment Amount is the
applicable ASP. CMS calculates payment in accordance with paragraph (b)
of this section as of the first day of the calendar quarter after the
date upon which the drug is no longer reported as ``Currently in
Shortage'' by FDA.
(3) Adjustment to phase-in formula. (i) CMS accelerates the phase-
in of the MFN Price by 5 percentage points at the next quarterly update
to calculate the MFN Drug Payment Amount for the MFN Model drug where
both of the following conditions are met:
(A) There is a greater cumulative percentage increase in either the
applicable ASP or any of the monthly U.S. list prices for the NDCs
assigned to the MFN Model drug's HCPCS code compared to the cumulative
percentage increase in the CPI-U.
(B) There is a greater cumulative percentage increase in either the
applicable ASP or any of the monthly U.S. list prices for the NDCs
assigned to the MFN Model drug's HCPCS code compared to the cumulative
percentage increase in the MFN Price.
(C) For purposes of paragraphs (d)(3)(i)(A) and (B) of this
section, the cumulative percentage increase means the cumulative
percentage change from the end of the baseline to the end of the
applicable ASP calendar quarter.
(D) The baseline in paragraph (d)(3)(i)(C) of this section for an
MFN Model drug is the ASP calendar quarter for the applicable ASP for
the first quarter of performance year 1. If there is not an applicable
ASP for the first quarter of performance year 1 for an MFN Model drug,
the baseline for that MFN Model drug is the ASP calendar quarter for
the first applicable ASP based on the manufacturer's average sales
price for that MFN Model drug that occurs after the ASP calendar
quarter for the applicable ASP for the first quarter of performance
year 1.
(ii) For purposes of paragraph (d)(3)(i) of this section, if the
cumulative percentage increase in CPI-U or MFN Price is negative, CMS
uses zero as the cumulative percentage increase in CPI-U or MFN Price,
as applicable.
(iii) The application of an acceleration of the phase-in formula
continues for the duration of the model performance period.
(iv) CMS applies an additional acceleration of the phase-in formula
for each calendar quarter where the conditions specified in paragraph
(i) are met.
(4) Adjustment for rapid increases in the applicable ASP or any
monthly U.S. list prices beyond inflation and MFN Price after the full
phase-in of the MFN Price. If the conditions described in paragraphs
(d)(3)(i)(A) and (B) of this section are met after the full phase-in of
the MFN Price for an MFN Model drug, for each calendar quarter
thereafter, CMS decreases the MFN Drug Payment Amount equal to largest
difference in the cumulative percentage increase in the applicable ASP
or any of the monthly U.S. list prices for the NDCs
[[Page 76255]]
assigned to the MFN Model drug's HCPCS code compared to the cumulative
percentage increase in the CPI-U and in the MFN Price, respectively,
determined quarterly.
(5) Limitation on MFN Drug Payment Amount. The MFN Drug Payment
Amount cannot exceed the non-model drug payment amount for claim lines
submitted with the JG modifier (or any successor modifier used to
identify drugs purchased under the 340B program) after removing any
add-on amount, if applicable.
(e) Blood clotting factor furnishing fee. When applicable, the
blood clotting furnishing fee under Sec. 410.63(c) of this chapter is
payable along with the MFN Drug Payment Amount.
Sec. 513.220 Model alternative add-on payment.
(a) Payment amount. (1) The total allowed alternative add-on
payment amount for a separately payable dose of an MFN Model drug
furnished to an MFN beneficiary by an MFN participant on a given date
of service within a calendar quarter is determined in accordance with
this section.
(2) The total allowed alternative add-on payment amount for a claim
line does not exceed the billed amount on that claim line.
(b) Calculation of the per-dose alternative add-on payment amount.
CMS calculates the per-dose alternative add-on payment for performance
year 1, quarter 1 for MFN Model drugs using the following steps:
(1) CMS identifies available Medicare Part B fee-for-service final
action claims lines, with dates of service in 2019, for drugs on the
initial MFN Model HCPCS Codes List described in Sec. 513.130(a)(1),
excluding claims for providers and suppliers specified in Sec.
513.100(c), and claims specified in Sec. 513.100(d), that were
furnished by Medicare-participating providers and suppliers, have a
separately paid allowed charge greater than $0, and for which Medicare
Part B was the primary payer. If a HCPCS code on the initial MFN Model
HCPCS Codes List was not in use during any calendar quarter in 2019,
CMS uses the HCPCS code that was applicable for the MFN Model drug
during 2019.
(2) CMS identifies the applicable ASP for each calendar quarter of
2019 for the drugs (by HCPCS code as specified in paragraph (b)(1) of
this section) included on the initial MFN Model HCPCS Codes List. In
the case of a biosimilar biological product, the applicable ASP for the
reference biological product is identified and used in paragraph (b)(3)
of this section.
(3) CMS multiplies the number of units billed for each claim line
described in paragraph (b)(1) of this section by 6.1224 percent of the
applicable ASP identified in paragraph (b)(2) of this section for the
HCPCS code on the claim line and date of service.
(4) CMS sums the products calculated in paragraph (b)(3) of this
section for all claim lines for each MFN Model drug to calculate the
total add-on spending amount for each MFN Model drug.
(5) CMS sums the amounts calculated in paragraph (b)(4) of this
section to calculate the total pooled add-on spending amount for all
MFN Model drugs.
(6) CMS divides the amount calculated in paragraph (b)(5) of this
section by the total number of claim lines retained in paragraph (b)(1)
of this section, excluding claim lines billed with the JW modifier.
(7) CMS trends the amount calculated in paragraph (b)(6) of this
section forward to the applicable ASP calendar quarter for quarter 1 of
performance year 1 using the percentage change in CPI-U from July 2019
through October 2020.
(c) Frequency of alternative add-on payment amount updates. For
each calendar quarter after quarter 1 of performance year 1, CMS
updates the alternative add-on payment by applying a cumulative
inflation factor based on the cumulative percentage change in CPI-U
from October 2020 through the first month of the prior calendar
quarter. If the cumulative percentage change in the CPI-U is negative,
CMS uses an inflation factor of 1.
(d) Limitation on the alternative add-on payment. The alternate
add-on payment is not payable for claim lines billed--
(1) With the JW modifier; or
(2) By MFN participants that receive an alternative add-on payment
for an MFN Model drug under any other model authorized by section 1115A
of the Act that tests an alternative approach to the add-on portion of
payment for Medicare Part B drugs.
Sec. 513.230 Financial hardship exemptions, request process, and
reconciliation payment.
(a) General. For purposes of the MFN Model, a financial hardship
exemption for a performance year may be granted to an MFN participant
by CMS, in its sole discretion and not subject to appeal, when the
provisions in this section are met.
(b) Request for financial hardship exemption. To be eligible for a
financial hardship exemption, the MFN participant must submit a request
for financial hardship exemption in the form and manner and with the
content specified by CMS, including without limitation the requirements
of this paragraph (b).
(1) Timing and form of request. The MFN participant must submit its
request for a financial hardship exemption to CMS in accordance the
submission process posted on the MFN Model website and such request
must be submitted within 60 calendar days following the end of the
performance year for which the MFN participant seeks a financial
hardship exemption.
(2) Request content. The MFN participant's request a financial
hardship exemption must include, at a minimum, all of the following:
(i) Evidence of methods used to obtain each MFN Model drug that was
furnished by the MFN participant during the performance year to any
patient.
(ii) Average net acquisition cost for each MFN Model drug
(inclusive of all on- and off-invoice discounts or adjustments, and any
other price concessions related to the purchase of the MFN Model drug)
that was furnished by the MFN participant during the performance year
to MFN beneficiaries.
(iii) Average net acquisition cost for each MFN Model drug
(inclusive of all on- and off-invoice discounts and adjustments, and
any other price concessions related to the purchase of the MFN Model
drug) that was furnished by the MFN participant during the performance
year to patients who were not MFN beneficiaries.
(iv) Statement of any remuneration received by the MFN participant
from manufacturers of MFN Model drugs, wholesalers, and distributors
that is not reflected in the MFN participant's average net acquisition
costs with a justification of why such remuneration should not be
treated as a price concession related to the purchase of an MFN Model
drug.
(v) Administrative information, including: MFN participant's name,
TIN or CCN (as applicable), contact name, phone number, and email
address.
(vi) The MFN participant's attestation that:
(A) The MFN participant experienced a reduction in Medicare Part B
FFS payments for separately payable drugs on a per beneficiary basis
during the performance year as compared to the prior year (that is, the
four calendar quarters immediately preceding the performance year) due
to its inability to obtain one or more of the MFN Model drugs at or
below the MFN Model Payments for such drugs during the performance
year;
[[Page 76256]]
(B) The MFN participant has not received and will not receive any
remuneration from manufacturers of MFN Model drugs, wholesalers, and
distributors related to the purchase of an MFN Model drug that was
furnished by the MFN participant during the performance year that is
not reflected in the MFN participant's submission; and
(C) The MFN participant submission is true, accurate and complete.
(c) Standard of review. (1) Incomplete requests for a financial
hardship exemption, as determined by CMS, are not reviewed.
(2) CMS grants a financial hardship exemption to an MFN participant
for a performance year, if the agency in its sole discretion determines
the following requirements have been met:
(i) The MFN participant submits a timely, complete request for
financial hardship exemption in accordance with the requirements of
this section which in the sole discretion of CMS demonstrates all of
the following:
(A) The MFN participant exhausted all reasonable methods to obtain
MFN Model drugs at or below the MFN Model Payment for such drugs during
the performance year.
(B) The MFN participant's average net acquisition cost for each MFN
Model drug (including invoices and off-invoice discounts or
adjustments) that was furnished by the MFN participant during the
performance year to patients who were not MFN beneficiaries was not
less than the MFN participant's average net acquisition costs for such
MFN Model drug (including invoices and off-invoice discounts or
adjustments) that was furnished by the MFN participant during the
performance year to MFN beneficiaries.
(C) Any remuneration the MFN participant received from
manufacturers of MFN Model drugs, wholesalers, and distributors that
was not reflected in the MFN participant's average net acquisition
costs was not a price concession related to the purchase of an MFN
Model drug.
(ii) The MFN participant's excess reduction amount per beneficiary
(as determined in paragraph (d)(6) of this section), is greater than
zero.
(d) Excess reduction amount per beneficiary. CMS calculates the MFN
participant's excess reduction amount per beneficiary using available
final action claims data where Medicare was the primary payer that is
estimated to be more than 90 percent complete in accordance with the
following steps:
(1) CMS calculates, separately for dates of service within the
performance year and prior year, the MFN participant's total allowed
charges for separately payable Medicare Part B drugs, and the total
number of beneficiaries that had at least one claim for a service
furnished by the MFN participant with a Medicare Part A or Medicare
Part B allowed charge greater than $0.
(2) CMS divides the MFN participant's total allowed charges for
separately payable Medicare Part B drugs for dates of service within
the performance year by the total number of beneficiaries that had at
least one claim for a service furnished by the MFN participant with a
Medicare Part A or Medicare Part B allowed charge greater than $0 with
a service date within the performance year, to calculate the MFN
participant's average per beneficiary total allowed charges for
separately payable Medicare Part B drugs for the performance year.
(3) CMS divides the MFN participant's total allowed charges for
separately payable Medicare Part B drugs for dates of service within
the prior year by the total number of beneficiaries that had at least
one claim for a service furnished by the MFN participant with a
Medicare Part A or Medicare Part B allowed charge greater than $0 with
a service date within the prior year, to calculate the MFN
participant's average per beneficiary total allowed charges for
separately payable Medicare Part B drugs for the prior year.
(4) CMS subtracts the MFN participant's average per beneficiary
total allowed charges for separately payable Medicare Part B drugs for
the performance year (as calculated in paragraph (d)(2) of this
section) from the MFN participant's average per beneficiary total
allowed charges for separately payable Medicare Part B drugs for the
prior year (as calculated in paragraph (d)(3) of this section).
(5) CMS calculates 25 percent of the MFN participant's total
allowed charges for all Medicare Part A and Part B claims with dates of
service within the prior year and divides that amount by the total
number of beneficiaries that had at least one claim for a service
furnished by the MFN participant with a Medicare Part A or Medicare
Part B allowed charge greater than $0 with a service date within the
prior year, to calculate 25 percent of the MFN participant's average
per beneficiary total allowed charges for all Medicare Part A and Part
B claims with dates of service within the prior year.
(6) CMS subtracts 25 percent of the MFN participant's average per
beneficiary total allowed charges for all Medicare Part A and Part B
claims with dates of service within the prior year (as calculated in
paragraph (d)(5) of this section) from the difference calculated in
paragraph (d)(4) of this section, to calculate the MFN participant's
excess reduction amount per beneficiary.
(e) Reconciliation payment. (1) If CMS in its sole discretion
grants a financial hardship exemption to an MFN participant for a
performance year, CMS provides such MFN participant a reconciliation
payment for the performance year that equals the amount calculated by
multiplying the excess reduction amount per beneficiary specified in
paragraph (d)(6) of this section by the total number of beneficiaries
that had at least one claim for a service furnished by the MFN
participant with a Medicare Part A or Medicare Part B allowed charge
greater than $0 with a service date within the performance year.
(2) The amount of a reconciliation payment provided in accordance
with this section is--
(i) Not subject to appeal;
(ii) Not subject to beneficiary cost-sharing, including any
deductible or coinsurance; and
(iii) Made by CMS (or a CMS contractor) as soon as practical.
Subpart D--[Reserved]
Subpart E--Quality Strategy, Beneficiary Protections, and
Compliance Activities
Sec. 513.400 Quality measures.
(a) General. Quality measures do not adjust model payments to MFN
participants and are used for monitoring purposes.
(b) Collection of quality measures. (1) CMS administers a patient
experience survey to a sample of beneficiaries who receive an MFN Model
drug. A sample of non-MFN beneficiaries may also be surveyed.
(2) If during the MFN Model CMS determines that the quality
measures specified in paragraph (b) of this section are not sufficient
to adequately monitor the quality of care that MFN beneficiaries are
receiving from MFN participants or that MFN participants are providing,
CMS may specify additional measures. CMS applies the following criteria
when specifying additional quality measures:
(i) Additional measures are among one or more of the following
categories:
(A) Patient experience of care.
(B) Patient activation
(C) Shared decision making.
(D) Adherence.
(E) Utilization.
(F) Process measures.
[[Page 76257]]
(ii) Additional measures will not add significant burden to MFN
participants or beneficiaries.
(iii) Additional measures utilize an instrument that CMS has used
previously in a model to adjust payment or for monitoring or
evaluation.
Sec. 513.410 Beneficiary protections.
(a) Beneficiary choice.
(1) MFN participants must not restrict beneficiaries' ability to
choose to receive care from any Medicare participating provider or
supplier or any provider or supplier who has opted out of Medicare.
(2) The MFN participant must not commit any act or omission, nor
adopt any policy that inhibits a beneficiary from exercising his or her
freedom to choose to receive care from any Medicare participating
provider or supplier or any provider or supplier who has opted out of
Medicare. Notwithstanding the foregoing, MFN participants may
communicate to beneficiaries the benefits of receiving care from an MFN
participant, if otherwise consistent with the requirements of this part
and applicable law.
(b) Appeals. An MFN beneficiary and his or her assignees retain
their right to appeal claims in accordance with part 405 subpart I of
this chapter.
(c) Availability of services. MFN participants must not take any
action to select or avoid treating beneficiaries based on their
diagnoses, care needs, income levels or other factors that would render
the beneficiary an ``at-risk beneficiary'' as defined at Sec. 425.20
of this chapter.
Sec. 513.420 Monitoring and compliance activities.
(a) Compliance with laws. (1) Agreement to comply. The MFN
participant must comply with all applicable laws and regulations.
(2) Notification. The MFN participant must notify CMS within 15
days after becoming aware that the MFN participant is under
investigation or has been sanctioned by the federal, state, or local
government, or any licensing authority (including, without limitation,
the imposition of program exclusion, debarment, civil monetary
penalties, corrective action plans, and revocation of Medicare billing
privileges).
(b) CMS monitoring and compliance activities. (1) CMS conducts
monitoring activities to ensure compliance by MFN participants with the
terms of the MFN Model, to obtain timely information about the effects
of the MFN Model on MFN beneficiaries, providers, suppliers, and on the
Medicare program and to facilitate real time identification and
response to potential issues. Such monitoring activities may include,
without limitation, the following:
(i) Documentation requests sent to the MFN participant including,
without limitation, surveys and questionnaires.
(ii) Audits of claims data, medical records, and other data from
the MFN participant.
(iii) Interviews with any individual or entity participating in the
MFN Model including members of the MFN participant's leadership,
management, and staff.
(iv) Interviews with beneficiaries and their caregivers.
(v) Site visits to the MFN participants, performed in a manner
consistent with Sec. 513.420(c).
(vi) Tracking patient complaints and appeals.
(2) In conducting monitoring and oversight activities, CMS or its
designees may use any relevant data or information including without
limitation, all Medicare claims submitted for items or services
furnished to beneficiaries in the MFN Model.
(3) The MFN participant must cooperate with evaluation and
monitoring activities as may be necessary to enable CMS to evaluate the
MFN Model in accordance with section 1115A(b)(4) of the Act and to
conduct monitoring activities under this section.
(c) Site visits. (1) To the extent practicable, CMS or its designee
provides the MFN participant with no less than 15 days advance notice
of any site visit. To the extent practicable, CMS attempts to
accommodate a request for particular dates in scheduling site visits.
However, the MFN participant may not request a date that is more than
60 days after the date of the initial site visit notice from CMS.
(2) The MFN participant must ensure that personnel with the
appropriate responsibilities and knowledge associated with the purpose
of the site visit are available during all site visits.
(3) Notwithstanding the foregoing, CMS may perform unannounced site
visits at all physical locations of the MFN participant at any time to
investigate concerns about the health or safety of beneficiaries or
other patients or other program integrity issues.
(4) Nothing in this part must be construed to limit or otherwise
prevent CMS from performing site visits permitted or required by
applicable law.
(d) Right to correct. If CMS discovers that it has made or received
an incorrect model-specific payment under the terms of the MFN Model,
CMS may make payment to, or demand payment from, the MFN participant.
Sec. 513.430 Audits and record retention.
(a) Right to audit. The Federal Government, including CMS, HHS, and
the Comptroller General, or their designees, has the right to audit,
inspect, investigate, and evaluate any documents and other evidence
regarding implementation of the MFN Model.
(b) Access to records. MFN participants must maintain and give the
Federal Government, including CMS, HHS, and the Comptroller General, or
their designees, access to all such documents and other evidence
sufficient to enable the audit, evaluation, inspection, or
investigation of the implementation of the MFN Model, including without
limitation, documents and other evidence regarding the following:
(1) The MFN participant's compliance with the terms of the MFN
Model, including this subpart.
(2) Quality measure information and the quality of services
performed under the terms of the MFN Model, including this subpart.
(3) Patient safety.
(4) The accuracy of model-specific payments made under the MFN
Model.
(5) Utilization of items and services furnished under the MFN
Model.
(6) Other program integrity issues.
(c) Record retention. The MFN participant must maintain the
documents and other evidence described in paragraph (b) of this section
and other evidence for a period of 6 years from the last payment
received by the MFN participant under the MFN Model or from the date of
completion of any audit, evaluation, inspection, or investigation,
whichever is later, unless--
(1) CMS determines there is a special need to retain a particular
record or group of records for a longer period and notifies the MFN
participant at least 30 days before the normal disposition date; or
(2) There has been a termination, dispute, or allegation of fraud
or similar fault against the MFN participant, in which case the records
must be maintained for an additional 6 years from the date of any
resulting final resolution of the termination, dispute, or allegation
of fraud or similar fault.
Sec. 513.440 Enforcement authority.
(a) Remedial action--(1) Grounds for remedial action. In addition
to any other grounds for remedial action that are permitted under the
terms of this part, CMS may take one or more of the remedial actions
set forth in paragraph (a)(2) of this section if CMS determines,
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in CMS' sole discretion, that an MFN participant:
(i) Has failed to comply with any applicable Medicare program
requirement, rule, or regulation.
(ii) Has failed to comply with any of the terms of the MFN Model,
including applicable requirements of this part.
(iii) Has systematically engaged in the under delivery or over
delivery of an MFN Model drug.
(iv) Has taken any action that threatens the health or safety of an
MFN beneficiary or other patient.
(v) Has undergone a change of control that presents a program
integrity risk.
(vi) Has submitted false data or made false representations,
warranties, certifications or attestations in connection with any
aspect of the MFN Model.
(vii) Has avoided at-risk beneficiaries, as this term is defined in
Sec. 425.20 of this chapter.
(viii) Has avoided patients on the basis of payer status.
(ix) Is subject to sanctions or final actions of an accrediting
organization or Federal, State, or local government agency.
(x) Takes any action that CMS determines for program integrity
reasons is not in the best interests of the MFN Model or the Medicare
program, or fails to take any action that CMS determines for program
integrity reasons should have been taken to further the best interests
of the MFN Model or Medicare program.
(xi) Is subject to investigation by HHS (including the HHS Office
of Inspector General (OIG)) or the Department of Justice due to an
allegation of fraud or significant misconduct, including being subject
to the filing of a complaint, filing of a criminal charge, being
subject to an indictment, being named as a defendant in a False Claims
Act qui tam matter in which the Federal Government has intervened, or
similar action;
(xii) Is the subject of administration enforcement action imposed
by CMS; or
(xiii) Has failed to demonstrate improved performance following any
remedial action imposed under this section.
(2) Taking remedial actions. If CMS determines that one or more
grounds for remedial action described in paragraph (a)(1) of this
section exist, CMS make take one or more of the following remedial
actions:
(i) Notifying the MFN participant of the violation.
(ii) Requiring the MFN participant to provide additional
information to CMS or its designees.
(iii) Requiring the MFN participant to develop and implement a
corrective action plan in a form and manner and by a deadline specified
by CMS.
(iv) Subjecting the MFN participant to additional monitoring,
auditing, or both.
(v) Removing the MFN participant from the MFN Model.
(vi) Recouping model-specific payments.
(vii) Other action as may be permitted under the terms of this
part.
(b) OIG authority. Nothing contained in the terms of the MFN Model
or this part limits or restricts the authority of the HHS Office of
Inspector General or any other Federal Government authority or agency,
including its authority to audit, evaluate, investigate, or inspect
model participant for violations of any statutes, rules, or regulations
administered by the Federal Government.
Sec. 513.450 Limitations on review.
There is no administrative or judicial review under sections 1869
or 1878 of the Act or otherwise for any of the following:
(a) The selection of models for testing or expansion under section
1115A of the Act.
(b) The selection of organizations, sites, or participants,
including MFN participants, to test the MFN Model, including a decision
by CMS to remove an MFN participant from the MFN Model.
(c) The elements, parameters, scope, and duration of such MFN Model
for testing or dissemination, including without limitation all of the
following:
(1) The selection of the model geographic area for the MFN Model by
CMS.
(2) The selection of MFN Model drugs by CMS.
(3) The selection of included international data, including
selection of countries, international drug pricing databases, and
international drug pricing data.
(d) Determinations regarding budget neutrality under section
1115A(b)(3) of the Act.
(e) The termination or modification of the design and
implementation of an MFN Model under section 1115A(b)(3)(B) of the Act.
(f) Determinations about expansion of the duration and scope of the
MFN Model under section 1115A(c) of the Act, including the
determination that the MFN Model is not expected to meet criteria
described in paragraphs (c)(1) or (2) of such section.
Subpart F--Waivers
Sec. 513.500 Waivers of Medicare program requirements for purposes
of testing the MFN Model.
CMS waives the Medicare program requirements in the following
provisions that are necessary solely for purposes of testing the MFN
Model:
(a) Sections 1833(t)(6) and 1833(t)(14) of the Act and Sec. Sec.
419.62 and 419.64 of this chapter related to Medicare payment amounts
for drugs and biologicals under the hospital outpatient prospective
payment system (OPPS) as necessary to permit testing of an alternative
payment amount for MFN Model drugs.
(b) Section 1833(i)(2)(D) of the Act related to Medicare payment to
ASCs for drugs and biologicals as necessary to permit testing of an
alternative payment amount for MFN Model drugs.
(c) Sections 1847A(b) and 1847A(c) of the Act and Sec. Sec.
414.904 and 414.802 of this chapter related to use of the ASP-based,
WAC-based, or other applicable payment methodology and calculation of
manufacturers' ASP as necessary to permit testing of an alternative
payment for MFN Model drugs and to exclude certain units of MFN Model
drugs from manufacturers' ASPs.
(d) Section 1833(a)(1) of the Act related to Medicare payment
portion of the allowed payment amount for an included MFN Model drug
that is determined under Sec. 513.220 as necessary to permit testing
of an innovative payment approach for the alternative add-on payment
amount.
(e) Section 1833(a)(1)(S) of the Act related to Medicare payment
for drugs and biologicals is 80 percent of the lesser of the actual
charge or the payment amount established in section 1842(o) of the Act
as necessary to permit testing of an innovative payment approach for
the total allowable MFN Model payment as determined under subpart C.
(f) Section 1833(a)(1)(G) of the Act related to the amounts paid
with respect to facility services furnished in connection with certain
surgical procedures and with respect to services furnished to an
individual in an ASC must be 80 percent of the lesser of the actual
charge for the services or the amount determined by the Secretary under
such revised payment system as necessary to permit testing of an
innovative payment approach for the total allowable MFN Model payment
as determined under subpart C.
(g) Section 1833(t) of the Act related to how beneficiary copayment
is calculated under the OPPS as necessary to permit testing of an
innovative
[[Page 76259]]
payment approach for the total allowable MFN Model payment as
determined under subpart C of this part.
(h) Section 1833(t)(9)(B) of the Act related to the requirement
that Medicare account for adjustments to ensure that the amount of
expenditures under the OPPS for the year does not increase or decrease
from the estimated amount of expenditures under the OPPS that would
have been made if the adjustments had not been made.
Subparts G through J--[Reserved]
Subpart K--Model Termination
Sec. 513.1000 Termination of the MFN Model.
(a) CMS may terminate the MFN Model for reasons including, but not
limited to, the following:
(1) CMS determines that it no longer has the funds to support the
MFN Model.
(2) CMS terminates the model in accordance with section
1115A(b)(3)(B) of the Act.
(b) As specified in section 1115A(d)(2) of the Act, termination of
the model in accordance with section 1115A(b)(3)(B) of the Act is not
subject to administrative or judicial review.
Dated: November 18, 2020.
Seema Verma,
Administrator, Centers for Medicare & Medicaid Services.
Dated: November 18, 2020.
Alex M. Azar II,
Secretary, Department of Health and Human Services.
[FR Doc. 2020-26037 Filed 11-20-20; 4:15 pm]
BILLING CODE 4120-01-P
