Medical Devices; Laboratory Developed Tests, 68006-68031 [2023-21662]
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68006
Federal Register / Vol. 88, No. 190 / Tuesday, October 3, 2023 / Proposed Rules
NAV CANADA is amending RNAV
route Q–801 in their airspace to ensure
continuity and cross-border
connectivity with the new RNAV route
Q–801 proposed in this NPRM. The
proposed Air Traffic Service (ATS)
route actions are described below.
J–133: Jet route J–133 currently
extends between Galena, AK, VOR/DME
and Sitka, AK, NDB. The FAA proposes
to revoke the portion between the
Anchorage, AK, VOR/DME and the
Sitka, AK, NDB. As amended, Jet route
J–133 would extend between Galena,
AK, VOR/DME and Anchorage, AK,
VOR/DME.
Q–801: Q–801 would extend between
the Anchorage, AK, VOR/DME and the
HARPR, OR, WP. The new route would
remain within United States airspace
between the Anchorage VOR/DME and
the EEVER, AK, Fix and between the
CYVIC, WA, WP and the HARPR WP.
The new EEVER route point is being
established on the Alaska/Canada
border north of the MOCHA, AK, Fix.
The new CYVIC route point is being
established on the United States/Canada
border in Washington state replacing,
the CFPXC computer navigation fix
(CNF) currently charted. This action is
part of an ongoing FAA initiative to
replace CNF and unpronounceable
border fix/waypoint names with
standard, pronounceable, five-letter
names. This proposed action would
establish RNAV route Q–801 within the
United States and exclude the airspace
in Canada.
ddrumheller on DSK120RN23PROD with PROPOSALS1
*
*
*
*
Issued in Washington, DC, on September
28, 2023.
Karen L. Chiodini,
Acting Manager, Rules and Regulations
Group.
[FR Doc. 2023–21811 Filed 10–2–23; 8:45 am]
Airspace, Incorporation by reference,
Navigation (air).
Regulatory Notices and Analyses
The FAA has determined that this
proposed regulation only involves an
established body of technical
regulations for which frequent and
routine amendments are necessary to
keep them operationally current. It,
therefore: (1) is not a ‘‘significant
regulatory action’’ under Executive
Order 12866; (2) is not a ‘‘significant
rule’’ under DOT Regulatory Policies
and Procedures (44 FR 11034; February
26, 1979); and (3) does not warrant
preparation of a regulatory evaluation as
the anticipated impact is so minimal.
Since this is a routine matter that will
only affect air traffic procedures and air
navigation, it is certified that this
proposed rule, when promulgated, will
not have a significant economic impact
on a substantial number of small entities
under the criteria of the Regulatory
Flexibility Act.
Environmental Review
This proposal will be subject to an
environmental analysis in accordance
with FAA Order 1050.1F,
‘‘Environmental Impacts: Policies and
Procedures’’ prior to any FAA final
regulatory action.
Q–801 HARPR, OR to Anchorage, AK (TED) [NEW]
HARPR, OR
WP
(Lat.
FELIX, OR
WP
(Lat.
ECTOF, OR
WP
(Lat.
WAPTO, WA
FIX
(Lat.
Tatoosh, WA (TOU)
VORTAC
(Lat.
CYVIC, WA
WP
(Lat.
GOVAD, Canada
FIX
(Lat.
FINGS, Canada
FIX
(Lat.
FIX
(Lat.
SIMSU, Canada
CAFTA, Canada
FIX
(Lat.
EEVER, AK
FIX
(Lat.
MACIE, AK
WP
(Lat.
LAIRE, AK
FIX
(Lat.
FROZN, AK
WP
(Lat.
Johnstone Point, AK (JOH)
VOR/DME
(Lat.
Anchorage, AK (TED)
VOR/DME
(Lat.
*
List of Subjects in 14 CFR Part 71
42°28′50.00″
43°19′13.98″
44°10′49.55″
47°28′19.54″
48°17′59.64″
48°29′59.97″
49°02′48.65″
50°15′00.00″
50°46′56.00″
51°17′43.00″
54°35′01.79″
57°43′38.87″
58°48′14.67″
59°40′34.90″
60°28′51.43″
61°10′04.32″
N,
N,
N,
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N,
N,
N,
N,
N,
N,
N,
N,
N,
N,
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long.
long.
long.
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long.
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21 CFR Part 809
[Docket No. FDA–2023–N–2177]
Medical Devices; Laboratory
Developed Tests
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Food and Drug Administration,
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Authority: 49 U.S.C. 106(f), 106(g); 40103,
40113, 40120; E.O. 10854, 24 FR 9565, 3 CFR,
1959–1963 Comp., p. 389.
§ 71.1
[Amended]
2. The incorporation by reference in
14 CFR 71.1 of FAA Order JO 7400.11H,
Airspace Designations and Reporting
Points, dated August 11, 2023, and
effective September 15, 2023, is
amended as follows:
■
Paragraph 2004
Jet Routes
*
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*
*
122°53′01.54″
123°05′39.51″
123°18′57.87″
124°13′50.38″
124°37′37.36″
124°54′39.80″
125°42′15.09″
127°34′00.00″
128°25′37.00″
129°05′19.00″
133°05′54.23″
137°50′47.74″
140°31′43.36″
143°29′31.48″
146°35′57.61″
149°57′36.52″
RIN 0910–AI85
18:38 Oct 02, 2023
1. The authority citation for 14 CFR
part 71 continues to read as follows:
■
*
Paragraph 2007
Routes.
BILLING CODE 4910–13–P
VerDate Sep<11>2014
PART 71—DESIGNATION OF CLASS A,
B, C, D, AND E AIRSPACE AREAS; AIR
TRAFFIC SERVICE ROUTES; AND
REPORTING POINTS
*
Food and Drug Administration
HHS.
In consideration of the foregoing, the
Federal Aviation Administration
proposes to amend 14 CFR part 71 as
follows:
*
J–133 [Amended]
From Galena, AK to Anchorage, AK.
DEPARTMENT OF HEALTH AND
HUMAN SERVICES
AGENCY:
The Proposed Amendment
ACTION:
*
*
Canadian Area Navigation
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Proposed rule.
The Food and Drug
Administration (FDA, the Agency, or
we) is proposing to amend its
regulations to make explicit that in vitro
diagnostic products (IVDs) are devices
under the Federal Food, Drug, and
Cosmetic Act (FD&C Act) including
when the manufacturer of the IVD is a
laboratory. In conjunction with this
amendment, FDA is proposing a policy
under which FDA intends to phase out
its general enforcement discretion
approach for laboratory developed tests
SUMMARY:
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Federal Register / Vol. 88, No. 190 / Tuesday, October 3, 2023 / Proposed Rules
(LDTs) so that IVDs manufactured by a
laboratory would generally fall under
the same enforcement approach as other
IVDs. FDA is proposing this phaseout to
better protect the public health by
helping to assure the safety and
effectiveness of LDTs. If finalized, this
phaseout may also foster the
manufacturing of innovative IVDs for
which FDA has determined there is a
reasonable assurance of safety and
effectiveness.
Either electronic or written
comments on the proposed rule must be
submitted by December 4, 2023.
ADDRESSES: You may submit comments
as follows. Please note that late,
untimely filed comments will not be
considered. The https://
www.regulations.gov electronic filing
system will accept comments until
11:59 p.m. Eastern Time at the end of
December 4, 2023. Comments received
by mail/hand delivery/courier (for
written/paper submissions) will be
considered timely if they are received
on or before that date.
DATES:
ddrumheller on DSK120RN23PROD with PROPOSALS1
Electronic Submissions
Submit electronic comments in the
following way:
• Federal eRulemaking Portal:
https://www.regulations.gov. Follow the
instructions for submitting comments.
Comments submitted electronically,
including attachments, to https://
www.regulations.gov will be posted to
the docket unchanged. Because your
comment will be made public, you are
solely responsible for ensuring that your
comment does not include any
confidential information that you or a
third party may not wish to be posted,
such as medical information, your or
anyone else’s Social Security number, or
confidential business information, such
as a manufacturing process. Please note
that if you include your name, contact
information, or other information that
identifies you in the body of your
comments, that information will be
posted on https://www.regulations.gov.
• If you want to submit a comment
with confidential information that you
do not wish to be made available to the
public, submit the comment as a
written/paper submission and in the
manner detailed (see ‘‘Written/Paper
Submissions’’ and ‘‘Instructions’’).
Written/Paper Submissions
Submit written/paper submissions as
follows:
• Mail/Hand Delivery/Courier (for
written/paper submissions): Dockets
Management Staff (HFA–305), Food and
Drug Administration, 5630 Fishers
Lane, Rm. 1061, Rockville, MD 20852.
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18:38 Oct 02, 2023
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• For written/paper comments
submitted to the Dockets Management
Staff, FDA will post your comment, as
well as any attachments, except for
information submitted, marked and
identified, as confidential, if submitted
as detailed in ‘‘Instructions.’’
Instructions: All submissions received
must include the Docket No. FDA–
2023–N–2177 for ‘‘Medical Devices;
Laboratory Developed Tests.’’ Received
comments, those filed in a timely
manner (see ADDRESSES), will be placed
in the docket and, except for those
submitted as ‘‘Confidential
Submissions,’’ publicly viewable at
https://www.regulations.gov or at the
Dockets Management Staff between 9
a.m. and 4 p.m., Monday through
Friday, 240–402–7500.
• Confidential Submissions—To
submit a comment with confidential
information that you do not wish to be
made publicly available, submit your
comments only as a written/paper
submission. You should submit two
copies total. One copy will include the
information you claim to be confidential
with a heading or cover note that states
‘‘THIS DOCUMENT CONTAINS
CONFIDENTIAL INFORMATION.’’ The
Agency will review this copy, including
the claimed confidential information, in
its consideration of comments. The
second copy, which will have the
claimed confidential information
redacted/blacked out, will be available
for public viewing and posted on
https://www.regulations.gov. Submit
both copies to the Dockets Management
Staff. If you do not wish your name and
contact information to be made publicly
available, you can provide this
information on the cover sheet and not
in the body of your comments and you
must identify this information as
‘‘confidential.’’ Any information marked
as ‘‘confidential’’ will not be disclosed
except in accordance with 21 CFR 10.20
and other applicable disclosure law. For
more information about FDA’s posting
of comments to public dockets, see 80
FR 56469, September 18, 2015, or access
the information at: https://
www.govinfo.gov/content/pkg/FR-201509-18/pdf/2015-23389.pdf.
Docket: For access to the docket to
read background documents or the
electronic and written/paper comments
received, go to https://
www.regulations.gov and insert the
docket number, found in brackets in the
heading of this document, into the
‘‘Search’’ box and follow the prompts
and/or go to the Dockets Management
Staff, 5630 Fishers Lane, Rm. 1061,
Rockville, MD 20852, 240–402–7500.
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68007
FOR FURTHER INFORMATION CONTACT:
Toby Lowe, Center for Devices and
Radiological Health, Food and Drug
Administration, 10903 New Hampshire
Ave., Silver Spring, MD 20993, 301–
796–6512, LDTProposedRule@
fda.hhs.gov.
SUPPLEMENTARY INFORMATION:
Table of Contents
I. Executive Summary
A. Purpose of the Proposed Rule
B. Summary of the Major Provisions of the
Proposed Rule
C. Legal Authority
D. Costs and Benefits
II. Table of Abbreviations/Commonly Used
Acronyms in This Document
III. Background
A. Introduction
B. Need for the Rule
C. FDA’s Current Regulatory Framework
D. History of the Rulemaking
IV. Legal Authority
V. Description of the Proposed Amendment
to the Definition of In Vitro Diagnostic
Products
A. Proposed Amendment
B. Legal Basis for the Proposed
Amendment
VI. Description of the Proposed Enforcement
Policy
A. Scope
B. Stages
VII. Proposed Effective Date
VIII. Preliminary Economic Analysis of
Impacts
IX. Analysis of Environmental Impact
X. Paperwork Reduction Act of 1995
XI. Federalism
XII. Consultation and Coordination With
Indian Tribal Governments
XIII. Other Issues for Consideration
XIV. References
I. Executive Summary
A. Purpose of the Proposed Rule
FDA is proposing to amend its
regulations to make explicit that IVDs
are devices under the FD&C Act
including when the manufacturer of the
IVD is a laboratory. This amendment
would reflect that the device definition
in the FD&C Act does not differentiate
between entities manufacturing the
device, and would provide further
clarity, including for stakeholders
affected by the accompanying changes
to FDA’s general enforcement discretion
approach for LDTs. In connection with
amending the regulation, FDA intends
to phase out its general enforcement
discretion approach for LDTs so that
IVDs manufactured by a laboratory
would generally fall under the same
enforcement approach as other IVDs.
For purposes of this document, we use
‘‘manufacture’’ and related terms as a
shorthand for the various activities that
constitute manufacturing as described
in FDA regulations (e.g., design,
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Federal Register / Vol. 88, No. 190 / Tuesday, October 3, 2023 / Proposed Rules
preparation, propagation, assembly, and
processing).
In 1976, the Medical Device
Amendments of 1976 (the MDA)
amended the FD&C Act to create a
comprehensive system for the regulation
of devices intended for human use. In
implementing the MDA, FDA has
generally exercised enforcement
discretion such that it generally has not
enforced applicable requirements with
respect to most LDTs. Enforcement
discretion for LDTs developed as a
matter of general practice. However, the
risks associated with LDTs are much
greater today than they were at the time
of enactment of the MDA. As discussed
more fully in section III.B, today’s LDTs
are generally, among other things, used
more widely, by a more diverse
population, with an increasing reliance
on high-tech instrumentation and
software, and more frequently for the
purpose of guiding critical healthcare
decisions. In this regard, today’s LDTs
are similar to other IVDs that have not
been under this general enforcement
discretion approach. Given these
changes, and for the additional reasons
discussed in section III.B, phasing out
the general enforcement discretion
approach for LDTs is important to
protect the public health. The phaseout
of FDA’s general enforcement discretion
approach for LDTs is intended to help
assure the safety and effectiveness of
LDTs, and may also foster the
manufacturing of innovative IVDs for
which FDA has determined there is a
reasonable assurance of safety and
effectiveness.
B. Summary of the Major Provisions of
the Proposed Rule
This rulemaking would amend the
definition of ‘‘in vitro diagnostic
products’’ in FDA regulations to state
that IVDs are devices under the FD&C
Act ‘‘including when the manufacturer
of these products is a laboratory.’’ In
conjunction with this amendment, FDA
is also proposing a policy under which
FDA intends to phase out its general
enforcement discretion approach for
LDTs so that IVDs manufactured by a
laboratory would generally fall under
the same enforcement approach as other
IVDs. Additional details regarding the
proposed phaseout policy are discussed
further in section VI.
C. Legal Authority
FDA is proposing to issue this rule
under the Agency’s general rulemaking
authorities and statutory authorities
relating to devices. These authorities
include sections 201(h)(1), 301, 501,
502, 510, 513, 514, 515, 518, 519, 520,
701, 702, 704, and 801 of the FD&C Act
(21 U.S.C. 321(h)(1), 331, 351, 352, 360,
360c, 360d, 360e, 360h, 360i, 360j, 371,
372, 374, and 381).
D. Costs and Benefits
We quantify benefits to patients from
averted health losses due to problematic
IVDs offered as LDTs.1 Due to
limitations in the data, we quantify
health benefits only with respect to
IVDs for certain diseases and
conditions; however, we would expect
additional health benefits associated
with averted health losses for other
diseases and conditions. We estimate
that the annualized benefits over 20
years would range from $2.67 billion to
$86.01 billion at a 7 percent discount
rate, with a primary estimate of $31.41
billion, and from $1.81 billion to $61.41
billion at a 3 percent discount rate, with
a primary estimate of $22.33 billion.
Additional benefits would include
ddrumheller on DSK120RN23PROD with PROPOSALS1
Abbreviation/acronym
1 See discussion of ‘‘IVDs offered as LDTs’’ in
section VI.A below.
2 This proposed rule would result in compliance
costs for laboratories that are ensuring their IVDs
offered as LDTs are compliant with applicable
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II. Table of Abbreviations/Commonly
Used Acronyms in This Document
What it means
510(k) ..................................................................
AMC ....................................................................
ASR .....................................................................
CFR .....................................................................
CGMP .................................................................
CLIA ....................................................................
CMS ....................................................................
EUA .....................................................................
FDA .....................................................................
FD&C Act ............................................................
HCT/Ps ...............................................................
HLA .....................................................................
IDE ......................................................................
IVD ......................................................................
IVDMIA ................................................................
LDT .....................................................................
VerDate Sep<11>2014
averted non-health losses from the
quantified reduction in costs of
problematic IVDs offered as LDTs and
unquantified reduction in costs from
lawsuits and costs to healthcare
systems. We quantify costs to affected
laboratories for complying with
applicable statutory and regulatory
requirements. Additional costs would
include some costs to FDA, which we
include in our estimates. The
annualized costs would range from
$2.52 billion to $19.45 billion at a 7
percent discount rate, with a primary
estimate of $5.87 billion, and from $2.39
billion to $18.55 billion at a 3 percent
discount rate, with a primary estimate of
$5.60 billion. The annualized transfers 2
would range from $100 million to $452
million at a 7 percent discount rate,
with a primary estimate of $226 million,
and from $121 million to $538 million
at a 3 percent discount rate, with a
primary estimate of $269 million. The
annualized costs to FDA would range
from $265 million to $1.06 billion at a
7 percent discount rate, with a primary
estimate of $530 million, and from $251
million to $1.00 billion at a 3 percent
discount rate, with a primary estimate of
$501 million. These estimates do not
include anticipated offsets from user
fees. Factoring in offsets from user fees
at current levels, estimated costs to FDA
are reduced to $165 million to $607
million at a 7 percent discount rate,
with a primary estimate of $304 million,
and to $103 million to $465 million at
a 7 percent discount rate, with a
primary estimate of $233 million,
covering approximately half of the
estimated costs to FDA.
Premarket Notification.
Academic Medical Center.
Analyte Specific Reagent.
Code of Federal Regulations.
Current Good Manufacturing Practice.
Clinical Laboratory Improvement Amendments of 1988.
Centers for Medicare & Medicaid Services.
Emergency Use Authorization.
Food and Drug Administration.
Federal Food, Drug, and Cosmetic Act.
Human Cells, Tissues, and Cellular and Tissue-Based Products.
Human Leukocyte Antigen.
Investigational Device Exemption.
In Vitro Diagnostic Product.
In Vitro Diagnostic Multivariate Index Assay.
Laboratory Developed Test.
statutory and regulatory requirements. These costs
overlap somewhat with effects associated with this
rule in the form of user fees including annual
registration fees, fees for premarket submissions,
and annual fees for periodic PMA reporting, which
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are paid from laboratories to FDA. These fees are
paid by laboratories but are considered revenue for
FDA. The approach to estimating fee effects is
distinct from the approaches for either benefits or
costs, so they will be presented as transfers.
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Abbreviation/acronym
What it means
MDA ....................................................................
MDR ....................................................................
MDUFA ...............................................................
NIPS ....................................................................
PMA ....................................................................
QS .......................................................................
ddrumheller on DSK120RN23PROD with PROPOSALS1
III. Background
A. Introduction
FDA’s regulations define IVDs as
reagents, instruments, and systems
intended for use in the diagnosis of
disease or other conditions, including a
determination of the state of health, in
order to cure, mitigate, treat, or prevent
disease or its sequelae, and intended for
use in the collection, preparation, and
examination of specimens taken from
the human body. IVDs include test
systems (also referred to in this
preamble as ‘‘tests’’) that are performed
on samples taken from the human body,
such as blood or tissue, for the purpose
of detecting diseases or other
conditions, monitoring a person’s
overall health, identifying patients who
are likely to benefit from specific
therapies, or otherwise helping to
diagnose, cure, mitigate, treat, or
prevent disease or its sequelae. Some
IVDs are manufactured by conventional
manufacturers for use by other entities
such as laboratories, healthcare
providers, or, in some cases, patients.
Such IVDs may include ‘‘test kits,’’
containing packaged sets of components
that are part of or comprise a test
system. Other IVDs are manufactured by
laboratories for use by the same or other
laboratories. Such IVDs include LDTs.
FDA has generally considered an LDT to
be an IVD that is intended for clinical
use and that is designed, manufactured,
and used within a single laboratory that
is certified under the Clinical
Laboratory Improvement Amendments
of 1988 (CLIA) and meets the regulatory
requirements under CLIA to perform
high complexity testing. Section V.B
sets forth the legal reasoning for FDA’s
position that IVDs manufactured by
laboratories, including LDTs, are
devices.
However, in implementing the MDA,
FDA generally has exercised
enforcement discretion such that it
generally has not enforced applicable
requirements with respect to most LDTs.
At the time of passage of the MDA,
LDTs were mostly manufactured in
small volumes by laboratories that
served their local communities. They
were typically intended for use in
diagnosing rare diseases or for other
uses to meet the needs of a local patient
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Medical Device Amendments of 1976.
Medical Device Report.
Medical Device User Fee Amendments.
Non-Invasive Prenatal Screening.
Premarket Approval Application.
Quality System.
population, or were generally similar to
well-characterized, standard tests. They
also tended to employ manual
techniques (and did not use automation)
performed by laboratory personnel with
specialized expertise; to be used and
interpreted by physicians or
pathologists in a single institution
responsible for the patient (and who
were actively involved in patient care);
and to be manufactured using
components legally marketed for
clinical use, such as general purpose
reagents or immunohistochemical stains
marketed in compliance with FDA
regulatory requirements. Due to these
and other factors, FDA generally
exercised enforcement discretion such
that it generally has not enforced
applicable requirements for most LDTs.3
However, the LDT landscape has
evolved significantly since 1976. Today,
many LDTs rely on high-tech or
complex instrumentation and software
to generate results and clinical
interpretations. They are often used in
laboratories outside of the patient’s
healthcare setting and are often
manufactured in high volume for large
and diverse populations. Many LDTs are
manufactured by laboratory
corporations that market the tests
nationwide, as they accept specimens
from patients across the country and run
their LDTs in very large volumes in a
single laboratory. Today’s LDTs are also
more commonly manufactured with
instruments or other components not
legally marketed for clinical use and are
more often used to inform or direct
critical treatment decisions, to widely
screen for common diseases, to predict
personal risk of developing certain
diseases, and to diagnose serious
medical conditions such as cancer and
heart disease.4 The risks associated with
most modern LDTs are therefore much
greater today than they were at the time
3 Although FDA’s general enforcement discretion
approach continues today, it does not apply to
LDTs in all contexts; for example, it does not apply
to, among other LDTs, those used for declared
emergencies/potential emergencies/material threats
under section 564 of the FD&C Act (21 U.S.C.
360bbb–3).
4 See, e.g., Refs. 1 to 3. These observations are also
informed by FDA’s own experience, including the
review of submissions and site visits, and staff with
prior experience in the laboratory industry
developing and running LDTs.
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FDA began implementing the MDA, and
most LDTs today are similar to other
IVDs that have not been under FDA’s
general enforcement discretion
approach. In addition, FDA is
concerned that firms are offering IVDs
as ‘‘LDTs’’ even when they are not
LDTs, because they are not actually
designed, manufactured, and used
within a single laboratory (see, e.g.,
Refs. 4 and 5).
As a result of this evolution in the
testing landscape, FDA has long
recognized the need for a change in the
Agency’s general enforcement discretion
approach for LDTs. The history of FDA’s
efforts with respect to LDTs is set forth
in the ‘‘History of the Rulemaking’’
section below (section III.D). Over the
past few years, FDA has accumulated
even more information supporting the
need for a change, as discussed below.
In light of these developments, FDA is
proposing to amend FDA’s regulations
to make explicit that IVDs are devices
under the FD&C Act including when the
manufacturer is a laboratory.5 FDA is
also proposing a policy under which
FDA intends to phase out FDA’s general
enforcement discretion approach for
LDTs so that IVDs manufactured by a
laboratory would generally fall under
the same enforcement approach as other
IVDs.
B. Need for the Rule
FDA is proposing a policy under
which FDA intends to phase out the
general enforcement discretion
approach for LDTs because that
approach has led to an oversight scheme
that does not best serve the public
health. LDTs that are under the general
enforcement discretion approach are
treated differently from other IVDs.
However, there is no longer a sound
basis for this distinction. In FDA’s
experience, including with COVID–19
tests and IVDs that are offered as LDTs
after FDA’s approval of a comparable
companion diagnostic, many test
systems made by laboratories today are
functionally the same as those made by
other manufacturers of IVDs. They
5 As discussed further in section V, FDA is also
proposing to amend the statutory citation for the
device definition included in § 809.3 (21 CFR 809.3)
to reflect that it is now codified at section 201(h)(1)
of the FD&C Act (21 U.S.C. 321(h)(1)).
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involve the same materials and
technologies, are intended for the same
or similar purposes, are developed by
and for individuals with similar
expertise, and are marketed to the same
patients, sometimes on a national scale.
For these reasons, tests made by
laboratories are often used
interchangeably by healthcare providers
and patients with tests made by other
manufacturers. In fact, today, the testing
industry has come to view FDA’s
general enforcement discretion
approach as an alternative pathway to
market for test systems, such that test
systems are often ‘‘launched as LDTs’’
with no assurance that they meet
requirements under the FD&C Act and
its implementing regulations (see, e.g.,
Refs. 6 and 7).6 These tests lack the
characteristics and institutional
safeguards that originally justified
FDA’s general enforcement discretion
approach, as discussed above, and may
directly compete with FDA-authorized
kit-based test systems. FDA views this
bifurcated system of oversight as
untenable and inconsistent with FDA’s
public health mission.
The proposed phaseout of FDA’s
general enforcement discretion
approach is designed to redress the
imbalance in oversight and protect the
public health. Diagnostic testing is a
cornerstone of modern medicine; CDC
estimates that 70 percent of medical
decisions are based on laboratory test
results (Ref. 8). IVDs offered as LDTs are
a growing sector of that market (Ref. 1).
Moreover, these tests are proliferating in
some of the most complicated and
sensitive areas of medical practice,
where the presence of a valid test can
be most important.
As the testing landscape has evolved,
information about these tests in the
scientific literature, news articles, and
anecdotal reports submitted to the
Agency, among other sources, has
exposed evidence of problems
associated with these tests. This
evidence is discussed in more detail
below. Particularly over the last few
years, this evidence has been growing
and likely does not reflect the full scale
of the problems. (Until FDA
systematically collects information on
these tests, such as adverse event
reports, it will not be able to assess more
fully the extent of the risks to patients
in the manner it does for other devices.)
Based on current safety signals, FDA is
proposing to phase out the general
enforcement discretion approach to help
6 The
references cited are examples of the
described practice. Their inclusion does not
represent FDA support for or approval of the
activities described.
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assure that patients are receiving
accurate and reliable diagnostic test
results regardless of where the tests are
made.
1. IVDs Offered as LDTs Have a
Significant Impact on Modern Medical
Care
Today, IVDs offered as LDTs are
ubiquitous, and are intended to
diagnose a broad range of diseases and
conditions (see Ref. 2). In many cases,
these IVDs are meant for use in complex
areas of medicine involving lifethreatening diseases, such as cancer,
neurological diseases, cardiovascular
illness, infectious diseases, and rare
diseases. They can proliferate in areas
where diagnosis is difficult, and the
healthcare community has few points of
reference for determining test validity.
Sometimes, they use complex
algorithms to calculate ‘‘scores’’ for
diagnosis with little transparency to the
user about the basis for these
algorithms. Increasingly, these IVDs are
intended to inform drug treatment,
directing physicians to choose certain
drugs based on a patient’s genetic or
other information. FDA has witnessed
an explosion in the volume, complexity,
and scope of IVDs offered as LDTs for
use in determining cancer treatments,7
and as discussed below, news coverage,
including as recently as this year, has
drawn attention to the use of IVDs
offered as LDTs for non-invasive
prenatal screening (NIPS), which
evaluate fetal DNA circulating in a
pregnant individual’s blood. In general,
IVDs offered as LDTs are occupying a
growing share of the testing market and
are used in some of the most complex
areas of medicine (see, e.g., Refs. 1 and
2).
Given the role these IVDs play in
modern medical care, their validity has
a significant impact on the public
health. False positive test results, which
erroneously indicate that a patient has
a certain disease or condition, can delay
diagnosis and treatment of the true
disease or condition, lead to
unwarranted interventions, and cause
needless distress. Interventions may
involve medication with serious side
effects or risky medical procedures.
False negative results can lead to
progression of disease, in some cases
without the opportunity for life-saving
treatment, and the spread of infectious
disease. The harms to patients from
false positive and negative results can
be significant. For example, the
7 FDA has initiated a pilot program for certain
oncology diagnostics as one step that may be
helpful in reducing the risks associated with using
certain LDTs to identify cancer biomarkers (see 88
FR 40273 (June 21, 2023)).
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application of an ineffective oncology
treatment due to a false positive for a
patient already weakened from disease,
or the failure to receive a life-saving
medication due to a false negative, can
be fatal. These false results can stem
from an analytical error or from a lack
of clinical validity where a measured
result is incorrectly associated with a
particular clinical state. Flaws in a test’s
algorithm can mean the difference in
whether a patient with cancer receives
a beneficial immunotherapy. Pregnant
people may use screening tests to make
decisions without obtaining appropriate
confirmatory testing. In 2016, FDA
learned of a false positive result from a
genetic test for long QT syndrome (a
heart signaling disorder) that led to the
erroneous implantation of a defibrillator
in a healthy individual. In addition to
the risks associated with the
implantation procedure, the defibrillator
delivered inappropriate shocks to the
patient, which posed the risk of sudden
cardiac death (Refs. 9 and 10). These are
just a few examples of how diagnostic
tests can and do have significant longterm consequences for patients.
2. Current Information Raises Serious
Questions About Whether Patients Can
Rely on IVDs Offered as LDTs
FDA has highlighted the risks
associated with IVDs offered as LDTs for
decades, and our concerns have grown
in recent years. As described in the
‘‘History of the Rulemaking’’ section, we
first took steps to address the issue in
the late 1990s, followed by a series of
different proposed strategies for
increasing oversight. In 2015, the
Agency published a report of 20 case
studies involving inaccurate, unsafe,
ineffective, or poor quality LDTs that
caused or may have caused patient harm
(‘‘2015 Report’’) (Ref. 11). More recent
evidence suggests that the situation is
getting worse. This evidence cuts across
test types and laboratories and is from
a variety of sources, including
published studies in the scientific
literature, allegations of problematic
tests reported to FDA, FDA’s own
experience in reviewing IVDs offered as
LDTs, news articles, and class-action
lawsuits. Overall, the evidence points to
fundamental uncertainty in the
marketplace about whether IVDs offered
as LDTs provide accurate and reliable
results.
Scientific literature is one source of
evidence. Over time, FDA has become
aware of various publications that
describe problems with IVDs offered as
LDTs. In the past 3 years, four different
studies have documented high
variability in performance among these
IVDs (Refs. 12 to 15). In one study, the
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same samples were sent to 19
laboratories for testing using their own
manufactured test and only 7 of those
laboratories correctly reported all results
(Ref. 12). For almost half of the tests
studied, analytical accuracy was
significantly lower than that of the
parallel test approved by FDA. In
another study, researchers sent identical
samples to two different laboratories to
detect tumor mutations and found over
70 percent discordance in the results
from their tests (Ref. 13). A study by
Friends of Cancer Research found
substantial variability among tumor
mutational burden (TMB) tests
manufactured by laboratories and used
to identify patients with cancer most
likely to benefit from immunotherapy
(Ref. 14). A fourth study highlighted
validity concerns specific to early
cancer detection tests, including one
IVD offered as an LDT that delivered
nine false positive results for every true
cancer diagnosis (Ref. 15). An article
published earlier this year detailed an
oncologist’s experience with false
results from an unapproved blood-based
multi-cancer early detection IVD offered
as an LDT and intended to screen for
more than 50 types of cancer (Ref. 16).
A 2016 study published in the New
England Journal of Medicine reported
false positive results from genetic IVDs
offered as LDTs for hypertrophic
cardiomyopathy in multiple patients of
African American descent (Ref. 17).
These studies do not mean that every
laboratory is manufacturing bad tests or
that no patient can rely on IVDs offered
as LDTs. Instead, they reflect a level of
variability, including the potential for
inaccurate or incomplete results, that
highlights the need for changes to the
basic oversight scheme.
FDA’s own experience has reinforced
concerns regarding IVDs offered as
LDTs. FDA has gathered information
about IVDs offered as LDTs through its
review of submissions. Although the
Agency generally has not enforced
requirements for LDTs, it has received
premarket submissions from some
laboratories seeking authorization for
their tests. We have received numerous
submissions for such tests, including
premarket review submissions,8 Qsubmissions,9 and investigational use
8 These submissions have been for a wide variety
of indications, including tests intended to detect
nucleic acids from viruses associated with head and
neck cancers; to identify patients with obesity due
to rare genetic conditions to inform treatment
eligibility; to aid in the management of therapy for
patients taking certain anticoagulants; and tests for
breast cancer prognosis, tumor profiling, and
treatment selection, for patients with cancer.
9 For discussion of FDA’s Q-submission program,
see FDA’s guidance document issued on June 2,
2023, entitled ‘‘Requests for Feedback and Meetings
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submissions for IVDs offered as LDTs, as
well as many emergency use
authorization (EUA) requests from
laboratories (which are discussed
further below). FDA’s review of these
submissions has provided insight into
laboratory test development and, in
some cases, revealed significant
concerns. For example, FDA has
observed that many laboratories fail to
perform appropriate or adequate
validation studies, have data
demonstrating their test does not work
as intended but offer the test anyway, or
use instruments and other components
that are not adequately controlled for
clinical use. The tests described in these
submissions have been intended for a
range of diseases or conditions, some of
which are very serious. FDA has
received submissions for IVDs offered as
LDTs to diagnose Alzheimer’s disease,
predict heart disease risk, diagnose
Fabry disease (a rare neurological
disorder), and inform treatment
considerations for a rare blood cancer,
all of which lacked adequate validation
to support authorization.
In addition, given that FDA’s general
enforcement discretion approach for
LDTs has not applied to IVDs for
emergency use (though FDA has issued
enforcement policies for such IVDs
during specific emergencies, as
explained elsewhere in this preamble),
FDA has received EUA requests for tests
from laboratories, including many for
COVID–19 diagnostics. Of the first 125
EUA requests for COVID–19 molecular
diagnostic tests submitted from
laboratories, 82 showed test design or
validation problems (Ref. 18). In one
case, the approach to validation was so
poor that when redone correctly, there
was a 400-fold difference in
performance, leading the laboratory to
take the test off the market. In another
example, an academic medical center
(AMC) laboratory purported to validate
its test with only 12 positive samples,
showing perfect performance. FDA
requested evaluation of additional
specimens to confirm. When an
additional 12 samples were evaluated,
the cumulative performance revealed an
unacceptably high false negative rate,
where the test identified only 71 percent
of known positive specimens as positive
and falsely identified 29 percent of
known positive samples as negative,
and the EUA request was withdrawn. In
addition, multiple laboratories that
offered their tests as described in FDA’s
COVID–19 test guidance (see discussion
in Ref. 19) did not provide any
for Medical Device Submissions: The QSubmissions Program,’’ available at https://
www.fda.gov/media/114034/download.
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analytical and/or clinical validation
data in the EUA requests that they
submitted after the tests were in use.
This experience provided a window
into the approach that many laboratories
may take to test validation, and not only
confirmed but increased FDA’s concerns
about the validation of IVDs offered as
LDTs. The experience also showed that
even tests involving relatively wellunderstood techniques (here, the
polymerase chain reaction, or PCR,
technique) may not perform well. In all,
test performance seen in this subset of
submissions from laboratories was far
worse than we expected. To the extent
that this sample represents larger trends
in the performance of IVDs offered as
LDTs, it underscores the need for greater
FDA oversight.
FDA has also received multiple
complaints, adverse event reports, and
other allegations identifying problems
with IVDs offered as LDTs.10 One
complaint alleged that an IVD offered as
an LDT to diagnose autism had
insufficient clinical validation to
support this use. In another complaint,
an informant alleged that a laboratory
was forging results when its liquid
biopsy test did not work. Additionally,
FDA has received multiple voluntary
medical device reports (primarily from
patients) of inaccurate NIPS test results,
as well as inaccurate results from an
oncology IVD offered as an LDT that
predicts risk of breast cancer recurrence
and informs the decision to pursue
chemotherapy, both of which can pose
serious, irreversible harm to patients.
Another report described a false
negative result from a BRCA test
marketed to predict one’s risk of breast
cancer. The patient was later diagnosed
with breast cancer and found to be
BRCA1 positive by another test. A
separate report from a healthcare
provider described a different patient
that received discrepant results from
testing with this BRCA test and with
another IVD offered as an LDT for
hereditary cancer risk prediction. In yet
another report, a patient described a
false positive breast cancer result from
an oncology blood IVD offered as an
LDT and that led to invasive followup
procedures, emotional anguish, and
unnecessary monetary expenses. FDA
also received a report regarding a bloodbased test for lung cancer that
underestimated cancer in about 40
percent of patients. Additionally, FDA
has received medical device reports
10 FDA has not confirmed the veracity of the
allegations or facts in every complaint, report, and
allegation. Nevertheless, collectively this
information points to potential problems among
IVDs offered as LDTs.
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regarding infectious disease genetic
IVDs offered as LDTs without
validation, from which inaccurate
results could lead to limb loss or
women’s health issues, and regarding
inaccurate results from an IVD offered
as an LDT to assess medication
adherence. As noted above, collectively,
this information, though anecdotal,
points to potential problems among
IVDs offered as LDTs, the scope and
scale of which FDA cannot fully assess
or address without phasing out the
general enforcement discretion
approach for applicable requirements
(such as adverse event reporting).
Aside from the scientific community
and FDA, the general public is coming
to recognize concerns with the current
scheme, in which most LDTs are
generally not overseen by FDA. General
news sources and other outlets have
reported on such concerns (see, e.g.,
Refs. 20 to 26). For example, the New
York Times recently conducted an
indepth investigation into NIPS tests
and found that positive results from the
tests are incorrect about 85 percent of
the time (Ref. 22). NIPS tests are
screening tests, so they should be
followed up with confirmatory
diagnostic testing, but the New York
Times article reported that patients and
healthcare providers are making
healthcare decisions based on results
from these screening tests alone due to
manufacturers’ marketing claims. A
device whose labeling is false or
misleading in any particular manner is
misbranded under the FD&C Act;
however, under the general enforcement
discretion approach, FDA generally has
not enforced this proscription for IVDs
offered as LDTs. As another example,
ProPublica reported on a COVID–19 test
offered by a laboratory under contract
with a university without EUA
authorization from FDA, which,
according to the report, missed 96
percent of the positive cases from the
university campus, and routinely sent
people infected with COVID–19 back
into the community (Ref. 26). In
addition, consumers, shareholders, and
investors are filing lawsuits against
laboratory manufacturers for false and
misleading statements about test
efficacy, including lawsuits related to
pharmacogenetic tests (genetic tests
intended to inform drug selection) and
NIPS (see, e.g., Complaint, In re Myriad
Genetics, Inc. Sec. Litig., No. 2:19–cv–
00707–PMW (D. Utah 2019); Complaint,
Hickok v. Capone, No. 2021–0686 (Del.
Ch. 2021); Complaint, Davis v. Natera,
Inc., No. 3:22–cv–00985 (N.D. Cal.
2022); Complaint, Carroll v. Myriad
Genetics Inc., No. 4:22–CV–00739 (N.D.
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Cal. 2022); Biesterfeld v. Ariosa
Diagnostics, Inc., No. 1:21–CV–03085,
2022 WL 972281 (N.D. Ill. 2022); and
Complaint, Kogus v. Capone, No. 2022–
0047–SG (Del. Ch. 2022)). The overall
picture presented by this evidence
indicates that a change in oversight is
needed to better assure the safety and
effectiveness of IVDs offered as LDTs.
3. Greater FDA Oversight is Needed To
Protect the Public Health
As described above, the evidence FDA
has collected points to flaws in
laboratory manufacturing of tests that
need to be addressed to protect the
public. Greater oversight by FDA would
help address these flaws.
In the past, FDA has communicated
with the public when it is particularly
concerned about a type of IVD offered
as an LDT. For example, in addition to
the 2015 Report, FDA has issued safety
communications about pharmacogenetic
tests, NIPS tests, ovarian cancer
screening tests, nipple aspirate tests,
and instruments used in the design of
many different LDTs (Refs. 27 to 31).
FDA has also taken compliance action
in some circumstances, such as issuing
a warning letter to a laboratory
manufacturing a pharmacogenetic test
in April 2019 (Ref. 32). However, more
structural change is needed. FDA’s
general enforcement discretion
approach emerged at a time when the
typical IVD offered as an LDT looked
very different from how it looks today.
FDA has made a preliminary
determination that this approach has
become outdated, and the proposed
steps to end this approach in this
rulemaking would better protect the
public health.
Increased oversight would help to
ensure the safety and effectiveness of
IVDs offered as LDTs. More accurate
diagnoses would lead to better care,
which would advance public health
overall. Through increased oversight,
the public, including patients and
healthcare professionals, could have
more confidence that the test results
they rely on are accurate. Greater FDA
oversight of IVDs offered as LDTs has
become particularly important as more
and more novel treatments require use
of a specialized test to identify patients
likely to benefit from them. This, in
turn, has led to increased development
of tests used as the primary driver for
therapeutic decisions. These include
tests to determine whether to administer
a therapeutic, which therapeutic to
administer, and at what dose to
administer the therapeutic. For
example, recent approvals of drug
products to treat diseases in their early
stages, such as for early-stage
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Alzheimer’s patients, make accurate and
early diagnosis of these diseases more
critical today than ever before. As
another example, gene therapy is an
emerging field with incredible potential
to treat many diseases or conditions.
Testing is required to identify patients
with the defective gene targeted by the
treatment and, in some cases, to assess
whether the patient has antibodies to
the vector delivering the treatment that
would prevent it from working. In these
and other cases, accurate and reliable
test results are essential for safe and
effective use of a therapeutic.
Increased oversight would also
address business strategies that take
advantage of the current bifurcated
system. For example, in a number of
cases, laboratories that have submitted
premarket submissions for their tests,
but whose tests did not meet applicable
requirements for authorization, have
still offered these IVDs as ‘‘LDTs.’’ Some
of these tests, such as a test intended to
diagnose Alzheimer’s disease, had
inadequate validation data to support
authorization (see Ref. 33). A
genotyping test purported to predict
heart disease risk, but FDA found that
there was no association between the
genetic information the test identified
(KIF6) and heart disease. A third test,
intended to diagnose Fabry disease,
showed a high level of false negatives.
The public health is not served by a
scheme in which tests that have these
types of problems are still offered to
patients simply because the
manufacturer is a laboratory. FDA is
also aware that some industry players
have created business models that claim
a connection to laboratories and offer
IVDs as LDTs. The increase in firms
using these business models, as well as
their substantial magnitude of reach,
underscores the need for more
oversight.
In addition, FDA anticipates that
consistent oversight would bring more
stability to the testing market overall,
which could help to encourage the
manufacture of IVDs for which there is
a reasonable assurance of safety and
effectiveness. FDA is aware of
arguments that better assuring the safety
and effectiveness of LDTs would foster
test innovation. FDA is also aware of
arguments that IVD manufacturers that
are not laboratories may currently be
discouraged from investing time and
resources into developing novel tests
due to the concern that once the
manufacturer receives marketing
authorization for its test, laboratories
will develop similar tests and market
their tests without complying with FDA
requirements. We anticipate that
applying the same oversight approach to
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laboratories and non-laboratories that
manufacture IVDs would better assure
the safety and effectiveness of LDTs,
and would remove a disincentive for
non-laboratory manufacturers to
develop novel tests, thereby spurring
innovation and access to IVDs for which
there is a reasonable assurance of safety
and effectiveness. As a result, we
anticipate that phasing out the general
enforcement discretion approach for
LDTs would advance responsible
innovation by both laboratory and nonlaboratory IVD manufacturers alike,
rather than discouraging it.
FDA is aware of other arguments that
ending the general enforcement
discretion approach for LDTs would
interfere with test innovation and
patient access due to the potential need
for premarket review of new tests.
However, under FDA’s device
authorities, FDA premarket review is
only required for certain tests (generally
those classified into class II or class III),
and FDA estimates that approximately
50 percent of IVDs offered as LDTs
would not require premarket review (see
section II.F.4 of the Preliminary
Economic Analysis of Impacts (Ref. 34)).
In addition, FDA review is only
required for device modifications in
certain circumstances. For devices that
are subject to PMA requirements, a PMA
supplement is required only for changes
that affect the safety or effectiveness of
the device, and in some cases the
change may be made prior to FDA
approval (see 21 CFR 814.39(d)); may be
made 30 days after a supplement has
been filed, unless FDA takes certain
action (see 21 CFR 814.39(e)); or may be
made 30 days after FDA receives a
notice describing the change (in lieu of
a supplement), unless FDA takes certain
action (see 21 CFR 814.39(f)). For
devices that are subject to 510(k)
requirements, a new 510(k) is only
required for a significant change or
modification in design, components,
method of manufacture, or intended
use, where a significant change or
modification is one that could
significantly affect the safety or
effectiveness of the device or that is a
major change or modification in the
device’s intended use (21 CFR
807.81(a)). FDA has published several
guidance documents to help
stakeholders determine whether a
certain change or modification may
require a PMA supplement, new 510(k),
or other submission to FDA, and FDA
has several mechanisms available
through which manufacturers may seek
FDA assistance in making this
determination. In addition, under
section 515C of the FD&C Act (21 U.S.C.
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360e–4), a PMA supplement or new
510(k) is not required for a change to a
device that would otherwise require a
supplement or new 510(k) if the change
is consistent with a predetermined
change control plan previously
approved or cleared by FDA. We also
note that as described in section VI.B,
FDA is proposing to phase out the
general enforcement discretion
approach for LDTs with respect to
premarket review requirements on a
date that aligns with or follows the
beginning of a new user fee cycle, such
that FDA’s review timelines and goals
would be reflected in commitments
newly negotiated with industry. For all
of these reasons, FDA does not
anticipate that ending the general
enforcement discretion approach for
LDTs would unduly impair test
innovation and patient access.
Furthermore, FDA’s approach was
never intended to selectively foster
laboratory innovation at a cost to public
health. Rather, the approach arose based
on certain test characteristics and
institutional safeguards that at the time
adequately protected patients. In
general, those characteristics and
safeguards are no longer present, putting
public health at risk. Further, FDA is
aware that this scheme is in some cases
fostering unfounded claims of
innovation rather than responsible
innovation. These claims are concerning
to FDA because they can mislead the
public, undermine legitimate
competition, and disincentivize
responsible, science-based innovation.
Finally, increased oversight may help
to advance health equity. FDA is aware
of concerns that IVDs offered as LDTs
may exacerbate health inequities due to
higher rates of inaccurate results among
underrepresented patient populations,
particularly racial and ethnic minorities
undergoing genetic testing (see, e.g.,
Refs. 17 and 35 to 38). Some IVDs
offered as LDTs have not been validated
for use in all patient populations within
a disease state, meaning that it is
unknown how well the test may
perform across diverse patient
populations expected to use the test and
the test may be less accurate in
underrepresented patient populations,
potentially contributing to health
disparities (see, e.g., Ref. 39). Increased
FDA oversight may help to ensure that
information is available pertaining to
device safety and effectiveness for
specific demographic characteristics if
performance differs within the target
population, through the enforcement of
applicable labeling requirements. In
addition, when FDA conducts
premarket review of a device, FDA may
ask that sponsors provide data for
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different intended patient populations,
and with new authorities under the
Food and Drug Omnibus Reform Act of
2022 (FDORA), sponsors generally are
required to submit diversity action
plans to FDA, including the sponsor’s
goals for enrollment in device clinical
studies. In contrast, with limited
oversight over these tests, FDA does not
know whether diverse patient
populations are being included in
validation studies for these IVDs. FDA
has made a preliminary determination
that increased oversight for these IVDs
would help ensure adequate
representation of the intended use
population in validation studies and
transparency regarding potential
differential performance, helping to
advance health equity. FDA also
recognizes that IVDs offered as LDTs
may serve communities in rural,
medically underserved areas with
disparities in access to diagnostic tests.
However, the benefits of test access
directly depend on the ability of tests to
work as intended. Thus, to the extent
that access to IVDs offered as LDTs may
benefit patients in rural, medically
underserved communities, the harms of
unsafe or ineffective IVDs offered as
LDTs may also be realized among these
underserved patient populations. By
increasing its oversight, FDA may better
prevent and mitigate such harms,
thereby better protecting the health of
these underserved populations.
We are aware of arguments that other
mechanisms—such as the medical
expertise of laboratorians or
requirements under CLIA—already
provide adequate oversight of IVDs
offered as LDTs. However, our review of
the evidence indicates otherwise.
Evidence suggests that under the current
scheme, the healthcare community lacks
adequate assurances about the safety
and effectiveness of IVDs offered as
LDTs. Although laboratories that offer
LDTs are also subject to CLIA, which is
primarily administered by the Centers
for Medicare & Medicaid Services
(CMS), CLIA is not a substitute for FDA
oversight. CLIA establishes
requirements for laboratories and
laboratory personnel pertaining to
operations, inspections, and
certification, with a focus on the
proficiency with which laboratories
perform clinical testing (see 42 U.S.C.
263a and 42 CFR part 493). Among
other requirements, clinical laboratories
generally must have a CLIA certificate
that corresponds to the complexity of
tests performed prior to accepting
human samples for testing. However,
under CLIA, CMS does not regulate
critical aspects of laboratory test
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development; does not evaluate the
performance of a test before it is offered
to patients and healthcare providers;
does not assess clinical validity (i.e., the
accuracy with which a test identifies,
measures, or predicts the presence or
absence of a clinical condition or
predisposition in a patient); does not
regulate certain manufacturing
activities, such as design controls and
acceptance activities; does not provide
human subject protections for patients
who participate in test clinical research
trials; and does not require adverse
event reporting. As such, CMS has
described the FDA and CMS ‘‘regulatory
schemes’’ as ‘‘different in focus, scope
and purpose, but they are intended to be
complementary’’ (Ref. 40). Where CLIA
does play a role (as discussed further
below, compliance with CLIA may
provide certain assurances relating to
quality system (QS) requirements), FDA
has tailored its proposed phaseout
policy accordingly.11
We are also aware of arguments that
any additional oversight of LDTs should
be accomplished by granting new
statutory authorities to CMS. However,
this would cause a problematic split in
oversight, with the same types of tests
being reviewed by different Agencies
depending on where the test was made.
For example, a cancer diagnostic test
developed by a conventional
manufacturer would be reviewed by
FDA while a similar cancer diagnostic
test (using the same sample type and
testing for the same analytes) developed
by a laboratory would be reviewed by
another Agency. Further, with that
divided oversight, an IVD developed by
a conventional manufacturer could even
be reviewed and cleared by FDA and
subsequently reviewed by another
Agency if a laboratory made certain
modifications to it. However, if those
same modifications were made by the
original manufacturer, they would be
reviewed by FDA. This could lead to
confusion and inconsistency.
FDA has both the authority and the
expertise to perform the necessary
oversight of IVDs offered as LDTs and is
the only Agency for which that is the
case. One of FDA’s most basic and wellunderstood responsibilities is helping to
ensure the safety and effectiveness of
medical products. FDA employs staff
across a wide range of disciplines,
11 When ‘‘QS’’ requirements are discussed
throughout this preamble, FDA is referring to the
current good manufacturing practice (CGMP)
requirements set forth in part 820 (21 CFR part 820).
Generally, the requirements are referred to as QS
requirements, but that terminology may change
when amendments to part 820 are finalized. See 87
FR 10119 (February 23, 2022) and section VI.B.3 for
a further discussion of FDA’s proposed
amendments to part 820.
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including physicians, statisticians,
engineers, biologists, chemists,
geneticists, and others, to evaluate the
science behind medical products before
they reach the market. Understanding
the complex technical information in
applications, such as clinical trial data,
bench testing results, and product
manufacturing and design
characteristics—and putting that
information in context to assess whether
a product can be marketed—is within
the unique expertise of FDA. This type
of expertise is no less important for
IVDs, which can have a wide variety of
public-health consequences, as
described elsewhere in this rule. During
review of an application for an IVD,
FDA reviewers closely examine data
relevant to analytical validity, clinical
validity, and safety, and draw on their
expertise and experience to understand
both the product and the science
supporting the product.
Review of the underlying science
behind an IVD is based on what the IVD
does and is in no way related to where
the IVD is made. Thus, FDA’s
experience and expertise with respect to
oversight of other IVDs is directly
applicable to oversight of LDTs. In fact,
FDA has already applied its expertise to
the review of some IVDs offered as
LDTs—for example, during public
health emergencies. As stated above,
FDA has reviewed many EUA requests
for tests from laboratories during the
public health response to COVID–19.
Entities outside FDA have also
recognized that FDA should oversee
LDTs, and that greater oversight is
needed. For example, the Secretary’s
Advisory Committee on Genetics,
Health, and Society, in its April 2008
report entitled ‘‘U.S. System of
Oversight of Genetic Testing,’’ stated
that ‘‘FDA should address all laboratory
tests, regardless of how they are
produced (i.e., as a commercial test kit
or laboratory-developed test), in a
manner that takes advantage of its
current experience’’ (Ref. 41). The
American Cancer Society Cancer Action
Network has taken a similar position,
noting in a November 2016 statement
that ‘‘[c]urrent oversight of LDTs falls
short of ensuring these tests produce
accurate and meaningful results . . .
[t]he FDA is the most appropriate
agency to evaluate the analytical and
clinical validity of diagnostic tests,
along with their safety, to help ensure
that cancer patients and their doctors
are able to make appropriate treatment
decisions based on accurate
information’’ (Ref. 42). Likewise, the
Advanced Medical Technology
Association (AdvaMed) stated in
November 2021 that the association has
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‘‘long supported the idea that all
diagnostic test developers . . . should
be subject to the same FDA standards
and processes’’ (Ref. 43).
4. FDA Should Increase Oversight in a
Manner That Recognizes the Current
State of the Testing Market
As discussed throughout this section,
increased oversight of IVDs offered as
LDTs is needed. However, FDA has also
made a preliminary determination that
our general enforcement discretion
approach should be phased out in a
manner that accounts for the level of
public health concern and the
importance of avoiding undue
disruption to the testing market,
including undue disruption to the
provision of care. Therefore, we are
proposing a gradual phaseout to occur
in stages over a total period of 4 years,
as described in section VI.B. FDA
anticipates that this phaseout policy
should ultimately enable IVDs offered as
LDTs that are supported by sound
science to remain on the market. FDA
also recognizes that some IVDs may
need to come off the market, because,
for example, the IVD cannot meet
applicable requirements under the
FD&C Act and its implementing
regulations, or the laboratory chooses
not to invest resources to meet those
requirements. To the extent that
withdrawal from the market of these
IVDs implicates any reliance interests,
FDA has made a preliminary
determination that the public-health
benefits associated with the reasonable
assurance of safety and effectiveness of
IVDs offered as LDTs outweigh any such
interests. In addition, in the long run, it
is possible that any reduction in the
number of current IVDs offered as LDTs
may be offset by the market entry of
IVDs from other manufacturers who will
have benefitted from a more consistent
oversight approach and increased
stability spurring innovation.
C. FDA’s Current Regulatory Framework
The FD&C Act, as amended by the
MDA and subsequent statutes,
establishes a comprehensive system for
the regulation of devices, defined in
section 201(h)(1) of the FD&C Act, that
are intended for human use. Section 513
of the FD&C Act (21 U.S.C. 360c)
establishes three categories (classes) of
devices depending on the regulatory
controls needed to provide reasonable
assurance of their safety and
effectiveness. The three categories of
devices are class I (general controls),
class II (special controls), and class III
(premarket approval).
Class I devices are those devices for
which the general controls of the FD&C
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Act (controls authorized by or under
section 501, 502, 510, 516, 518, 519, or
520 (21 U.S.C. 351, 352, 360, 360f, 360h,
360i, or 360j) or any combination of
such sections) are sufficient to provide
reasonable assurance of safety and
effectiveness of the device; or those
devices for which insufficient
information exists to determine that
general controls are sufficient to provide
reasonable assurance of safety and
effectiveness or to establish special
controls to provide such assurance, but
because the devices are not purported or
represented to be for a use in supporting
or sustaining human life or for a use
which is of substantial importance in
preventing impairment of human
health, and do not present a potential
unreasonable risk of illness or injury,
are to be regulated by general controls
(section 513(a)(1)(A) of the FD&C Act).
General controls include, but are not
limited to, provisions that relate to
establishment registration and device
listing; premarket notification;
prohibitions against adulteration and
misbranding (e.g., labeling that fails to
bear adequate directions for use);
recordkeeping and reporting, including
adverse event reporting and reporting of
corrections and removals initiated to
reduce a risk to health posed by the
device or to remedy a violation of the
FD&C Act caused by the device which
may present a risk to health; and current
good manufacturing practice (CGMP)
requirements. These controls apply to
all devices unless an exemption applies.
Class II devices are those devices for
which general controls by themselves
are insufficient to provide reasonable
assurance of safety and effectiveness,
but for which there is sufficient
information to establish special controls
to provide such assurance, including the
promulgation of performance standards,
post-market surveillance, patient
registries, development and
dissemination of guidelines,
recommendations, and other
appropriate actions the Agency deems
necessary to provide such assurance
(section 513(a)(1)(B) of the FD&C Act).
Class III devices are those devices for
which insufficient information exists to
determine that general controls and
special controls would provide a
reasonable assurance of safety and
effectiveness, and are purported or
represented for a use in supporting or
sustaining human life or for a use which
is of substantial importance in
preventing impairment of human
health, or present a potential
unreasonable risk of illness or injury
(section 513(a)(1)(C) of the FD&C Act).
Under section 513(d)(1) of the FD&C
Act, devices that were introduced or
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delivered for introduction into interstate
commerce for commercial distribution
before the enactment of the MDA on
May 28, 1976 (generally referred to as
‘‘preamendments devices’’) are
classified after FDA: (1) receives a
recommendation from a device
classification panel (an FDA advisory
committee); (2) publishes the panel’s
recommendation, along with a proposed
regulation classifying the device, and
provides an opportunity for interested
persons to submit comments; and (3)
publishes a final regulation classifying
the device. A preamendments device for
which a classification regulation has not
been promulgated is known as an
‘‘unclassified device.’’ Until an
unclassified device type has been
formally classified by regulation, the
marketing of new devices within the
device type requires FDA premarket
review through a premarket notification
(510(k)) under section 510(k) of the
FD&C Act.
Devices that were not introduced or
delivered for introduction into interstate
commerce for commercial distribution
before May 28, 1976 (generally referred
to as ‘‘postamendments devices’’) are
classified automatically by section
513(f) of the FD&C Act into class III
without any FDA rulemaking process.
Those devices remain in class III and
require approval of a premarket
approval application (PMA), unless and
until: (1) FDA classifies or reclassifies
the device into class I or II under section
513(f)(2) or (3) of the FD&C Act, or (2)
FDA issues an order finding the device
to be substantially equivalent, in
accordance with section 513(i) of the
FD&C Act, to a predicate device that
does not require premarket approval.
The Agency determines whether new
devices are substantially equivalent to
predicate devices by means of
premarket notification procedures in
section 510(k) of the FD&C Act and part
807 of the regulations (21 CFR part 807).
In addition, under section 520(g) of
the FD&C Act and part 812 of FDA’s
regulations (21 CFR part 812), a clinical
investigation to determine the safety
and effectiveness of certain devices
must be the subject of an approved
investigational device exemption (IDE)
before such investigation may
commence. If an IDE has been granted,
a failure to comply with a requirement
under which the device was exempted
for investigational use renders the
device adulterated (see section 501(i) of
the FD&C Act).
Failure to comply with applicable
requirements of the FD&C Act and FDA
regulations may render the device
adulterated and misbranded under
sections 501 and 502 of the FD&C Act
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and may constitute a prohibited act
under section 301 of the FD&C Act (21
U.S.C. 331).
IVDs, as defined in § 809.3 (21 CFR
809.3), are devices intended for human
use and are subject to the FD&C Act.
They include class I, class II, and class
III devices, as well as both
preamendments and postamendments
devices. Like other devices, IVDs are
subject to general controls, including
premarket notification, reporting
requirements regarding adverse events
and corrections and removals, IDE
requirements (though most
investigations of IVDs are exempt from
most provisions of the IDE regulation),
and other applicable requirements
under the FD&C Act and FDA’s
regulations. IVDs are also subject to
specific labeling requirements in part
809 of the regulations (21 CFR part 809).
D. History of the Rulemaking
1. FDA’s Longstanding Recognition That
IVDs Manufactured by Laboratories Are
Devices
FDA has made clear, on many
occasions and over many years, that
LDTs are devices under the FD&C Act
(for the legal reasoning for this
conclusion, see section V.B). Over 25
years ago, FDA explained that clinical
laboratories that develop tests are acting
as manufacturers of medical devices (62
FR 62243 at 62249 (November 21,
1997)). FDA reiterated that position in a
citizen petition response a year later
(Ref. 44), and in the preamble to a final
rule 3 years after that (65 FR 18230 at
18231 (April 7, 2000)). In 2006, FDA
again cited its prior statement that
clinical laboratories that develop tests
are acting as manufacturers of medical
devices (Ref. 45 (quoting 62 FR 62243 at
62249)). In 2014, FDA expressly
considered and rejected arguments that
LDTs are not devices under the FD&C
Act, stating in a citizen petition
response that ‘‘LDTs are devices within
the plain language of the [statutory]
definition’’ (Ref. 46). Five years later,
FDA issued a warning letter stating that
‘‘FDA has not created a legal ‘carve-out’
for LDTs such that they are not required
to comply with the requirements under
the Act that otherwise would
apply. . . . Although FDA has
generally exercised enforcement
discretion for LDTs, the Agency always
retains discretion to take action when
appropriate, such as when it is
appropriate to address significant public
health concerns’’ (Ref. 47). A wide range
of other FDA documents, including
guidance documents, safety
communications, compliance letters,
and other public statements, have
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indicated or otherwise taken as their
premise that IVDs are devices even
when the manufacturer is a laboratory
(see, e.g., Refs. 11, 18, 27, 28, and 48 to
56).
FDA has also taken regulatory actions
consistent with these statements and
documents. Since 2017, the Agency has
reviewed over 40 PMAs, 510(k)s, and De
Novo classification requests for tests
identified by the manufacturer as LDTs,
and has approved, cleared, or granted
De Novo classification for roughly half
of those tests under authorities in the
FD&C Act specifically reserved for
‘‘devices.’’ FDA has also received many
EUA requests from laboratories and has
authorized over 150 such tests for
emergency use, an authority that is also
limited to ‘‘devices’’ or other FDAregulated medical products.
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2. Past FDA Initiatives To Address LDTs
In light of FDA’s recognition that
LDTs are devices and our increasing
concerns about IVDs offered as LDTs (as
detailed in the ‘‘Need for the Rule’’
section, section III.B of this document),
over the years the Agency has
considered various ways to address
IVDs manufactured by laboratories that
raise safety or effectiveness concerns. In
1997, FDA sought to address these
concerns by establishing restrictions on
the sale, distribution, and use of analyte
specific reagents (ASRs), which the
Agency described as the ‘‘primary
ingredients’’ of most LDTs (62 FR 62243
at 62249). In 2006, FDA issued a draft
guidance outlining a different
enforcement approach for a type of LDT
known as an in vitro diagnostic
multivariate index assay (IVDMIA),12
which raised particular safety and
effectiveness concerns (Ref. 45). FDA
later determined that it should engage in
a more comprehensive effort to oversee
LDTs, in part due to stakeholder
feedback.
Consistent with this determination, in
2010, FDA announced plans to develop
12 As defined in the draft guidance document,
IVDMIAs are ‘‘test systems that employ data,
derived in part from one or more in vitro assays,
and an algorithm that usually, but not necessarily,
runs on software to generate a result that diagnoses
a disease or condition or is used in the cure,
mitigation, treatment, or prevention of disease.’’
The draft guidance document further characterized
IVDMIAs as having the following three features:
they use clinical data to empirically identify
variables and derive weights/coefficients used in an
algorithm; they employ that algorithm to calculate
a patient-specific result, which cannot be
independently derived and confirmed by another
laboratory (absent access to proprietary information
used in the development and derivation of the test);
and they report that result, which cannot be
interpreted by a well-trained healthcare practitioner
using prior knowledge of medicine in the absence
of information from the test developer regarding
clinical performance and effectiveness.
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a broader approach to the oversight of
LDTs. The Agency held a 2-day public
meeting and opened a docket for public
comment (75 FR 34463 (June 17, 2010)).
Input received through those
proceedings informed two draft
guidance documents issued by FDA on
October 3, 2014, entitled ‘‘Framework
for Regulatory Oversight of Laboratory
Developed Tests (LDTs)’’ (79 FR 59776)
and ‘‘FDA Notification and Medical
Device Reporting for Laboratory
Developed Tests (LDTs)’’ (79 FR 59779)
(Refs. 48 and 49). In those draft
guidance documents, FDA proposed to
implement a risk-based oversight
framework for IVDs offered as LDTs,
with a phased enforcement strategy.
FDA solicited public feedback on the
draft guidance documents and held a
public workshop on January 8 and 9,
2015 (79 FR 69860 (November 24,
2014)).
From October 2014 through 2016,
FDA analyzed more than 300 sets of
comments on the draft guidance
documents, as well as discussion from
the public workshop, and engaged
extensively with stakeholders in
meetings and conferences. A number of
interested parties provided feedback,
including laboratories, healthcare
providers, patients, conventional IVD
manufacturers, government agencies,
and Congress. The feedback ranged
generally from strong opposition to
strong support for FDA’s proposed
increased oversight of LDTs and
addressed a wide range of topics,
including FDA’s authority to regulate
LDTs, the risks posed by LDTs without
increased FDA enforcement, the effect
of a new enforcement approach on test
access and innovation, the potential
interplay between FDA regulation and
CLIA, and the implications of increased
FDA oversight for competition in the
IVD market.
On January 13, 2017, FDA issued a
discussion paper (2017 Discussion
Paper) synthesizing the feedback that
had been provided to the Agency,
following a choice by FDA not to
finalize the draft guidance documents to
allow for further public discussion and
to provide an opportunity for Congress
to develop legislation for a new
regulatory framework encompassing all
IVDs that appropriately balances patient
protection with continued access and
innovation (Ref. 50).
In August 2020, HHS posted a
statement on its website entitled
‘‘Rescission of Guidances and Other
Informal Issuances,’’ which stated,
among other things, that ‘‘the
department has determined that the
Food and Drug Administration (‘FDA’)
will not require premarket review of
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laboratory developed tests (‘LDT’)
absent notice-and-comment
rulemaking’’ (Ref. 57).13 This statement
was informed by advice in a legal
memorandum from the HHS Office of
General Counsel (see Ref. 59). In
November 2021, based on new advice
from the HHS Office of General Counsel,
HHS leadership determined that the
August 2020 statement no longer
represented the Department’s policy or
legal views (Ref. 59). HHS Secretary
Xavier Becerra publicly announced the
withdrawal of the statement on
November 15, 2021 (Ref. 60). Various
news outlets have reported on these
events (Refs. 61 to 64).
IV. Legal Authority
FDA is proposing to issue this rule
under the Agency’s general rulemaking
authorities and statutory authorities
relating to devices. These authorities
include sections 201(h)(1), 301, 501,
502, 510, 513, 514, 515, 518, 519, 520,
701, 702, 704, and 801 (21 U.S.C.
321(h)(1), 331, 351, 352, 360, 360c,
360d, 360e, 360h, 360i, 360j, 371, 372,
374, and 381). In particular:
• Under section 201(h)(1) of the
FD&C Act, a device is defined as ‘‘an
instrument, apparatus, implement,
machine, contrivance, implant, in vitro
reagent, or other similar or related
article, including any component, part,
or accessory, which is (A) recognized in
the official National Formulary, or the
United States Pharmacopeia, or any
supplement to them, (B) intended for
use in the diagnosis of disease or other
conditions, or in the cure, mitigation,
treatment, or prevention of disease, in
man or other animals, or (C) intended to
affect the structure or any function of
the body of man or other animals, and
which does not achieve its primary
intended purposes through chemical
action within or on the body of man or
other animals and which is not
dependent upon being metabolized for
the achievement of its primary intended
purposes.’’
• Section 701(a) of the FD&C Act
authorizes FDA to issue regulations for
the efficient enforcement of the FD&C
Act.
For additional descriptions of some of
the authorities referenced above, see
‘‘FDA’s Current Regulatory Framework’’
section (section III.C.). For additional
discussion of how these legal authorities
apply to LDTs, see ‘‘Legal Basis for the
Proposed Amendment’’ section (section
V.B.).
13 HHS also posted an accompanying document
entitled ‘‘FAQs on Laboratory Developed Tests
(LDTs)’’ on its website (Ref. 58).
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V. Description of the Proposed
Amendment to the Definition of In Vitro
Diagnostic Products
A. Proposed Amendment
We are proposing to amend part 809,
subpart A, specifically § 809.3, by
updating the definition of ‘‘in vitro
diagnostic products’’ to make explicit
that IVDs are devices under the FD&C
Act including when the manufacturer of
the IVD is a laboratory. IVDs are defined
as ‘‘those reagents, instruments, and
systems intended for use in the
diagnosis of disease or other conditions,
including a determination of the state of
health, in order to cure, mitigate, treat,
or prevent disease or its sequelae. Such
products are intended for use in the
collection, preparation, and
examination of specimens taken from
the human body’’ (§ 809.3). This
amendment would reflect FDA’s
longstanding view that LDTs are devices
under the FD&C Act, and would reflect
the fact that the device definition in the
FD&C Act does not differentiate
between entities manufacturing the
device. In other words, whether an IVD
is a device does not depend on where
or by whom the IVD is manufactured.
FDA is also proposing to amend the
statutory citation for the device
definition included in § 809.3 to reflect
amendments to section 201(h) of the
FD&C Act as a result of the enactment
of the Safeguarding Therapeutics Act
(Pub. L. 116–304, 134 Stat. 4915). For
many years, the definition of ‘‘device’’
had been codified at section 201(h) of
the FD&C Act. Upon enactment of the
Safeguarding Therapeutics Act, the
definition of ‘‘device’’ was redesignated
as paragraph (h)(1) and a new definition
of ‘‘counterfeit device’’ was codified at
paragraph (h)(2).
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B. Legal Basis for the Proposed
Amendment
If amended as proposed, § 809.3
would express in plain terms that IVDs,
including test systems, fall within the
definition of a device in section
201(h)(1) of the FD&C Act when they
have been manufactured by laboratories.
In this subsection, FDA sets forth the
legal reasoning for this position.
1. In Vitro Diagnostic Test Systems Are
Devices
The FD&C Act defines a device as, in
relevant part, ‘‘an instrument,
apparatus, implement, machine,
contrivance, implant, in vitro reagent, or
other similar or related article,
including any component, part, or
accessory, which is . . . intended for
use in the diagnosis of disease or other
conditions, or in the cure, mitigation,
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treatment, or prevention of disease’’ (see
21 U.S.C. 321(h)(1); see also 21 U.S.C.
360j(o) (identifying circumstances under
which software is and is not within the
device definition)). This definition
includes IVD test systems. Test systems
are sets of IVDs—for example, reagents,
instruments, specimen collection
devices, software, and other related
materials—that function together to
produce a test result. See, e.g.,
§ 809.10(a)(9)(iii) (21 CFR
809.10(a)(9)(iii)) (discussing ‘‘multiple
unit products which require the use of
included units together as a system’’);
id. § 809.10(b) (referring to reagents and
instruments within a system).
According to a straightforward reading
of the statutory text, these systems are
‘‘apparatus[es],’’ ‘‘contrivance[s],’’ and
articles that are ‘‘similar or related’’ to
‘‘instrument[s]’’ and ‘‘in vitro
reagent[s],’’ that are intended for use in
the diagnosis of disease or other
conditions or in the cure, mitigation,
treatment, or prevention of disease.
They consist of individual parts that
have their own regulatory identity, but,
when combined, constitute a new
device.
The device definition expressly
contemplates this scenario because it
provides that both an overall article and
each of its ‘‘components’’ and ‘‘parts’’
are devices subject to regulation. (21
U.S.C. 321(h)(1); cf. Shuker v. Smith &
Nephew, PLC, 885 F.3d 760, 768 (3d Cir.
2018) (describing the distinct status of a
‘‘system that is itself a ‘device’ but that
is comprised of Class II [device]
components in addition to one or more
Class III [device] components’’).) The
word ‘‘apparatus,’’ which is defined as
‘‘a set of materials or equipment
designed for a particular use,’’
encompasses test systems by its plain
terms. (See Apparatus, MerriamWebster.com (last accessed June 28,
2023); see also United States v. BactoUnidisk, 394 U.S. 784, 798 (1969)
(‘‘Congress fully intended that the
[FD&C] Act’s coverage be as broad as its
literal language indicates’’).) Consistent
with this analysis, FDA’s definition of
an ‘‘in vitro diagnostic product,’’ which
was first promulgated in 1973 and is
still in effect today, identifies a
‘‘system’’ as a type of IVD and a device
under the FD&C Act. (Section 809.3
(IVDs include ‘‘reagents, instruments,
and systems’’); see 38 FR 7096 at 7098
(March 15, 1973).)
The regulation of test systems is
important because test systems are
generally the IVDs that produce a
result—a ‘‘positive’’ or ‘‘negative’’ (such
as what patients receive in the context
of COVID–19 diagnostic tests), a
quantitative value (such as a
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concentration of glucose), or perhaps a
more detailed report of results. The
quality of test results is generally what
defines both the risks and benefits of
IVDs: the risks stem from inaccurate,
unreliable, incomplete, or misleading
test results, and the benefits stem from
accurate, reliable, and complete test
results. For that reason, test systems and
their results are a key focus of FDA’s
regulation of IVDs. FDA has issued over
350 regulations classifying different
types of test systems (see generally 21
CFR parts 862, 864, 866) and has
evaluated the performance and results
of innumerable test systems over the
course of decades. Patients and
healthcare professionals rely on FDA to
help ensure the validity of test systems,
and conventional IVD manufacturers
have built their business around this
premise.
The focus on test systems and their
results is not new; it has been a
consistent theme throughout the history
of FDA’s regulation of IVDs. Congress
expressly granted FDA authority over
diagnostic products in 1938. (Federal
Food, Drug and Cosmetic Act (June 25,
1938), Pub. L. 75–717, 52 Stat. 1040
(defining ‘‘drug’’ and ‘‘device’’ with
reference to an intended use in
‘‘diagnosis,’’ among other things).)
Following the 1938 Act, FDA took
action against diagnostic products,
including against a system intended to
diagnose illness based on human blood
samples. (See Drown v. United States,
198 F.2d 999, 1001 (9th Cir. 1952).)
And, in the early 1970s, FDA
established a specific IVD regulatory
program in response to ‘‘rapid growth in
development of in vitro diagnostic
products combined with the increasing
use and reliance on the results by
physicians, hospital personnel, and
clinical laboratories.’’ (37 FR 819,
January 19, 1972). This program
addressed the ‘‘need [for] closer scrutiny
because of the possibility that
inaccurate and unreliable results may be
obtained.’’ Id. FDA issued final
regulations establishing controls over
IVDs, including ‘‘systems,’’ in 1973 (38
FR 7096 at 7098) (creating, among other
things, ‘‘product class standards’’ to set
‘‘performance requirements necessary to
assure accuracy and reliability of
results’’). FDA’s increasing concerns
about these products was evident from
the fact that—even before Congress
expanded the Agency’s device
authorities in 1976—it applied the drug
authorities to certain IVDs. The
Supreme Court upheld that application
in Bacto-Unidisk, 394 U.S. at 800–01.
In 1976, Congress enacted the MDA,
sweeping legislation meant to broaden
and strengthen FDA’s authority over
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devices. (See, e.g., H.R. Rep. 94–853 at
11 (February 29, 1976).) The MDA
included revisions to the definition of
‘‘device’’ to clarify that IVDs should be
regulated under the new, more robust
device authorities. (Medical Device
Amendments of 1976, Pub. L. 94–295,
90 Stat. 539 (adding the term ‘‘in vitro
reagent’’ to the definition of a device);
S. Rep. No. 93–670 at 16 (January 29,
1974) (‘‘The Committee recognizes that
there is confusion at the present time
about whether certain articles are to be
treated as devices or drugs under the
Food, Drug and Cosmetic Act.
Therefore, the Committee reported bill
has carefully defined ‘device’ so as to
specifically include implants, in vitro
diagnostic products, and other similar
or related articles.’’). The legislative
history shows that Congress had serious
concerns about test systems and sought
to empower FDA to address them. (See,
e.g., S. Rep. No. 93–670 at 3–4 (January
29, 1974) (describing with concern
‘‘quack devices’’ such as a ‘‘diagnostic
service’’ in which ‘‘[p]ractitioners . . .
mailed in the blood spots taken from
their patients,’’ ‘‘[t]he blood-spotted
paper was put into a slot of the
electrical device called the ‘Radioscope’
while the operator stroked with a wand
the abdomen of a person holding metal
plates connected to the device,’’ and
‘‘the operator determined from this the
identity, kind, location, and significance
of any disease present’’).) Congress also
contemplated performance standards
relevant to test systems, such as
required labeling with ‘‘ranges of
accuracy of diagnosis.’’ (H.R. Rep. 94–
853 at 27.) Thus, in the MDA, Congress
endorsed FDA’s focus on test systems
and their results.
2. Test Systems Manufactured by
Laboratories Are Devices
The definition of ‘‘device’’ in the
FD&C Act encompasses test systems
regardless of where or by whom they are
manufactured. (See 21 U.S.C. 321(h)(1).)
In particular, the definition contains no
exception or limitation for devices
manufactured by laboratories. ‘‘Congress
expresses its intentions through
statutory text passed by both Houses
and signed by the President (or passed
over a Presidential veto).’’ (Oklahoma v.
Castro-Huerta, 142 S. Ct. 2486, 2496
(2022).) If Congress had intended such
a limitation, it could have said so.
Instead, Congress made clear that the
definition does not turn on the type of
entity manufacturing the device: for
example, the statute expressly
recognizes that even ‘‘practitioners
licensed by law to prescribe or
administer . . . devices’’ (the
professionals most closely associated
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with traditional medical practice) can
‘‘manufacture . . . devices,’’ though
they may be exempt from certain
requirements when they do so ‘‘solely
for use in the course of their
professional practice.’’ 14 (See 21 U.S.C.
360(g)(2); see also 21 U.S.C. 360i(c)(1),
374(a)(2)(B).)
Courts have repeatedly recognized
that articles manufactured by medical
professionals fall within FDA’s
jurisdiction (e.g., United States v.
Regenerative Sciences, 741 F.3d 1314
(D.C. Cir. 2014) (holding that doctors
‘‘producing, as part of their medical
practice,’’ a ‘‘drug’’ under the FD&C Act
violated the FD&C Act); Drown v.
United States, 198 F.2d 999, 1001 (9th
Cir. 1952) (upholding FDA action
against chiropractor who
‘‘manufacture[d] certain photographic,
therapeutic and diagnostic instruments
of her own design which she use[d] in
her practice’’)). As the D.C. Circuit in
Regenerative Sciences observed, an
approach that rejects ‘‘the [FD&C Act]’s
regulation of doctors’’ would ‘‘create an
enormous gap in the [FD&C Act]’s
coverage.’’ (741 F.3d at 1320.)
The inclusion of articles in the FD&C
Act’s definition of a device without
regard to the identity of their
manufacturer makes particular sense in
the context of test systems. Today, in
FDA’s experience, there is little
distinction between the test systems
manufactured by laboratories and other
manufacturers. These systems generally
consist of highly specialized
components with complex functionality
working in combination; they rarely
resemble the ‘‘1976-type’’ tests
discussed in this rule. For example, a
modern-day next generation sequencing
(NGS) test system for genetic testing
typically consists of (among other
things) a DNA extraction kit to extract
nucleic acids from a human sample; an
14 These exemptions apply when a practitioner (1)
is licensed by law to prescribe or administer a
device such as an IVD, (2) manufactures that device,
and (3) does so ‘‘solely for use in the course of [his
or her] professional practice.’’ Thus, these
exemptions apply to practitioners, not entities such
as corporate or hospital laboratories that employ
licensed practitioners. For example, FDA has long
held that hospitals that reprocess single-use devices
are subject to registration and other requirements
under the FD&C Act because they are the owners/
operators, manufacturers, etc. even though those
hospitals employ licensed practitioners. See
Frequently-Asked-Questions about the Reprocessing
and Reuse of Single-Use Devices by Third-Party and
Hospital Reprocessors; Final Guidance for Industry
and FDA Staff (July 2001), available at https://
www.fda.gov/media/71057/download (stating
‘‘Third-party and hospital reprocessors of single-use
devices (SUDs) are subject to all the regulatory
requirements currently applicable to original
equipment manufacturers, including premarket
submission requirements’’ and including a Q&A
that provides instructions on how to register and
list for such entities).
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NGS instrument that analyzes the
nucleic-acid output and (after days)
generates gigabytes of sequencing raw
data; and multiple pieces of computer
software that translate that raw data into
a test report. The systems look the same,
and function the same way, regardless
of who manufactures them. And
although not all systems look exactly
like an NGS system, they do typically
involve sophisticated instruments with
advanced software that, when used in
conjunction with other test components,
produce the system’s results. Their
manufacture generally requires
knowledge of bioinformatics, software
development, and an underlying
specialty, such as medical genetics—
knowledge that is neither traditionally
associated with nor unique to
laboratories. FDA understands that
many test systems offered as LDTs are
designed at Fortune 500 companies (see
Ref. 65) by a ‘‘development team,’’
similar to how systems from
conventional manufacturers are
designed. And in FDA’s experience, the
individuals on these development teams
generally have the same training and
expertise regardless of whether they are
employed by a ‘‘laboratory’’
organization or a conventional
manufacturer. Even smaller laboratories
use the same complex equipment for
their systems, although they may
purchase and use components that are
labeled by other companies for
‘‘research use only.’’ In short, there is
nothing inherent in the nature or design
of laboratory developed test systems
that would justify exclusion from FDA’s
jurisdiction.
That is not to say that laboratories and
conventional IVD manufacturers are
identical. Laboratories do occupy a
distinct role in diagnostic testing
because they are the entities that
generally perform the tests. Like many
devices, such as a magnetic resonance
imaging unit used by a trained
technician, test systems are usually used
by trained professionals. Laboratories
that are certified under CLIA and that
meet the regulatory requirements under
CLIA to perform high complexity testing
employ trained laboratorians to ‘‘run’’
test systems, and CLIA is the statutory
scheme that governs that work, as
discussed in more detail in section III.B.
However, a laboratory’s role in
performing test systems does not change
its obligations under the FD&C Act
when it is manufacturing test systems.
As previously noted, the FD&C Act does
not exclude medical professionals who
manufacture devices from its scope, and
the mere fact that a device is
manufactured in connection with a
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medical service or procedure does not
eliminate FDA’s jurisdiction. (See
United States v. Regenerative Sciences,
741 F.3d at 1319 (‘‘Notwithstanding
appellants’ attempt to characterize this
case as an effort by the FDA to ‘restrict[ ]
the use of an autologous stem cell
procedure,’ the focus of the FDA’s
regulation is on the Mixture [that is, the
product that is created in connection
with the procedure].’’).)
Although some commentators have
argued that laboratory manufacturing is
immune from regulation because it is
within the ‘‘practice of medicine,’’ that
argument misconstrues the scope of the
FD&C Act’s ‘‘practice of medicine’’
provision. Section 1006 of the FD&C Act
(21 U.S.C. 396) provides: ‘‘Nothing in
this [Act] shall be construed to limit or
interfere with the authority of a health
care practitioner to prescribe or
administer any legally marketed device
to a patient for any condition or disease
within a legitimate health care
practitioner-patient relationship.’’
Section 1006 carves out a specific zone
of protected conduct that does not reach
laboratory manufacturing of test
systems. The purpose of the provision is
to ‘‘ensure[ ] that once the FDA permits
a device to be marketed for one use,
health care practitioners have the
flexibility to draw on their expertise to
prescribe or administer the device’’ for
other uses. (Judge Rotenberg Educ. Ctr.,
Inc. v. United States, 3 F.4th at 395
(emphases added); see also Conf. Rep.
105–399 at 97 (November 9, 1997)
(provision intended to cover ‘‘off-label
use of a medical device by a physician
using his or her best medical judgment
in determining how and when to use the
medical product for the care of a
particular patient’’).) The statutory
provision applies only in the context of
use of a ‘‘legally marketed device’’—that
is, a device that is already manufactured
and lawfully on the market—and only
applies to ‘‘prescrib[ing] or
administer[ing] . . . within a legitimate
health care practitioner-patient
relationship.’’ It does not apply to the
manufacture of new test systems. The
manufacture of a new device falls
squarely within FDA’s realm. Cf. United
States v. Regenerative Sciences, 741
F.3d at 1320 (‘‘[W]hile the [FD&C Act]
was not intended to regulate the
practice of medicine, it was obviously
intended to control the availability of
drugs for prescribing by physicians.’’)
(quoting United States v. Evers, 643
F.2d 1043, 1048 (1981)). The fact that
healthcare practitioners may prescribe a
device, such as a test system, in the
context of a healthcare practitionerpatient relationship does not mean that
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entities manufacturing that device can
escape regulation. If that were the case,
few devices would be regulated, because
most are intended for use by healthcare
practitioners in the context of a
healthcare practitioner-patient
relationship.
Furthermore, contrary to what some
commentators have suggested, CLIA did
not repeal FDA’s authority over IVDs
manufactured by laboratories, which
dates back to at least 1938. CLIA does
not expressly repeal FDA’s authority,
nor was FDA’s authority repealed by
implication. ‘‘An implied repeal will
only be found where provisions in two
statutes are in irreconcilable conflict, or
where the latter Act covers the whole
subject of the earlier one and is clearly
intended as a substitute.’’ (Branch v.
Smith, 538 U.S. 254, 273 (2003)
(cleaned up).) Here, as CMS itself has
explained, ‘‘the regulatory schemes of
the two agencies are different in focus,
scope and purpose’’ and ‘‘are intended
to be complementary’’ (Ref. 40). As
explained in section III.B, CLIA puts a
focus on the proficiency with which
laboratories perform clinical testing, and
the FD&C Act puts a focus on the
manufacturing of test systems. CMS and
FDA have different areas of expertise,
and CLIA does not address a wide range
of activities regulated under the FD&C
Act, such as clinical validation and
design activities. Thus, ‘‘CLIA does not
preempt the FDA’s authority to regulate
facilities like [Clinical Reference
Laboratory]. When two statutes are
‘capable of co-existence, it is the duty of
the courts, absent a clearly expressed
congressional intent to the contrary, to
regard each as effective.’ ’’ (Clinical
Reference Lab. v. Sullivan, 791 F. Supp.
1499, 1509 (D. Kan. 1992) (quoting
Ruckelshaus v. Monsanto Co., 467 U.S.
986, 1018, (1984)), aff’d in part and
rev’d in part on other grounds sub nom.,
United States v. Undetermined No. of
Unlabeled Cases, 21 F.3d 1026 (10th
Cir. 1994).)
In fact, Congress has affirmed that test
systems manufactured by laboratories
are devices under the FD&C Act. In the
Protecting Access to Medicare Act of
2014 (PAMA) (Pub. L. 113–93),
Congress listed 510(k) clearance or
premarket approval under the FD&C Act
as one of several bases for Medicare
payment for an ‘‘advanced diagnostic
laboratory test,’’ which is defined in
part as a clinical diagnostic laboratory
test ‘‘that is offered and furnished only
by a single laboratory and not sold for
use by a laboratory other than the
original developing laboratory (or a
successor owner)’’ (section 216(a) of
PAMA). If such laboratory tests were not
devices, the 510(k) clearance and
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premarket approval provisions would
not apply to them and the inclusion of
such provisions would be pointless and
ineffectual. In addition, Congress
indicated that clinical laboratory tests
are devices in 2016 amendments to the
FD&C Act. (21 U.S.C. 360j(o)(1)(D)
(repeatedly referring to ‘‘clinical
laboratory test or other device data’’)
(emphasis added).)
The FD&C Act confers jurisdiction on
FDA to regulate test systems, a point
that has been codified in FDA’s
regulations for more than half a century.
And nothing in the text, history, or
purpose of the statute suggests that test
systems manufactured by laboratories
are excluded from that jurisdiction. This
interpretation is not only the most
straightforward reading of the statute, it
is also the most reasonable: any other
interpretation would create a bifurcated
scheme in which systems that are
functionally identical are treated
differently under the law.
3. FDA’s Jurisdiction Over IVDs
Manufactured by Laboratories Is Not
Altered by the FD&C Act’s Provisions
Related to Interstate Commerce and
Commercial Distribution
Modern Commerce Clause
jurisprudence holds that Congress has
‘‘authority to regulate even purely local
activities that are part of an economic
‘class of activities’ that have a
substantial effect on interstate
commerce.’’ (United States v.
Regenerative Sciences, 741 F.3d at 1320
(quoting Gonzales v. Raich, 545 U.S. 1,
17 (2005)).) Thus, few have disputed
that Congress possesses the power to
grant FDA authority to regulate even
purely intrastate activities. However,
some commentators have asserted that
language in the FD&C Act referencing
‘‘interstate commerce’’ and ‘‘commercial
distribution’’ precludes FDA from
regulating IVDs that are designed,
manufactured, and used in a single
laboratory. As discussed below, these
assertions lack merit.
a. Interstate commerce. There is no
overarching requirement in the FD&C
Act that FDA-regulated articles have a
particular nexus with interstate
commerce. Interstate commerce is not a
prerequisite to FDA jurisdiction (beyond
the constitutional minimum). Rather,
under the FD&C Act, a limited number
of provisions include specific interstate
commerce ‘‘elements,’’ and thus require
a particular connection with interstate
commerce in order for those provisions
to apply. For example, certain of the
FD&C Act’s ‘‘prohibited acts’’ contain an
interstate commerce element that must
be satisfied before the government can
bring an enforcement action under those
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provisions (e.g., 21 U.S.C. 331(a), (c),
(d), and (k)). But relatively few of the
FD&C Act’s device provisions include a
specific interstate commerce element,
and most of the device-related
prohibited acts do not. (See, e.g., 21
U.S.C. 331(e) (prohibiting the failure to
establish or maintain any record, or
make any report, required under the
device adverse-event reporting
requirements without reference to
interstate commerce); id. 331(p)
(prohibiting the failure to register a
device establishment without reference
to interstate commerce); id. 331(q)(1)
(prohibiting the failure to comply with
device investigational-use requirements
without reference to interstate
commerce); id. 331(fff)(3) (prohibiting
the doing of any act which causes a
device to be a counterfeit device, or the
sale or dispensing, or holding for sale or
dispensing, of a counterfeit device
without reference to interstate
commerce); see generally United States
v. Walsh, 331 U.S. 432, 434–36 (1947)
(finding no interstate commerce element
to 21 U.S.C. 331(h), which prohibits
false guaranties) (‘‘[21 U.S.C. 331(a)] is
directed to illegal interstate shipments,
while [21 U.S.C. 331(h)] is directed to
the giving of false guaranties’’).) If an
FD&C Act provision does not contain an
interstate commerce element, ‘‘interstate
commerce’’ imposes no limit on FDA’s
powers beyond the constitutional
minimum. For devices, the FD&C Act
imposes obligations even where there is
no interstate commerce element and
likewise gives FDA authority to take
action when there is a violation of those
obligations. Thus, FDA does not, for
example, somehow lose jurisdiction if a
particular device has not been
‘‘introduced’’ into interstate commerce.
In fact, Congress intentionally revised
a provision of the FD&C Act to ensure
that FDA could take action against
devices without satisfying any
particular interstate commerce element.
In the MDA, Congress revised the
seizure provisions in section 304 of the
FD&C Act to ‘‘permit seizure of devices
without reference to interstate
commerce’’ because the previous
interstate commerce requirement ‘‘ha[d]
been a burden to the effective
enforcement of existing authorities’’ and
‘‘whether or not a medical device
actually crosses state lines has nothing
to do with the principal intent of this
proposal: to assure the safety and
effectiveness of medical devices.’’ (H.R.
Rep. 94–853 at 15; see 21 U.S.C.
334(a)(2).) In other words, Congress
recognized that the interstate commerce
element in this provision did not
advance the goals of the MDA.
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Consistent with that view, the FD&C Act
grants FDA wide-ranging authority over
devices, including IVDs, and that
general authority does not turn on a
connection with interstate commerce
above the constitutional minimum.
In addition, one of the key prohibited
acts on which FDA relies, section 301(k)
of the FD&C Act (21 U.S.C. 331(k)),
contains an interstate commerce
element, but applies even when a
problematic device has not been
introduced in interstate commerce. That
provision prohibits ‘‘the doing of any
. . . act with respect to[ ] a . . . device
. . . if such act is done while such
article is held for sale (whether or not
the first sale) after shipment in interstate
commerce and results in such article
being adulterated or misbranded.’’
Courts have held that even if a product
is wholly manufactured and sold
intrastate, the interstate commerce
element is satisfied if the components
used in manufacturing the product have
traveled in interstate commerce. (See
United States v. Regenerative Sciences,
741 F.3d at 1320–21 (upholding FDA
enforcement action under 331(k)
because a drug component had traveled
in interstate commerce); Baker v. United
States, 932 F.2d 813, 815 (9th Cir. 1991);
United States v. Dianovin Pharm., Inc.,
475 F.2d 100, 102 (1st Cir. 1973).) At
least some components of test systems,
such as general purpose reagents, ASRs,
instruments, and collection devices, are
usually shipped in interstate commerce
even if the system itself is designed,
manufactured, and used solely in the
laboratory (i.e., intrastate). And section
709 of the FD&C Act (21 U.S.C. 379a)
establishes a presumption of interstate
commerce in enforcement actions,
meaning that the burden is on regulated
parties to demonstrate, for example, that
no component of a system traveled
across State lines. (‘‘In any action to
enforce the requirements of this Act
respecting a device . . . the connection
with interstate commerce . . . shall be
presumed to exist.’’).
Some commentators have cited the
interstate commerce element in section
510(k) of the FD&C Act to raise
questions about FDA’s authority over
LDTs. Section 510(k) provides that a
person who is required to register and
‘‘proposes to begin the introduction or
delivery for introduction into interstate
commerce’’ of a device ‘‘shall’’ submit a
premarket notification. Under this line
of argument, laboratories that design,
manufacture, and use an IVD in a single
laboratory are not proposing to
introduce their IVD into interstate
commerce, and therefore section 510(k)
does not apply to them. That argument,
however, does not lead to the
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conclusion that FDA lacks jurisdiction
over LDTs or that none of the FD&C Act
requirements apply to LDTs. It would
mean only that section 510(k) does not
apply. And if accepted, the only
practical consequence of that assertion
would be that affected laboratories are
subject to more burdensome
requirements under the FD&C Act.
In particular, if section 510(k) is
construed to mean that such IVDs are
not eligible for the premarket
notification pathway, that would only
mean that those IVDs (unless they are
510(k)-exempt, in which case section
510(k) would not apply anyway, or are
for investigational use) would be forced
into the more rigorous review pathways
of premarket approval or authorization
through the De Novo pathway. That is
because under section 513(f)(l) of the
FD&C Act, a postamendments device,
i.e., a device that was ‘‘not introduced
or delivered for introduction into
interstate commerce for commercial
distribution before [May 28, 1976],’’ is a
class III device by operation of law (21
U.S.C. 360c(f)(1)). If such a device
cannot be found to be substantially
equivalent through the premarket
notification pathway, it must either
have an approved PMA (21 U.S.C.
360e(a)), or be reclassified and gain
authorization through a pathway such
as the De Novo process (21 U.S.C.
360c(f)(2)(A)(ii)). Thus, under this
theory, laboratories would not escape
FDA regulation—they would face
heavier regulation. However, because
section 510(k) does not, in fact, preclude
regulated entities from submitting
premarket notifications even assuming
their devices are not introduced into
interstate commerce, and because
laboratories have every incentive to take
the less burdensome path to market of
510(k) notification, the 510(k) pathway
should play the same role in device
reclassification (21 U.S.C. 360c(f)) for
IVDs offered as LDTs as for any other
device. Regardless, the inclusion of an
interstate commerce element in section
510(k) in no way affects FDA’s overall
authority to regulate IVDs manufactured
by laboratories.
b. Commercial distribution. The
phrase ‘‘for commercial distribution’’
also appears in various device
provisions of the FD&C Act, and some
commentators have asserted that this
phrase, too, signals that FDA lacks
authority over LDTs. For example, they
point to the 510(k) premarket
notification requirement, which is
triggered when a person who is required
to register ‘‘proposes to begin the
introduction or delivery for introduction
into interstate commerce for commercial
distribution of a device intended for
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human use’’ (21 U.S.C. 360(k)). As with
‘‘interstate commerce,’’ the presence of
this phrase in that provision and certain
other specific device provisions does
not bear on the Agency’s overall
jurisdiction. Furthermore, LDTs are for
commercial distribution, so the
presence of the phrase does not change
the operation of those provisions with
respect to these IVDs.
Under our longstanding, judicially
endorsed interpretation, ‘‘commercial
distribution’’ does not require the
physical transfer of an object, as some
commentators have argued. Instead, the
legislative history, FDA’s nearcontemporaneous regulation, and at
least one judicial decision reflect that
the phrase ‘‘commercial distribution’’
means ‘‘on the market.’’ A House Report
issued 3 months before enactment of the
MDA contains an unusually clear
statement of the intended meaning of
the phrase: ‘‘‘Commercial distribution’
is the functional equivalent of the
popular phrase ‘on the market.’ ’’ (H.R.
Rep. No. 94–853 at 36) FDA’s
regulations implementing the
registration, listing, and 510(k)
provisions, which were finalized in
1977 (soon after enactment of the MDA),
similarly define commercial distribution
as ‘‘any distribution of a device
intended for human use which is held
or offered for sale.’’ (21 CFR 807.3(b)) In
the preambles to the proposed and final
rule, FDA equated the term with the
phrase ‘‘on the market’’ (41 FR 37458 at
37459 (September 3, 1976); 42 FR 42520
at 42524 (August 23, 1977)). A court has
also endorsed this interpretation of the
term (United States v. An Article of
Device Consisting of 1,217 Cardboard
Boxes, 607 F. Supp. 990, 994–95 (W.D.
Mich. 1985) (giving deference to FDA’s
reasonable interpretation of
‘‘commercial distribution’’ to mean, ‘‘in
its popular sense, ‘on the market’ ’’)).
These sources show that the term does
not relate to physical movement, and
because IVDs manufactured by
laboratories (including LDTs) generally
are ‘‘on the market,’’ they are for
commercial distribution.
VI. Description of the Proposed
Enforcement Policy
Based on the considerations set forth
in this preamble, FDA is proposing to
end the general enforcement discretion
approach for LDTs. However, FDA also
recognizes that many IVDs
manufactured by laboratories are
currently being marketed as LDTs, and
that a sudden change could negatively
affect the public, including patients and
industry. In particular, FDA
understands that the healthcare
community and patients have been
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using these IVDs, and that coming into
compliance will take time for
manufacturers. FDA also recognizes that
we should consider Agency resources.
For additional information regarding the
estimated costs associated with this
rulemaking, see the Preliminary
Economic Analysis of Impacts (Ref. 34).
To achieve greater oversight in a
manner that accounts for the various
considerations, FDA is proposing to
gradually end its general enforcement
discretion approach in stages, as
described below (hereinafter ‘‘the
phaseout policy’’). FDA’s intent is that,
following a 4-year phaseout period,
IVDs offered as LDTs generally would
be expected to meet applicable
requirements.
Although FDA is proposing to
gradually end its current general
enforcement discretion approach over a
period of years, the phaseout policy
does not in any way alter the fact that
it is illegal to offer IVDs without
complying with applicable
requirements. Regardless of the
phaseout timeline and continued
enforcement discretion approach for
certain IVDs discussed below, FDA
retains discretion to pursue enforcement
action at any time against violative IVDs
when appropriate.
Moreover, FDA has adopted and
intends to continue adopting
enforcement discretion policies for
certain types of IVDs in certain
circumstances, as appropriate. For
example, FDA issued guidance
documents with enforcement discretion
policies for certain COVID–19 and
Mpox tests at the beginning of each
declared emergency (as described
further below), and intends to issue a
draft guidance with an enforcement
policy for IVDs for emerging outbreaks
offered prior to FDA review to address
the immediate public health need. FDA
will seek public comment on such draft
guidance in accordance with good
guidance practices (see 21 CFR 10.115).
With this notice of proposed
rulemaking, FDA seeks public comment
on whether specific enforcement
discretion policies would be appropriate
for IVDs offered as LDTs for other public
health scenarios. If so, please provide a
description of those scenarios, an
explanation of why enforcement
discretion policies with respect to those
scenarios would be appropriate, and any
relevant evidence to support such
policies. FDA would also appreciate
public comment on what, if any,
unintended consequences may result
from the proposed phaseout policy to
certain patient populations (for
example, Medicare beneficiaries, rural
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populations, etc.) and what steps could
be taken to mitigate those consequences.
FDA’s proposed phaseout policy,
including the scope and phaseout
timeline, is set forth below.
A. Scope
While FDA’s general enforcement
discretion approach has been focused
on LDTs, FDA is proposing a broader
scope for the phaseout policy.
Specifically, FDA is proposing to apply
the phaseout policy to IVDs that are
manufactured and offered as LDTs by
laboratories that are certified under
CLIA and that meet the regulatory
requirements under CLIA to perform
high complexity testing,15 even if those
IVDs do not fall within FDA’s
traditional understanding of an LDT
because they are not designed,
manufactured, and used within a single
laboratory.16 Throughout this preamble,
these IVDs are referred to as ‘‘IVDs
offered as LDTs.’’ FDA is proposing this
scope because it recognizes that not all
laboratories have understood the limited
nature of FDA’s general enforcement
discretion approach and have been
offering IVDs based on the approach
even when they do not fit what FDA
generally considers to be an LDT. As
previously discussed, FDA has made a
preliminary determination to structure
the phaseout in a way that avoids undue
disruption to the testing market. This is
important even for certain IVDs
currently on the market that do not fall
within the scope of FDA’s general
enforcement discretion approach.
Although FDA is proposing this
broader scope for the phaseout policy, it
does not intend to sweep in certain tests
that were excluded from the general
enforcement discretion approach, as
reflected in compliance patterns,
multiple public FDA actions and
communications, or both. These tests
are:
1. Tests that are intended as blood
donor screening or human cells, tissues,
and cellular and tissue-based products
(HCT/Ps) donor screening tests required
for infectious disease testing under 21
CFR 610.40 and 1271.80(c),
respectively, or for determination of
15 Other laboratories would be out of compliance
with CLIA regulations if they were developing and
performing tests that are not FDA authorized. Such
tests have never fallen within FDA’s general
enforcement discretion approach (see, e.g., Refs. 32,
40, and 54).
16 As discussed elsewhere in this preamble, FDA
has generally considered the term ‘‘laboratory
developed test (LDT)’’ to mean an IVD that is
intended for clinical use and that is designed,
manufactured, and used within a single CLIAcertified laboratory that meets the regulatory
requirements under CLIA to perform high
complexity testing.
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blood group and Rh factors required
under 21 CFR 640.5. Under the cited
regulations, a blood or HCT/P
establishment must not use a test for the
purposes listed here unless the test is
licensed, approved, or cleared by FDA
for such use. Blood and HCT/P
establishments must register with FDA
and are subject to FDA inspection (see
21 CFR parts 207, 607, 807 and 1271).
FDA’s general enforcement discretion
approach for LDTs has never applied to
these tests because these tests are a
critical part of the overall process of
ensuring the safety of blood and blood
components and HCT/Ps by preventing
infectious disease transmission and
incompatible blood transfusions which
can have life-threatening consequences.
Based on FDA experience,
establishments have been generally
complying with these requirements (see,
e.g., Refs. 66 and 67).
2. Tests intended for emergencies,
potential emergencies, or material
threats declared under section 564 of
the FD&C Act. After all previous
declarations under section 564(b), FDA
has generally expected LDTs to comply
with applicable requirements in the
FD&C Act and FDA regulations. FDA’s
general enforcement discretion
approach has not applied to these tests
because of the significant risk posed by
the disease (as signified by the unusual
step of issuing a declaration) and
because false results can have serious
implications for disease progression and
public health decision-making, in
addition to the individual patient’s care.
As it has done in other areas, FDA has
adopted (and may continue to adopt)
specific enforcement discretion policies
for such tests (see, e.g., Refs. 51 and 52).
In addition, consistent with the
Government Accountability Office’s
2022 recommendation that ‘‘FDA
should develop a policy for the use of
enforcement discretion regarding
unauthorized tests in future public
health emergencies,’’ FDA intends to
issue guidance on factors to consider in
adopting such enforcement discretion
policies (Ref. 68). FDA has
communicated its expectations
regarding tests for emergency use in
guidance and elsewhere, including ‘‘It
has come to our attention’’ letters posted
on FDA’s website and other public
communications (see, e.g., Refs. 51 to
54, 69, and 70).
3. Direct-to-consumer tests. FDA’s
general enforcement discretion
approach has not applied to tests
intended for consumer use (without
meaningful involvement by a licensed
healthcare professional), given the
greater risks to patients presented by
these tests (see, e.g., Refs. 48, 55, and 71
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to 75). FDA’s enforcement discretion
approach for LDTs was originally
premised, in part, on the participation
of medical professionals to help
determine whether a particular test was
appropriate, counsel patients on the
significance and limitations of a test,
assist in interpreting results, assess how
the results fit in the overall clinical
picture, and consider next steps. When
patients order tests, receive results, and
make decisions (such as a decision to
stop medication) without this expert
intermediary, there is a heightened need
for FDA oversight.
For these categories of tests, FDA has
generally expected applicable
requirements to be met, and we are not
proposing to change that approach.
FDA notes that the manufacturing of
test components outside of a
laboratory—for example, when the same
entity owns both the laboratory and a
manufacturing facility separate from the
laboratory—does not fall within FDA’s
general enforcement discretion
approach. FDA’s approach has long
been specific to laboratory development
(e.g., 61 FR 10484 (‘‘in-house developed
tests have not been actively regulated by
the Agency’’) (emphasis added); Ref. 48
(describing an LDT as an IVD that is
‘‘designed, manufactured, and used
within a single laboratory’’). The
proposed phaseout policy would not
change FDA’s longstanding expectation
that IVD manufacturing activities
occurring outside of a CLIA-certified
laboratory comply with applicable
device requirements.
In addition, for certain categories of
tests manufactured by laboratories, FDA
is proposing to continue to apply the
current general enforcement discretion
approach going forward. One such
category of tests is referred to in this
preamble as ‘‘1976-Type LDTs.’’ Such
tests have the following characteristics
common among LDTs offered in 1976:
use of manual techniques (without
automation) performed by laboratory
personnel with specialized expertise;
use of components legally marketed for
clinical use; and design, manufacture,
and use within a single CLIA-certified
laboratory that meets the requirements
under CLIA for high complexity testing.
The characteristics associated with
LDTs offered in 1976 resulted in the
emergence of FDA’s general
enforcement discretion approach for
LDTs, and the specific characteristics
listed above provide the greatest risk
mitigation among the characteristics
that were commonly associated with
LDTs offered in 1976 (discussed in
section III.A). Based on changes to the
LDT landscape since 1976, the risks
associated with most modern LDTs are
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generally much greater today than they
were in 1976; however, for tests that
share the characteristics listed above,
FDA has made a preliminary
determination that the risks are
sufficiently mitigated such that FDA’s
general enforcement discretion
approach for LDTs should continue to
apply. These tests might include, for
example, immunohistochemistry tests
that involve no automated preparation
or interpretation, but would not include,
for example, lateral flow tests, as they
do not generally rely on laboratory
personnel expertise.
FDA is also proposing to continue to
apply the general enforcement
discretion approach to Human
Leukocyte Antigen (HLA) tests that are
designed, manufactured, and used in a
single laboratory certified under CLIA
that meets the requirements to perform
high-complexity histocompatibility
testing when used in connection with
organ, stem cell, and tissue
transplantation to perform HLA allele
typing, for HLA antibody screening and
monitoring, or for conducting real and
‘‘virtual’’ HLA crossmatch tests. FDA
has made a preliminary determination
that HLA LDTs for transplantation used
in histocompatibility laboratories that
meet the regulatory requirements under
CLIA to perform high complexity
testing, when used in connection with
organ, stem cell, and tissue
transplantation for certain purposes as
described in this paragraph, are unique
in that they are generally developed,
and the testing is generally performed,
in urgent, life-saving situations for the
patient. Physicians must often make
prompt decisions about transplantation
based on medical judgment regarding
their patient’s condition and degree of
mismatch between the donor and
patient should an organ, stem cells, or
tissue become available. Further, these
tests are often individualized within
each medical facility, for example, they
include reagents that reflect local HLA
polymorphisms and patient
demographics. Note that the general
enforcement discretion approach does
not apply to HLA tests used for blood
transfusion as such tests are highly
standardized across institutions; FDA
intends to continue to enforce
applicable requirements for HLA tests
used for blood transfusion.
FDA also intends to maintain its
longstanding enforcement discretion
approach for tests intended solely for
forensic (law enforcement) purposes.
This approach has been in place for over
20 years and applies to such tests
regardless of whether they are offered as
an LDT. See, e.g., 65 FR 18230 (April 7,
2000). Tests used in the law
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enforcement setting are subject to
protections and requirements associated
with the judicial process that mitigate
risk related to test accuracy and sample
collection and that generally are not
available in the home, workplace,
insurance, and sports settings. These
protections include the use of rules of
evidence in judicial proceedings and
legal representation of the accused (i.e.,
the person being tested) through the
judicial process during which the
accuracy of the test may be raised
during the adjudication. We seek
comment on any implications of
continued enforcement discretion with
regard to LDTs used for law
enforcement purposes and any factors
that FDA should consider—particularly
as it relates to civil rights and equity—
related to the scientific validity and
accuracy of these tests.
In addition, tests exclusively used for
public health surveillance are distinct
from other tests where: (1) they are
intended solely for use on
systematically collected samples for
analysis and interpretation of health
data in connection with disease
prevention and control, and (2) test
results are not reported to patients or
their healthcare providers. These tests
would not be affected by the phaseout
policy. The results of these tests are
generally used for trending on a
population basis. Public health
authorities also have access to test
results from non-surveillance tests that
are FDA approved, cleared, or
authorized and that are reported under
State reporting laws for infectious and
other diseases. In addition, during a
public health emergency, if there was a
564 declaration (as there was for past
public health emergencies), FDA could
require test result reporting to public
health authorities under emergency use
authorizations, as appropriate.
In 2017, FDA indicated support for
less oversight of other categories of tests,
such as low-risk tests (class I devices),
tests currently on the market, and tests
for rare diseases. However, FDA has
accumulated information in the
intervening years that suggests we
should treat these categories of tests
similarly to other FDA-regulated tests.
For example, as discussed above in
section III.B, FDA has gained additional
information showing that there is a high
variability in the performance of IVDs
offered as LDTs that are currently on the
market, including in circumstances
where the test technology is relatively
simple and well-understood, where the
tests are for rare diseases, and where the
tests are low risk. Among other things,
FDA’s recent experience with tests for
COVID–19 suggests that many tests
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manufactured by laboratories are not
appropriately validated. Compliance
with premarket review requirements
(when applicable), QS requirements,
and registration and listing
requirements would help assure that
these IVDs work as intended, enable
FDA to keep track of IVDs offered as
LDTs (and, for example, help FDA
locate IVDs that are raising concerns or
independently evaluate the risk status of
marketed IVDs), assist with FDA’s
inspection and planning efforts, and
make information available to patients
and healthcare providers that may
inform the selection of particular IVDs
for use. Therefore, FDA is now
proposing to end the general
enforcement discretion approach, via a
phaseout approach, with respect to
premarket review requirements (as
applicable), QS requirements, and
registration and listing requirements for
these tests, in addition to medical
device reporting (MDR) requirements
(i.e., reporting of adverse events),
correction and removal reporting
requirements, and other requirements
applicable to such tests. Based on the
information available at this time, FDA
has made a preliminary determination
that this proposal appropriately
balances the relevant considerations
with respect to these tests, including
currently marketed IVDs offered as
LDTs.
However, FDA expects that some
stakeholders will suggest that FDA
continue to maintain the current general
enforcement discretion approach with
respect to premarket review and some or
all QS requirements for currently
marketed LDTs or a subset of currently
marketed LDTs (i.e., what some
previously referred to as
‘‘grandfathering’’). To the extent
commenters suggest such an approach
for FDA’s consideration, FDA requests
information to support such an
approach, including the following:
• Given the information in the ‘‘Need
for the Rule’’ section of this preamble in
particular, what would be the public
health rationale for generally exercising
enforcement discretion with respect to
premarket review and some or all QS
requirements, for LDTs that are being
offered as of the date of issuance of this
proposed rule and are not changed with
respect to indications for use or
performance after that date? Please
provide data to support such an
approach. Also, if you think there are
steps that might help support such an
approach, including ideas that might
help to address the public health
concerns discussed in the ‘‘Need for the
Rule’’ section, please describe them, and
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include a rationale and any supporting
evidence.
• If commenters suggest maintaining
the general enforcement discretion
approach with respect to premarket
review and QS requirements for a subset
of LDTs (e.g., low and moderate risk
LDTs) currently on the market that are
being offered as of the date of issuance
of this proposed rule and are not
changed with respect to indications for
use or performance after that date, what
would be the public health rationale to
support such an approach? Please
provide any data supporting such an
approach. Also, if you think there are
steps that might help support such an
approach, including ideas that might
help to address the public health
concerns discussed in the ‘‘Need for the
Rule’’ section, please describe them and
include a rationale and any supporting
evidence.
FDA recognizes that the phaseout of
the general enforcement discretion
approach described in this section may
have a relatively greater impact on small
laboratories. Therefore, FDA seeks
comment on the following:
• Is there a public health rationale to
have a longer phaseout period for IVDs
offered as LDTs by laboratories with
annual receipts below a certain
threshold (e.g., $150,000) (see Table 43
in the Preliminary Economic Analysis of
Impacts (Ref. 34))? If so, please provide
relevant data and comment specifically
on an alternative recommended
timeline.
In addition, FDA is aware that some
AMCs have claimed that their
laboratories operate under unique
circumstances (such as being integrated
into direct patient care) and therefore
their tests should be treated differently
than tests manufactured by other
laboratories. Although FDA is not aware
of an established definition of an AMC
laboratory, one possible description is: a
laboratory for which a certificate is in
effect under CLIA and that meets the
requirements under CLIA to perform
tests of high-complexity; that is part of
an accredited public or nonprofit
private AMC that has a medical
residency training program or
fellowship program related to test
development, application, and
interpretation; and that is integrated
into the direct medical care for a
patient, including specimen collection,
testing, interaction with the treating
provider, and, as appropriate, patient
treatment based on the test, all at the
same physical location. FDA seeks
comments on the following:
• What are the characteristics of AMC
laboratories? Do the characteristics
included above accurately describe
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AMC laboratories and in fact distinguish
them from other laboratories?
• Should FDA continue the general
enforcement discretion approach with
respect to any requirements, such as
premarket review requirements, for tests
manufactured by AMC laboratories?
• If FDA should continue the general
enforcement discretion approach with
respect to any requirements, such as
premarket review requirements, for tests
manufactured by AMC laboratories, are
there any additional considerations that
should be taken into account with
respect to this approach, for example,
whether an FDA cleared or approved
test is available for the same intended
use as the test manufactured by an AMC
laboratory? Please provide a rationale
and other information (e.g., data) to
support any additional considerations.
• If FDA should have a different
policy for AMC laboratories, what
would be the public health rationale to
support such a policy? For example, if
integration of an AMC laboratory into
direct patient care is included as a basis
for a different policy, please include a
public health rationale when explaining
why and how such integration supports
the different policy, and how integration
could ensure that there is a reasonable
assurance of IVD safety and
effectiveness.
• If FDA should have a different
policy for AMC laboratories, is there
evidence to support such a policy?
FDA also is interested in and seeks
comment on leveraging programs such
as the New York State Department of
Health Clinical Laboratory Evaluation
Program (NYSDOH CLEP) or those
within the Veterans Health
Administration (VHA), as appropriate.
In particular, FDA requests comment on
whether it may be appropriate to
continue the general enforcement
discretion approach, such that FDA
generally would not enforce any
applicable device requirements, where
outside programs can be leveraged. If
FDA should continue to exercise
enforcement discretion under these
circumstances:
• What specific characteristics of and
activities within these programs justify
such an approach?
• Should the scope of such a policy
be more limited for each program in
question? For example, should FDA
continue enforcement discretion for
premarket review requirements and
intend to enforce other requirements,
such as reporting adverse events?
• Are there any additional
considerations that should be taken into
account?
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Please provide a rationale and other
information (e.g., data) to support any
suggestions.
B. Stages
As previously discussed, FDA is
proposing to gradually phase out its
current general enforcement discretion
approach so that most IVDs offered as
LDTs would generally fall under the
same enforcement approach as other
IVDs. In developing the proposed
phaseout policy, FDA has considered a
number of factors, including the public
health importance of better assuring the
safety and effectiveness of IVDs offered
as LDTs, the desire to avoid undue
disruption to the testing market, the
time it may take for laboratories to come
into compliance with FDA
requirements, the need for adequate
resources to implement the phaseout
policy in a manner that does not
undermine reasonable expectations with
regards to premarket review timing (per
the Medical Device User Fee
Amendments (MDUFA) V agreement),
and the benefits of a relatively simple
policy that can be easily understood and
implemented. Keeping these factors in
mind, FDA has structured the phaseout
policy to contain five key stages:
• Stage 1: End the general
enforcement discretion approach with
respect to MDR requirements and
correction and removal reporting
requirements 1 year after FDA publishes
a final phaseout policy, which FDA
intends to issue in the preamble of the
final rule.
• Stage 2: End the general
enforcement discretion approach with
respect to requirements other than MDR,
correction and removal reporting, QS,
and premarket review requirements 2
years after FDA publishes a final
phaseout policy.
• Stage 3: End the general
enforcement discretion approach with
respect to QS requirements 3 years after
FDA publishes a final phaseout policy.
• Stage 4: End the general
enforcement discretion approach with
respect to premarket review
requirements for high-risk IVDs 31⁄2
years after FDA publishes a final
phaseout policy, but not before October
1, 2027.
• Stage 5: End the general
enforcement discretion approach with
respect to premarket review
requirements for moderate risk and low
risk IVDs (that require premarket
submissions) 4 years after FDA
publishes a final phaseout policy, but
not before April 1, 2028.
Each of these stages is discussed in
further detail below. For each stage,
FDA is proposing a period of time for
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laboratories to come into compliance
before FDA intends to end the general
enforcement discretion approach. FDA
encourages laboratory manufacturers to
begin early and work toward
compliance with requirements sooner
than the end of the specified
timeframes. FDA also intends to
consider providing more targeted
guidance and/or making additional
resources available on specific topics,
such as compliance with applicable
labeling requirements, over the course
of the phaseout period.
1. Stage 1: End the general
enforcement discretion approach with
respect to MDR requirements and
correction and removal reporting
requirements 1 year after FDA publishes
a final phaseout policy.
FDA has structured the phaseout
policy to obtain information about
potentially harmful IVDs offered as
LDTs as soon as feasible. As detailed
elsewhere in this preamble, FDA is
concerned that some of the IVDs offered
as LDTs may be posing risks to patients.
Therefore, FDA is prioritizing the
phaseout of the general enforcement
discretion approach for requirements
that would help FDA identify and
monitor significant issues with IVDs
offered as LDTs, consistent with other
considerations described in this
proposed policy.
Enforcement of the MDR requirements
under 21 U.S.C. 360i(a) through (c) and
21 CFR part 803, in particular, would
enable FDA to systematically monitor
significant adverse events to identify
problematic IVDs offered as LDTs, such
as those with poor performance or other
safety issues. FDA has made a
preliminary determination that
gathering this information is important
for IVDs that do not have the safeguards
associated with compliance with other
FDA requirements, such as
manufacturing under QS requirements
or confirmation of analytical and
clinical validity through premarket
review.
For similar reasons, FDA is
prioritizing the collection of information
about when a manufacturer has initiated
a correction or removal of its IVD to
reduce a risk to health or to remedy a
violation of the FD&C Act that may
present a risk to health. Under 21 U.S.C.
360i(g) and part 806 (21 CFR part 806),
manufacturers are required to report
such corrections or removals to FDA,
and FDA intends to phase out the
general enforcement discretion
approach for these requirements at the
same time it does so for MDR
requirements. Because FDA intends for
the phaseout of the general enforcement
discretion approach with respect to
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correction and removal reporting
requirements to occur before phaseout
of the general enforcement discretion
approach with respect to registration
and listing requirements, FDA intends
to exercise enforcement discretion, such
that it generally does not intend to
enforce, the requirement to use the
establishment registration number on
such reports (21 CFR 806.10) when
laboratories use their CLIA certificate
number instead prior to registering.
FDA’s proposal to phase out
enforcement discretion for MDR
requirements within 1 year after
finalization of the policy is informed by
comments FDA received in response to
the draft guidance documents that FDA
issued in 2014 proposing to implement
an oversight framework for IVDs offered
as LDTs. In 2014, FDA proposed a 6month timeline for laboratory
compliance with MDR requirements
(Ref. 48), and we received comments
suggesting that a longer period may be
appropriate for the establishment of a
system to identify, review, and report
adverse events. Based in part on those
comments, FDA is now proposing a 1year time period for laboratories to come
into compliance with the MDR
requirements. In conjunction with the
phaseout of the general enforcement
discretion approach with respect to the
MDR requirements, FDA is also
proposing to end the general
enforcement discretion approach with
respect to the requirements of part 806,
concerning reports of corrections and
removals. Because MDRs frequently are
a basis for corrections and removals,
FDA views these requirements as
working together to provide information
to FDA about issues with device
performance or quality. We anticipate
that this 1-year time period is adequate,
particularly given that laboratories
should already have some processes in
place for detecting problems with their
IVDs to comply with CLIA regulations.
2. Stage 2: End the general
enforcement discretion approach with
respect to requirements not covered
during other stages of the phaseout
policy 2 years after FDA publishes a
final phaseout policy.
FDA is proposing to end the general
enforcement discretion approach for
requirements besides MDR, correction
and removal reporting, QS, and
premarket review requirements 2 years
after the final policy is published. These
other requirements include registration
and listing requirements under 21
U.S.C. 360 and part 807 (excluding
subpart E); labeling requirements under
21 U.S.C. 352 and parts 801 and 809,
subpart B; and investigational use
requirements under 21 U.S.C. 360j(g)
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and part 812. We have included
compliance with investigational use
requirements at this stage, in
recognition that there has been some
confusion about our enforcement
approach in this area. Our
understanding is that laboratories often
are not complying with investigational
use requirements currently, even though
FDA has generally expected compliance
with these requirements.17 We are
therefore including these requirements
in the phaseout policy.
FDA recognizes that this proposal is
different from FDA’s prior statements in
the 2017 Discussion Paper regarding
oversight of IVDs manufactured by
laboratories with respect to certain
requirements, for which the timing of
FDA’s expectations for compliance
generally depended on the type of
premarket review applicable to the
device. However, upon review, FDA
anticipates that it would better serve the
public health and be simpler to phase
out the general enforcement discretion
approach for these requirements at the
2-year mark. For example, under this
timeline, laboratories could work
toward compliance with the stage 2
requirements without necessarily
determining the risk category of their
IVDs until later stages of the proposed
phaseout policy. Another advantage of
this timeline is that FDA would obtain
registration and listing information
before the enforcement discretion
phaseout date for premarket review
requirements, which could give the
Agency an initial understanding of the
universe of IVDs offered as LDTs to
facilitate premarket review of those
IVDs. Based on its experience, FDA
anticipates that 2 years is adequate time
to come into compliance with the
various requirements.
3. Stage 3: End the general
enforcement discretion approach with
respect to QS requirements 3 years after
FDA publishes a final phaseout policy.
At the 3-year mark, FDA would
expect compliance with the device
CGMP requirements of the QS
requirements under 21 U.S.C. 360j(f)
and part 820 (21 CFR part 820).
However, for IVDs for which all
manufacturing activities occur within a
single CLIA-certified laboratory that
meets the regulatory requirements to
perform high complexity testing and for
which distribution of the IVD does not
17 For example, FDA stated in the ‘‘Framework for
Regulatory Oversight of Laboratory Developed Tests
(LDTs)’’ draft guidance that ‘‘FDA intends to
continue to enforce investigational device
requirements under 21 CFR part 812 for all clinical
investigations of LDTs that are conducted under
clinical protocols that require institutional review
board approval’’ (Ref. 48).
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occur outside that single laboratory,
FDA would expect compliance at the 3year mark with some, but not all, of the
QS requirements. Although FDA and
CMS regulation are different and
complementary, compliance with CLIA
requirements provides some quality
assurances that may be relevant to
laboratories’ manufacturing practices. In
particular, laboratories may in practice
be able to apply concepts set forth under
CLIA requirements for laboratory
operations to manufacturing activities
regulated by FDA. For FDA to
effectively leverage the CLIA
assurances, this proposed approach
would apply only when all
manufacturing activities occur within a
single laboratory and the IVD is not
distributed outside that laboratory.
However, even in the context of this
approach, there are certain QS
requirements for which CLIA
regulations do not provide the
assurances that FDA requirements
would provide. These requirements
include design controls under 21 CFR
820.30; purchasing controls (including
supplier controls) under 21 CFR 820.50;
acceptance activities (receiving, inprocess, and finished device
acceptance) under 21 CFR 820.80 and
21 CFR 820.86; corrective and
preventative actions (CAPA) under 21
CFR 820.100; and records requirements
under part 820, subpart M. Because
CLIA does not provide assurances
relevant to these requirements, FDA is
proposing to end the general
enforcement discretion approach for
these specific requirements for IVDs for
which all manufacturing activities occur
within a single CLIA-certified laboratory
that meets the regulatory requirements
to perform high complexity testing, and
which are not distributed outside that
laboratory, 3 years after finalizing this
policy. For all other IVDs offered as
LDTs and subject to this phaseout
policy, FDA is proposing to end the
general enforcement discretion
approach for all QS requirements 3
years after finalizing this policy.
Based on its experience, FDA
anticipates that 3 years is adequate time
for laboratories to come into compliance
with QS requirements. In addition,
based on the discussion above regarding
concerns with the quality and validation
of IVDs offered as LDTs, FDA has made
a preliminary determination that
phasing out the general enforcement
discretion approach for QS
requirements later than 3 years would
not be in the best interest of the public
health. Compliance with QS
requirements is critical to the quality
and validity of IVDs offered as LDTs.
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For example, under the design controls
of the QS requirements, laboratories
would, among other things, generally
have better procedures for validating the
design of their tests, which would help
to ensure that they are analytically and
clinically valid (see Ref. 76).
FDA also notes that on February 23,
2022, FDA proposed to amend the
device QS regulation, part 820, to align
more closely with international
consensus standards for devices (87 FR
10119). As stated in that proposed rule,
the requirements, if finalized, would be
substantially similar to the requirements
of the current part 820, providing a
similar level of assurance in a firm’s
quality management system, and FDA
intends for this phaseout policy to apply
with respect to any regulations
promulgated through that rulemaking.
FDA intends to finalize amendments
to the QS regulation expeditiously, such
that the amended QS requirements
would be in effect before the proposed
beginning of stage 3. Upon the start of
stage 3, or if the laboratory complies
with QS requirements prior to the start
of stage 3, FDA would expect
compliance with the QS requirements
that are in effect at that time. For further
information on the QS requirements that
would be established pursuant to the
amendments to the QS regulation, if
finalized as proposed, please refer to the
proposed codified at 87 FR 10119 at
10133 and 10134. Notably, the
requirements relating to design controls,
purchasing controls, acceptance
activities, CAPA, and records
requirements are set forth in the
following ISO 13485 clauses as
modified by the proposed codified for
part 820: Clause 4. Quality Management
System, Subclause 4.2.5; Clause 6.
Resource Management; Clause 7.
Product Realization, Subclause 7.1,
Subclause 7.3, Subclause 7.4, and
Subclause 7.4.3; and Clause 8.
Measurement, Analysis, &
Improvement, Subclause 8.2.5,
Subclause 8.2.6, and Subclause 8.3.
In addition, FDA notes that under
section 515(d)(2) of the FD&C Act, the
Agency may not approve a PMA if the
applicant fails to demonstrate
conformity with the QS requirements.
Therefore, compliance with the QS
requirements is needed to support
approval of a PMA. As provided in
section 520(f)(2) of the FD&C Act, any
person subject to the QS requirements
may petition for an exemption or
variance from any QS requirement (see
also 21 CFR 820.1).
4. Stage 4: End the general
enforcement discretion approach with
respect to premarket review
requirements for high-risk IVDs 31⁄2
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years after FDA publishes a final
phaseout policy, but not before October
1, 2027.
FDA proposes that the phaseout date
for the general enforcement discretion
approach with respect to premarket
review requirements for high-risk IVDs
offered as LDTs (IVDs that may be
eligible for classification into class III)
should occur 31⁄2 years from the time
that FDA issues a final phaseout policy.
The premarket review requirements are
set forth in 21 U.S.C. 360e and 21 CFR
part 814. FDA is proposing this time
period because it is mindful that
phasing out the general enforcement
discretion approach on a timeline that is
too short could cause undue disruption
in the testing market. Among other
things, we anticipate that 31⁄2 years
would provide sufficient notice and
opportunity for laboratories
manufacturing IVDs to plan for and
prepare PMAs and would appropriately
account for any reliance interests. We
note that 31⁄2 years is a longer time
period than was discussed in either the
2014 draft guidance documents or the
2017 Discussion Paper for the phaseout
of the general enforcement discretion
approach for premarket review
requirements.
This timeline is also intended to align
the phaseout date for the general
enforcement discretion approach for
premarket review requirements for highrisk IVDs offered as LDTs with the start
of fiscal year 2028, which coincides
with the beginning of a new user fee
cycle. This alignment would provide an
opportunity for industry participation in
negotiations regarding the next user fee
cycle with the knowledge that
laboratory manufacturers would be
expected to comply with premarket
review requirements. (Although a trade
association representing laboratories
previously has participated in MDUFA
negotiations, the prior negotiations have
not incorporated similar expectations
regarding laboratory compliance with
premarket requirements.) Thus, we
propose that this amount of time is
appropriate to foster stability and
consistency in the marketplace for the
current MDUFA cycle, and would take
into account the need for adequate FDA
resources to implement the phaseout
policy in a manner that does not
compromise the capacity to achieve
MDUFA V performance expectations.
FDA anticipates that during this 31⁄2year period, laboratories would work
with FDA to determine whether PMAs
should be submitted for their IVDs.
Under FDA’s proposed policy, FDA
generally would not intend to enforce
against IVDs offered as LDTs after a
PMA has been submitted (within the
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31⁄2-year timeframe) until FDA
completes its review of the application.
Given that such IVDs may already be on
the market and available to patients,
FDA generally does not intend to
interrupt access at the point when a
submission is made.
Finally, FDA recognizes that the 2017
Discussion Paper described a possible
premarket-review approach specific to
LDTs for unmet needs. FDA has not
included such an approach in this
proposed policy because we anticipate
that the 31⁄2-year timeframe should be
sufficient for laboratories to meet
premarket review requirements for each
of their marketed IVDs, as applicable,
including IVDs for unmet needs. FDA
also anticipates that programs currently
in place may facilitate the development
and premarket authorization of IVDs for
unmet needs. These programs include
the Humanitarian Use Devices (HUD)/
Humanitarian Device Exemption (HDE)
program,18 which, among other things,
provides an exemption from the
requirement to establish a reasonable
assurance of effectiveness for devices
intended for use in the treatment or
diagnosis of rare diseases or conditions
(21 U.S.C. 360j(m); 21 CFR part 814,
subpart H), and the Breakthrough
Devices program, which is intended to
help expedite the development and
review of certain devices that provide
for more effective treatment or diagnosis
of life-threatening or irreversibly
debilitating diseases or conditions (21
U.S.C. 360e–3).
5. Stage 5: End the general enforcement
discretion approach with respect to
premarket review requirements for moderate
risk and low risk IVDs (that require
premarket submissions) 4 years after FDA
publishes a final phaseout policy, but not
before April 1, 2028.
FDA is proposing to end the general
enforcement discretion approach with
respect to premarket review
requirements for moderate risk IVDs
offered as LDTs (IVDs that may be
eligible for classification into class II)
and low risk IVDs offered as LDTs (IVDs
that may be eligible for classification
into class I) that require a premarket
submission 4 years after FDA publishes
the final phaseout policy. These
premarket submissions include 510(k)
submissions, the requirements for
which are set forth at 21 U.S.C. 360(k),
18 Under the proposed phaseout policy,
laboratories that intend to submit an HDE
application should do so within the same 31⁄2-year
timeframe provided for submission of PMAs. As in
the case of PMAs, under FDA’s proposed policy,
FDA generally would not intend to enforce against
IVDs after an HDE application has been submitted
(within the 31⁄2-year timeframe) until FDA
completes its review of the application.
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360c(i), and part 807, subpart E. These
submissions also include De Novo
requests, which laboratories may submit
for IVDs offered as LDTs for which there
is no legally marketed device upon
which to base a determination of
substantial equivalence, and for which
the laboratory seeks classification into
class I or class II. These requirements
are set forth at 21 U.S.C. 360c(f)(2) and
21 CFR part 860, subpart D.
FDA intends this stage to begin no
earlier than April 1, 2028. FDA’s
reasons for proposing this time period to
phase out the general enforcement
discretion approach with respect to
premarket review requirements for
moderate risk and low risk IVDs offered
as LDTs are similar to those for the
‘‘stage 4’’ time period, except that FDA
has lengthened the time period by 6
months in order to prioritize the review
of applications for high-risk IVDs
offered as LDTs (subject to premarket
approval requirements), so that FDA can
focus first on IVDs for which the
consequences of a false result are most
significant. FDA also recognizes that a
greater number of IVDs are subject to the
510(k) requirements, as compared with
premarket approval requirements, so a
longer period of time for laboratories to
come into compliance with these
requirements may be appropriate,
particularly for laboratories with large
test menus.
FDA generally would not intend to
enforce against IVDs offered as LDTs
after a 510(k) or De Novo request has
been submitted (within the 4-year
timeframe) until FDA completes its
review of the submission.
FDA also anticipates that laboratories
may seek to utilize FDA’s Third Party
review program. FDA currently operates
a Third Party review program for
medical devices, and multiple
organizations are accredited to conduct
reviews of 510(k) submissions for
certain IVDs (see Ref. 77). We anticipate
interest in the Third Party review
program among test manufacturers, as
well as potential new Third Party
review organizations. In particular, FDA
is aware of certain CLIA accreditation
organizations that may be interested in
potentially becoming Third Party
reviewers under FDA’s program, and to
the extent laboratories are already
familiar with these organizations,
laboratories may be inclined to use the
Third Party review program. In
addition, under the MDUFA V
agreement, FDA is currently working to
enhance the Third Party review
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program, which may make it more
attractive to manufacturers including
laboratories.
VII. Proposed Effective Date
The Agency proposes that any final
rule based on this proposed rule will
become effective 60 days after the date
of publication of the final rule in the
Federal Register.
VIII. Preliminary Economic Analysis of
Impacts
We have examined the impacts of the
proposed rule under Executive Order
12866, Executive Order 13563,
Executive Order 14094, the Regulatory
Flexibility Act (5 U.S.C. 601–612), and
the Unfunded Mandates Reform Act of
1995 (Pub. L. 104–4).
Executive Orders 12866, 13563, and
14094 direct us to assess all benefits,
costs, and transfers of available
regulatory alternatives and to select
regulatory approaches that maximize
net benefits (including potential
economic, environmental, public health
and safety, and other advantages;
distributive impacts; and equity). Rules
are ‘‘significant’’ under Executive Order
12866 Section 3(f)(1) (as amended by
Executive Order 14094) if they ‘‘have an
annual effect on the economy of $200
million or more (adjusted every 3 years
by the Administrator of [the Office of
Information and Regulatory Affairs
(OIRA)] for changes in gross domestic
product); or adversely affect in a
material way the economy, a sector of
the economy, productivity, competition,
jobs, the environment, public health or
safety, or State, local, territorial, or tribal
governments or communities.’’ OIRA
has determined that this proposed rule
is a significant regulatory action under
Executive Order 12866 Section 3(f)(1).
The Regulatory Flexibility Act
requires Agencies to analyze regulatory
options that would minimize any
significant impact of a rule on small
entities. Because most facilities that will
be affected by this rule are defined as
small businesses and the proposed rule
is likely to impose a substantial burden
on the affected small entities, we find
that the proposed rule will have a
significant economic impact on a
substantial number of small entities.
We prepared an analysis consistent
with the Unfunded Mandates Reform
Act of 1995 (section 202(a)), which
requires us to prepare a written
statement that includes estimates of
anticipated impacts, before proposing
‘‘any rule that includes any Federal
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68027
mandate that may result in the
expenditure by State, local, and tribal
governments, in the aggregate, or by the
private sector, of $100,000,000 or more
(adjusted annually for inflation) in any
one year.’’ The current threshold after
adjustment for inflation is $177 million,
using the most current (2022) Implicit
Price Deflator for the Gross Domestic
Product. This proposed rule would
result in an expenditure in at least one
year that meets or exceeds this amount.
This proposed rule, if finalized,
would amend FDA’s regulations to
make explicit that IVDs are devices
under the FD&C Act including when the
manufacturer of the IVD is a laboratory.
As discussed in section VI, FDA intends
to phase out its general enforcement
discretion approach for LDTs so that
IVDs manufactured by a laboratory
would generally fall under the same
enforcement approach as other IVDs.
We anticipate that the benefits of
phasing out FDA’s general enforcement
discretion approach for LDTs would
include a reduction in healthcare costs
associated with unsafe or ineffective
tests, including tests promoted with
false or misleading claims, and from
therapeutic decisions based on the
results of those tests. Quantified benefits
are the annualized sum of both health
and non-health benefits. Unquantified
benefits would include the reduction in
costs from lawsuits and reduction in
costs to healthcare systems.
Table 1 summarizes the annualized
benefits, costs, and transfers of the
proposed rule. At a 7 percent discount
rate, 20-year annualized benefits range
from $2.67 billion to $86.01 billion,
with a primary estimate of $31.41
billion per year. At a 3 percent discount
rate, 20-year annualized benefits range
from $1.81 billion to $61.41 billion,
with a primary estimate of $22.33
billion per year. At a 7 percent discount
rate, 20-year annualized costs range
from about $2.52 billion to $19.45
billion, with a primary estimate of $5.87
billion per year. At a 3 percent discount
rate, annualized costs range from about
$2.39 billion to $18.55 billion, with a
primary estimate of $5.60 billion per
year. At a 7 percent discount rate, 20year annualized transfers range from
$100 million to $452 million, with a
primary estimate of $226 million per
year. At a 3 percent discount rate, 20year annualized transfers range from
$121 million to $538 million, with a
primary estimate of $269 million per
year.
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TABLE 1—SUMMARY OF BENEFITS, COSTS AND TRANSFERS OF THE PROPOSED RULE
[Millions of 2022 U.S. dollars]
Units
Category
Primary
estimate
Low
estimate
High
estimate
Benefits:
Annualized Monetized
($m/year).
Annualized Quantified ..
$31,408
22,332
..................
$2,670
1,810
..................
$86,013
61,413
..................
2022
2022
..................
7
3
7
3
20
20
5,874
5,598
2,522
2,394
19,452
18,549
2022
2022
7
3
20
20
..................
..................
..................
..................
7
3
226
269
100
121
452
538
2022
2022
7
3
Year
dollars
Discount
rate
(%)
Period
covered
(years)
Notes
Qualitative .....................
Costs:
Annualized Monetized
($m/year).
Annualized Quantified ..
A portion of foreign costs could be passed on to domestic consumers. We estimate that up to $30.73
million in annualized costs (7%, 20 years) to foreign facilities could be passed on to domestic consumers.
Qualitative .....................
Transfers:
Federal Annualized
Monetized ($m/year).
From: Device Industry
Other Annualized Monetized ($m/year).
..................
..................
20
20
To: FDA
..................
From:
..................
7
3
To:
Effects:
State, Local, or Tribal Government:
Small Business: The proposed rule is likely to have a significant economic impact on a substantial number of small laboratories that manufacture IVDs offered
as LDTs.
Wages:
Growth:
We have developed a comprehensive
Preliminary Economic Analysis of
Impacts that assesses the impacts of the
proposed rule. The full preliminary
analysis of economic impacts is
available in the docket for this proposed
rule (Ref. 34) and at https://
www.fda.gov/about-fda/economicsstaff/regulatory-impact-analyses-ria.
IX. Analysis of Environmental Impact
We have determined under 21 CFR
25.30(h) that this action is of a type that
does not individually or cumulatively
have a significant effect on the human
environment. Therefore, neither an
environmental assessment nor an
environmental impact statement is
required.
ddrumheller on DSK120RN23PROD with PROPOSALS1
X. Paperwork Reduction Act of 1995
FDA tentatively concludes that this
proposed rule contains no new
collections of information. However,
FDA does assume that there will need
to be corresponding adjustments to the
burden estimates for relevant approved
collections of information before the
relevant phaseout stage begins and any
such collection of information would
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not be as a result of the implementation
of the proposed rule. FDA tentatively
concludes that the following
information collections will need
adjustment before the relevant phaseout
stage begins: Office of Management and
Budget (OMB) control number 0910–
0437, Medical Device Reporting; OMB
control number 0910–0359, Corrections
and Removals; OMB control number
0910–0625, Device Registration and
Listing; OMB control number 0910–
0485, Labeling; OMB control number
0910–0078, Investigational Device
Exemption; OMB control number 0910–
0073, Quality Systems; OMB control
number 0910–0231, Premarket
Approval; OMB control number 0910–
0332, Humanitarian Device Exemption;
OMB control number 0910–0756, QSubmissions; OMB control number
0910–0120, Premarket Notification; and
OMB control number 0910–0844 De
Novo. Such adjustments will be
submitted for review and clearance by
OMB under the Paperwork Reduction
Act of 1995 (PRA) (44 U.S.C. 3501–
3521).
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XI. Federalism
We have analyzed this proposed rule
in accordance with the principles set
forth in Executive Order 13132. We
have determined that this proposed rule
does not contain policies that have
substantial direct effects on the States,
on the relationship between the
National Government and the States, or
on the distribution of power and
responsibilities among the various
levels of government. Accordingly, we
conclude that the rule does not contain
policies that have federalism
implications as defined in the Executive
order and, consequently, a federalism
summary impact statement is not
required. Through publication of this
proposed rule, we are providing notice
and an opportunity for State and local
officials to comment on this rulemaking.
XII. Consultation and Coordination
With Indian Tribal Governments
We have analyzed this proposed rule
in accordance with the principles set
forth in Executive Order 13175. We
have tentatively determined that the
rule does not contain policies that
would have a substantial direct effect on
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one or more Indian Tribes, on the
relationship between the Federal
Government and Indian Tribes, or on
the distribution of power and
responsibilities between the Federal
Government and Indian Tribes. The
Agency solicits comments from tribal
officials on any potential impact on
Indian Tribes from this proposed action.
XIII. Other Issues for Consideration
FDA anticipates that this proposed
rule, if finalized, may require
conforming amendments to other FDA
regulations, including provisions
regarding IVD labeling and ASRs in part
809. FDA intends to consider and
propose conforming amendments,
where appropriate, at a future date.
In addition, we note that various bills
have been introduced in Congress that
would change the legal status of IVDs as
devices (under these bills, IVDs would
generally be regulated as ‘‘in vitro
clinical tests’’ and would be subject to
new statutory authorities).19 We
recognize that the enactment of such
legislation would directly impact this
rule, given that it is being proposed
under the statutory device authorities
and other authorities under the FD&C
Act.
ddrumheller on DSK120RN23PROD with PROPOSALS1
XIV. References
The following references marked with
an asterisk (*) are on display at the
Dockets Management Staff (see
ADDRESSES) and are available for
viewing by interested persons between
9 a.m. and 4 p.m., Monday through
Friday; they also are available
electronically at https://
www.regulations.gov. References
without asterisks are not on public
display at https://www.regulations.gov
because they have copyright restriction.
Some may be available at the website
address, if listed. References without
asterisks are available for viewing only
at the Dockets Management Staff. FDA
has verified the website addresses, as of
the date this document publishes in the
Federal Register, but websites are
subject to change over time.
1. Grand View Research, ‘‘Laboratory
Developed Tests Market Size, Share & Trends
Analysis Report By Technology
(Immunoassay, Molecular Diagnostics), By
Application (Oncology, Nutritional &
Metabolic Disease), By Region, and Segment
Forecasts, 2023–2030: Report Summary,’’
available at https://
www.grandviewresearch.com/industry19 See, e.g. H.R.4128—117th Congress (2021–
2022): VALID Act of 2021, H.R.4128, 117th Cong.
(2021), https://www.congress.gov/bill/117thcongress/house-bill/4128/text; S.2209—117th
Congress (2021–2022): VALID Act of 2021, S.2209,
117th Cong. (2021), https://www.congress.gov/bill/
117th-congress/senate-bill/2209.
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analysis/laboratory-developed-tests-marketreport (last accessed on April 28, 2023).
2. The Pew Charitable Trusts, ‘‘The Role of
Lab-Developed Tests in the In Vitro
Diagnostics Market,’’ October 2021. Available
at https://www.pewtrusts.org/en/researchand-analysis/reports/2021/10/the-role-of-labdeveloped-tests-in-the-in-vitro-diagnosticsmarket.
* 3. Congressional Research Service, ‘‘FDA
Regulation of Laboratory-Developed Tests
(LDTs),’’ December 7, 2022. Available at
https://crsreports.congress.gov/product/pdf/
IF/IF11389.
* 4. Warning Letter to deCODE Genetics re:
deCODEme Complete Scan (June 10, 2010).
Available at https://www.fda.gov/media/
79216/download.
* 5. Warning Letter to 23andMe, Inc. re:
23andMe Personal Genome Service (June 10,
2010). Available at https://web.archive.org/
web/20191214010336/https:/www.fda.gov/
media/79205/download.
6. ThermoFisher Scientific, ‘‘Demystify
Molecular Test Development and
Implementation: How Do Labs Implement
Molecular Tests To Meet Complex Clinical
Needs?’’ Available at https://
www.thermofisher.com/us/en/home/clinical/
clinical-genomics/molecular-diagnostics/
molecular-diagnostic-education.html (last
accessed on March 28, 2023).
7. Lighthouse Lab Services, ‘‘Industry
Insights: Paths To Consider When
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(last accessed on March 31, 2023).
* 8. Centers for Disease Control and
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www.fda.gov/MedicalDevices/Safety/
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www.fda.gov/Safety/MedWatch/
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(IVDs) Offered as Laboratory Developed Tests
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35. Gerhard, G.S., S.G. Fisher, and A.M.
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journals/jamacardiology/fullarticle/2673291.
36. Martin, A.R., M. Kanai, Y. Kamatani, et
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37. Wang, Y., K. Tsuo, M. Kanai, et al.,
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Developing More Generalizable Polygenic
Risk Scores,’’ Annual Review of Biomedical
Data Science, 5:293–320. Available at https://
doi.org/10.1146%2Fannurev-biodatasci111721-074830.
38. Duncan L., H. Shen, B. Gelaye, et al.,
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Performance in Diverse Human Populations,’’
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39. Hoskins, K.F., O.C. Danciu, N.Y. Ko, et
al., ‘‘Association of Race/Ethnicity and the
21-Gene Recurrence Score With Breast
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* 40. CMS, ‘‘Laboratory Developed Tests
(LDTs) Frequently Asked Questions,’’
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2023).
* 41. Teutsch, S. and R. Tuckson, ‘‘U.S.
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Health, and Society,’’ 2008. Available at
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report.pdf?sequence=l&isAllowed=y.
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43. Advanced Medical Technology
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* 44. Letter from D. Bruce Burlington, M.D.,
Director, FDA/CDRH, to Jeffrey N. Gibbs,
Esq., Hyman, Phelps & McNamara, P.C.,
Docket No. 92P–0405 (August 12, 1998).
Available at https://www.regulations.gov/
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* 46. Letter from Leslie Kux, Assistant
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(July 31, 2014). Available at https://
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* 47. Warning Letter to Inova Genomics
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(LDTs); Draft Guidance for Industry, Food
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Laboratories,’’ October 3, 2014. Available at
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* 49. FDA, ‘‘FDA Notification and Medical
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Clinical Laboratories,’’ October 3, 2014.
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89837/download.
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13, 2017. Available at https://www.fda.gov/
media/102367/download.
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Address the Public Health Emergency;
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161443/download.
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Disease-2019 Tests (Revised); Guidance for
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to Texas Children’s Hospital and Houston
Methodist Hospital re: Zika Direct Test
(March 4, 2016). Available at https://
public4.pagefreezer.com/browse/FDA/22-022023T10:21/https://www.fda.gov/media/
96740/download.
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Medical Devices,’’ January 27, 2023, available
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accessed on March 9, 2023).
* 55. Untitled Letter to Navigenics Corp.
(June 10, 2010). Available at https://
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79235/download.
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accessed on April 12, 2023).
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Other Informal Issuances,’’ August 19, 2020.
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Xavier Becerra on Withdrawal of HHS Policy
on Laboratory-Developed Tests,’’ November
15, 2021.
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Oversight,’’ Politico, October 2, 2020.
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62. Kaplan, S., ‘‘Trump Administration
Says Some Coronavirus Tests Can Bypass
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63. Baumann, J., ‘‘Virus Testing Push
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64. Howard, J., ‘‘HHS Withdraws Trump
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* 69. ‘‘It Has Come to Our Attention’’ Letter
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media/94365/download.
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media/93493/download.
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UCM249858.pdf.
76. Bradley, P.L., J.S. Dickey, J.D. Levin, et
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* 77. FDA, ‘‘510(k) Third Party Review
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premarket-submissions-selecting-andpreparing-correct-submission/510k-thirdparty-reviewprogram(lastaccessedonSeptember22,2023).
List of Subjects in 21 CFR Part 809
Labeling, Medical devices.
Therefore, under the Federal Food,
Drug, and Cosmetic Act and under
authority delegated to the Commissioner
of Food and Drugs, FDA proposes to
amend 21 CFR part 809 as follows:
PART 809—IN VITRO DIAGNOSTIC
PRODUCTS FOR HUMAN USE
1. The authority citation for part 809
is revised to read as follows:
■
Authority: 21 U.S.C. 321(h)(1), 331, 351,
352, 360, 360c, 360d, 360e, 360h, 360i, 360j,
371, 372, 374, 381.
2. In § 809.3, revise the last sentence
of paragraph (a) to read as follows:
■
§ 809.3
Definitions.
(a) * * * These products are devices
as defined in section 201(h)(1) of the
Federal Food, Drug, and Cosmetic Act
(the act) and may also be biological
products subject to section 351 of the
Public Health Service Act, including
when the manufacturer of these
products is a laboratory.
*
*
*
*
*
Dated: September 27, 2023.
Robert M. Califf,
Commissioner of Food and Drugs.
[FR Doc. 2023–21662 Filed 9–29–23; 8:45 am]
BILLING CODE 4164–01–P
PO 00000
68031
DEPARTMENT OF HOMELAND
SECURITY
Coast Guard
33 CFR Part 117
[Docket No. USCG–2023–0530]
RIN 1625–AA09
Drawbridge Operation Regulation;
Long Creek, Nassau County, NY
Coast Guard, Department of
Homeland Security (DHS).
ACTION: Notice of proposed rulemaking.
AGENCY:
The Coast Guard proposes to
temporarily modify the operating
schedule that governs the Loop Parkway
Bridge across Long Creek, mile 0.7,
Nassau County, NY. The bridge owner,
New York State Department of
Transportation (NYSDOT), submitted a
request to operate the bridge under
single leaf openings to perform bridge
deck replacement. We invite your
comments on this proposed rulemaking.
DATES: Comments and related material
must reach the Coast Guard on or before
November 2, 2023.
ADDRESSES: You may submit comments
identified by docket number USCG–
2023–0530 using Federal Decision
Making Portal at https://
www.regulations.gov.
See the ‘‘Public Participation and
Request for Comments’’ portion of the
SUPPLEMENTARY INFORMATION section
below for instructions on submitting
comments.
SUMMARY:
If
you have questions on this proposed
rule, call or email Ms. Stephanie E.
Lopez, First Coast Guard District,
Project Officer, telephone 212–514–
4335, email Stephanie.E.Lopez@
uscg.mil.
FOR FURTHER INFORMATION CONTACT:
SUPPLEMENTARY INFORMATION:
I. Table of Abbreviations
CFR Code of Federal Regulations
DHS Department of Homeland Security
FR Federal Register
OMB Office of Management and Budget
NPRM Notice of proposed rulemaking
(advance, supplemental)
§ Section
U.S.C. United States Code
NYSDOT New York State Department of
Transportation
II. Background, Purpose, and Legal
Basis
The Loop Parkway Bridge across Long
Creek, mile 0.7, Nassau County, NY, has
a vertical clearance of 21 feet at mean
high water and a horizontal clearance of
75.5 feet at mean high water. Waterway
Frm 00045
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]]>Agencies
[Federal Register Volume 88, Number 190 (Tuesday, October 3, 2023)]
[Proposed Rules]
[Pages 68006-68031]
From the Federal Register Online via the Government Publishing Office [www.gpo.gov]
[FR Doc No: 2023-21662]
=======================================================================
-----------------------------------------------------------------------
DEPARTMENT OF HEALTH AND HUMAN SERVICES
Food and Drug Administration
21 CFR Part 809
[Docket No. FDA-2023-N-2177]
RIN 0910-AI85
Medical Devices; Laboratory Developed Tests
AGENCY: Food and Drug Administration, HHS.
ACTION: Proposed rule.
-----------------------------------------------------------------------
SUMMARY: The Food and Drug Administration (FDA, the Agency, or we) is
proposing to amend its regulations to make explicit that in vitro
diagnostic products (IVDs) are devices under the Federal Food, Drug,
and Cosmetic Act (FD&C Act) including when the manufacturer of the IVD
is a laboratory. In conjunction with this amendment, FDA is proposing a
policy under which FDA intends to phase out its general enforcement
discretion approach for laboratory developed tests
[[Page 68007]]
(LDTs) so that IVDs manufactured by a laboratory would generally fall
under the same enforcement approach as other IVDs. FDA is proposing
this phaseout to better protect the public health by helping to assure
the safety and effectiveness of LDTs. If finalized, this phaseout may
also foster the manufacturing of innovative IVDs for which FDA has
determined there is a reasonable assurance of safety and effectiveness.
DATES: Either electronic or written comments on the proposed rule must
be submitted by December 4, 2023.
ADDRESSES: You may submit comments as follows. Please note that late,
untimely filed comments will not be considered. The https://www.regulations.gov electronic filing system will accept comments until
11:59 p.m. Eastern Time at the end of December 4, 2023. Comments
received by mail/hand delivery/courier (for written/paper submissions)
will be considered timely if they are received on or before that date.
Electronic Submissions
Submit electronic comments in the following way:
Federal eRulemaking Portal: https://www.regulations.gov.
Follow the instructions for submitting comments. Comments submitted
electronically, including attachments, to https://www.regulations.gov
will be posted to the docket unchanged. Because your comment will be
made public, you are solely responsible for ensuring that your comment
does not include any confidential information that you or a third party
may not wish to be posted, such as medical information, your or anyone
else's Social Security number, or confidential business information,
such as a manufacturing process. Please note that if you include your
name, contact information, or other information that identifies you in
the body of your comments, that information will be posted on https://www.regulations.gov.
If you want to submit a comment with confidential
information that you do not wish to be made available to the public,
submit the comment as a written/paper submission and in the manner
detailed (see ``Written/Paper Submissions'' and ``Instructions'').
Written/Paper Submissions
Submit written/paper submissions as follows:
Mail/Hand Delivery/Courier (for written/paper
submissions): Dockets Management Staff (HFA-305), Food and Drug
Administration, 5630 Fishers Lane, Rm. 1061, Rockville, MD 20852.
For written/paper comments submitted to the Dockets
Management Staff, FDA will post your comment, as well as any
attachments, except for information submitted, marked and identified,
as confidential, if submitted as detailed in ``Instructions.''
Instructions: All submissions received must include the Docket No.
FDA-2023-N-2177 for ``Medical Devices; Laboratory Developed Tests.''
Received comments, those filed in a timely manner (see ADDRESSES), will
be placed in the docket and, except for those submitted as
``Confidential Submissions,'' publicly viewable at https://www.regulations.gov or at the Dockets Management Staff between 9 a.m.
and 4 p.m., Monday through Friday, 240-402-7500.
Confidential Submissions--To submit a comment with
confidential information that you do not wish to be made publicly
available, submit your comments only as a written/paper submission. You
should submit two copies total. One copy will include the information
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``THIS DOCUMENT CONTAINS CONFIDENTIAL INFORMATION.'' The Agency will
review this copy, including the claimed confidential information, in
its consideration of comments. The second copy, which will have the
claimed confidential information redacted/blacked out, will be
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Submit both copies to the Dockets Management Staff. If you do not wish
your name and contact information to be made publicly available, you
can provide this information on the cover sheet and not in the body of
your comments and you must identify this information as
``confidential.'' Any information marked as ``confidential'' will not
be disclosed except in accordance with 21 CFR 10.20 and other
applicable disclosure law. For more information about FDA's posting of
comments to public dockets, see 80 FR 56469, September 18, 2015, or
access the information at: https://www.govinfo.gov/content/pkg/FR-2015-09-18/pdf/2015-23389.pdf.
Docket: For access to the docket to read background documents or
the electronic and written/paper comments received, go to https://www.regulations.gov and insert the docket number, found in brackets in
the heading of this document, into the ``Search'' box and follow the
prompts and/or go to the Dockets Management Staff, 5630 Fishers Lane,
Rm. 1061, Rockville, MD 20852, 240-402-7500.
FOR FURTHER INFORMATION CONTACT: Toby Lowe, Center for Devices and
Radiological Health, Food and Drug Administration, 10903 New Hampshire
Ave., Silver Spring, MD 20993, 301-796-6512,
[email protected].
SUPPLEMENTARY INFORMATION:
Table of Contents
I. Executive Summary
A. Purpose of the Proposed Rule
B. Summary of the Major Provisions of the Proposed Rule
C. Legal Authority
D. Costs and Benefits
II. Table of Abbreviations/Commonly Used Acronyms in This Document
III. Background
A. Introduction
B. Need for the Rule
C. FDA's Current Regulatory Framework
D. History of the Rulemaking
IV. Legal Authority
V. Description of the Proposed Amendment to the Definition of In
Vitro Diagnostic Products
A. Proposed Amendment
B. Legal Basis for the Proposed Amendment
VI. Description of the Proposed Enforcement Policy
A. Scope
B. Stages
VII. Proposed Effective Date
VIII. Preliminary Economic Analysis of Impacts
IX. Analysis of Environmental Impact
X. Paperwork Reduction Act of 1995
XI. Federalism
XII. Consultation and Coordination With Indian Tribal Governments
XIII. Other Issues for Consideration
XIV. References
I. Executive Summary
A. Purpose of the Proposed Rule
FDA is proposing to amend its regulations to make explicit that
IVDs are devices under the FD&C Act including when the manufacturer of
the IVD is a laboratory. This amendment would reflect that the device
definition in the FD&C Act does not differentiate between entities
manufacturing the device, and would provide further clarity, including
for stakeholders affected by the accompanying changes to FDA's general
enforcement discretion approach for LDTs. In connection with amending
the regulation, FDA intends to phase out its general enforcement
discretion approach for LDTs so that IVDs manufactured by a laboratory
would generally fall under the same enforcement approach as other IVDs.
For purposes of this document, we use ``manufacture'' and related terms
as a shorthand for the various activities that constitute manufacturing
as described in FDA regulations (e.g., design,
[[Page 68008]]
preparation, propagation, assembly, and processing).
In 1976, the Medical Device Amendments of 1976 (the MDA) amended
the FD&C Act to create a comprehensive system for the regulation of
devices intended for human use. In implementing the MDA, FDA has
generally exercised enforcement discretion such that it generally has
not enforced applicable requirements with respect to most LDTs.
Enforcement discretion for LDTs developed as a matter of general
practice. However, the risks associated with LDTs are much greater
today than they were at the time of enactment of the MDA. As discussed
more fully in section III.B, today's LDTs are generally, among other
things, used more widely, by a more diverse population, with an
increasing reliance on high-tech instrumentation and software, and more
frequently for the purpose of guiding critical healthcare decisions. In
this regard, today's LDTs are similar to other IVDs that have not been
under this general enforcement discretion approach. Given these
changes, and for the additional reasons discussed in section III.B,
phasing out the general enforcement discretion approach for LDTs is
important to protect the public health. The phaseout of FDA's general
enforcement discretion approach for LDTs is intended to help assure the
safety and effectiveness of LDTs, and may also foster the manufacturing
of innovative IVDs for which FDA has determined there is a reasonable
assurance of safety and effectiveness.
B. Summary of the Major Provisions of the Proposed Rule
This rulemaking would amend the definition of ``in vitro diagnostic
products'' in FDA regulations to state that IVDs are devices under the
FD&C Act ``including when the manufacturer of these products is a
laboratory.'' In conjunction with this amendment, FDA is also proposing
a policy under which FDA intends to phase out its general enforcement
discretion approach for LDTs so that IVDs manufactured by a laboratory
would generally fall under the same enforcement approach as other IVDs.
Additional details regarding the proposed phaseout policy are discussed
further in section VI.
C. Legal Authority
FDA is proposing to issue this rule under the Agency's general
rulemaking authorities and statutory authorities relating to devices.
These authorities include sections 201(h)(1), 301, 501, 502, 510, 513,
514, 515, 518, 519, 520, 701, 702, 704, and 801 of the FD&C Act (21
U.S.C. 321(h)(1), 331, 351, 352, 360, 360c, 360d, 360e, 360h, 360i,
360j, 371, 372, 374, and 381).
D. Costs and Benefits
We quantify benefits to patients from averted health losses due to
problematic IVDs offered as LDTs.\1\ Due to limitations in the data, we
quantify health benefits only with respect to IVDs for certain diseases
and conditions; however, we would expect additional health benefits
associated with averted health losses for other diseases and
conditions. We estimate that the annualized benefits over 20 years
would range from $2.67 billion to $86.01 billion at a 7 percent
discount rate, with a primary estimate of $31.41 billion, and from
$1.81 billion to $61.41 billion at a 3 percent discount rate, with a
primary estimate of $22.33 billion. Additional benefits would include
averted non-health losses from the quantified reduction in costs of
problematic IVDs offered as LDTs and unquantified reduction in costs
from lawsuits and costs to healthcare systems. We quantify costs to
affected laboratories for complying with applicable statutory and
regulatory requirements. Additional costs would include some costs to
FDA, which we include in our estimates. The annualized costs would
range from $2.52 billion to $19.45 billion at a 7 percent discount
rate, with a primary estimate of $5.87 billion, and from $2.39 billion
to $18.55 billion at a 3 percent discount rate, with a primary estimate
of $5.60 billion. The annualized transfers \2\ would range from $100
million to $452 million at a 7 percent discount rate, with a primary
estimate of $226 million, and from $121 million to $538 million at a 3
percent discount rate, with a primary estimate of $269 million. The
annualized costs to FDA would range from $265 million to $1.06 billion
at a 7 percent discount rate, with a primary estimate of $530 million,
and from $251 million to $1.00 billion at a 3 percent discount rate,
with a primary estimate of $501 million. These estimates do not include
anticipated offsets from user fees. Factoring in offsets from user fees
at current levels, estimated costs to FDA are reduced to $165 million
to $607 million at a 7 percent discount rate, with a primary estimate
of $304 million, and to $103 million to $465 million at a 7 percent
discount rate, with a primary estimate of $233 million, covering
approximately half of the estimated costs to FDA.
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\1\ See discussion of ``IVDs offered as LDTs'' in section VI.A
below.
\2\ This proposed rule would result in compliance costs for
laboratories that are ensuring their IVDs offered as LDTs are
compliant with applicable statutory and regulatory requirements.
These costs overlap somewhat with effects associated with this rule
in the form of user fees including annual registration fees, fees
for premarket submissions, and annual fees for periodic PMA
reporting, which are paid from laboratories to FDA. These fees are
paid by laboratories but are considered revenue for FDA. The
approach to estimating fee effects is distinct from the approaches
for either benefits or costs, so they will be presented as
transfers.
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II. Table of Abbreviations/Commonly Used Acronyms in This Document
------------------------------------------------------------------------
Abbreviation/acronym What it means
------------------------------------------------------------------------
510(k)....................... Premarket Notification.
AMC.......................... Academic Medical Center.
ASR.......................... Analyte Specific Reagent.
CFR.......................... Code of Federal Regulations.
CGMP......................... Current Good Manufacturing Practice.
CLIA......................... Clinical Laboratory Improvement
Amendments of 1988.
CMS.......................... Centers for Medicare & Medicaid Services.
EUA.......................... Emergency Use Authorization.
FDA.......................... Food and Drug Administration.
FD&C Act..................... Federal Food, Drug, and Cosmetic Act.
HCT/Ps....................... Human Cells, Tissues, and Cellular and
Tissue-Based Products.
HLA.......................... Human Leukocyte Antigen.
IDE.......................... Investigational Device Exemption.
IVD.......................... In Vitro Diagnostic Product.
IVDMIA....................... In Vitro Diagnostic Multivariate Index
Assay.
LDT.......................... Laboratory Developed Test.
[[Page 68009]]
MDA.......................... Medical Device Amendments of 1976.
MDR.......................... Medical Device Report.
MDUFA........................ Medical Device User Fee Amendments.
NIPS......................... Non-Invasive Prenatal Screening.
PMA.......................... Premarket Approval Application.
QS........................... Quality System.
------------------------------------------------------------------------
III. Background
A. Introduction
FDA's regulations define IVDs as reagents, instruments, and systems
intended for use in the diagnosis of disease or other conditions,
including a determination of the state of health, in order to cure,
mitigate, treat, or prevent disease or its sequelae, and intended for
use in the collection, preparation, and examination of specimens taken
from the human body. IVDs include test systems (also referred to in
this preamble as ``tests'') that are performed on samples taken from
the human body, such as blood or tissue, for the purpose of detecting
diseases or other conditions, monitoring a person's overall health,
identifying patients who are likely to benefit from specific therapies,
or otherwise helping to diagnose, cure, mitigate, treat, or prevent
disease or its sequelae. Some IVDs are manufactured by conventional
manufacturers for use by other entities such as laboratories,
healthcare providers, or, in some cases, patients. Such IVDs may
include ``test kits,'' containing packaged sets of components that are
part of or comprise a test system. Other IVDs are manufactured by
laboratories for use by the same or other laboratories. Such IVDs
include LDTs. FDA has generally considered an LDT to be an IVD that is
intended for clinical use and that is designed, manufactured, and used
within a single laboratory that is certified under the Clinical
Laboratory Improvement Amendments of 1988 (CLIA) and meets the
regulatory requirements under CLIA to perform high complexity testing.
Section V.B sets forth the legal reasoning for FDA's position that IVDs
manufactured by laboratories, including LDTs, are devices.
However, in implementing the MDA, FDA generally has exercised
enforcement discretion such that it generally has not enforced
applicable requirements with respect to most LDTs. At the time of
passage of the MDA, LDTs were mostly manufactured in small volumes by
laboratories that served their local communities. They were typically
intended for use in diagnosing rare diseases or for other uses to meet
the needs of a local patient population, or were generally similar to
well-characterized, standard tests. They also tended to employ manual
techniques (and did not use automation) performed by laboratory
personnel with specialized expertise; to be used and interpreted by
physicians or pathologists in a single institution responsible for the
patient (and who were actively involved in patient care); and to be
manufactured using components legally marketed for clinical use, such
as general purpose reagents or immunohistochemical stains marketed in
compliance with FDA regulatory requirements. Due to these and other
factors, FDA generally exercised enforcement discretion such that it
generally has not enforced applicable requirements for most LDTs.\3\
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\3\ Although FDA's general enforcement discretion approach
continues today, it does not apply to LDTs in all contexts; for
example, it does not apply to, among other LDTs, those used for
declared emergencies/potential emergencies/material threats under
section 564 of the FD&C Act (21 U.S.C. 360bbb-3).
---------------------------------------------------------------------------
However, the LDT landscape has evolved significantly since 1976.
Today, many LDTs rely on high-tech or complex instrumentation and
software to generate results and clinical interpretations. They are
often used in laboratories outside of the patient's healthcare setting
and are often manufactured in high volume for large and diverse
populations. Many LDTs are manufactured by laboratory corporations that
market the tests nationwide, as they accept specimens from patients
across the country and run their LDTs in very large volumes in a single
laboratory. Today's LDTs are also more commonly manufactured with
instruments or other components not legally marketed for clinical use
and are more often used to inform or direct critical treatment
decisions, to widely screen for common diseases, to predict personal
risk of developing certain diseases, and to diagnose serious medical
conditions such as cancer and heart disease.\4\ The risks associated
with most modern LDTs are therefore much greater today than they were
at the time FDA began implementing the MDA, and most LDTs today are
similar to other IVDs that have not been under FDA's general
enforcement discretion approach. In addition, FDA is concerned that
firms are offering IVDs as ``LDTs'' even when they are not LDTs,
because they are not actually designed, manufactured, and used within a
single laboratory (see, e.g., Refs. 4 and 5).
---------------------------------------------------------------------------
\4\ See, e.g., Refs. 1 to 3. These observations are also
informed by FDA's own experience, including the review of
submissions and site visits, and staff with prior experience in the
laboratory industry developing and running LDTs.
---------------------------------------------------------------------------
As a result of this evolution in the testing landscape, FDA has
long recognized the need for a change in the Agency's general
enforcement discretion approach for LDTs. The history of FDA's efforts
with respect to LDTs is set forth in the ``History of the Rulemaking''
section below (section III.D). Over the past few years, FDA has
accumulated even more information supporting the need for a change, as
discussed below. In light of these developments, FDA is proposing to
amend FDA's regulations to make explicit that IVDs are devices under
the FD&C Act including when the manufacturer is a laboratory.\5\ FDA is
also proposing a policy under which FDA intends to phase out FDA's
general enforcement discretion approach for LDTs so that IVDs
manufactured by a laboratory would generally fall under the same
enforcement approach as other IVDs.
---------------------------------------------------------------------------
\5\ As discussed further in section V, FDA is also proposing to
amend the statutory citation for the device definition included in
Sec. 809.3 (21 CFR 809.3) to reflect that it is now codified at
section 201(h)(1) of the FD&C Act (21 U.S.C. 321(h)(1)).
---------------------------------------------------------------------------
B. Need for the Rule
FDA is proposing a policy under which FDA intends to phase out the
general enforcement discretion approach for LDTs because that approach
has led to an oversight scheme that does not best serve the public
health. LDTs that are under the general enforcement discretion approach
are treated differently from other IVDs. However, there is no longer a
sound basis for this distinction. In FDA's experience, including with
COVID-19 tests and IVDs that are offered as LDTs after FDA's approval
of a comparable companion diagnostic, many test systems made by
laboratories today are functionally the same as those made by other
manufacturers of IVDs. They
[[Page 68010]]
involve the same materials and technologies, are intended for the same
or similar purposes, are developed by and for individuals with similar
expertise, and are marketed to the same patients, sometimes on a
national scale. For these reasons, tests made by laboratories are often
used interchangeably by healthcare providers and patients with tests
made by other manufacturers. In fact, today, the testing industry has
come to view FDA's general enforcement discretion approach as an
alternative pathway to market for test systems, such that test systems
are often ``launched as LDTs'' with no assurance that they meet
requirements under the FD&C Act and its implementing regulations (see,
e.g., Refs. 6 and 7).\6\ These tests lack the characteristics and
institutional safeguards that originally justified FDA's general
enforcement discretion approach, as discussed above, and may directly
compete with FDA-authorized kit-based test systems. FDA views this
bifurcated system of oversight as untenable and inconsistent with FDA's
public health mission.
---------------------------------------------------------------------------
\6\ The references cited are examples of the described practice.
Their inclusion does not represent FDA support for or approval of
the activities described.
---------------------------------------------------------------------------
The proposed phaseout of FDA's general enforcement discretion
approach is designed to redress the imbalance in oversight and protect
the public health. Diagnostic testing is a cornerstone of modern
medicine; CDC estimates that 70 percent of medical decisions are based
on laboratory test results (Ref. 8). IVDs offered as LDTs are a growing
sector of that market (Ref. 1). Moreover, these tests are proliferating
in some of the most complicated and sensitive areas of medical
practice, where the presence of a valid test can be most important.
As the testing landscape has evolved, information about these tests
in the scientific literature, news articles, and anecdotal reports
submitted to the Agency, among other sources, has exposed evidence of
problems associated with these tests. This evidence is discussed in
more detail below. Particularly over the last few years, this evidence
has been growing and likely does not reflect the full scale of the
problems. (Until FDA systematically collects information on these
tests, such as adverse event reports, it will not be able to assess
more fully the extent of the risks to patients in the manner it does
for other devices.) Based on current safety signals, FDA is proposing
to phase out the general enforcement discretion approach to help assure
that patients are receiving accurate and reliable diagnostic test
results regardless of where the tests are made.
1. IVDs Offered as LDTs Have a Significant Impact on Modern Medical
Care
Today, IVDs offered as LDTs are ubiquitous, and are intended to
diagnose a broad range of diseases and conditions (see Ref. 2). In many
cases, these IVDs are meant for use in complex areas of medicine
involving life-threatening diseases, such as cancer, neurological
diseases, cardiovascular illness, infectious diseases, and rare
diseases. They can proliferate in areas where diagnosis is difficult,
and the healthcare community has few points of reference for
determining test validity. Sometimes, they use complex algorithms to
calculate ``scores'' for diagnosis with little transparency to the user
about the basis for these algorithms. Increasingly, these IVDs are
intended to inform drug treatment, directing physicians to choose
certain drugs based on a patient's genetic or other information. FDA
has witnessed an explosion in the volume, complexity, and scope of IVDs
offered as LDTs for use in determining cancer treatments,\7\ and as
discussed below, news coverage, including as recently as this year, has
drawn attention to the use of IVDs offered as LDTs for non-invasive
prenatal screening (NIPS), which evaluate fetal DNA circulating in a
pregnant individual's blood. In general, IVDs offered as LDTs are
occupying a growing share of the testing market and are used in some of
the most complex areas of medicine (see, e.g., Refs. 1 and 2).
---------------------------------------------------------------------------
\7\ FDA has initiated a pilot program for certain oncology
diagnostics as one step that may be helpful in reducing the risks
associated with using certain LDTs to identify cancer biomarkers
(see 88 FR 40273 (June 21, 2023)).
---------------------------------------------------------------------------
Given the role these IVDs play in modern medical care, their
validity has a significant impact on the public health. False positive
test results, which erroneously indicate that a patient has a certain
disease or condition, can delay diagnosis and treatment of the true
disease or condition, lead to unwarranted interventions, and cause
needless distress. Interventions may involve medication with serious
side effects or risky medical procedures. False negative results can
lead to progression of disease, in some cases without the opportunity
for life-saving treatment, and the spread of infectious disease. The
harms to patients from false positive and negative results can be
significant. For example, the application of an ineffective oncology
treatment due to a false positive for a patient already weakened from
disease, or the failure to receive a life-saving medication due to a
false negative, can be fatal. These false results can stem from an
analytical error or from a lack of clinical validity where a measured
result is incorrectly associated with a particular clinical state.
Flaws in a test's algorithm can mean the difference in whether a
patient with cancer receives a beneficial immunotherapy. Pregnant
people may use screening tests to make decisions without obtaining
appropriate confirmatory testing. In 2016, FDA learned of a false
positive result from a genetic test for long QT syndrome (a heart
signaling disorder) that led to the erroneous implantation of a
defibrillator in a healthy individual. In addition to the risks
associated with the implantation procedure, the defibrillator delivered
inappropriate shocks to the patient, which posed the risk of sudden
cardiac death (Refs. 9 and 10). These are just a few examples of how
diagnostic tests can and do have significant long-term consequences for
patients.
2. Current Information Raises Serious Questions About Whether Patients
Can Rely on IVDs Offered as LDTs
FDA has highlighted the risks associated with IVDs offered as LDTs
for decades, and our concerns have grown in recent years. As described
in the ``History of the Rulemaking'' section, we first took steps to
address the issue in the late 1990s, followed by a series of different
proposed strategies for increasing oversight. In 2015, the Agency
published a report of 20 case studies involving inaccurate, unsafe,
ineffective, or poor quality LDTs that caused or may have caused
patient harm (``2015 Report'') (Ref. 11). More recent evidence suggests
that the situation is getting worse. This evidence cuts across test
types and laboratories and is from a variety of sources, including
published studies in the scientific literature, allegations of
problematic tests reported to FDA, FDA's own experience in reviewing
IVDs offered as LDTs, news articles, and class-action lawsuits.
Overall, the evidence points to fundamental uncertainty in the
marketplace about whether IVDs offered as LDTs provide accurate and
reliable results.
Scientific literature is one source of evidence. Over time, FDA has
become aware of various publications that describe problems with IVDs
offered as LDTs. In the past 3 years, four different studies have
documented high variability in performance among these IVDs (Refs. 12
to 15). In one study, the
[[Page 68011]]
same samples were sent to 19 laboratories for testing using their own
manufactured test and only 7 of those laboratories correctly reported
all results (Ref. 12). For almost half of the tests studied, analytical
accuracy was significantly lower than that of the parallel test
approved by FDA. In another study, researchers sent identical samples
to two different laboratories to detect tumor mutations and found over
70 percent discordance in the results from their tests (Ref. 13). A
study by Friends of Cancer Research found substantial variability among
tumor mutational burden (TMB) tests manufactured by laboratories and
used to identify patients with cancer most likely to benefit from
immunotherapy (Ref. 14). A fourth study highlighted validity concerns
specific to early cancer detection tests, including one IVD offered as
an LDT that delivered nine false positive results for every true cancer
diagnosis (Ref. 15). An article published earlier this year detailed an
oncologist's experience with false results from an unapproved blood-
based multi-cancer early detection IVD offered as an LDT and intended
to screen for more than 50 types of cancer (Ref. 16). A 2016 study
published in the New England Journal of Medicine reported false
positive results from genetic IVDs offered as LDTs for hypertrophic
cardiomyopathy in multiple patients of African American descent (Ref.
17). These studies do not mean that every laboratory is manufacturing
bad tests or that no patient can rely on IVDs offered as LDTs. Instead,
they reflect a level of variability, including the potential for
inaccurate or incomplete results, that highlights the need for changes
to the basic oversight scheme.
FDA's own experience has reinforced concerns regarding IVDs offered
as LDTs. FDA has gathered information about IVDs offered as LDTs
through its review of submissions. Although the Agency generally has
not enforced requirements for LDTs, it has received premarket
submissions from some laboratories seeking authorization for their
tests. We have received numerous submissions for such tests, including
premarket review submissions,\8\ Q-submissions,\9\ and investigational
use submissions for IVDs offered as LDTs, as well as many emergency use
authorization (EUA) requests from laboratories (which are discussed
further below). FDA's review of these submissions has provided insight
into laboratory test development and, in some cases, revealed
significant concerns. For example, FDA has observed that many
laboratories fail to perform appropriate or adequate validation
studies, have data demonstrating their test does not work as intended
but offer the test anyway, or use instruments and other components that
are not adequately controlled for clinical use. The tests described in
these submissions have been intended for a range of diseases or
conditions, some of which are very serious. FDA has received
submissions for IVDs offered as LDTs to diagnose Alzheimer's disease,
predict heart disease risk, diagnose Fabry disease (a rare neurological
disorder), and inform treatment considerations for a rare blood cancer,
all of which lacked adequate validation to support authorization.
---------------------------------------------------------------------------
\8\ These submissions have been for a wide variety of
indications, including tests intended to detect nucleic acids from
viruses associated with head and neck cancers; to identify patients
with obesity due to rare genetic conditions to inform treatment
eligibility; to aid in the management of therapy for patients taking
certain anticoagulants; and tests for breast cancer prognosis, tumor
profiling, and treatment selection, for patients with cancer.
\9\ For discussion of FDA's Q-submission program, see FDA's
guidance document issued on June 2, 2023, entitled ``Requests for
Feedback and Meetings for Medical Device Submissions: The Q-
Submissions Program,'' available at https://www.fda.gov/media/114034/download.
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In addition, given that FDA's general enforcement discretion
approach for LDTs has not applied to IVDs for emergency use (though FDA
has issued enforcement policies for such IVDs during specific
emergencies, as explained elsewhere in this preamble), FDA has received
EUA requests for tests from laboratories, including many for COVID-19
diagnostics. Of the first 125 EUA requests for COVID-19 molecular
diagnostic tests submitted from laboratories, 82 showed test design or
validation problems (Ref. 18). In one case, the approach to validation
was so poor that when redone correctly, there was a 400-fold difference
in performance, leading the laboratory to take the test off the market.
In another example, an academic medical center (AMC) laboratory
purported to validate its test with only 12 positive samples, showing
perfect performance. FDA requested evaluation of additional specimens
to confirm. When an additional 12 samples were evaluated, the
cumulative performance revealed an unacceptably high false negative
rate, where the test identified only 71 percent of known positive
specimens as positive and falsely identified 29 percent of known
positive samples as negative, and the EUA request was withdrawn. In
addition, multiple laboratories that offered their tests as described
in FDA's COVID-19 test guidance (see discussion in Ref. 19) did not
provide any analytical and/or clinical validation data in the EUA
requests that they submitted after the tests were in use. This
experience provided a window into the approach that many laboratories
may take to test validation, and not only confirmed but increased FDA's
concerns about the validation of IVDs offered as LDTs. The experience
also showed that even tests involving relatively well-understood
techniques (here, the polymerase chain reaction, or PCR, technique) may
not perform well. In all, test performance seen in this subset of
submissions from laboratories was far worse than we expected. To the
extent that this sample represents larger trends in the performance of
IVDs offered as LDTs, it underscores the need for greater FDA
oversight.
FDA has also received multiple complaints, adverse event reports,
and other allegations identifying problems with IVDs offered as
LDTs.\10\ One complaint alleged that an IVD offered as an LDT to
diagnose autism had insufficient clinical validation to support this
use. In another complaint, an informant alleged that a laboratory was
forging results when its liquid biopsy test did not work. Additionally,
FDA has received multiple voluntary medical device reports (primarily
from patients) of inaccurate NIPS test results, as well as inaccurate
results from an oncology IVD offered as an LDT that predicts risk of
breast cancer recurrence and informs the decision to pursue
chemotherapy, both of which can pose serious, irreversible harm to
patients. Another report described a false negative result from a BRCA
test marketed to predict one's risk of breast cancer. The patient was
later diagnosed with breast cancer and found to be BRCA1 positive by
another test. A separate report from a healthcare provider described a
different patient that received discrepant results from testing with
this BRCA test and with another IVD offered as an LDT for hereditary
cancer risk prediction. In yet another report, a patient described a
false positive breast cancer result from an oncology blood IVD offered
as an LDT and that led to invasive followup procedures, emotional
anguish, and unnecessary monetary expenses. FDA also received a report
regarding a blood-based test for lung cancer that underestimated cancer
in about 40 percent of patients. Additionally, FDA has received medical
device reports
[[Page 68012]]
regarding infectious disease genetic IVDs offered as LDTs without
validation, from which inaccurate results could lead to limb loss or
women's health issues, and regarding inaccurate results from an IVD
offered as an LDT to assess medication adherence. As noted above,
collectively, this information, though anecdotal, points to potential
problems among IVDs offered as LDTs, the scope and scale of which FDA
cannot fully assess or address without phasing out the general
enforcement discretion approach for applicable requirements (such as
adverse event reporting).
---------------------------------------------------------------------------
\10\ FDA has not confirmed the veracity of the allegations or
facts in every complaint, report, and allegation. Nevertheless,
collectively this information points to potential problems among
IVDs offered as LDTs.
---------------------------------------------------------------------------
Aside from the scientific community and FDA, the general public is
coming to recognize concerns with the current scheme, in which most
LDTs are generally not overseen by FDA. General news sources and other
outlets have reported on such concerns (see, e.g., Refs. 20 to 26). For
example, the New York Times recently conducted an indepth investigation
into NIPS tests and found that positive results from the tests are
incorrect about 85 percent of the time (Ref. 22). NIPS tests are
screening tests, so they should be followed up with confirmatory
diagnostic testing, but the New York Times article reported that
patients and healthcare providers are making healthcare decisions based
on results from these screening tests alone due to manufacturers'
marketing claims. A device whose labeling is false or misleading in any
particular manner is misbranded under the FD&C Act; however, under the
general enforcement discretion approach, FDA generally has not enforced
this proscription for IVDs offered as LDTs. As another example,
ProPublica reported on a COVID-19 test offered by a laboratory under
contract with a university without EUA authorization from FDA, which,
according to the report, missed 96 percent of the positive cases from
the university campus, and routinely sent people infected with COVID-19
back into the community (Ref. 26). In addition, consumers,
shareholders, and investors are filing lawsuits against laboratory
manufacturers for false and misleading statements about test efficacy,
including lawsuits related to pharmacogenetic tests (genetic tests
intended to inform drug selection) and NIPS (see, e.g., Complaint, In
re Myriad Genetics, Inc. Sec. Litig., No. 2:19-cv-00707-PMW (D. Utah
2019); Complaint, Hickok v. Capone, No. 2021-0686 (Del. Ch. 2021);
Complaint, Davis v. Natera, Inc., No. 3:22-cv-00985 (N.D. Cal. 2022);
Complaint, Carroll v. Myriad Genetics Inc., No. 4:22-CV-00739 (N.D.
Cal. 2022); Biesterfeld v. Ariosa Diagnostics, Inc., No. 1:21-CV-03085,
2022 WL 972281 (N.D. Ill. 2022); and Complaint, Kogus v. Capone, No.
2022-0047-SG (Del. Ch. 2022)). The overall picture presented by this
evidence indicates that a change in oversight is needed to better
assure the safety and effectiveness of IVDs offered as LDTs.
3. Greater FDA Oversight is Needed To Protect the Public Health
As described above, the evidence FDA has collected points to flaws
in laboratory manufacturing of tests that need to be addressed to
protect the public. Greater oversight by FDA would help address these
flaws.
In the past, FDA has communicated with the public when it is
particularly concerned about a type of IVD offered as an LDT. For
example, in addition to the 2015 Report, FDA has issued safety
communications about pharmacogenetic tests, NIPS tests, ovarian cancer
screening tests, nipple aspirate tests, and instruments used in the
design of many different LDTs (Refs. 27 to 31). FDA has also taken
compliance action in some circumstances, such as issuing a warning
letter to a laboratory manufacturing a pharmacogenetic test in April
2019 (Ref. 32). However, more structural change is needed. FDA's
general enforcement discretion approach emerged at a time when the
typical IVD offered as an LDT looked very different from how it looks
today. FDA has made a preliminary determination that this approach has
become outdated, and the proposed steps to end this approach in this
rulemaking would better protect the public health.
Increased oversight would help to ensure the safety and
effectiveness of IVDs offered as LDTs. More accurate diagnoses would
lead to better care, which would advance public health overall. Through
increased oversight, the public, including patients and healthcare
professionals, could have more confidence that the test results they
rely on are accurate. Greater FDA oversight of IVDs offered as LDTs has
become particularly important as more and more novel treatments require
use of a specialized test to identify patients likely to benefit from
them. This, in turn, has led to increased development of tests used as
the primary driver for therapeutic decisions. These include tests to
determine whether to administer a therapeutic, which therapeutic to
administer, and at what dose to administer the therapeutic. For
example, recent approvals of drug products to treat diseases in their
early stages, such as for early-stage Alzheimer's patients, make
accurate and early diagnosis of these diseases more critical today than
ever before. As another example, gene therapy is an emerging field with
incredible potential to treat many diseases or conditions. Testing is
required to identify patients with the defective gene targeted by the
treatment and, in some cases, to assess whether the patient has
antibodies to the vector delivering the treatment that would prevent it
from working. In these and other cases, accurate and reliable test
results are essential for safe and effective use of a therapeutic.
Increased oversight would also address business strategies that
take advantage of the current bifurcated system. For example, in a
number of cases, laboratories that have submitted premarket submissions
for their tests, but whose tests did not meet applicable requirements
for authorization, have still offered these IVDs as ``LDTs.'' Some of
these tests, such as a test intended to diagnose Alzheimer's disease,
had inadequate validation data to support authorization (see Ref. 33).
A genotyping test purported to predict heart disease risk, but FDA
found that there was no association between the genetic information the
test identified (KIF6) and heart disease. A third test, intended to
diagnose Fabry disease, showed a high level of false negatives. The
public health is not served by a scheme in which tests that have these
types of problems are still offered to patients simply because the
manufacturer is a laboratory. FDA is also aware that some industry
players have created business models that claim a connection to
laboratories and offer IVDs as LDTs. The increase in firms using these
business models, as well as their substantial magnitude of reach,
underscores the need for more oversight.
In addition, FDA anticipates that consistent oversight would bring
more stability to the testing market overall, which could help to
encourage the manufacture of IVDs for which there is a reasonable
assurance of safety and effectiveness. FDA is aware of arguments that
better assuring the safety and effectiveness of LDTs would foster test
innovation. FDA is also aware of arguments that IVD manufacturers that
are not laboratories may currently be discouraged from investing time
and resources into developing novel tests due to the concern that once
the manufacturer receives marketing authorization for its test,
laboratories will develop similar tests and market their tests without
complying with FDA requirements. We anticipate that applying the same
oversight approach to
[[Page 68013]]
laboratories and non-laboratories that manufacture IVDs would better
assure the safety and effectiveness of LDTs, and would remove a
disincentive for non-laboratory manufacturers to develop novel tests,
thereby spurring innovation and access to IVDs for which there is a
reasonable assurance of safety and effectiveness. As a result, we
anticipate that phasing out the general enforcement discretion approach
for LDTs would advance responsible innovation by both laboratory and
non-laboratory IVD manufacturers alike, rather than discouraging it.
FDA is aware of other arguments that ending the general enforcement
discretion approach for LDTs would interfere with test innovation and
patient access due to the potential need for premarket review of new
tests. However, under FDA's device authorities, FDA premarket review is
only required for certain tests (generally those classified into class
II or class III), and FDA estimates that approximately 50 percent of
IVDs offered as LDTs would not require premarket review (see section
II.F.4 of the Preliminary Economic Analysis of Impacts (Ref. 34)). In
addition, FDA review is only required for device modifications in
certain circumstances. For devices that are subject to PMA
requirements, a PMA supplement is required only for changes that affect
the safety or effectiveness of the device, and in some cases the change
may be made prior to FDA approval (see 21 CFR 814.39(d)); may be made
30 days after a supplement has been filed, unless FDA takes certain
action (see 21 CFR 814.39(e)); or may be made 30 days after FDA
receives a notice describing the change (in lieu of a supplement),
unless FDA takes certain action (see 21 CFR 814.39(f)). For devices
that are subject to 510(k) requirements, a new 510(k) is only required
for a significant change or modification in design, components, method
of manufacture, or intended use, where a significant change or
modification is one that could significantly affect the safety or
effectiveness of the device or that is a major change or modification
in the device's intended use (21 CFR 807.81(a)). FDA has published
several guidance documents to help stakeholders determine whether a
certain change or modification may require a PMA supplement, new
510(k), or other submission to FDA, and FDA has several mechanisms
available through which manufacturers may seek FDA assistance in making
this determination. In addition, under section 515C of the FD&C Act (21
U.S.C. 360e-4), a PMA supplement or new 510(k) is not required for a
change to a device that would otherwise require a supplement or new
510(k) if the change is consistent with a predetermined change control
plan previously approved or cleared by FDA. We also note that as
described in section VI.B, FDA is proposing to phase out the general
enforcement discretion approach for LDTs with respect to premarket
review requirements on a date that aligns with or follows the beginning
of a new user fee cycle, such that FDA's review timelines and goals
would be reflected in commitments newly negotiated with industry. For
all of these reasons, FDA does not anticipate that ending the general
enforcement discretion approach for LDTs would unduly impair test
innovation and patient access.
Furthermore, FDA's approach was never intended to selectively
foster laboratory innovation at a cost to public health. Rather, the
approach arose based on certain test characteristics and institutional
safeguards that at the time adequately protected patients. In general,
those characteristics and safeguards are no longer present, putting
public health at risk. Further, FDA is aware that this scheme is in
some cases fostering unfounded claims of innovation rather than
responsible innovation. These claims are concerning to FDA because they
can mislead the public, undermine legitimate competition, and
disincentivize responsible, science-based innovation.
Finally, increased oversight may help to advance health equity. FDA
is aware of concerns that IVDs offered as LDTs may exacerbate health
inequities due to higher rates of inaccurate results among
underrepresented patient populations, particularly racial and ethnic
minorities undergoing genetic testing (see, e.g., Refs. 17 and 35 to
38). Some IVDs offered as LDTs have not been validated for use in all
patient populations within a disease state, meaning that it is unknown
how well the test may perform across diverse patient populations
expected to use the test and the test may be less accurate in
underrepresented patient populations, potentially contributing to
health disparities (see, e.g., Ref. 39). Increased FDA oversight may
help to ensure that information is available pertaining to device
safety and effectiveness for specific demographic characteristics if
performance differs within the target population, through the
enforcement of applicable labeling requirements. In addition, when FDA
conducts premarket review of a device, FDA may ask that sponsors
provide data for different intended patient populations, and with new
authorities under the Food and Drug Omnibus Reform Act of 2022 (FDORA),
sponsors generally are required to submit diversity action plans to
FDA, including the sponsor's goals for enrollment in device clinical
studies. In contrast, with limited oversight over these tests, FDA does
not know whether diverse patient populations are being included in
validation studies for these IVDs. FDA has made a preliminary
determination that increased oversight for these IVDs would help ensure
adequate representation of the intended use population in validation
studies and transparency regarding potential differential performance,
helping to advance health equity. FDA also recognizes that IVDs offered
as LDTs may serve communities in rural, medically underserved areas
with disparities in access to diagnostic tests. However, the benefits
of test access directly depend on the ability of tests to work as
intended. Thus, to the extent that access to IVDs offered as LDTs may
benefit patients in rural, medically underserved communities, the harms
of unsafe or ineffective IVDs offered as LDTs may also be realized
among these underserved patient populations. By increasing its
oversight, FDA may better prevent and mitigate such harms, thereby
better protecting the health of these underserved populations.
We are aware of arguments that other mechanisms--such as the
medical expertise of laboratorians or requirements under CLIA--already
provide adequate oversight of IVDs offered as LDTs. However, our review
of the evidence indicates otherwise. Evidence suggests that under the
current scheme, the healthcare community lacks adequate assurances
about the safety and effectiveness of IVDs offered as LDTs. Although
laboratories that offer LDTs are also subject to CLIA, which is
primarily administered by the Centers for Medicare & Medicaid Services
(CMS), CLIA is not a substitute for FDA oversight. CLIA establishes
requirements for laboratories and laboratory personnel pertaining to
operations, inspections, and certification, with a focus on the
proficiency with which laboratories perform clinical testing (see 42
U.S.C. 263a and 42 CFR part 493). Among other requirements, clinical
laboratories generally must have a CLIA certificate that corresponds to
the complexity of tests performed prior to accepting human samples for
testing. However, under CLIA, CMS does not regulate critical aspects of
laboratory test
[[Page 68014]]
development; does not evaluate the performance of a test before it is
offered to patients and healthcare providers; does not assess clinical
validity (i.e., the accuracy with which a test identifies, measures, or
predicts the presence or absence of a clinical condition or
predisposition in a patient); does not regulate certain manufacturing
activities, such as design controls and acceptance activities; does not
provide human subject protections for patients who participate in test
clinical research trials; and does not require adverse event reporting.
As such, CMS has described the FDA and CMS ``regulatory schemes'' as
``different in focus, scope and purpose, but they are intended to be
complementary'' (Ref. 40). Where CLIA does play a role (as discussed
further below, compliance with CLIA may provide certain assurances
relating to quality system (QS) requirements), FDA has tailored its
proposed phaseout policy accordingly.\11\
---------------------------------------------------------------------------
\11\ When ``QS'' requirements are discussed throughout this
preamble, FDA is referring to the current good manufacturing
practice (CGMP) requirements set forth in part 820 (21 CFR part
820). Generally, the requirements are referred to as QS
requirements, but that terminology may change when amendments to
part 820 are finalized. See 87 FR 10119 (February 23, 2022) and
section VI.B.3 for a further discussion of FDA's proposed amendments
to part 820.
---------------------------------------------------------------------------
We are also aware of arguments that any additional oversight of
LDTs should be accomplished by granting new statutory authorities to
CMS. However, this would cause a problematic split in oversight, with
the same types of tests being reviewed by different Agencies depending
on where the test was made. For example, a cancer diagnostic test
developed by a conventional manufacturer would be reviewed by FDA while
a similar cancer diagnostic test (using the same sample type and
testing for the same analytes) developed by a laboratory would be
reviewed by another Agency. Further, with that divided oversight, an
IVD developed by a conventional manufacturer could even be reviewed and
cleared by FDA and subsequently reviewed by another Agency if a
laboratory made certain modifications to it. However, if those same
modifications were made by the original manufacturer, they would be
reviewed by FDA. This could lead to confusion and inconsistency.
FDA has both the authority and the expertise to perform the
necessary oversight of IVDs offered as LDTs and is the only Agency for
which that is the case. One of FDA's most basic and well-understood
responsibilities is helping to ensure the safety and effectiveness of
medical products. FDA employs staff across a wide range of disciplines,
including physicians, statisticians, engineers, biologists, chemists,
geneticists, and others, to evaluate the science behind medical
products before they reach the market. Understanding the complex
technical information in applications, such as clinical trial data,
bench testing results, and product manufacturing and design
characteristics--and putting that information in context to assess
whether a product can be marketed--is within the unique expertise of
FDA. This type of expertise is no less important for IVDs, which can
have a wide variety of public-health consequences, as described
elsewhere in this rule. During review of an application for an IVD, FDA
reviewers closely examine data relevant to analytical validity,
clinical validity, and safety, and draw on their expertise and
experience to understand both the product and the science supporting
the product.
Review of the underlying science behind an IVD is based on what the
IVD does and is in no way related to where the IVD is made. Thus, FDA's
experience and expertise with respect to oversight of other IVDs is
directly applicable to oversight of LDTs. In fact, FDA has already
applied its expertise to the review of some IVDs offered as LDTs--for
example, during public health emergencies. As stated above, FDA has
reviewed many EUA requests for tests from laboratories during the
public health response to COVID-19.
Entities outside FDA have also recognized that FDA should oversee
LDTs, and that greater oversight is needed. For example, the
Secretary's Advisory Committee on Genetics, Health, and Society, in its
April 2008 report entitled ``U.S. System of Oversight of Genetic
Testing,'' stated that ``FDA should address all laboratory tests,
regardless of how they are produced (i.e., as a commercial test kit or
laboratory-developed test), in a manner that takes advantage of its
current experience'' (Ref. 41). The American Cancer Society Cancer
Action Network has taken a similar position, noting in a November 2016
statement that ``[c]urrent oversight of LDTs falls short of ensuring
these tests produce accurate and meaningful results . . . [t]he FDA is
the most appropriate agency to evaluate the analytical and clinical
validity of diagnostic tests, along with their safety, to help ensure
that cancer patients and their doctors are able to make appropriate
treatment decisions based on accurate information'' (Ref. 42).
Likewise, the Advanced Medical Technology Association (AdvaMed) stated
in November 2021 that the association has ``long supported the idea
that all diagnostic test developers . . . should be subject to the same
FDA standards and processes'' (Ref. 43).
4. FDA Should Increase Oversight in a Manner That Recognizes the
Current State of the Testing Market
As discussed throughout this section, increased oversight of IVDs
offered as LDTs is needed. However, FDA has also made a preliminary
determination that our general enforcement discretion approach should
be phased out in a manner that accounts for the level of public health
concern and the importance of avoiding undue disruption to the testing
market, including undue disruption to the provision of care. Therefore,
we are proposing a gradual phaseout to occur in stages over a total
period of 4 years, as described in section VI.B. FDA anticipates that
this phaseout policy should ultimately enable IVDs offered as LDTs that
are supported by sound science to remain on the market. FDA also
recognizes that some IVDs may need to come off the market, because, for
example, the IVD cannot meet applicable requirements under the FD&C Act
and its implementing regulations, or the laboratory chooses not to
invest resources to meet those requirements. To the extent that
withdrawal from the market of these IVDs implicates any reliance
interests, FDA has made a preliminary determination that the public-
health benefits associated with the reasonable assurance of safety and
effectiveness of IVDs offered as LDTs outweigh any such interests. In
addition, in the long run, it is possible that any reduction in the
number of current IVDs offered as LDTs may be offset by the market
entry of IVDs from other manufacturers who will have benefitted from a
more consistent oversight approach and increased stability spurring
innovation.
C. FDA's Current Regulatory Framework
The FD&C Act, as amended by the MDA and subsequent statutes,
establishes a comprehensive system for the regulation of devices,
defined in section 201(h)(1) of the FD&C Act, that are intended for
human use. Section 513 of the FD&C Act (21 U.S.C. 360c) establishes
three categories (classes) of devices depending on the regulatory
controls needed to provide reasonable assurance of their safety and
effectiveness. The three categories of devices are class I (general
controls), class II (special controls), and class III (premarket
approval).
Class I devices are those devices for which the general controls of
the FD&C
[[Page 68015]]
Act (controls authorized by or under section 501, 502, 510, 516, 518,
519, or 520 (21 U.S.C. 351, 352, 360, 360f, 360h, 360i, or 360j) or any
combination of such sections) are sufficient to provide reasonable
assurance of safety and effectiveness of the device; or those devices
for which insufficient information exists to determine that general
controls are sufficient to provide reasonable assurance of safety and
effectiveness or to establish special controls to provide such
assurance, but because the devices are not purported or represented to
be for a use in supporting or sustaining human life or for a use which
is of substantial importance in preventing impairment of human health,
and do not present a potential unreasonable risk of illness or injury,
are to be regulated by general controls (section 513(a)(1)(A) of the
FD&C Act).
General controls include, but are not limited to, provisions that
relate to establishment registration and device listing; premarket
notification; prohibitions against adulteration and misbranding (e.g.,
labeling that fails to bear adequate directions for use); recordkeeping
and reporting, including adverse event reporting and reporting of
corrections and removals initiated to reduce a risk to health posed by
the device or to remedy a violation of the FD&C Act caused by the
device which may present a risk to health; and current good
manufacturing practice (CGMP) requirements. These controls apply to all
devices unless an exemption applies.
Class II devices are those devices for which general controls by
themselves are insufficient to provide reasonable assurance of safety
and effectiveness, but for which there is sufficient information to
establish special controls to provide such assurance, including the
promulgation of performance standards, post-market surveillance,
patient registries, development and dissemination of guidelines,
recommendations, and other appropriate actions the Agency deems
necessary to provide such assurance (section 513(a)(1)(B) of the FD&C
Act).
Class III devices are those devices for which insufficient
information exists to determine that general controls and special
controls would provide a reasonable assurance of safety and
effectiveness, and are purported or represented for a use in supporting
or sustaining human life or for a use which is of substantial
importance in preventing impairment of human health, or present a
potential unreasonable risk of illness or injury (section 513(a)(1)(C)
of the FD&C Act).
Under section 513(d)(1) of the FD&C Act, devices that were
introduced or delivered for introduction into interstate commerce for
commercial distribution before the enactment of the MDA on May 28, 1976
(generally referred to as ``preamendments devices'') are classified
after FDA: (1) receives a recommendation from a device classification
panel (an FDA advisory committee); (2) publishes the panel's
recommendation, along with a proposed regulation classifying the
device, and provides an opportunity for interested persons to submit
comments; and (3) publishes a final regulation classifying the device.
A preamendments device for which a classification regulation has not
been promulgated is known as an ``unclassified device.'' Until an
unclassified device type has been formally classified by regulation,
the marketing of new devices within the device type requires FDA
premarket review through a premarket notification (510(k)) under
section 510(k) of the FD&C Act.
Devices that were not introduced or delivered for introduction into
interstate commerce for commercial distribution before May 28, 1976
(generally referred to as ``postamendments devices'') are classified
automatically by section 513(f) of the FD&C Act into class III without
any FDA rulemaking process. Those devices remain in class III and
require approval of a premarket approval application (PMA), unless and
until: (1) FDA classifies or reclassifies the device into class I or II
under section 513(f)(2) or (3) of the FD&C Act, or (2) FDA issues an
order finding the device to be substantially equivalent, in accordance
with section 513(i) of the FD&C Act, to a predicate device that does
not require premarket approval. The Agency determines whether new
devices are substantially equivalent to predicate devices by means of
premarket notification procedures in section 510(k) of the FD&C Act and
part 807 of the regulations (21 CFR part 807).
In addition, under section 520(g) of the FD&C Act and part 812 of
FDA's regulations (21 CFR part 812), a clinical investigation to
determine the safety and effectiveness of certain devices must be the
subject of an approved investigational device exemption (IDE) before
such investigation may commence. If an IDE has been granted, a failure
to comply with a requirement under which the device was exempted for
investigational use renders the device adulterated (see section 501(i)
of the FD&C Act).
Failure to comply with applicable requirements of the FD&C Act and
FDA regulations may render the device adulterated and misbranded under
sections 501 and 502 of the FD&C Act and may constitute a prohibited
act under section 301 of the FD&C Act (21 U.S.C. 331).
IVDs, as defined in Sec. 809.3 (21 CFR 809.3), are devices
intended for human use and are subject to the FD&C Act. They include
class I, class II, and class III devices, as well as both preamendments
and postamendments devices. Like other devices, IVDs are subject to
general controls, including premarket notification, reporting
requirements regarding adverse events and corrections and removals, IDE
requirements (though most investigations of IVDs are exempt from most
provisions of the IDE regulation), and other applicable requirements
under the FD&C Act and FDA's regulations. IVDs are also subject to
specific labeling requirements in part 809 of the regulations (21 CFR
part 809).
D. History of the Rulemaking
1. FDA's Longstanding Recognition That IVDs Manufactured by
Laboratories Are Devices
FDA has made clear, on many occasions and over many years, that
LDTs are devices under the FD&C Act (for the legal reasoning for this
conclusion, see section V.B). Over 25 years ago, FDA explained that
clinical laboratories that develop tests are acting as manufacturers of
medical devices (62 FR 62243 at 62249 (November 21, 1997)). FDA
reiterated that position in a citizen petition response a year later
(Ref. 44), and in the preamble to a final rule 3 years after that (65
FR 18230 at 18231 (April 7, 2000)). In 2006, FDA again cited its prior
statement that clinical laboratories that develop tests are acting as
manufacturers of medical devices (Ref. 45 (quoting 62 FR 62243 at
62249)). In 2014, FDA expressly considered and rejected arguments that
LDTs are not devices under the FD&C Act, stating in a citizen petition
response that ``LDTs are devices within the plain language of the
[statutory] definition'' (Ref. 46). Five years later, FDA issued a
warning letter stating that ``FDA has not created a legal `carve-out'
for LDTs such that they are not required to comply with the
requirements under the Act that otherwise would apply. . . . Although
FDA has generally exercised enforcement discretion for LDTs, the Agency
always retains discretion to take action when appropriate, such as when
it is appropriate to address significant public health concerns'' (Ref.
47). A wide range of other FDA documents, including guidance documents,
safety communications, compliance letters, and other public statements,
have
[[Page 68016]]
indicated or otherwise taken as their premise that IVDs are devices
even when the manufacturer is a laboratory (see, e.g., Refs. 11, 18,
27, 28, and 48 to 56).
FDA has also taken regulatory actions consistent with these
statements and documents. Since 2017, the Agency has reviewed over 40
PMAs, 510(k)s, and De Novo classification requests for tests identified
by the manufacturer as LDTs, and has approved, cleared, or granted De
Novo classification for roughly half of those tests under authorities
in the FD&C Act specifically reserved for ``devices.'' FDA has also
received many EUA requests from laboratories and has authorized over
150 such tests for emergency use, an authority that is also limited to
``devices'' or other FDA-regulated medical products.
2. Past FDA Initiatives To Address LDTs
In light of FDA's recognition that LDTs are devices and our
increasing concerns about IVDs offered as LDTs (as detailed in the
``Need for the Rule'' section, section III.B of this document), over
the years the Agency has considered various ways to address IVDs
manufactured by laboratories that raise safety or effectiveness
concerns. In 1997, FDA sought to address these concerns by establishing
restrictions on the sale, distribution, and use of analyte specific
reagents (ASRs), which the Agency described as the ``primary
ingredients'' of most LDTs (62 FR 62243 at 62249). In 2006, FDA issued
a draft guidance outlining a different enforcement approach for a type
of LDT known as an in vitro diagnostic multivariate index assay
(IVDMIA),\12\ which raised particular safety and effectiveness concerns
(Ref. 45). FDA later determined that it should engage in a more
comprehensive effort to oversee LDTs, in part due to stakeholder
feedback.
---------------------------------------------------------------------------
\12\ As defined in the draft guidance document, IVDMIAs are
``test systems that employ data, derived in part from one or more in
vitro assays, and an algorithm that usually, but not necessarily,
runs on software to generate a result that diagnoses a disease or
condition or is used in the cure, mitigation, treatment, or
prevention of disease.'' The draft guidance document further
characterized IVDMIAs as having the following three features: they
use clinical data to empirically identify variables and derive
weights/coefficients used in an algorithm; they employ that
algorithm to calculate a patient-specific result, which cannot be
independently derived and confirmed by another laboratory (absent
access to proprietary information used in the development and
derivation of the test); and they report that result, which cannot
be interpreted by a well-trained healthcare practitioner using prior
knowledge of medicine in the absence of information from the test
developer regarding clinical performance and effectiveness.
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Consistent with this determination, in 2010, FDA announced plans to
develop a broader approach to the oversight of LDTs. The Agency held a
2-day public meeting and opened a docket for public comment (75 FR
34463 (June 17, 2010)). Input received through those proceedings
informed two draft guidance documents issued by FDA on October 3, 2014,
entitled ``Framework for Regulatory Oversight of Laboratory Developed
Tests (LDTs)'' (79 FR 59776) and ``FDA Notification and Medical Device
Reporting for Laboratory Developed Tests (LDTs)'' (79 FR 59779) (Refs.
48 and 49). In those draft guidance documents, FDA proposed to
implement a risk-based oversight framework for IVDs offered as LDTs,
with a phased enforcement strategy. FDA solicited public feedback on
the draft guidance documents and held a public workshop on January 8
and 9, 2015 (79 FR 69860 (November 24, 2014)).
From October 2014 through 2016, FDA analyzed more than 300 sets of
comments on the draft guidance documents, as well as discussion from
the public workshop, and engaged extensively with stakeholders in
meetings and conferences. A number of interested parties provided
feedback, including laboratories, healthcare providers, patients,
conventional IVD manufacturers, government agencies, and Congress. The
feedback ranged generally from strong opposition to strong support for
FDA's proposed increased oversight of LDTs and addressed a wide range
of topics, including FDA's authority to regulate LDTs, the risks posed
by LDTs without increased FDA enforcement, the effect of a new
enforcement approach on test access and innovation, the potential
interplay between FDA regulation and CLIA, and the implications of
increased FDA oversight for competition in the IVD market.
On January 13, 2017, FDA issued a discussion paper (2017 Discussion
Paper) synthesizing the feedback that had been provided to the Agency,
following a choice by FDA not to finalize the draft guidance documents
to allow for further public discussion and to provide an opportunity
for Congress to develop legislation for a new regulatory framework
encompassing all IVDs that appropriately balances patient protection
with continued access and innovation (Ref. 50).
In August 2020, HHS posted a statement on its website entitled
``Rescission of Guidances and Other Informal Issuances,'' which stated,
among other things, that ``the department has determined that the Food
and Drug Administration (`FDA') will not require premarket review of
laboratory developed tests (`LDT') absent notice-and-comment
rulemaking'' (Ref. 57).\13\ This statement was informed by advice in a
legal memorandum from the HHS Office of General Counsel (see Ref. 59).
In November 2021, based on new advice from the HHS Office of General
Counsel, HHS leadership determined that the August 2020 statement no
longer represented the Department's policy or legal views (Ref. 59).
HHS Secretary Xavier Becerra publicly announced the withdrawal of the
statement on November 15, 2021 (Ref. 60). Various news outlets have
reported on these events (Refs. 61 to 64).
---------------------------------------------------------------------------
\13\ HHS also posted an accompanying document entitled ``FAQs on
Laboratory Developed Tests (LDTs)'' on its website (Ref. 58).
---------------------------------------------------------------------------
IV. Legal Authority
FDA is proposing to issue this rule under the Agency's general
rulemaking authorities and statutory authorities relating to devices.
These authorities include sections 201(h)(1), 301, 501, 502, 510, 513,
514, 515, 518, 519, 520, 701, 702, 704, and 801 (21 U.S.C. 321(h)(1),
331, 351, 352, 360, 360c, 360d, 360e, 360h, 360i, 360j, 371, 372, 374,
and 381). In particular:
Under section 201(h)(1) of the FD&C Act, a device is
defined as ``an instrument, apparatus, implement, machine, contrivance,
implant, in vitro reagent, or other similar or related article,
including any component, part, or accessory, which is (A) recognized in
the official National Formulary, or the United States Pharmacopeia, or
any supplement to them, (B) intended for use in the diagnosis of
disease or other conditions, or in the cure, mitigation, treatment, or
prevention of disease, in man or other animals, or (C) intended to
affect the structure or any function of the body of man or other
animals, and which does not achieve its primary intended purposes
through chemical action within or on the body of man or other animals
and which is not dependent upon being metabolized for the achievement
of its primary intended purposes.''
Section 701(a) of the FD&C Act authorizes FDA to issue
regulations for the efficient enforcement of the FD&C Act.
For additional descriptions of some of the authorities referenced
above, see ``FDA's Current Regulatory Framework'' section (section
III.C.). For additional discussion of how these legal authorities apply
to LDTs, see ``Legal Basis for the Proposed Amendment'' section
(section V.B.).
[[Page 68017]]
V. Description of the Proposed Amendment to the Definition of In Vitro
Diagnostic Products
A. Proposed Amendment
We are proposing to amend part 809, subpart A, specifically Sec.
809.3, by updating the definition of ``in vitro diagnostic products''
to make explicit that IVDs are devices under the FD&C Act including
when the manufacturer of the IVD is a laboratory. IVDs are defined as
``those reagents, instruments, and systems intended for use in the
diagnosis of disease or other conditions, including a determination of
the state of health, in order to cure, mitigate, treat, or prevent
disease or its sequelae. Such products are intended for use in the
collection, preparation, and examination of specimens taken from the
human body'' (Sec. 809.3). This amendment would reflect FDA's
longstanding view that LDTs are devices under the FD&C Act, and would
reflect the fact that the device definition in the FD&C Act does not
differentiate between entities manufacturing the device. In other
words, whether an IVD is a device does not depend on where or by whom
the IVD is manufactured.
FDA is also proposing to amend the statutory citation for the
device definition included in Sec. 809.3 to reflect amendments to
section 201(h) of the FD&C Act as a result of the enactment of the
Safeguarding Therapeutics Act (Pub. L. 116-304, 134 Stat. 4915). For
many years, the definition of ``device'' had been codified at section
201(h) of the FD&C Act. Upon enactment of the Safeguarding Therapeutics
Act, the definition of ``device'' was redesignated as paragraph (h)(1)
and a new definition of ``counterfeit device'' was codified at
paragraph (h)(2).
B. Legal Basis for the Proposed Amendment
If amended as proposed, Sec. 809.3 would express in plain terms
that IVDs, including test systems, fall within the definition of a
device in section 201(h)(1) of the FD&C Act when they have been
manufactured by laboratories. In this subsection, FDA sets forth the
legal reasoning for this position.
1. In Vitro Diagnostic Test Systems Are Devices
The FD&C Act defines a device as, in relevant part, ``an
instrument, apparatus, implement, machine, contrivance, implant, in
vitro reagent, or other similar or related article, including any
component, part, or accessory, which is . . . intended for use in the
diagnosis of disease or other conditions, or in the cure, mitigation,
treatment, or prevention of disease'' (see 21 U.S.C. 321(h)(1); see
also 21 U.S.C. 360j(o) (identifying circumstances under which software
is and is not within the device definition)). This definition includes
IVD test systems. Test systems are sets of IVDs--for example, reagents,
instruments, specimen collection devices, software, and other related
materials--that function together to produce a test result. See, e.g.,
Sec. 809.10(a)(9)(iii) (21 CFR 809.10(a)(9)(iii)) (discussing
``multiple unit products which require the use of included units
together as a system''); id. Sec. 809.10(b) (referring to reagents and
instruments within a system). According to a straightforward reading of
the statutory text, these systems are ``apparatus[es],''
``contrivance[s],'' and articles that are ``similar or related'' to
``instrument[s]'' and ``in vitro reagent[s],'' that are intended for
use in the diagnosis of disease or other conditions or in the cure,
mitigation, treatment, or prevention of disease. They consist of
individual parts that have their own regulatory identity, but, when
combined, constitute a new device.
The device definition expressly contemplates this scenario because
it provides that both an overall article and each of its ``components''
and ``parts'' are devices subject to regulation. (21 U.S.C. 321(h)(1);
cf. Shuker v. Smith & Nephew, PLC, 885 F.3d 760, 768 (3d Cir. 2018)
(describing the distinct status of a ``system that is itself a `device'
but that is comprised of Class II [device] components in addition to
one or more Class III [device] components'').) The word ``apparatus,''
which is defined as ``a set of materials or equipment designed for a
particular use,'' encompasses test systems by its plain terms. (See
Apparatus, Merriam-Webster.com (last accessed June 28, 2023); see also
United States v. Bacto-Unidisk, 394 U.S. 784, 798 (1969) (``Congress
fully intended that the [FD&C] Act's coverage be as broad as its
literal language indicates'').) Consistent with this analysis, FDA's
definition of an ``in vitro diagnostic product,'' which was first
promulgated in 1973 and is still in effect today, identifies a
``system'' as a type of IVD and a device under the FD&C Act. (Section
809.3 (IVDs include ``reagents, instruments, and systems''); see 38 FR
7096 at 7098 (March 15, 1973).)
The regulation of test systems is important because test systems
are generally the IVDs that produce a result--a ``positive'' or
``negative'' (such as what patients receive in the context of COVID-19
diagnostic tests), a quantitative value (such as a concentration of
glucose), or perhaps a more detailed report of results. The quality of
test results is generally what defines both the risks and benefits of
IVDs: the risks stem from inaccurate, unreliable, incomplete, or
misleading test results, and the benefits stem from accurate, reliable,
and complete test results. For that reason, test systems and their
results are a key focus of FDA's regulation of IVDs. FDA has issued
over 350 regulations classifying different types of test systems (see
generally 21 CFR parts 862, 864, 866) and has evaluated the performance
and results of innumerable test systems over the course of decades.
Patients and healthcare professionals rely on FDA to help ensure the
validity of test systems, and conventional IVD manufacturers have built
their business around this premise.
The focus on test systems and their results is not new; it has been
a consistent theme throughout the history of FDA's regulation of IVDs.
Congress expressly granted FDA authority over diagnostic products in
1938. (Federal Food, Drug and Cosmetic Act (June 25, 1938), Pub. L. 75-
717, 52 Stat. 1040 (defining ``drug'' and ``device'' with reference to
an intended use in ``diagnosis,'' among other things).) Following the
1938 Act, FDA took action against diagnostic products, including
against a system intended to diagnose illness based on human blood
samples. (See Drown v. United States, 198 F.2d 999, 1001 (9th Cir.
1952).) And, in the early 1970s, FDA established a specific IVD
regulatory program in response to ``rapid growth in development of in
vitro diagnostic products combined with the increasing use and reliance
on the results by physicians, hospital personnel, and clinical
laboratories.'' (37 FR 819, January 19, 1972). This program addressed
the ``need [for] closer scrutiny because of the possibility that
inaccurate and unreliable results may be obtained.'' Id. FDA issued
final regulations establishing controls over IVDs, including
``systems,'' in 1973 (38 FR 7096 at 7098) (creating, among other
things, ``product class standards'' to set ``performance requirements
necessary to assure accuracy and reliability of results''). FDA's
increasing concerns about these products was evident from the fact
that--even before Congress expanded the Agency's device authorities in
1976--it applied the drug authorities to certain IVDs. The Supreme
Court upheld that application in Bacto-Unidisk, 394 U.S. at 800-01.
In 1976, Congress enacted the MDA, sweeping legislation meant to
broaden and strengthen FDA's authority over
[[Page 68018]]
devices. (See, e.g., H.R. Rep. 94-853 at 11 (February 29, 1976).) The
MDA included revisions to the definition of ``device'' to clarify that
IVDs should be regulated under the new, more robust device authorities.
(Medical Device Amendments of 1976, Pub. L. 94-295, 90 Stat. 539
(adding the term ``in vitro reagent'' to the definition of a device);
S. Rep. No. 93-670 at 16 (January 29, 1974) (``The Committee recognizes
that there is confusion at the present time about whether certain
articles are to be treated as devices or drugs under the Food, Drug and
Cosmetic Act. Therefore, the Committee reported bill has carefully
defined `device' so as to specifically include implants, in vitro
diagnostic products, and other similar or related articles.''). The
legislative history shows that Congress had serious concerns about test
systems and sought to empower FDA to address them. (See, e.g., S. Rep.
No. 93-670 at 3-4 (January 29, 1974) (describing with concern ``quack
devices'' such as a ``diagnostic service'' in which ``[p]ractitioners .
. . mailed in the blood spots taken from their patients,'' ``[t]he
blood-spotted paper was put into a slot of the electrical device called
the `Radioscope' while the operator stroked with a wand the abdomen of
a person holding metal plates connected to the device,'' and ``the
operator determined from this the identity, kind, location, and
significance of any disease present'').) Congress also contemplated
performance standards relevant to test systems, such as required
labeling with ``ranges of accuracy of diagnosis.'' (H.R. Rep. 94-853 at
27.) Thus, in the MDA, Congress endorsed FDA's focus on test systems
and their results.
2. Test Systems Manufactured by Laboratories Are Devices
The definition of ``device'' in the FD&C Act encompasses test
systems regardless of where or by whom they are manufactured. (See 21
U.S.C. 321(h)(1).) In particular, the definition contains no exception
or limitation for devices manufactured by laboratories. ``Congress
expresses its intentions through statutory text passed by both Houses
and signed by the President (or passed over a Presidential veto).''
(Oklahoma v. Castro-Huerta, 142 S. Ct. 2486, 2496 (2022).) If Congress
had intended such a limitation, it could have said so. Instead,
Congress made clear that the definition does not turn on the type of
entity manufacturing the device: for example, the statute expressly
recognizes that even ``practitioners licensed by law to prescribe or
administer . . . devices'' (the professionals most closely associated
with traditional medical practice) can ``manufacture . . . devices,''
though they may be exempt from certain requirements when they do so
``solely for use in the course of their professional practice.'' \14\
(See 21 U.S.C. 360(g)(2); see also 21 U.S.C. 360i(c)(1), 374(a)(2)(B).)
---------------------------------------------------------------------------
\14\ These exemptions apply when a practitioner (1) is licensed
by law to prescribe or administer a device such as an IVD, (2)
manufactures that device, and (3) does so ``solely for use in the
course of [his or her] professional practice.'' Thus, these
exemptions apply to practitioners, not entities such as corporate or
hospital laboratories that employ licensed practitioners. For
example, FDA has long held that hospitals that reprocess single-use
devices are subject to registration and other requirements under the
FD&C Act because they are the owners/operators, manufacturers, etc.
even though those hospitals employ licensed practitioners. See
Frequently-Asked-Questions about the Reprocessing and Reuse of
Single-Use Devices by Third-Party and Hospital Reprocessors; Final
Guidance for Industry and FDA Staff (July 2001), available at
https://www.fda.gov/media/71057/download (stating ``Third-party and
hospital reprocessors of single-use devices (SUDs) are subject to
all the regulatory requirements currently applicable to original
equipment manufacturers, including premarket submission
requirements'' and including a Q&A that provides instructions on how
to register and list for such entities).
---------------------------------------------------------------------------
Courts have repeatedly recognized that articles manufactured by
medical professionals fall within FDA's jurisdiction (e.g., United
States v. Regenerative Sciences, 741 F.3d 1314 (D.C. Cir. 2014)
(holding that doctors ``producing, as part of their medical practice,''
a ``drug'' under the FD&C Act violated the FD&C Act); Drown v. United
States, 198 F.2d 999, 1001 (9th Cir. 1952) (upholding FDA action
against chiropractor who ``manufacture[d] certain photographic,
therapeutic and diagnostic instruments of her own design which she
use[d] in her practice'')). As the D.C. Circuit in Regenerative
Sciences observed, an approach that rejects ``the [FD&C Act]'s
regulation of doctors'' would ``create an enormous gap in the [FD&C
Act]'s coverage.'' (741 F.3d at 1320.)
The inclusion of articles in the FD&C Act's definition of a device
without regard to the identity of their manufacturer makes particular
sense in the context of test systems. Today, in FDA's experience, there
is little distinction between the test systems manufactured by
laboratories and other manufacturers. These systems generally consist
of highly specialized components with complex functionality working in
combination; they rarely resemble the ``1976-type'' tests discussed in
this rule. For example, a modern-day next generation sequencing (NGS)
test system for genetic testing typically consists of (among other
things) a DNA extraction kit to extract nucleic acids from a human
sample; an NGS instrument that analyzes the nucleic-acid output and
(after days) generates gigabytes of sequencing raw data; and multiple
pieces of computer software that translate that raw data into a test
report. The systems look the same, and function the same way,
regardless of who manufactures them. And although not all systems look
exactly like an NGS system, they do typically involve sophisticated
instruments with advanced software that, when used in conjunction with
other test components, produce the system's results. Their manufacture
generally requires knowledge of bioinformatics, software development,
and an underlying specialty, such as medical genetics--knowledge that
is neither traditionally associated with nor unique to laboratories.
FDA understands that many test systems offered as LDTs are designed at
Fortune 500 companies (see Ref. 65) by a ``development team,'' similar
to how systems from conventional manufacturers are designed. And in
FDA's experience, the individuals on these development teams generally
have the same training and expertise regardless of whether they are
employed by a ``laboratory'' organization or a conventional
manufacturer. Even smaller laboratories use the same complex equipment
for their systems, although they may purchase and use components that
are labeled by other companies for ``research use only.'' In short,
there is nothing inherent in the nature or design of laboratory
developed test systems that would justify exclusion from FDA's
jurisdiction.
That is not to say that laboratories and conventional IVD
manufacturers are identical. Laboratories do occupy a distinct role in
diagnostic testing because they are the entities that generally perform
the tests. Like many devices, such as a magnetic resonance imaging unit
used by a trained technician, test systems are usually used by trained
professionals. Laboratories that are certified under CLIA and that meet
the regulatory requirements under CLIA to perform high complexity
testing employ trained laboratorians to ``run'' test systems, and CLIA
is the statutory scheme that governs that work, as discussed in more
detail in section III.B. However, a laboratory's role in performing
test systems does not change its obligations under the FD&C Act when it
is manufacturing test systems. As previously noted, the FD&C Act does
not exclude medical professionals who manufacture devices from its
scope, and the mere fact that a device is manufactured in connection
with a
[[Page 68019]]
medical service or procedure does not eliminate FDA's jurisdiction.
(See United States v. Regenerative Sciences, 741 F.3d at 1319
(``Notwithstanding appellants' attempt to characterize this case as an
effort by the FDA to `restrict[ ] the use of an autologous stem cell
procedure,' the focus of the FDA's regulation is on the Mixture [that
is, the product that is created in connection with the procedure].'').)
Although some commentators have argued that laboratory
manufacturing is immune from regulation because it is within the
``practice of medicine,'' that argument misconstrues the scope of the
FD&C Act's ``practice of medicine'' provision. Section 1006 of the FD&C
Act (21 U.S.C. 396) provides: ``Nothing in this [Act] shall be
construed to limit or interfere with the authority of a health care
practitioner to prescribe or administer any legally marketed device to
a patient for any condition or disease within a legitimate health care
practitioner-patient relationship.'' Section 1006 carves out a specific
zone of protected conduct that does not reach laboratory manufacturing
of test systems. The purpose of the provision is to ``ensure[ ] that
once the FDA permits a device to be marketed for one use, health care
practitioners have the flexibility to draw on their expertise to
prescribe or administer the device'' for other uses. (Judge Rotenberg
Educ. Ctr., Inc. v. United States, 3 F.4th at 395 (emphases added); see
also Conf. Rep. 105-399 at 97 (November 9, 1997) (provision intended to
cover ``off-label use of a medical device by a physician using his or
her best medical judgment in determining how and when to use the
medical product for the care of a particular patient'').) The statutory
provision applies only in the context of use of a ``legally marketed
device''--that is, a device that is already manufactured and lawfully
on the market--and only applies to ``prescrib[ing] or administer[ing] .
. . within a legitimate health care practitioner-patient
relationship.'' It does not apply to the manufacture of new test
systems. The manufacture of a new device falls squarely within FDA's
realm. Cf. United States v. Regenerative Sciences, 741 F.3d at 1320
(``[W]hile the [FD&C Act] was not intended to regulate the practice of
medicine, it was obviously intended to control the availability of
drugs for prescribing by physicians.'') (quoting United States v.
Evers, 643 F.2d 1043, 1048 (1981)). The fact that healthcare
practitioners may prescribe a device, such as a test system, in the
context of a healthcare practitioner-patient relationship does not mean
that entities manufacturing that device can escape regulation. If that
were the case, few devices would be regulated, because most are
intended for use by healthcare practitioners in the context of a
healthcare practitioner-patient relationship.
Furthermore, contrary to what some commentators have suggested,
CLIA did not repeal FDA's authority over IVDs manufactured by
laboratories, which dates back to at least 1938. CLIA does not
expressly repeal FDA's authority, nor was FDA's authority repealed by
implication. ``An implied repeal will only be found where provisions in
two statutes are in irreconcilable conflict, or where the latter Act
covers the whole subject of the earlier one and is clearly intended as
a substitute.'' (Branch v. Smith, 538 U.S. 254, 273 (2003) (cleaned
up).) Here, as CMS itself has explained, ``the regulatory schemes of
the two agencies are different in focus, scope and purpose'' and ``are
intended to be complementary'' (Ref. 40). As explained in section
III.B, CLIA puts a focus on the proficiency with which laboratories
perform clinical testing, and the FD&C Act puts a focus on the
manufacturing of test systems. CMS and FDA have different areas of
expertise, and CLIA does not address a wide range of activities
regulated under the FD&C Act, such as clinical validation and design
activities. Thus, ``CLIA does not preempt the FDA's authority to
regulate facilities like [Clinical Reference Laboratory]. When two
statutes are `capable of co-existence, it is the duty of the courts,
absent a clearly expressed congressional intent to the contrary, to
regard each as effective.' '' (Clinical Reference Lab. v. Sullivan, 791
F. Supp. 1499, 1509 (D. Kan. 1992) (quoting Ruckelshaus v. Monsanto
Co., 467 U.S. 986, 1018, (1984)), aff'd in part and rev'd in part on
other grounds sub nom., United States v. Undetermined No. of Unlabeled
Cases, 21 F.3d 1026 (10th Cir. 1994).)
In fact, Congress has affirmed that test systems manufactured by
laboratories are devices under the FD&C Act. In the Protecting Access
to Medicare Act of 2014 (PAMA) (Pub. L. 113-93), Congress listed 510(k)
clearance or premarket approval under the FD&C Act as one of several
bases for Medicare payment for an ``advanced diagnostic laboratory
test,'' which is defined in part as a clinical diagnostic laboratory
test ``that is offered and furnished only by a single laboratory and
not sold for use by a laboratory other than the original developing
laboratory (or a successor owner)'' (section 216(a) of PAMA). If such
laboratory tests were not devices, the 510(k) clearance and premarket
approval provisions would not apply to them and the inclusion of such
provisions would be pointless and ineffectual. In addition, Congress
indicated that clinical laboratory tests are devices in 2016 amendments
to the FD&C Act. (21 U.S.C. 360j(o)(1)(D) (repeatedly referring to
``clinical laboratory test or other device data'') (emphasis added).)
The FD&C Act confers jurisdiction on FDA to regulate test systems,
a point that has been codified in FDA's regulations for more than half
a century. And nothing in the text, history, or purpose of the statute
suggests that test systems manufactured by laboratories are excluded
from that jurisdiction. This interpretation is not only the most
straightforward reading of the statute, it is also the most reasonable:
any other interpretation would create a bifurcated scheme in which
systems that are functionally identical are treated differently under
the law.
3. FDA's Jurisdiction Over IVDs Manufactured by Laboratories Is Not
Altered by the FD&C Act's Provisions Related to Interstate Commerce and
Commercial Distribution
Modern Commerce Clause jurisprudence holds that Congress has
``authority to regulate even purely local activities that are part of
an economic `class of activities' that have a substantial effect on
interstate commerce.'' (United States v. Regenerative Sciences, 741
F.3d at 1320 (quoting Gonzales v. Raich, 545 U.S. 1, 17 (2005)).) Thus,
few have disputed that Congress possesses the power to grant FDA
authority to regulate even purely intrastate activities. However, some
commentators have asserted that language in the FD&C Act referencing
``interstate commerce'' and ``commercial distribution'' precludes FDA
from regulating IVDs that are designed, manufactured, and used in a
single laboratory. As discussed below, these assertions lack merit.
a. Interstate commerce. There is no overarching requirement in the
FD&C Act that FDA-regulated articles have a particular nexus with
interstate commerce. Interstate commerce is not a prerequisite to FDA
jurisdiction (beyond the constitutional minimum). Rather, under the
FD&C Act, a limited number of provisions include specific interstate
commerce ``elements,'' and thus require a particular connection with
interstate commerce in order for those provisions to apply. For
example, certain of the FD&C Act's ``prohibited acts'' contain an
interstate commerce element that must be satisfied before the
government can bring an enforcement action under those
[[Page 68020]]
provisions (e.g., 21 U.S.C. 331(a), (c), (d), and (k)). But relatively
few of the FD&C Act's device provisions include a specific interstate
commerce element, and most of the device-related prohibited acts do
not. (See, e.g., 21 U.S.C. 331(e) (prohibiting the failure to establish
or maintain any record, or make any report, required under the device
adverse-event reporting requirements without reference to interstate
commerce); id. 331(p) (prohibiting the failure to register a device
establishment without reference to interstate commerce); id. 331(q)(1)
(prohibiting the failure to comply with device investigational-use
requirements without reference to interstate commerce); id. 331(fff)(3)
(prohibiting the doing of any act which causes a device to be a
counterfeit device, or the sale or dispensing, or holding for sale or
dispensing, of a counterfeit device without reference to interstate
commerce); see generally United States v. Walsh, 331 U.S. 432, 434-36
(1947) (finding no interstate commerce element to 21 U.S.C. 331(h),
which prohibits false guaranties) (``[21 U.S.C. 331(a)] is directed to
illegal interstate shipments, while [21 U.S.C. 331(h)] is directed to
the giving of false guaranties'').) If an FD&C Act provision does not
contain an interstate commerce element, ``interstate commerce'' imposes
no limit on FDA's powers beyond the constitutional minimum. For
devices, the FD&C Act imposes obligations even where there is no
interstate commerce element and likewise gives FDA authority to take
action when there is a violation of those obligations. Thus, FDA does
not, for example, somehow lose jurisdiction if a particular device has
not been ``introduced'' into interstate commerce.
In fact, Congress intentionally revised a provision of the FD&C Act
to ensure that FDA could take action against devices without satisfying
any particular interstate commerce element. In the MDA, Congress
revised the seizure provisions in section 304 of the FD&C Act to
``permit seizure of devices without reference to interstate commerce''
because the previous interstate commerce requirement ``ha[d] been a
burden to the effective enforcement of existing authorities'' and
``whether or not a medical device actually crosses state lines has
nothing to do with the principal intent of this proposal: to assure the
safety and effectiveness of medical devices.'' (H.R. Rep. 94-853 at 15;
see 21 U.S.C. 334(a)(2).) In other words, Congress recognized that the
interstate commerce element in this provision did not advance the goals
of the MDA. Consistent with that view, the FD&C Act grants FDA wide-
ranging authority over devices, including IVDs, and that general
authority does not turn on a connection with interstate commerce above
the constitutional minimum.
In addition, one of the key prohibited acts on which FDA relies,
section 301(k) of the FD&C Act (21 U.S.C. 331(k)), contains an
interstate commerce element, but applies even when a problematic device
has not been introduced in interstate commerce. That provision
prohibits ``the doing of any . . . act with respect to[ ] a . . .
device . . . if such act is done while such article is held for sale
(whether or not the first sale) after shipment in interstate commerce
and results in such article being adulterated or misbranded.'' Courts
have held that even if a product is wholly manufactured and sold
intrastate, the interstate commerce element is satisfied if the
components used in manufacturing the product have traveled in
interstate commerce. (See United States v. Regenerative Sciences, 741
F.3d at 1320-21 (upholding FDA enforcement action under 331(k) because
a drug component had traveled in interstate commerce); Baker v. United
States, 932 F.2d 813, 815 (9th Cir. 1991); United States v. Dianovin
Pharm., Inc., 475 F.2d 100, 102 (1st Cir. 1973).) At least some
components of test systems, such as general purpose reagents, ASRs,
instruments, and collection devices, are usually shipped in interstate
commerce even if the system itself is designed, manufactured, and used
solely in the laboratory (i.e., intrastate). And section 709 of the
FD&C Act (21 U.S.C. 379a) establishes a presumption of interstate
commerce in enforcement actions, meaning that the burden is on
regulated parties to demonstrate, for example, that no component of a
system traveled across State lines. (``In any action to enforce the
requirements of this Act respecting a device . . . the connection with
interstate commerce . . . shall be presumed to exist.'').
Some commentators have cited the interstate commerce element in
section 510(k) of the FD&C Act to raise questions about FDA's authority
over LDTs. Section 510(k) provides that a person who is required to
register and ``proposes to begin the introduction or delivery for
introduction into interstate commerce'' of a device ``shall'' submit a
premarket notification. Under this line of argument, laboratories that
design, manufacture, and use an IVD in a single laboratory are not
proposing to introduce their IVD into interstate commerce, and
therefore section 510(k) does not apply to them. That argument,
however, does not lead to the conclusion that FDA lacks jurisdiction
over LDTs or that none of the FD&C Act requirements apply to LDTs. It
would mean only that section 510(k) does not apply. And if accepted,
the only practical consequence of that assertion would be that affected
laboratories are subject to more burdensome requirements under the FD&C
Act.
In particular, if section 510(k) is construed to mean that such
IVDs are not eligible for the premarket notification pathway, that
would only mean that those IVDs (unless they are 510(k)-exempt, in
which case section 510(k) would not apply anyway, or are for
investigational use) would be forced into the more rigorous review
pathways of premarket approval or authorization through the De Novo
pathway. That is because under section 513(f)(l) of the FD&C Act, a
postamendments device, i.e., a device that was ``not introduced or
delivered for introduction into interstate commerce for commercial
distribution before [May 28, 1976],'' is a class III device by
operation of law (21 U.S.C. 360c(f)(1)). If such a device cannot be
found to be substantially equivalent through the premarket notification
pathway, it must either have an approved PMA (21 U.S.C. 360e(a)), or be
reclassified and gain authorization through a pathway such as the De
Novo process (21 U.S.C. 360c(f)(2)(A)(ii)). Thus, under this theory,
laboratories would not escape FDA regulation--they would face heavier
regulation. However, because section 510(k) does not, in fact, preclude
regulated entities from submitting premarket notifications even
assuming their devices are not introduced into interstate commerce, and
because laboratories have every incentive to take the less burdensome
path to market of 510(k) notification, the 510(k) pathway should play
the same role in device reclassification (21 U.S.C. 360c(f)) for IVDs
offered as LDTs as for any other device. Regardless, the inclusion of
an interstate commerce element in section 510(k) in no way affects
FDA's overall authority to regulate IVDs manufactured by laboratories.
b. Commercial distribution. The phrase ``for commercial
distribution'' also appears in various device provisions of the FD&C
Act, and some commentators have asserted that this phrase, too, signals
that FDA lacks authority over LDTs. For example, they point to the
510(k) premarket notification requirement, which is triggered when a
person who is required to register ``proposes to begin the introduction
or delivery for introduction into interstate commerce for commercial
distribution of a device intended for
[[Page 68021]]
human use'' (21 U.S.C. 360(k)). As with ``interstate commerce,'' the
presence of this phrase in that provision and certain other specific
device provisions does not bear on the Agency's overall jurisdiction.
Furthermore, LDTs are for commercial distribution, so the presence of
the phrase does not change the operation of those provisions with
respect to these IVDs.
Under our longstanding, judicially endorsed interpretation,
``commercial distribution'' does not require the physical transfer of
an object, as some commentators have argued. Instead, the legislative
history, FDA's near-contemporaneous regulation, and at least one
judicial decision reflect that the phrase ``commercial distribution''
means ``on the market.'' A House Report issued 3 months before
enactment of the MDA contains an unusually clear statement of the
intended meaning of the phrase: ```Commercial distribution' is the
functional equivalent of the popular phrase `on the market.' '' (H.R.
Rep. No. 94-853 at 36) FDA's regulations implementing the registration,
listing, and 510(k) provisions, which were finalized in 1977 (soon
after enactment of the MDA), similarly define commercial distribution
as ``any distribution of a device intended for human use which is held
or offered for sale.'' (21 CFR 807.3(b)) In the preambles to the
proposed and final rule, FDA equated the term with the phrase ``on the
market'' (41 FR 37458 at 37459 (September 3, 1976); 42 FR 42520 at
42524 (August 23, 1977)). A court has also endorsed this interpretation
of the term (United States v. An Article of Device Consisting of 1,217
Cardboard Boxes, 607 F. Supp. 990, 994-95 (W.D. Mich. 1985) (giving
deference to FDA's reasonable interpretation of ``commercial
distribution'' to mean, ``in its popular sense, `on the market' '')).
These sources show that the term does not relate to physical movement,
and because IVDs manufactured by laboratories (including LDTs)
generally are ``on the market,'' they are for commercial distribution.
VI. Description of the Proposed Enforcement Policy
Based on the considerations set forth in this preamble, FDA is
proposing to end the general enforcement discretion approach for LDTs.
However, FDA also recognizes that many IVDs manufactured by
laboratories are currently being marketed as LDTs, and that a sudden
change could negatively affect the public, including patients and
industry. In particular, FDA understands that the healthcare community
and patients have been using these IVDs, and that coming into
compliance will take time for manufacturers. FDA also recognizes that
we should consider Agency resources. For additional information
regarding the estimated costs associated with this rulemaking, see the
Preliminary Economic Analysis of Impacts (Ref. 34).
To achieve greater oversight in a manner that accounts for the
various considerations, FDA is proposing to gradually end its general
enforcement discretion approach in stages, as described below
(hereinafter ``the phaseout policy''). FDA's intent is that, following
a 4-year phaseout period, IVDs offered as LDTs generally would be
expected to meet applicable requirements.
Although FDA is proposing to gradually end its current general
enforcement discretion approach over a period of years, the phaseout
policy does not in any way alter the fact that it is illegal to offer
IVDs without complying with applicable requirements. Regardless of the
phaseout timeline and continued enforcement discretion approach for
certain IVDs discussed below, FDA retains discretion to pursue
enforcement action at any time against violative IVDs when appropriate.
Moreover, FDA has adopted and intends to continue adopting
enforcement discretion policies for certain types of IVDs in certain
circumstances, as appropriate. For example, FDA issued guidance
documents with enforcement discretion policies for certain COVID-19 and
Mpox tests at the beginning of each declared emergency (as described
further below), and intends to issue a draft guidance with an
enforcement policy for IVDs for emerging outbreaks offered prior to FDA
review to address the immediate public health need. FDA will seek
public comment on such draft guidance in accordance with good guidance
practices (see 21 CFR 10.115).
With this notice of proposed rulemaking, FDA seeks public comment
on whether specific enforcement discretion policies would be
appropriate for IVDs offered as LDTs for other public health scenarios.
If so, please provide a description of those scenarios, an explanation
of why enforcement discretion policies with respect to those scenarios
would be appropriate, and any relevant evidence to support such
policies. FDA would also appreciate public comment on what, if any,
unintended consequences may result from the proposed phaseout policy to
certain patient populations (for example, Medicare beneficiaries, rural
populations, etc.) and what steps could be taken to mitigate those
consequences.
FDA's proposed phaseout policy, including the scope and phaseout
timeline, is set forth below.
A. Scope
While FDA's general enforcement discretion approach has been
focused on LDTs, FDA is proposing a broader scope for the phaseout
policy. Specifically, FDA is proposing to apply the phaseout policy to
IVDs that are manufactured and offered as LDTs by laboratories that are
certified under CLIA and that meet the regulatory requirements under
CLIA to perform high complexity testing,\15\ even if those IVDs do not
fall within FDA's traditional understanding of an LDT because they are
not designed, manufactured, and used within a single laboratory.\16\
Throughout this preamble, these IVDs are referred to as ``IVDs offered
as LDTs.'' FDA is proposing this scope because it recognizes that not
all laboratories have understood the limited nature of FDA's general
enforcement discretion approach and have been offering IVDs based on
the approach even when they do not fit what FDA generally considers to
be an LDT. As previously discussed, FDA has made a preliminary
determination to structure the phaseout in a way that avoids undue
disruption to the testing market. This is important even for certain
IVDs currently on the market that do not fall within the scope of FDA's
general enforcement discretion approach.
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\15\ Other laboratories would be out of compliance with CLIA
regulations if they were developing and performing tests that are
not FDA authorized. Such tests have never fallen within FDA's
general enforcement discretion approach (see, e.g., Refs. 32, 40,
and 54).
\16\ As discussed elsewhere in this preamble, FDA has generally
considered the term ``laboratory developed test (LDT)'' to mean an
IVD that is intended for clinical use and that is designed,
manufactured, and used within a single CLIA-certified laboratory
that meets the regulatory requirements under CLIA to perform high
complexity testing.
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Although FDA is proposing this broader scope for the phaseout
policy, it does not intend to sweep in certain tests that were excluded
from the general enforcement discretion approach, as reflected in
compliance patterns, multiple public FDA actions and communications, or
both. These tests are:
1. Tests that are intended as blood donor screening or human cells,
tissues, and cellular and tissue-based products (HCT/Ps) donor
screening tests required for infectious disease testing under 21 CFR
610.40 and 1271.80(c), respectively, or for determination of
[[Page 68022]]
blood group and Rh factors required under 21 CFR 640.5. Under the cited
regulations, a blood or HCT/P establishment must not use a test for the
purposes listed here unless the test is licensed, approved, or cleared
by FDA for such use. Blood and HCT/P establishments must register with
FDA and are subject to FDA inspection (see 21 CFR parts 207, 607, 807
and 1271). FDA's general enforcement discretion approach for LDTs has
never applied to these tests because these tests are a critical part of
the overall process of ensuring the safety of blood and blood
components and HCT/Ps by preventing infectious disease transmission and
incompatible blood transfusions which can have life-threatening
consequences. Based on FDA experience, establishments have been
generally complying with these requirements (see, e.g., Refs. 66 and
67).
2. Tests intended for emergencies, potential emergencies, or
material threats declared under section 564 of the FD&C Act. After all
previous declarations under section 564(b), FDA has generally expected
LDTs to comply with applicable requirements in the FD&C Act and FDA
regulations. FDA's general enforcement discretion approach has not
applied to these tests because of the significant risk posed by the
disease (as signified by the unusual step of issuing a declaration) and
because false results can have serious implications for disease
progression and public health decision-making, in addition to the
individual patient's care. As it has done in other areas, FDA has
adopted (and may continue to adopt) specific enforcement discretion
policies for such tests (see, e.g., Refs. 51 and 52). In addition,
consistent with the Government Accountability Office's 2022
recommendation that ``FDA should develop a policy for the use of
enforcement discretion regarding unauthorized tests in future public
health emergencies,'' FDA intends to issue guidance on factors to
consider in adopting such enforcement discretion policies (Ref. 68).
FDA has communicated its expectations regarding tests for emergency use
in guidance and elsewhere, including ``It has come to our attention''
letters posted on FDA's website and other public communications (see,
e.g., Refs. 51 to 54, 69, and 70).
3. Direct-to-consumer tests. FDA's general enforcement discretion
approach has not applied to tests intended for consumer use (without
meaningful involvement by a licensed healthcare professional), given
the greater risks to patients presented by these tests (see, e.g.,
Refs. 48, 55, and 71 to 75). FDA's enforcement discretion approach for
LDTs was originally premised, in part, on the participation of medical
professionals to help determine whether a particular test was
appropriate, counsel patients on the significance and limitations of a
test, assist in interpreting results, assess how the results fit in the
overall clinical picture, and consider next steps. When patients order
tests, receive results, and make decisions (such as a decision to stop
medication) without this expert intermediary, there is a heightened
need for FDA oversight.
For these categories of tests, FDA has generally expected
applicable requirements to be met, and we are not proposing to change
that approach.
FDA notes that the manufacturing of test components outside of a
laboratory--for example, when the same entity owns both the laboratory
and a manufacturing facility separate from the laboratory--does not
fall within FDA's general enforcement discretion approach. FDA's
approach has long been specific to laboratory development (e.g., 61 FR
10484 (``in-house developed tests have not been actively regulated by
the Agency'') (emphasis added); Ref. 48 (describing an LDT as an IVD
that is ``designed, manufactured, and used within a single
laboratory''). The proposed phaseout policy would not change FDA's
longstanding expectation that IVD manufacturing activities occurring
outside of a CLIA-certified laboratory comply with applicable device
requirements.
In addition, for certain categories of tests manufactured by
laboratories, FDA is proposing to continue to apply the current general
enforcement discretion approach going forward. One such category of
tests is referred to in this preamble as ``1976-Type LDTs.'' Such tests
have the following characteristics common among LDTs offered in 1976:
use of manual techniques (without automation) performed by laboratory
personnel with specialized expertise; use of components legally
marketed for clinical use; and design, manufacture, and use within a
single CLIA-certified laboratory that meets the requirements under CLIA
for high complexity testing. The characteristics associated with LDTs
offered in 1976 resulted in the emergence of FDA's general enforcement
discretion approach for LDTs, and the specific characteristics listed
above provide the greatest risk mitigation among the characteristics
that were commonly associated with LDTs offered in 1976 (discussed in
section III.A). Based on changes to the LDT landscape since 1976, the
risks associated with most modern LDTs are generally much greater today
than they were in 1976; however, for tests that share the
characteristics listed above, FDA has made a preliminary determination
that the risks are sufficiently mitigated such that FDA's general
enforcement discretion approach for LDTs should continue to apply.
These tests might include, for example, immunohistochemistry tests that
involve no automated preparation or interpretation, but would not
include, for example, lateral flow tests, as they do not generally rely
on laboratory personnel expertise.
FDA is also proposing to continue to apply the general enforcement
discretion approach to Human Leukocyte Antigen (HLA) tests that are
designed, manufactured, and used in a single laboratory certified under
CLIA that meets the requirements to perform high-complexity
histocompatibility testing when used in connection with organ, stem
cell, and tissue transplantation to perform HLA allele typing, for HLA
antibody screening and monitoring, or for conducting real and
``virtual'' HLA crossmatch tests. FDA has made a preliminary
determination that HLA LDTs for transplantation used in
histocompatibility laboratories that meet the regulatory requirements
under CLIA to perform high complexity testing, when used in connection
with organ, stem cell, and tissue transplantation for certain purposes
as described in this paragraph, are unique in that they are generally
developed, and the testing is generally performed, in urgent, life-
saving situations for the patient. Physicians must often make prompt
decisions about transplantation based on medical judgment regarding
their patient's condition and degree of mismatch between the donor and
patient should an organ, stem cells, or tissue become available.
Further, these tests are often individualized within each medical
facility, for example, they include reagents that reflect local HLA
polymorphisms and patient demographics. Note that the general
enforcement discretion approach does not apply to HLA tests used for
blood transfusion as such tests are highly standardized across
institutions; FDA intends to continue to enforce applicable
requirements for HLA tests used for blood transfusion.
FDA also intends to maintain its longstanding enforcement
discretion approach for tests intended solely for forensic (law
enforcement) purposes. This approach has been in place for over 20
years and applies to such tests regardless of whether they are offered
as an LDT. See, e.g., 65 FR 18230 (April 7, 2000). Tests used in the
law
[[Page 68023]]
enforcement setting are subject to protections and requirements
associated with the judicial process that mitigate risk related to test
accuracy and sample collection and that generally are not available in
the home, workplace, insurance, and sports settings. These protections
include the use of rules of evidence in judicial proceedings and legal
representation of the accused (i.e., the person being tested) through
the judicial process during which the accuracy of the test may be
raised during the adjudication. We seek comment on any implications of
continued enforcement discretion with regard to LDTs used for law
enforcement purposes and any factors that FDA should consider--
particularly as it relates to civil rights and equity--related to the
scientific validity and accuracy of these tests.
In addition, tests exclusively used for public health surveillance
are distinct from other tests where: (1) they are intended solely for
use on systematically collected samples for analysis and interpretation
of health data in connection with disease prevention and control, and
(2) test results are not reported to patients or their healthcare
providers. These tests would not be affected by the phaseout policy.
The results of these tests are generally used for trending on a
population basis. Public health authorities also have access to test
results from non-surveillance tests that are FDA approved, cleared, or
authorized and that are reported under State reporting laws for
infectious and other diseases. In addition, during a public health
emergency, if there was a 564 declaration (as there was for past public
health emergencies), FDA could require test result reporting to public
health authorities under emergency use authorizations, as appropriate.
In 2017, FDA indicated support for less oversight of other
categories of tests, such as low-risk tests (class I devices), tests
currently on the market, and tests for rare diseases. However, FDA has
accumulated information in the intervening years that suggests we
should treat these categories of tests similarly to other FDA-regulated
tests. For example, as discussed above in section III.B, FDA has gained
additional information showing that there is a high variability in the
performance of IVDs offered as LDTs that are currently on the market,
including in circumstances where the test technology is relatively
simple and well-understood, where the tests are for rare diseases, and
where the tests are low risk. Among other things, FDA's recent
experience with tests for COVID-19 suggests that many tests
manufactured by laboratories are not appropriately validated.
Compliance with premarket review requirements (when applicable), QS
requirements, and registration and listing requirements would help
assure that these IVDs work as intended, enable FDA to keep track of
IVDs offered as LDTs (and, for example, help FDA locate IVDs that are
raising concerns or independently evaluate the risk status of marketed
IVDs), assist with FDA's inspection and planning efforts, and make
information available to patients and healthcare providers that may
inform the selection of particular IVDs for use. Therefore, FDA is now
proposing to end the general enforcement discretion approach, via a
phaseout approach, with respect to premarket review requirements (as
applicable), QS requirements, and registration and listing requirements
for these tests, in addition to medical device reporting (MDR)
requirements (i.e., reporting of adverse events), correction and
removal reporting requirements, and other requirements applicable to
such tests. Based on the information available at this time, FDA has
made a preliminary determination that this proposal appropriately
balances the relevant considerations with respect to these tests,
including currently marketed IVDs offered as LDTs.
However, FDA expects that some stakeholders will suggest that FDA
continue to maintain the current general enforcement discretion
approach with respect to premarket review and some or all QS
requirements for currently marketed LDTs or a subset of currently
marketed LDTs (i.e., what some previously referred to as
``grandfathering''). To the extent commenters suggest such an approach
for FDA's consideration, FDA requests information to support such an
approach, including the following:
Given the information in the ``Need for the Rule'' section
of this preamble in particular, what would be the public health
rationale for generally exercising enforcement discretion with respect
to premarket review and some or all QS requirements, for LDTs that are
being offered as of the date of issuance of this proposed rule and are
not changed with respect to indications for use or performance after
that date? Please provide data to support such an approach. Also, if
you think there are steps that might help support such an approach,
including ideas that might help to address the public health concerns
discussed in the ``Need for the Rule'' section, please describe them,
and include a rationale and any supporting evidence.
If commenters suggest maintaining the general enforcement
discretion approach with respect to premarket review and QS
requirements for a subset of LDTs (e.g., low and moderate risk LDTs)
currently on the market that are being offered as of the date of
issuance of this proposed rule and are not changed with respect to
indications for use or performance after that date, what would be the
public health rationale to support such an approach? Please provide any
data supporting such an approach. Also, if you think there are steps
that might help support such an approach, including ideas that might
help to address the public health concerns discussed in the ``Need for
the Rule'' section, please describe them and include a rationale and
any supporting evidence.
FDA recognizes that the phaseout of the general enforcement
discretion approach described in this section may have a relatively
greater impact on small laboratories. Therefore, FDA seeks comment on
the following:
Is there a public health rationale to have a longer
phaseout period for IVDs offered as LDTs by laboratories with annual
receipts below a certain threshold (e.g., $150,000) (see Table 43 in
the Preliminary Economic Analysis of Impacts (Ref. 34))? If so, please
provide relevant data and comment specifically on an alternative
recommended timeline.
In addition, FDA is aware that some AMCs have claimed that their
laboratories operate under unique circumstances (such as being
integrated into direct patient care) and therefore their tests should
be treated differently than tests manufactured by other laboratories.
Although FDA is not aware of an established definition of an AMC
laboratory, one possible description is: a laboratory for which a
certificate is in effect under CLIA and that meets the requirements
under CLIA to perform tests of high-complexity; that is part of an
accredited public or nonprofit private AMC that has a medical residency
training program or fellowship program related to test development,
application, and interpretation; and that is integrated into the direct
medical care for a patient, including specimen collection, testing,
interaction with the treating provider, and, as appropriate, patient
treatment based on the test, all at the same physical location. FDA
seeks comments on the following:
What are the characteristics of AMC laboratories? Do the
characteristics included above accurately describe
[[Page 68024]]
AMC laboratories and in fact distinguish them from other laboratories?
Should FDA continue the general enforcement discretion
approach with respect to any requirements, such as premarket review
requirements, for tests manufactured by AMC laboratories?
If FDA should continue the general enforcement discretion
approach with respect to any requirements, such as premarket review
requirements, for tests manufactured by AMC laboratories, are there any
additional considerations that should be taken into account with
respect to this approach, for example, whether an FDA cleared or
approved test is available for the same intended use as the test
manufactured by an AMC laboratory? Please provide a rationale and other
information (e.g., data) to support any additional considerations.
If FDA should have a different policy for AMC
laboratories, what would be the public health rationale to support such
a policy? For example, if integration of an AMC laboratory into direct
patient care is included as a basis for a different policy, please
include a public health rationale when explaining why and how such
integration supports the different policy, and how integration could
ensure that there is a reasonable assurance of IVD safety and
effectiveness.
If FDA should have a different policy for AMC
laboratories, is there evidence to support such a policy?
FDA also is interested in and seeks comment on leveraging programs
such as the New York State Department of Health Clinical Laboratory
Evaluation Program (NYSDOH CLEP) or those within the Veterans Health
Administration (VHA), as appropriate. In particular, FDA requests
comment on whether it may be appropriate to continue the general
enforcement discretion approach, such that FDA generally would not
enforce any applicable device requirements, where outside programs can
be leveraged. If FDA should continue to exercise enforcement discretion
under these circumstances:
What specific characteristics of and activities within
these programs justify such an approach?
Should the scope of such a policy be more limited for each
program in question? For example, should FDA continue enforcement
discretion for premarket review requirements and intend to enforce
other requirements, such as reporting adverse events?
Are there any additional considerations that should be
taken into account?
Please provide a rationale and other information (e.g., data) to
support any suggestions.
B. Stages
As previously discussed, FDA is proposing to gradually phase out
its current general enforcement discretion approach so that most IVDs
offered as LDTs would generally fall under the same enforcement
approach as other IVDs. In developing the proposed phaseout policy, FDA
has considered a number of factors, including the public health
importance of better assuring the safety and effectiveness of IVDs
offered as LDTs, the desire to avoid undue disruption to the testing
market, the time it may take for laboratories to come into compliance
with FDA requirements, the need for adequate resources to implement the
phaseout policy in a manner that does not undermine reasonable
expectations with regards to premarket review timing (per the Medical
Device User Fee Amendments (MDUFA) V agreement), and the benefits of a
relatively simple policy that can be easily understood and implemented.
Keeping these factors in mind, FDA has structured the phaseout policy
to contain five key stages:
Stage 1: End the general enforcement discretion approach
with respect to MDR requirements and correction and removal reporting
requirements 1 year after FDA publishes a final phaseout policy, which
FDA intends to issue in the preamble of the final rule.
Stage 2: End the general enforcement discretion approach
with respect to requirements other than MDR, correction and removal
reporting, QS, and premarket review requirements 2 years after FDA
publishes a final phaseout policy.
Stage 3: End the general enforcement discretion approach
with respect to QS requirements 3 years after FDA publishes a final
phaseout policy.
Stage 4: End the general enforcement discretion approach
with respect to premarket review requirements for high-risk IVDs 3\1/2\
years after FDA publishes a final phaseout policy, but not before
October 1, 2027.
Stage 5: End the general enforcement discretion approach
with respect to premarket review requirements for moderate risk and low
risk IVDs (that require premarket submissions) 4 years after FDA
publishes a final phaseout policy, but not before April 1, 2028.
Each of these stages is discussed in further detail below. For each
stage, FDA is proposing a period of time for laboratories to come into
compliance before FDA intends to end the general enforcement discretion
approach. FDA encourages laboratory manufacturers to begin early and
work toward compliance with requirements sooner than the end of the
specified timeframes. FDA also intends to consider providing more
targeted guidance and/or making additional resources available on
specific topics, such as compliance with applicable labeling
requirements, over the course of the phaseout period.
1. Stage 1: End the general enforcement discretion approach with
respect to MDR requirements and correction and removal reporting
requirements 1 year after FDA publishes a final phaseout policy.
FDA has structured the phaseout policy to obtain information about
potentially harmful IVDs offered as LDTs as soon as feasible. As
detailed elsewhere in this preamble, FDA is concerned that some of the
IVDs offered as LDTs may be posing risks to patients. Therefore, FDA is
prioritizing the phaseout of the general enforcement discretion
approach for requirements that would help FDA identify and monitor
significant issues with IVDs offered as LDTs, consistent with other
considerations described in this proposed policy.
Enforcement of the MDR requirements under 21 U.S.C. 360i(a) through
(c) and 21 CFR part 803, in particular, would enable FDA to
systematically monitor significant adverse events to identify
problematic IVDs offered as LDTs, such as those with poor performance
or other safety issues. FDA has made a preliminary determination that
gathering this information is important for IVDs that do not have the
safeguards associated with compliance with other FDA requirements, such
as manufacturing under QS requirements or confirmation of analytical
and clinical validity through premarket review.
For similar reasons, FDA is prioritizing the collection of
information about when a manufacturer has initiated a correction or
removal of its IVD to reduce a risk to health or to remedy a violation
of the FD&C Act that may present a risk to health. Under 21 U.S.C.
360i(g) and part 806 (21 CFR part 806), manufacturers are required to
report such corrections or removals to FDA, and FDA intends to phase
out the general enforcement discretion approach for these requirements
at the same time it does so for MDR requirements. Because FDA intends
for the phaseout of the general enforcement discretion approach with
respect to
[[Page 68025]]
correction and removal reporting requirements to occur before phaseout
of the general enforcement discretion approach with respect to
registration and listing requirements, FDA intends to exercise
enforcement discretion, such that it generally does not intend to
enforce, the requirement to use the establishment registration number
on such reports (21 CFR 806.10) when laboratories use their CLIA
certificate number instead prior to registering.
FDA's proposal to phase out enforcement discretion for MDR
requirements within 1 year after finalization of the policy is informed
by comments FDA received in response to the draft guidance documents
that FDA issued in 2014 proposing to implement an oversight framework
for IVDs offered as LDTs. In 2014, FDA proposed a 6-month timeline for
laboratory compliance with MDR requirements (Ref. 48), and we received
comments suggesting that a longer period may be appropriate for the
establishment of a system to identify, review, and report adverse
events. Based in part on those comments, FDA is now proposing a 1-year
time period for laboratories to come into compliance with the MDR
requirements. In conjunction with the phaseout of the general
enforcement discretion approach with respect to the MDR requirements,
FDA is also proposing to end the general enforcement discretion
approach with respect to the requirements of part 806, concerning
reports of corrections and removals. Because MDRs frequently are a
basis for corrections and removals, FDA views these requirements as
working together to provide information to FDA about issues with device
performance or quality. We anticipate that this 1-year time period is
adequate, particularly given that laboratories should already have some
processes in place for detecting problems with their IVDs to comply
with CLIA regulations.
2. Stage 2: End the general enforcement discretion approach with
respect to requirements not covered during other stages of the phaseout
policy 2 years after FDA publishes a final phaseout policy.
FDA is proposing to end the general enforcement discretion approach
for requirements besides MDR, correction and removal reporting, QS, and
premarket review requirements 2 years after the final policy is
published. These other requirements include registration and listing
requirements under 21 U.S.C. 360 and part 807 (excluding subpart E);
labeling requirements under 21 U.S.C. 352 and parts 801 and 809,
subpart B; and investigational use requirements under 21 U.S.C. 360j(g)
and part 812. We have included compliance with investigational use
requirements at this stage, in recognition that there has been some
confusion about our enforcement approach in this area. Our
understanding is that laboratories often are not complying with
investigational use requirements currently, even though FDA has
generally expected compliance with these requirements.\17\ We are
therefore including these requirements in the phaseout policy.
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\17\ For example, FDA stated in the ``Framework for Regulatory
Oversight of Laboratory Developed Tests (LDTs)'' draft guidance that
``FDA intends to continue to enforce investigational device
requirements under 21 CFR part 812 for all clinical investigations
of LDTs that are conducted under clinical protocols that require
institutional review board approval'' (Ref. 48).
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FDA recognizes that this proposal is different from FDA's prior
statements in the 2017 Discussion Paper regarding oversight of IVDs
manufactured by laboratories with respect to certain requirements, for
which the timing of FDA's expectations for compliance generally
depended on the type of premarket review applicable to the device.
However, upon review, FDA anticipates that it would better serve the
public health and be simpler to phase out the general enforcement
discretion approach for these requirements at the 2-year mark. For
example, under this timeline, laboratories could work toward compliance
with the stage 2 requirements without necessarily determining the risk
category of their IVDs until later stages of the proposed phaseout
policy. Another advantage of this timeline is that FDA would obtain
registration and listing information before the enforcement discretion
phaseout date for premarket review requirements, which could give the
Agency an initial understanding of the universe of IVDs offered as LDTs
to facilitate premarket review of those IVDs. Based on its experience,
FDA anticipates that 2 years is adequate time to come into compliance
with the various requirements.
3. Stage 3: End the general enforcement discretion approach with
respect to QS requirements 3 years after FDA publishes a final phaseout
policy.
At the 3-year mark, FDA would expect compliance with the device
CGMP requirements of the QS requirements under 21 U.S.C. 360j(f) and
part 820 (21 CFR part 820). However, for IVDs for which all
manufacturing activities occur within a single CLIA-certified
laboratory that meets the regulatory requirements to perform high
complexity testing and for which distribution of the IVD does not occur
outside that single laboratory, FDA would expect compliance at the 3-
year mark with some, but not all, of the QS requirements. Although FDA
and CMS regulation are different and complementary, compliance with
CLIA requirements provides some quality assurances that may be relevant
to laboratories' manufacturing practices. In particular, laboratories
may in practice be able to apply concepts set forth under CLIA
requirements for laboratory operations to manufacturing activities
regulated by FDA. For FDA to effectively leverage the CLIA assurances,
this proposed approach would apply only when all manufacturing
activities occur within a single laboratory and the IVD is not
distributed outside that laboratory. However, even in the context of
this approach, there are certain QS requirements for which CLIA
regulations do not provide the assurances that FDA requirements would
provide. These requirements include design controls under 21 CFR
820.30; purchasing controls (including supplier controls) under 21 CFR
820.50; acceptance activities (receiving, in-process, and finished
device acceptance) under 21 CFR 820.80 and 21 CFR 820.86; corrective
and preventative actions (CAPA) under 21 CFR 820.100; and records
requirements under part 820, subpart M. Because CLIA does not provide
assurances relevant to these requirements, FDA is proposing to end the
general enforcement discretion approach for these specific requirements
for IVDs for which all manufacturing activities occur within a single
CLIA-certified laboratory that meets the regulatory requirements to
perform high complexity testing, and which are not distributed outside
that laboratory, 3 years after finalizing this policy. For all other
IVDs offered as LDTs and subject to this phaseout policy, FDA is
proposing to end the general enforcement discretion approach for all QS
requirements 3 years after finalizing this policy.
Based on its experience, FDA anticipates that 3 years is adequate
time for laboratories to come into compliance with QS requirements. In
addition, based on the discussion above regarding concerns with the
quality and validation of IVDs offered as LDTs, FDA has made a
preliminary determination that phasing out the general enforcement
discretion approach for QS requirements later than 3 years would not be
in the best interest of the public health. Compliance with QS
requirements is critical to the quality and validity of IVDs offered as
LDTs.
[[Page 68026]]
For example, under the design controls of the QS requirements,
laboratories would, among other things, generally have better
procedures for validating the design of their tests, which would help
to ensure that they are analytically and clinically valid (see Ref.
76).
FDA also notes that on February 23, 2022, FDA proposed to amend the
device QS regulation, part 820, to align more closely with
international consensus standards for devices (87 FR 10119). As stated
in that proposed rule, the requirements, if finalized, would be
substantially similar to the requirements of the current part 820,
providing a similar level of assurance in a firm's quality management
system, and FDA intends for this phaseout policy to apply with respect
to any regulations promulgated through that rulemaking.
FDA intends to finalize amendments to the QS regulation
expeditiously, such that the amended QS requirements would be in effect
before the proposed beginning of stage 3. Upon the start of stage 3, or
if the laboratory complies with QS requirements prior to the start of
stage 3, FDA would expect compliance with the QS requirements that are
in effect at that time. For further information on the QS requirements
that would be established pursuant to the amendments to the QS
regulation, if finalized as proposed, please refer to the proposed
codified at 87 FR 10119 at 10133 and 10134. Notably, the requirements
relating to design controls, purchasing controls, acceptance
activities, CAPA, and records requirements are set forth in the
following ISO 13485 clauses as modified by the proposed codified for
part 820: Clause 4. Quality Management System, Subclause 4.2.5; Clause
6. Resource Management; Clause 7. Product Realization, Subclause 7.1,
Subclause 7.3, Subclause 7.4, and Subclause 7.4.3; and Clause 8.
Measurement, Analysis, & Improvement, Subclause 8.2.5, Subclause 8.2.6,
and Subclause 8.3.
In addition, FDA notes that under section 515(d)(2) of the FD&C
Act, the Agency may not approve a PMA if the applicant fails to
demonstrate conformity with the QS requirements. Therefore, compliance
with the QS requirements is needed to support approval of a PMA. As
provided in section 520(f)(2) of the FD&C Act, any person subject to
the QS requirements may petition for an exemption or variance from any
QS requirement (see also 21 CFR 820.1).
4. Stage 4: End the general enforcement discretion approach with
respect to premarket review requirements for high-risk IVDs 3\1/2\
years after FDA publishes a final phaseout policy, but not before
October 1, 2027.
FDA proposes that the phaseout date for the general enforcement
discretion approach with respect to premarket review requirements for
high-risk IVDs offered as LDTs (IVDs that may be eligible for
classification into class III) should occur 3\1/2\ years from the time
that FDA issues a final phaseout policy. The premarket review
requirements are set forth in 21 U.S.C. 360e and 21 CFR part 814. FDA
is proposing this time period because it is mindful that phasing out
the general enforcement discretion approach on a timeline that is too
short could cause undue disruption in the testing market. Among other
things, we anticipate that 3\1/2\ years would provide sufficient notice
and opportunity for laboratories manufacturing IVDs to plan for and
prepare PMAs and would appropriately account for any reliance
interests. We note that 3\1/2\ years is a longer time period than was
discussed in either the 2014 draft guidance documents or the 2017
Discussion Paper for the phaseout of the general enforcement discretion
approach for premarket review requirements.
This timeline is also intended to align the phaseout date for the
general enforcement discretion approach for premarket review
requirements for high-risk IVDs offered as LDTs with the start of
fiscal year 2028, which coincides with the beginning of a new user fee
cycle. This alignment would provide an opportunity for industry
participation in negotiations regarding the next user fee cycle with
the knowledge that laboratory manufacturers would be expected to comply
with premarket review requirements. (Although a trade association
representing laboratories previously has participated in MDUFA
negotiations, the prior negotiations have not incorporated similar
expectations regarding laboratory compliance with premarket
requirements.) Thus, we propose that this amount of time is appropriate
to foster stability and consistency in the marketplace for the current
MDUFA cycle, and would take into account the need for adequate FDA
resources to implement the phaseout policy in a manner that does not
compromise the capacity to achieve MDUFA V performance expectations.
FDA anticipates that during this 3\1/2\-year period, laboratories would
work with FDA to determine whether PMAs should be submitted for their
IVDs.
Under FDA's proposed policy, FDA generally would not intend to
enforce against IVDs offered as LDTs after a PMA has been submitted
(within the 3\1/2\-year timeframe) until FDA completes its review of
the application. Given that such IVDs may already be on the market and
available to patients, FDA generally does not intend to interrupt
access at the point when a submission is made.
Finally, FDA recognizes that the 2017 Discussion Paper described a
possible premarket-review approach specific to LDTs for unmet needs.
FDA has not included such an approach in this proposed policy because
we anticipate that the 3\1/2\-year timeframe should be sufficient for
laboratories to meet premarket review requirements for each of their
marketed IVDs, as applicable, including IVDs for unmet needs. FDA also
anticipates that programs currently in place may facilitate the
development and premarket authorization of IVDs for unmet needs. These
programs include the Humanitarian Use Devices (HUD)/Humanitarian Device
Exemption (HDE) program,\18\ which, among other things, provides an
exemption from the requirement to establish a reasonable assurance of
effectiveness for devices intended for use in the treatment or
diagnosis of rare diseases or conditions (21 U.S.C. 360j(m); 21 CFR
part 814, subpart H), and the Breakthrough Devices program, which is
intended to help expedite the development and review of certain devices
that provide for more effective treatment or diagnosis of life-
threatening or irreversibly debilitating diseases or conditions (21
U.S.C. 360e-3).
---------------------------------------------------------------------------
\18\ Under the proposed phaseout policy, laboratories that
intend to submit an HDE application should do so within the same
3\1/2\-year timeframe provided for submission of PMAs. As in the
case of PMAs, under FDA's proposed policy, FDA generally would not
intend to enforce against IVDs after an HDE application has been
submitted (within the 3\1/2\-year timeframe) until FDA completes its
review of the application.
5. Stage 5: End the general enforcement discretion approach with
respect to premarket review requirements for moderate risk and low
risk IVDs (that require premarket submissions) 4 years after FDA
---------------------------------------------------------------------------
publishes a final phaseout policy, but not before April 1, 2028.
FDA is proposing to end the general enforcement discretion approach
with respect to premarket review requirements for moderate risk IVDs
offered as LDTs (IVDs that may be eligible for classification into
class II) and low risk IVDs offered as LDTs (IVDs that may be eligible
for classification into class I) that require a premarket submission 4
years after FDA publishes the final phaseout policy. These premarket
submissions include 510(k) submissions, the requirements for which are
set forth at 21 U.S.C. 360(k),
[[Page 68027]]
360c(i), and part 807, subpart E. These submissions also include De
Novo requests, which laboratories may submit for IVDs offered as LDTs
for which there is no legally marketed device upon which to base a
determination of substantial equivalence, and for which the laboratory
seeks classification into class I or class II. These requirements are
set forth at 21 U.S.C. 360c(f)(2) and 21 CFR part 860, subpart D.
FDA intends this stage to begin no earlier than April 1, 2028.
FDA's reasons for proposing this time period to phase out the general
enforcement discretion approach with respect to premarket review
requirements for moderate risk and low risk IVDs offered as LDTs are
similar to those for the ``stage 4'' time period, except that FDA has
lengthened the time period by 6 months in order to prioritize the
review of applications for high-risk IVDs offered as LDTs (subject to
premarket approval requirements), so that FDA can focus first on IVDs
for which the consequences of a false result are most significant. FDA
also recognizes that a greater number of IVDs are subject to the 510(k)
requirements, as compared with premarket approval requirements, so a
longer period of time for laboratories to come into compliance with
these requirements may be appropriate, particularly for laboratories
with large test menus.
FDA generally would not intend to enforce against IVDs offered as
LDTs after a 510(k) or De Novo request has been submitted (within the
4-year timeframe) until FDA completes its review of the submission.
FDA also anticipates that laboratories may seek to utilize FDA's
Third Party review program. FDA currently operates a Third Party review
program for medical devices, and multiple organizations are accredited
to conduct reviews of 510(k) submissions for certain IVDs (see Ref.
77). We anticipate interest in the Third Party review program among
test manufacturers, as well as potential new Third Party review
organizations. In particular, FDA is aware of certain CLIA
accreditation organizations that may be interested in potentially
becoming Third Party reviewers under FDA's program, and to the extent
laboratories are already familiar with these organizations,
laboratories may be inclined to use the Third Party review program. In
addition, under the MDUFA V agreement, FDA is currently working to
enhance the Third Party review program, which may make it more
attractive to manufacturers including laboratories.
VII. Proposed Effective Date
The Agency proposes that any final rule based on this proposed rule
will become effective 60 days after the date of publication of the
final rule in the Federal Register.
VIII. Preliminary Economic Analysis of Impacts
We have examined the impacts of the proposed rule under Executive
Order 12866, Executive Order 13563, Executive Order 14094, the
Regulatory Flexibility Act (5 U.S.C. 601-612), and the Unfunded
Mandates Reform Act of 1995 (Pub. L. 104-4).
Executive Orders 12866, 13563, and 14094 direct us to assess all
benefits, costs, and transfers of available regulatory alternatives and
to select regulatory approaches that maximize net benefits (including
potential economic, environmental, public health and safety, and other
advantages; distributive impacts; and equity). Rules are
``significant'' under Executive Order 12866 Section 3(f)(1) (as amended
by Executive Order 14094) if they ``have an annual effect on the
economy of $200 million or more (adjusted every 3 years by the
Administrator of [the Office of Information and Regulatory Affairs
(OIRA)] for changes in gross domestic product); or adversely affect in
a material way the economy, a sector of the economy, productivity,
competition, jobs, the environment, public health or safety, or State,
local, territorial, or tribal governments or communities.'' OIRA has
determined that this proposed rule is a significant regulatory action
under Executive Order 12866 Section 3(f)(1).
The Regulatory Flexibility Act requires Agencies to analyze
regulatory options that would minimize any significant impact of a rule
on small entities. Because most facilities that will be affected by
this rule are defined as small businesses and the proposed rule is
likely to impose a substantial burden on the affected small entities,
we find that the proposed rule will have a significant economic impact
on a substantial number of small entities.
We prepared an analysis consistent with the Unfunded Mandates
Reform Act of 1995 (section 202(a)), which requires us to prepare a
written statement that includes estimates of anticipated impacts,
before proposing ``any rule that includes any Federal mandate that may
result in the expenditure by State, local, and tribal governments, in
the aggregate, or by the private sector, of $100,000,000 or more
(adjusted annually for inflation) in any one year.'' The current
threshold after adjustment for inflation is $177 million, using the
most current (2022) Implicit Price Deflator for the Gross Domestic
Product. This proposed rule would result in an expenditure in at least
one year that meets or exceeds this amount.
This proposed rule, if finalized, would amend FDA's regulations to
make explicit that IVDs are devices under the FD&C Act including when
the manufacturer of the IVD is a laboratory. As discussed in section
VI, FDA intends to phase out its general enforcement discretion
approach for LDTs so that IVDs manufactured by a laboratory would
generally fall under the same enforcement approach as other IVDs.
We anticipate that the benefits of phasing out FDA's general
enforcement discretion approach for LDTs would include a reduction in
healthcare costs associated with unsafe or ineffective tests, including
tests promoted with false or misleading claims, and from therapeutic
decisions based on the results of those tests. Quantified benefits are
the annualized sum of both health and non-health benefits. Unquantified
benefits would include the reduction in costs from lawsuits and
reduction in costs to healthcare systems.
Table 1 summarizes the annualized benefits, costs, and transfers of
the proposed rule. At a 7 percent discount rate, 20-year annualized
benefits range from $2.67 billion to $86.01 billion, with a primary
estimate of $31.41 billion per year. At a 3 percent discount rate, 20-
year annualized benefits range from $1.81 billion to $61.41 billion,
with a primary estimate of $22.33 billion per year. At a 7 percent
discount rate, 20-year annualized costs range from about $2.52 billion
to $19.45 billion, with a primary estimate of $5.87 billion per year.
At a 3 percent discount rate, annualized costs range from about $2.39
billion to $18.55 billion, with a primary estimate of $5.60 billion per
year. At a 7 percent discount rate, 20-year annualized transfers range
from $100 million to $452 million, with a primary estimate of $226
million per year. At a 3 percent discount rate, 20-year annualized
transfers range from $121 million to $538 million, with a primary
estimate of $269 million per year.
[[Page 68028]]
Table 1--Summary of Benefits, Costs and Transfers of the Proposed Rule
[Millions of 2022 U.S. dollars]
--------------------------------------------------------------------------------------------------------------------------------------------------------
Units
------------------------------------
Category Primary Low High Period Notes
estimate estimate estimate Year Discount covered
dollars rate (%) (years)
--------------------------------------------------------------------------------------------------------------------------------------------------------
Benefits:
Annualized Monetized ($m/year)............ $31,408 $2,670 $86,013 2022 7 20
22,332 1,810 61,413 2022 3 20
Annualized Quantified..................... .......... .......... .......... .......... 7
3
---------------------------------------------------------------------------------------------------------
Qualitative...............................
--------------------------------------------------------------------------------------------------------------------------------------------------------
Costs:
Annualized Monetized ($m/year)............ 5,874 2,522 19,452 2022 7 20 A portion of foreign costs could
5,598 2,394 18,549 2022 3 20 be passed on to domestic
consumers. We estimate that up
to $30.73 million in annualized
costs (7%, 20 years) to foreign
facilities could be passed on
to domestic consumers.
Annualized Quantified..................... .......... .......... .......... .......... 7
3
---------------------------------------------------------------------------------------------------------
Qualitative...............................
--------------------------------------------------------------------------------------------------------------------------------------------------------
Transfers:
Federal Annualized Monetized ($m/year).... 226 100 452 2022 7 20
269 121 538 2022 3 20
------------------------------------------------------------------------
From: Device Industry
To: FDA
---------------------------------------------------------------------------------------------------------
Other Annualized Monetized ($m/year)...... .......... .......... .......... .......... 7
3
------------------------------------------------------------------------
From:
To:
--------------------------------------------------------------------------------------------------------------------------------------------------------
Effects:
State, Local, or Tribal Government:.................................................................................................................
Small Business: The proposed rule is likely to have a significant economic impact on a substantial number of small laboratories that manufacture
IVDs offered as LDTs..
Wages:..............................................................................................................................................
Growth:.............................................................................................................................................
--------------------------------------------------------------------------------------------------------------------------------------------------------
We have developed a comprehensive Preliminary Economic Analysis of
Impacts that assesses the impacts of the proposed rule. The full
preliminary analysis of economic impacts is available in the docket for
this proposed rule (Ref. 34) and at https://www.fda.gov/about-fda/economics-staff/regulatory-impact-analyses-ria.
IX. Analysis of Environmental Impact
We have determined under 21 CFR 25.30(h) that this action is of a
type that does not individually or cumulatively have a significant
effect on the human environment. Therefore, neither an environmental
assessment nor an environmental impact statement is required.
X. Paperwork Reduction Act of 1995
FDA tentatively concludes that this proposed rule contains no new
collections of information. However, FDA does assume that there will
need to be corresponding adjustments to the burden estimates for
relevant approved collections of information before the relevant
phaseout stage begins and any such collection of information would not
be as a result of the implementation of the proposed rule. FDA
tentatively concludes that the following information collections will
need adjustment before the relevant phaseout stage begins: Office of
Management and Budget (OMB) control number 0910-0437, Medical Device
Reporting; OMB control number 0910-0359, Corrections and Removals; OMB
control number 0910-0625, Device Registration and Listing; OMB control
number 0910-0485, Labeling; OMB control number 0910-0078,
Investigational Device Exemption; OMB control number 0910-0073, Quality
Systems; OMB control number 0910-0231, Premarket Approval; OMB control
number 0910-0332, Humanitarian Device Exemption; OMB control number
0910-0756, Q-Submissions; OMB control number 0910-0120, Premarket
Notification; and OMB control number 0910-0844 De Novo. Such
adjustments will be submitted for review and clearance by OMB under the
Paperwork Reduction Act of 1995 (PRA) (44 U.S.C. 3501-3521).
XI. Federalism
We have analyzed this proposed rule in accordance with the
principles set forth in Executive Order 13132. We have determined that
this proposed rule does not contain policies that have substantial
direct effects on the States, on the relationship between the National
Government and the States, or on the distribution of power and
responsibilities among the various levels of government. Accordingly,
we conclude that the rule does not contain policies that have
federalism implications as defined in the Executive order and,
consequently, a federalism summary impact statement is not required.
Through publication of this proposed rule, we are providing notice and
an opportunity for State and local officials to comment on this
rulemaking.
XII. Consultation and Coordination With Indian Tribal Governments
We have analyzed this proposed rule in accordance with the
principles set forth in Executive Order 13175. We have tentatively
determined that the rule does not contain policies that would have a
substantial direct effect on
[[Page 68029]]
one or more Indian Tribes, on the relationship between the Federal
Government and Indian Tribes, or on the distribution of power and
responsibilities between the Federal Government and Indian Tribes. The
Agency solicits comments from tribal officials on any potential impact
on Indian Tribes from this proposed action.
XIII. Other Issues for Consideration
FDA anticipates that this proposed rule, if finalized, may require
conforming amendments to other FDA regulations, including provisions
regarding IVD labeling and ASRs in part 809. FDA intends to consider
and propose conforming amendments, where appropriate, at a future date.
In addition, we note that various bills have been introduced in
Congress that would change the legal status of IVDs as devices (under
these bills, IVDs would generally be regulated as ``in vitro clinical
tests'' and would be subject to new statutory authorities).\19\ We
recognize that the enactment of such legislation would directly impact
this rule, given that it is being proposed under the statutory device
authorities and other authorities under the FD&C Act.
---------------------------------------------------------------------------
\19\ See, e.g. H.R.4128--117th Congress (2021-2022): VALID Act
of 2021, H.R.4128, 117th Cong. (2021), https://www.congress.gov/bill/117th-congress/house-bill/4128/text; S.2209--117th Congress
(2021-2022): VALID Act of 2021, S.2209, 117th Cong. (2021), https://www.congress.gov/bill/117th-congress/senate-bill/2209.
---------------------------------------------------------------------------
XIV. References
The following references marked with an asterisk (*) are on display
at the Dockets Management Staff (see ADDRESSES) and are available for
viewing by interested persons between 9 a.m. and 4 p.m., Monday through
Friday; they also are available electronically at https://www.regulations.gov. References without asterisks are not on public
display at https://www.regulations.gov because they have copyright
restriction. Some may be available at the website address, if listed.
References without asterisks are available for viewing only at the
Dockets Management Staff. FDA has verified the website addresses, as of
the date this document publishes in the Federal Register, but websites
are subject to change over time.
1. Grand View Research, ``Laboratory Developed Tests Market
Size, Share & Trends Analysis Report By Technology (Immunoassay,
Molecular Diagnostics), By Application (Oncology, Nutritional &
Metabolic Disease), By Region, and Segment Forecasts, 2023-2030:
Report Summary,'' available at https://www.grandviewresearch.com/industry-analysis/laboratory-developed-tests-market-report (last
accessed on April 28, 2023).
2. The Pew Charitable Trusts, ``The Role of Lab-Developed Tests
in the In Vitro Diagnostics Market,'' October 2021. Available at
https://www.pewtrusts.org/en/research-and-analysis/reports/2021/10/the-role-of-lab-developed-tests-in-the-in-vitro-diagnostics-market.
* 3. Congressional Research Service, ``FDA Regulation of
Laboratory-Developed Tests (LDTs),'' December 7, 2022. Available at
https://crsreports.congress.gov/product/pdf/IF/IF11389.
* 4. Warning Letter to deCODE Genetics re: deCODEme Complete
Scan (June 10, 2010). Available at https://www.fda.gov/media/79216/download.
* 5. Warning Letter to 23andMe, Inc. re: 23andMe Personal Genome
Service (June 10, 2010). Available at https://web.archive.org/web/20191214010336/https:/www.fda.gov/media/79205/download.
6. ThermoFisher Scientific, ``Demystify Molecular Test
Development and Implementation: How Do Labs Implement Molecular
Tests To Meet Complex Clinical Needs?'' Available at https://www.thermofisher.com/us/en/home/clinical/clinical-genomics/molecular-diagnostics/molecular-diagnostic-education.html (last
accessed on March 28, 2023).
7. Lighthouse Lab Services, ``Industry Insights: Paths To
Consider When Commercializing Your LDT,'' December 19, 2022;
available at https://www.lighthouselabservices.com/paths-to-consider-when-commercializing-your-ldt/ (last accessed on March 31,
2023).
* 8. Centers for Disease Control and Prevention, Division of
Laboratory Systems (DLS), ``Strengthening Clinical Laboratories,''
November 15, 2018, available at https://www.cdc.gov/csels/dls/strengthening-clinical-labs.html (last accessed on March 31, 2023).
9. Ackerman, J.P., DC Bartos, J.D. Kapplinger, et al., ``The
Promise and Peril of Precision Medicine: Phenotyping Still Matters
Most,'' Mayo Clinic Proceedings, 91(11):1606-1616, 2016. Available
at https://doi.org/10.1016/j.mayocp.2016.08.008.
10. Begley, S., ``Genetic Testing Fumbles, Revealing `Dark Side'
of Precision Medicine,'' STAT, October 31, 2016. Available at
https://www.statnews.com/2016/10/31/genetic-testing-precision-medicine/.
* 11. FDA, ``The Public Health Evidence for FDA Oversight of
Laboratory Developed Tests: 20 Case Studies,'' November 16, 2015,
available at https://web.archive.org/web/20151122235012/https://www.fda.gov/downloads/AboutFDA/ReportsManualsForms/Reports/UCM472777.pdf.
12. Pfeifer, J.D., R. Loberg, C. Lofton-Day, et al., ``Reference
Samples To Compare Next-Generation Sequencing Test Performance for
Oncology Therapeutics and Diagnostics,'' American Journal of
Clinical Pathology, 157(4):628-638, 2022. Available at https://doi.org/10.1093/ajcp/aqab164.
13. Quy, P.N., K. Fukuyama, M. Kanai, et al., ``Inter-Assay
Variability of Next-Generation Sequencing-Based Gene Panels,'' BMC
Medical Genomics, 15: 86, 2022. Available at https://doi.org/10.1186/s12920-022-01230-y.
14. Vega, D.M., L.M. Yee, L.M. McShane, et al., ``Aligning Tumor
Mutational Burden (TMB) Quantification Across Diagnostic Platforms:
Phase II of the Friends of Cancer Research TMB Harmonization
Project,'' Annals of Oncology, 32(12):1626-1636, 2021. Available at
https://doi.org/10.1016/j.annonc.2021.09.016.
15. Offit, K., C.M. Sharkey, D. Green, et al., ``Regulation of
Laboratory-Developed Tests in Preventive Oncology: Emerging Needs
and Opportunities,'' Journal of Clinical Oncology, 41(1): 11-21,
2023. Available at https://doi.org/10.1200/jco.22.00995.
16. Coffey, D., ``Blood Test Positive for Cancer, but Is There
Really a Tumor?'' Medscape, February 17, 2023. Available at https://www.medscape.com/viewarticle/988431.
17. Manrai, A.K., B.H. Funke, H.L. Rehm, et al., ``Genetic
Misdiagnoses and the Potential for Health Disparities,'' New England
Journal of Medicine, 375(7):655-665, 2016. Available at https://doi.org/10.1056/NEJMsa1507092.
18. Shuren, J. and T. Stenzel, ``Covid-19 Molecular Diagnostic
Testing--Lessons Learned,'' New England Journal of Medicine,
387:e97, 2020. Available at https://doi.org/10.1056/nejmp2023830.
* 19. FDA, ``Policy for Coronavirus Disease-2019 Tests During
the Public Health Emergency (Revised)*; Guidance for Developers and
Food and Drug Administration Staff,'' November 15, 2021.
20. Clark, A., ``For a Host of Vital Lab Tests, No FDA Oversight
Exists,'' Undark Magazine, February 1, 2023. Available at https://undark.org/2023/02/01/for-a-host-of-vital-lab-tests-no-fda-oversight-exists/.
21. Clark, A., A. Gallardo, J. Deam, et al., ``They Trusted
Their Prenatal Test. They Didn't Know the Industry Is an Unregulated
`Wild West,''' ProPublica, December 6, 2022. Available at https://www.propublica.org/article/how-prenatal-screenings-have-escaped-regulation.
22. Kliff, S. and A. Bhatia, ``When They Warn of Rare Disorders,
These Prenatal Tests Are Usually Wrong,'' New York Times, January 1,
2022. Available at https://www.nytimes.com/2022/01/01/upshot/pregnancy-birth-genetic-testing.html.
23. Robinson, S.A., A.R. Carter, and D.A. Brindley, ``The
Changing Regulatory Landscape for Laboratory Developed Tests,''
Regulatory Focus, August 30, 2021. Available at https://www.raps.org/news-and-articles/news-articles/2021/8/the-changing-regulatory-landscape-for-laboratory-d.
24. Adashi, E.Y. and I.G. Cohen, ``SARS-CoV-2 Laboratory-
Developed Tests: Integrity Restored,'' JAMA, 2022;327(13):1229-1230.
Available at https://doi.org/10.1001/jama.2022.3382.
25. Rogus, S. and P. Lurie, ``FDA Is Letting Harmful Lab-
Developed Tests Fall Through the Cracks,'' MedPage Today, December
9, 2022. Available at https://www.medpagetoday.com/opinion/second-opinions/102161.
26. Damon, A., ``The COVID Testing Company That Missed 96% of
Cases,'' ProPublica, May 16, 2022. Available at https://www.propublica.org/article/covid-testing-nevada-false-negatives-northshore.
[[Page 68030]]
* 27. FDA, ``The FDA Warns Against the Use of Many Genetic Tests
With Unapproved Claims To Predict Patient Response to Specific
Medications: FDA Safety Communication,'' October 31, 2018. Available
at https://web.archive.org/web/20190909184258/https://www.fda.gov/medical-devices/safety-communications/fda-warns-against-use-many-genetic-tests-unapproved-claims-predict-patient-response-specific.
* 28. FDA, ``Genetic Non-Invasive Prenatal Screening Tests May
Have False Results: FDA Safety Communication,'' April 19, 2022.
Available at https://www.fda.gov/medical-devices/safety-communications/genetic-non-invasive-prenatal-screening-tests-may-have-false-results-fda-safety-communication.
* 29. FDA, ``Ovarian Cancer Screening Tests: Safety
Communication--FDA Recommends Against Use,'' September 7, 2016.
Available at https://web.archive.org/web/20160912081959/https:/www.fda.gov/Safety/MedWatch/SafetyInformation/SafetyAlertsforHumanMedicalProducts/ucm519540.htm?source=govdelivery&utm_medium=email&utm_source=govdelivery.
* 30. FDA, ``FDA Safety Communication: Breast Cancer Screening--
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List of Subjects in 21 CFR Part 809
Labeling, Medical devices.
Therefore, under the Federal Food, Drug, and Cosmetic Act and under
authority delegated to the Commissioner of Food and Drugs, FDA proposes
to amend 21 CFR part 809 as follows:
PART 809--IN VITRO DIAGNOSTIC PRODUCTS FOR HUMAN USE
0
1. The authority citation for part 809 is revised to read as follows:
Authority: 21 U.S.C. 321(h)(1), 331, 351, 352, 360, 360c, 360d,
360e, 360h, 360i, 360j, 371, 372, 374, 381.
0
2. In Sec. 809.3, revise the last sentence of paragraph (a) to read as
follows:
Sec. 809.3 Definitions.
(a) * * * These products are devices as defined in section
201(h)(1) of the Federal Food, Drug, and Cosmetic Act (the act) and may
also be biological products subject to section 351 of the Public Health
Service Act, including when the manufacturer of these products is a
laboratory.
* * * * *
Dated: September 27, 2023.
Robert M. Califf,
Commissioner of Food and Drugs.
[FR Doc. 2023-21662 Filed 9-29-23; 8:45 am]
BILLING CODE 4164-01-P
