List of Bulk Drug Substances That Can Be Used To Compound Drug Products in Accordance With Section 503A of the Federal Food, Drug, and Cosmetic Act, 91071-91082 [2016-30109]
Download as PDF
<![CDATA[
Federal Register / Vol. 81, No. 242 / Friday, December 16, 2016 / Proposed Rules
Report SE–623, Issue 16’’). Accomplishing
the revision required by this paragraph
terminates the requirements of paragraph (g)
of this AD. Accomplishing the revision
required by this paragraph also terminates
the requirements of paragraph (g) of AD
2012–12–07.
(1) The initial compliance times for the
tasks specified in Fokker Services B.V.
Engineering Report SE–623, Issue 16, are at
the later of the applicable compliance times
specified in Fokker Services B.V. Engineering
Report SE–623, Issue 16, or within 30 days
after the effective date of this AD, whichever
is later.
(2) If any discrepancy is found, before
further flight, repair using a method
approved by the Manager, International
Branch, ANM–116, Transport Airplane
Directorate, FAA; or the EASA; or Fokker
B.V. Service’s EASA DOA.
asabaliauskas on DSK3SPTVN1PROD with PROPOSALS
(l) No Alternative Actions or Intervals
After the maintenance or inspection
program, as applicable, has been revised as
required by paragraph (k) of this AD, no
alternative actions (e.g., inspections) or
intervals may be used unless the actions or
intervals are approved as an AMOC in
accordance with the procedures specified in
paragraph (m)(1) of this AD.
(m) Other FAA AD Provisions
The following provisions also apply to this
AD:
(1) Alternative Methods of Compliance
(AMOCs): The Manager, International
Branch, ANM–116, Transport Airplane
Directorate, FAA, has the authority to
approve AMOCs for this AD, if requested
using the procedures found in 14 CFR 39.19.
In accordance with 14 CFR 39.19, send your
request to your principal inspector or local
Flight Standards District Office, as
appropriate. If sending information directly
to the International Branch, send it to ATTN:
Tom Rodriguez, Aerospace Engineer,
International Branch, ANM–116, Transport
Airplane Directorate, FAA, 1601 Lind
Avenue SW., Renton, WA 98057–3356;
telephone 425–227–1137; fax 425–227–1149.
Information may be emailed to: 9-ANM-116AMOC-REQUESTS@faa.gov. Before using
any approved AMOC, notify your appropriate
principal inspector, or lacking a principal
inspector, the manager of the local flight
standards district office/certificate holding
district office.
(2) Contacting the Manufacturer: As of the
effective date of this AD, for any requirement
in this AD to obtain corrective actions from
a manufacturer, the action must be
accomplished using a method approved by
the Manager, International Branch, ANM–
116, Transport Airplane Directorate, FAA; or
EASA; or Fokker B.V. Services’ EASA DOA.
If approved by the DOA, the approval must
include the DOA-authorized signature.
(n) Related Information
(1) Refer to Mandatory Continuing
Airworthiness Information (MCAI) EASA AD
2016–0125, dated June 21, 2016, for related
information. You may examine the MCAI on
the Internet at https://www.regulations.gov by
searching for and locating Docket No. FAA–
2016–9435.
VerDate Sep<11>2014
18:25 Dec 15, 2016
Jkt 241001
(2) For service information identified in
this AD, contact Fokker Services B.V.,
Technical Services Dept., P.O. Box 1357,
2130 EL Hoofddorp, the Netherlands;
telephone: +31 (0)88–6280–350; fax: +31
(0)88–6280–111; email: technicalservices@
fokker.com; Internet https://
www.myfokkerfleet.com. You may view this
service information at the FAA, Transport
Airplane Directorate, 1601 Lind Avenue SW.,
Renton, WA. For information on the
availability of this material at the FAA, call
425–227–1221.
Issued in Renton, Washington, on
November 17, 2016.
Phil Forde,
Acting Manager, Transport Airplane
Directorate, Aircraft Certification Service.
[FR Doc. 2016–28669 Filed 12–15–16; 8:45 am]
BILLING CODE 4910–13–P
DEPARTMENT OF HEALTH AND
HUMAN SERVICES
Food and Drug Administration
21 CFR Part 216
[Docket No. FDA–2016–N–3464]
RIN 0910–AH29
List of Bulk Drug Substances That Can
Be Used To Compound Drug Products
in Accordance With Section 503A of
the Federal Food, Drug, and Cosmetic
Act
AGENCY:
Food and Drug Administration,
HHS.
ACTION:
Proposed rule.
The Food and Drug
Administration (FDA or Agency) is
proposing a regulation to identify an
initial list of bulk drug substances that
can be used to compound drug products
in accordance with certain
compounding provisions of the Federal
Food, Drug, and Cosmetic Act (the
FD&C Act), although they are neither
the subject of an applicable United
States Pharmacopeia (USP) or National
Formulary (NF) monograph nor
components of FDA-approved drugs.
Specifically, the Agency proposes to
place six bulk drug substances on the
list. This proposed rule also identifies
four bulk drug substances that FDA has
considered and proposes not to include
on the list. Additional substances
nominated by the public for inclusion
on this list are currently under
consideration and will be the subject of
a future rulemaking.
DATES: Submit either electronic or
written comments on the bulk drug
substances list by March 16, 2017. See
section VI for the proposed effective
SUMMARY:
PO 00000
Frm 00023
Fmt 4702
Sfmt 4702
91071
date of a final rule based on this
proposed rule.
ADDRESSES: You may submit comments
as follows:
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): Division of
Dockets Management (HFA–305), Food
and Drug Administration, 5630 Fishers
Lane, Rm. 1061, Rockville, MD 20852.
• For written/paper comments
submitted to the Division of Dockets
Management, 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–
2016–N–3464 for ‘‘List of Bulk Drug
Substances That Can Be Used To
Compound Drug Products in
Accordance With Section 503A of the
Federal Food, Drug, and Cosmetic Act.’’
Received comments will be placed in
the docket and, except for those
submitted as ‘‘Confidential
Submissions,’’ publicly viewable at
https://www.regulations.gov or at the
Division of Dockets Management
between 9 a.m. and 4 p.m., Monday
through Friday.
E:\FR\FM\16DEP1.SGM
16DEP1
91072
Federal Register / Vol. 81, No. 242 / Friday, December 16, 2016 / Proposed Rules
• 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 Division of Dockets
Management. 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.fda.gov/
regulatoryinformation/dockets/
default.htm.
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 Division of Dockets
Management, 5630 Fishers Lane, Rm.
1061, Rockville, MD 20852.
FOR FURTHER INFORMATION CONTACT:
James Flahive, Center for Drug
Evaluation and Research, Food and
Drug Administration, 10903 New
Hampshire Ave., Bldg. 51, Rm. 5108,
Silver Spring, MD 20993–0002, 301–
796–9293.
SUPPLEMENTARY INFORMATION:
asabaliauskas on DSK3SPTVN1PROD with PROPOSALS
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 and Acronyms
Commonly Used in This Document
III. Background
A. Statutory and Regulatory Background
B. Regulatory History of the 503A Bulks
List
VerDate Sep<11>2014
18:25 Dec 15, 2016
Jkt 241001
C. Requests for Nominations
IV. Legal Authority
V. Description of the Proposed Rule
A. Criteria for Evaluating Bulk Drug
Substances for the 503A Bulks List
B. Methodology for Developing the 503A
Bulks List
C. Substances Proposed for Inclusion on
the 503A Bulks List
D. Substances Considered and Not
Proposed for Inclusion on the 503A
Bulks List
VI. Proposed Effective Date
VII. Analysis of Environmental Impact
VIII. Economic Analysis of Impacts
A. Summary of the Costs of the Rule
B. Summary of the Benefits of the Rule
C. Summary of the Impact on Small
Entities
IX. Paperwork Reduction Act of 1995
X. Federalism
XI. References
I. Executive Summary
A. Purpose of the Proposed Rule
FDA is proposing to amend its
regulations to add a list of bulk drug
substances that can be used in
compounding under section 503A of the
FD&C Act (21 U.S.C. 353a) (referred to
as ‘‘the 503A Bulks List’’). Bulk drug
substances that appear on the 503A
Bulks List can be used to compound
drug products subject to the conditions
of section 503A, although those
substances are not the subject of a USP
or NF monograph or components of
approved drug products.
B. Summary of the Major Provisions of
the Proposed Rule
FDA is proposing to establish the
criteria by which bulk drug substances
will be evaluated for inclusion on the
503A Bulks List. Based on the results of
its evaluation of nominated bulk drug
substances to date, as well as
consultation with the Pharmacy
Compounding Advisory Committee
(PCAC), FDA is also proposing to
include six bulk drug substances on the
list: Brilliant Blue G, also known as
Coomassie Brilliant Blue G–250;
cantharidin (for topical use only);
diphenylcyclopropenone (for topical
use only); N-acetyl-D-glucosamine (for
topical use only); squaric acid dibutyl
ester (for topical use only); and thymol
iodide (for topical use only) and that
four other substances not be included
on the list: Oxitriptan, piracetam, silver
protein mild, and tranilast.
C. Legal Authority
Section 503A of the FD&C Act, in
conjunction with our general
rulemaking authority in section 701(a)
of the FD&C Act (21 U.S.C. 371(a)),
serves as our principal legal authority
for this proposed rule.
PO 00000
Frm 00024
Fmt 4702
Sfmt 4702
D. Costs and Benefits
FDA is proposing to place six bulk
substances on the 503A Bulks List and
not to place four bulk substances on the
503A Bulks List. Because we lack
sufficient information to quantify the
costs and benefits of this proposed rule,
we include a qualitative description of
potential benefits and potential costs.
We expect that the rule would affect
compounding pharmacies and other
entities that market the affected
substances or drug products made from
the affected substances, consumers of
drug products containing the affected
drug substances, and payers that cover
these drug products or alternative drug
products.
II. Table of Abbreviations and
Acronyms Commonly Used in This
Document
5-HTP 5-hydroxytryptophan
BLA Biologics License Application
CFR Code of Federal Regulations
CSA Controlled Substances Act
DPCP Diphenylcyclopropenone
DQSA Drug Quality and Security Act
FD&C Act Federal Food, Drug, and
Cosmetic Act
FDA Food and Drug Administration
IND Investigational New Drug
NAG N-acetyl-D-glucosamine
NAICS North American Industry
Classification System
NF National Formulary
NPRM Notice of Proposed Rulemaking
OTC Over-The-Counter
PCAC Pharmacy Compounding Advisory
Committee
PHS Act Public Health Service Act
PRESTO Prevention of REStenosis with
Tranilast and its Outcomes
RFA Regulatory Flexibility Analysis
SADBE Squaric acid dibutyl ester
SBA Small Business Administration
UGT1A1 Uridine diphosphate
glucuronosyltransferase 1A1
UK United Kingdom
USP United States Pharmacopeia
III. Background
A. Statutory and Regulatory Background
Section 503A of the FD&C Act (21
U.S.C. 353a) describes the conditions
under which a compounded drug
product may qualify for an exemption
from certain sections of the FD&C Act.
Those conditions include that a licensed
pharmacist in a State-licensed pharmacy
or Federal facility or a licensed
physician compounds the drug product
using bulk drug substances that: (1)
Comply with the standards of an
applicable USP or NF monograph,1 if a
1 FDA has interpreted the statutory language
‘‘applicable USP or NF monographs’’ to refer to
official USP or NF drug substance monographs.
Therefore, a substance that is the subject of a
dietary supplement monograph, but not a USP or
NF drug substance monograph, does not satisfy the
E:\FR\FM\16DEP1.SGM
16DEP1
asabaliauskas on DSK3SPTVN1PROD with PROPOSALS
Federal Register / Vol. 81, No. 242 / Friday, December 16, 2016 / Proposed Rules
monograph exists, and the USP chapter
on pharmacy compounding; (2) if such
a monograph does not exist, are drug
substances that are components of drugs
approved by the Secretary; or (3) if such
a monograph does not exist and the
drug substance is not a component of a
drug approved by the Secretary, that
appear on the 503A Bulks List. See
section 503A(b)(1)(A)(i) of the FD&C
Act. This proposed rule proposes
criteria for evaluating substances for
inclusion on the 503A Bulks List and
identifies six substances the Secretary
proposes to place on the list. The
Agency considered four other
substances and is proposing not to
include those substances on the 503A
Bulks List. Additional substances are
under evaluation, and new substances
may be added to the list through
subsequent rulemaking.
Section 503A adopts the definition of
‘‘bulk drug substance’’ in FDA’s drug
establishment registration and listing
regulations, which was codified at
§ 207.3(a)(4) (21 CFR 207.3(a)(4)) at the
time section 503A was enacted. See
section 503A(b)(1)(A) of the FD&C Act.
Under the definition, bulk drug
substance means any substance that is
represented for use in a drug and that,
when used in the manufacturing,
processing, or packaging of a drug,
becomes an active ingredient or a
finished dosage form of the drug, but the
term does not include intermediates
used in the synthesis of such
substances.
On August 31, 2016, FDA published
a final rule in the Federal Register to
update its registration and listing
regulations in part 207 (21 CFR part
207), which included minor changes to
the definition of bulk drug substance
and moved the definition to § 207.3 (see
81 FR 60170). This definition becomes
effective on November 29, 2016. As set
forth in § 207.3, ‘‘bulk drug substance,’’
as referenced in section 503A(b)(1)(A) of
the FD&C Act, means the same as
‘‘active pharmaceutical ingredient’’ as
defined in § 207.1(b). An ‘‘active
pharmaceutical ingredient’’ is any
substance that is intended for
incorporation into a finished drug
product and is intended to furnish
pharmacological activity or other direct
effect in the diagnosis, cure, mitigation,
treatment, or prevention of disease, or to
affect the structure or any function of
the body. Active pharmaceutical
ingredient does not include
condition regarding bulk drug substances in section
503A(b)(1)(A)(i)(I) of the Act. Such a substance may
only be used as a bulk drug substance under section
503A of the FD&C Act if it is a component of an
FDA-approved drug product or is on the 503A
Bulks List.
VerDate Sep<11>2014
18:25 Dec 15, 2016
Jkt 241001
intermediates used in the synthesis of
the substance (§ 207.1).
Inactive ingredients used in
compounded drug products, such as
flavorings, dyes, or diluents, need not
appear on the 503A Bulks List to be
eligible for use in compounding drug
products and will not be included on
the list.
B. Regulatory History of the 503A Bulks
List
Section 503A of the FD&C Act was
enacted in 1997. In the Federal Register
of April 7, 1998 (63 FR 17011), FDA
invited all interested persons to
nominate bulk drug substances for
inclusion on the 503A Bulks List. In
1998, FDA received nominations for 41
different drug substances. Ten of these
drug substances were the subject of an
applicable USP or NF monograph or
were components of FDA-approved
drugs and did not need to go on the list
to be used in compounding. After
evaluating the nominated drug
substances and consulting with the
PCAC as required by section 503A(c)(2),
FDA published a proposed rule listing
20 drug substances for potential
inclusion on the initial section 503A
Bulks List (64 FR 996, January 7, 1999)
(the 1999 Proposed 503A Bulks List).
The proposed rule also described 10
nominated drug substances that were
still under consideration for the 503A
Bulks List. The PCAC reconvened in
May 1999 to discuss bulk drug
substances included in the proposed
rule, in addition to other bulk drug
substances (see 64 FR 19791, April 22,
1999).
In February 2001, the U.S. Court of
Appeals for the Ninth Circuit held that
certain provisions of section 503A of the
FD&C Act were unconstitutional
restrictions on commercial speech. (See
Western States Med. Ctr. v. Shalala, 238
F.3d 1090 (9th Cir. 2001).) Furthermore,
the Ninth Circuit held that the
advertising and solicitation provisions
could not be severed from the rest of
section 503A and, as a result, found
section 503A of the FD&C Act to be
invalid in its entirety. In April 2002, the
U.S. Supreme Court affirmed the Ninth
Circuit’s decision that the advertising
and solicitation provisions were
unconstitutional; it did not, however,
rule on the severability of section 503A
of the FD&C Act. (See Thompson v.
Western States Med. Ctr., 535 U.S. 357
(2002).) In 2008, the U.S. Court of
Appeals for the Fifth Circuit held that
compounded drugs are subject to
regulation by FDA, and that the
advertising and solicitation provisions
are severable from the rest of section
503A of the FD&C Act. (See Medical Ctr.
PO 00000
Frm 00025
Fmt 4702
Sfmt 4702
91073
Pharm. v. Mukasey, 536 F.3d 383 (5th
Cir. 2008).)
Following a fungal meningitis
outbreak in September 2012, FDA
sought legislation to, among other
things, resolve the split in the Circuits
to clarify that section 503A of the FD&C
Act was valid nationwide. On
November 27, 2013, President Obama
signed the Drug Quality and Security
Act (Pub. L. 113–54) (DQSA), which
contains important provisions relating
to the oversight of human drug product
compounding. Among other things, the
DQSA removed from section 503A of
the FD&C Act the provisions that had
been held unconstitutional by the U.S.
Supreme Court in 2002. By removing
these provisions, the DQSA clarified
that section 503A of the FD&C Act
applies nationwide.
C. Requests for Nominations
Because of the amount of time that
had passed between the publication of
the 1999 proposed rule and the
enactment of the DQSA, FDA felt it was
necessary to begin again to develop the
503A Bulks List. In the Federal Register
of December 4, 2013 (78 FR 72841), FDA
published a notice withdrawing the
1999 proposed rule and inviting all
interested persons to nominate bulk
drug substances for inclusion on the
503A Bulks List.
Over 2,000 substances were
nominated. However, many of those
nominations were for a substance that is
the subject of an applicable USP or NF
monograph or a component of an FDAapproved drug, were not for substances
used in compounding as active
ingredients, or did not include sufficient
information for FDA to evaluate
whether the substances should be
proposed for inclusion on the 503A
Bulks List. To improve the efficiency of
the process for developing the 503A
Bulks List, FDA reopened the
nomination process in July 2014 (79 FR
37747, July 2, 2014) and provided a
more detailed description about what
information should be included in a
nomination to support the Agency’s
evaluation. FDA stated that bulk drug
substances that were previously
nominated would not be further
considered unless they were
renominated and the new nominations
were adequately supported. Substances
that were already eligible for use in
compounding or that were not
adequately supported would not be
placed on the list.
In response to that solicitation,
approximately 740 unique substances
were nominated. Of those substances,
approximately 315 are components of
an FDA-approved drug product or the
E:\FR\FM\16DEP1.SGM
16DEP1
asabaliauskas on DSK3SPTVN1PROD with PROPOSALS
91074
Federal Register / Vol. 81, No. 242 / Friday, December 16, 2016 / Proposed Rules
subject of an applicable USP or NF
monograph. Such substances can be
used in compounding under section
503A(b)(1)(A)(i)(I) and (II) of the FD&C
Act and, therefore, are not eligible for
inclusion on the 503A Bulks List.
At least one of the nominated
substances is a finished drug product
that was nominated by its brand name.
Finished drug products are not eligible
for the 503A Bulks List because they do
not meet the definition of a bulk drug
substance in § 207.3(4).
At least one of the nominated
substances is a biological product
subject to approval in a biologics license
application (BLA) under section 351 of
the Public Health Service (PHS) Act (42
U.S.C. 262) when used for the
indication proposed in the nomination.
This substance is not eligible for the
503A Bulks List because biological
products subject to approval in a BLA
under section 351 of the PHS Act are
not eligible for the exemptions in
section 503A of the FD&C Act. No
biological products subject to approval
in a BLA will be considered for the
503A Bulks List.
At least four of the nominated
substances appear on the list published
by FDA of substances that have been
withdrawn or removed from the market
because the drug products or
components of the drug products have
been found to be unsafe or not effective
(section 503A(b)(1)(C) of the FD&C Act)
(Withdrawn or Removed List). Such
substances cannot be used in
compounding under section 503A of the
FD&C Act, and therefore, are not eligible
for inclusion on the 503A Bulks List.
One of the nominated substances has
no currently accepted medical use and
is included on Schedule I of the
Controlled Substances Act (CSA) (21
U.S.C. 812(c)). The CSA does not allow
possession or distribution of Schedule I
substances (see 21 U.S.C. 841(a)(1) and
829), except for research purposes (see
21 U.S.C. 823(f)), and Schedule I
substances will not be considered for
the 503A Bulks List. Those desiring to
do research on a Schedule I substance
may apply to do so under an
investigational new drug (IND)
application.
Of the substances that are not
components of an approved drug
product or the subject of an applicable
USP or NF monograph, finished drug
products, biological products subject to
licensure in a BLA, and do not appear
on the Withdrawn or Removed List or
Schedule I of the CSA, about 350
substances were nominated with
insufficient supporting evidence for
FDA to evaluate them.
VerDate Sep<11>2014
18:25 Dec 15, 2016
Jkt 241001
The remaining substances may be
eligible for inclusion on the 503A Bulks
List and were nominated with sufficient
supporting information for FDA to
evaluate them. Ten of those substances
have been evaluated and are discussed
in section V. The rest will be discussed
in future notices of proposed
rulemaking (NPRMs) after they have
been evaluated. Once the Agency
completes its review of the substances
that were nominated for the 503A Bulks
List with adequate supporting
information under the July 2, 2014,
request for nominations, FDA will
consider additional substances
nominated for inclusion on the list if
they are eligible and adequate
supporting information is submitted to
permit FDA to meaningfully evaluate
them (see section III).
With regard to the substances
nominated with sufficient supporting
information for FDA to evaluate them,
including the 10 nominated substances
discussed in this proposed rule, FDA
generally does not intend to take
regulatory action against a Statelicensed pharmacy, Federal facility, or
licensed physician for compounding a
drug product using a bulk drug
substance that is not the subject of an
applicable USP or NF monograph or a
component of an FDA-approved drug
product, provided that the other
conditions in section 503A and the
FD&C Act are met, until the substance
is addressed in a final rule. FDA is not
applying this interim policy to a
nominated substance however, if the
Agency has identified the substance as
posing a significant safety risk,2 or if the
substance was nominated without
adequate support. For further
information on this subject, see the
guidance for industry entitled ‘‘Interim
Policy on Compounding Using Bulk
Drug Substances Under Section 503A of
the Federal Food, Drug, and Cosmetic
Act’’ (Ref. 1). As described in the
guidance, the following categories of
bulk drug substances are identified on
FDA’s Web site at https://www.fda.gov/
downloads/Drugs/GuidanceCompliance
RegulatoryInformation/
PharmacyCompounding/
UCM467373.pdf: (1) The substances
nominated with sufficient supporting
information that are under evaluation,
(2) the substances nominated with
sufficient supporting information but
with which FDA has identified
significant safety risks relating to the
2 This is not a determination regarding whether
the substances will be added to the 503A Bulks list.
FDA intends to make that determination after notice
and comment rulemaking, as set forth in this
proposal.
PO 00000
Frm 00026
Fmt 4702
Sfmt 4702
use of these bulk drug substances in
compounding, and (3) the substances
nominated with insufficient supporting
evidence for FDA to evaluate them.
IV. Legal Authority
As described in the Background
section, section 503A of the FD&C Act
describes the conditions that must be
satisfied for human drug products
compounded by a licensed pharmacist
or licensed physician to be exempt from
three sections of the FD&C Act (sections
501(a)(2)(B), 502(f)(1), and 505 (21
U.S.C. 351(a)(2)(B), 352(f)(1), and 355)).
One of the conditions that must be
satisfied for a compounded drug to
qualify for the exemptions under section
503A of the FD&C Act is that a licensed
pharmacist in a State-licensed pharmacy
or Federal facility or a licensed
physician compounds the drug product
using bulk drug substances that: (1)
Comply with the standards of an
applicable USP or NF monograph, if a
monograph exists, and the USP chapter
on pharmacy compounding; (2) if such
a monograph does not exist, are drug
substances that are components of drugs
approved by the Secretary; or (3) if such
a monograph does not exist and the
drug substance is not a component of a
drug approved by the Secretary, that
appear on the 503A Bulks List. See
section 503A(b)(1)(A)(i) of the FD&C
Act. Section 503A(c)(1) of the FD&C Act
also states that the Secretary shall issue
regulations to implement section 503A,
and that before issuing regulations to
implement section 503A(b)(1)(A)(i)(III)
pertaining to the 503A bulks list, among
other sections, the Secretary shall
convene and consult an advisory
committee on compounding unless the
Secretary determines that the issuance
of such regulations before consultation
is necessary to protect the public health.
Section 503A(c)(2) of the FD&C Act
requires the Secretary to issue the
regulations in consultation with the
USP, and to include in the regulation
the criteria for such substances that
shall include historical use, reports in
peer reviewed journals, and any other
criteria the Secretary identifies. Thus,
section 503A of the FD&C Act, in
conjunction with our general
rulemaking authority in section 701(a)
of the FD&C Act, serves as our principal
legal authority for this proposed rule.
V. Description of the Proposed Rule
FDA is proposing to add § 216.23 to
title 21 of the Code of Federal
Regulations (CFR) to set forth criteria to
evaluate bulk drug substances for
inclusion on the 503A Bulks List.
Additionally, after considering 10 bulk
drug substances for the 503A Bulks List,
E:\FR\FM\16DEP1.SGM
16DEP1
Federal Register / Vol. 81, No. 242 / Friday, December 16, 2016 / Proposed Rules
asabaliauskas on DSK3SPTVN1PROD with PROPOSALS
FDA proposes to codify the initial 503A
Bulks List to include 6 of the bulk drug
substances that were considered and to
identify 4 substances that were
considered and would not be placed on
the list. The criteria and the bulk drug
substances considered for inclusion on
the list are described in the paragraphs
that follow.
A. Criteria for Evaluating Bulk Drug
Substances for the 503A Bulks List
Section 503A(c)(2) of the FD&C Act
provides that the criteria for
determining which substances should
appear on the 503A Bulks List shall
include historical use, reports in peer
reviewed medical literature, or other
criteria the Secretary of Health and
Human Services may identify.
Consistent with the July 2, 2014,
Federal Register notice (79 FR 37747)
soliciting nominations for this list, and
as presented to and discussed with the
PCAC in February 2015 (Ref. 2), FDA
proposes that the following criteria be
used to evaluate the nominated
substances:
• The physical and chemical
characterization of the substance;
• Any safety issues raised by the use
of the substance in compounded drug
products;
• The available evidence of
effectiveness or lack of effectiveness of
a drug product compounded with the
substance, if any such evidence exists;
and
• Historical use of the substance in
compounded drug products, including
information about the medical
condition(s) the substance has been
used to treat and any references in peerreviewed medical literature.
In evaluating candidates for the 503A
Bulks List under these criteria, the
Agency proposes to use a balancing test.
Specifically, the Agency proposes to
consider each criterion in the context of
the others and balance them, on a
substance-by-substance basis, to decide
whether a particular substance is
appropriate for inclusion on the 503A
Bulks List.
Under the first criterion, the physical
and chemical characterization of the
substance, FDA would consider each
substance’s purity, identity, and quality.
Based on attributes such as the
substance’s molecular structure,
stability, melting point, appearance,
likely impurities, and solubilities, FDA
would determine whether the substance
can be identified consistently based on
its physical and chemical
characteristics. If a substance cannot be
well characterized chemically and
physically, the Agency proposes that
this criterion weigh against its inclusion
VerDate Sep<11>2014
18:25 Dec 15, 2016
Jkt 241001
on the 503A Bulks List because there
can be no assurance that its properties
and toxicities, when used in
compounding, would be the same as the
properties and toxicities reported in the
literature and considered by the Agency.
Under the second criterion, FDA
would consider the safety issues raised
by the use of each substance in
pharmacy compounding. Based on
FDA’s review of the substances
nominated to date, it is unlikely that
candidates for the 503A Bulks List will
have been thoroughly investigated in in
vitro or in animal toxicology studies, or
that there will be well-controlled
clinical trials to substantiate their safe
use in humans. Thus, in evaluating list
candidates, the Agency is likely to have
at its disposal very limited information,
or in some cases no information, of the
type and quality that is ordinarily
required and evaluated as part of the
drug approval process.
To evaluate the safety of the
substances then, the Agency proposes to
rely on available information, including
reports in peer-reviewed medical
literature, about each substance’s
pharmacology, acute toxicity, repeat
dose toxicity, mutagenicity,
developmental and reproductive
toxicity, and carcinogenicity. The
Agency would also rely on reports and
abstracts in the literature about adverse
reactions the substances have caused in
humans. In applying the safety criterion,
FDA also proposes to consider the
availability of approved drug products
or drug products that follow an OTC
monograph (OTC monograph products).
The existence of approved drug
products or OTC monograph products
would likely weigh against inclusion on
the proposed list when the toxicity of a
particular substance appears to be
significant or where there are other
safety concerns associated with the use
of the substance in compounded drug
products.
Under the third criterion, FDA
proposes to consider the available
evidence of the substance’s effectiveness
or lack of effectiveness for a particular
use, including reports in peer-reviewed
medical literature, if any such evidence
exists. In the new drug approval
process, applicants are required to
demonstrate effectiveness under the
substantial evidence standard described
in section 505(d) of the FD&C Act. FDA
recognizes that few, if any, of the
candidates for the 503A Bulks List will
have been studied in adequate and wellcontrolled investigations sufficient to
satisfy this standard. Thus, in its
balancing of the relevant criteria, the
Agency would take into account
PO 00000
Frm 00027
Fmt 4702
Sfmt 4702
91075
whatever relevant evidence concerning
effectiveness is available.
For example, for substances that have
been widely used for a long period of
time, the literature may include
anecdotal reports of effectiveness for a
particular use or reports of one or more
trials suggesting possible effectiveness.
Conversely, the literature may contain
anecdotal or clinical evidence that a
particular bulk drug substance was not
effective for a particular use (negative
effectiveness data). When evaluating a
bulk drug substance that is proposed for
the treatment of a less serious illness,
FDA would generally be more
concerned about the safety of the
substance than about its effectiveness.
Thus, the availability of minimal
effectiveness data, or the existence of
mere anecdotal reports, would be less
likely to preclude inclusion of the
substance on the list. However, for a
bulk drug substance that is proposed to
treat a more serious or life-threatening
disease, there may be more serious
consequences associated with
ineffective therapy, particularly when
there are approved drug products or
OTC monograph products. In those
cases, the existence of approved drug
products or OTC monograph products
would likely weigh against inclusion on
the proposed list, and the availability of
minimal effectiveness data, or the
presence of negative effectiveness data,
would weigh more heavily against
placement on the list in FDA’s
balancing of the relevant criteria.
Under the fourth criterion, the
historical use of the substance in
pharmacy compounding, FDA proposes
to consider the length of time the
substance has been used in pharmacy
compounding, the medical conditions it
has been used to treat, how widespread
its use has been, including use in other
countries, and any references in peerreviewed medical literature. The
Agency proposes that the longer a
substance has been used in pharmacy
compounding and the broader its use,
the more this criterion will weigh in
favor of inclusion of the substance on
the list.
B. Methodology for Developing the 503A
Bulks List
FDA reviewed the substances
addressed in this proposed rule in the
context of adequately supported
nominated uses. In certain
circumstances, FDA also reviewed
substances in the context of
unnominated or inadequately supported
uses because, for example, such uses
appear to be widespread, are intended
to treat serious conditions, or pose
serious risks to patients. The
E:\FR\FM\16DEP1.SGM
16DEP1
asabaliauskas on DSK3SPTVN1PROD with PROPOSALS
91076
Federal Register / Vol. 81, No. 242 / Friday, December 16, 2016 / Proposed Rules
information that FDA assessed to
evaluate the substances addressed in
this proposed rule under each of the
proposed evaluation criteria was
obtained from publicly available
sources, including peer-reviewed
medical literature. Some of this
information was referenced in the
nominations, and the remainder FDA
gathered through independent searches
of medical and pharmaceutical
databases. FDA did not review raw data.
The nature, quantity, and quality of the
information FDA assessed varied
considerably from substance to
substance. In some cases, there were
very little data. For other substances,
reports in the literature were more
plentiful and sometimes comprised
hundreds or thousands of articles. In
those cases, generally the Agency
limited its review to a sample of the best
literature sources available (e.g., review
articles in widely known, peer-reviewed
journals; meta-analyses; reports of
randomized controlled trials).
FDA’s evaluation of the nominated
substances was, necessarily, far less
rigorous and less comprehensive than
the Agency’s review of drugs as part of
the new drug approval process. The new
drug approval process is conducted
based on extensive data compiled and
submitted with new drug and
abbreviated new drug applications,
which are not available for the
nominated substances. Additionally, the
Agency’s review during the drug
approval process includes premarketing
evaluation of a specific drug
formulation, the sponsor’s chemistry
and manufacturing controls, and the
establishments where approved drugs
will be manufactured. In contrast, these
bulk drug substances will be evaluated
only for possible use in compounded
drugs.
Therefore, the proposed inclusion of a
drug substance on the 503A Bulks List
should not, in any way, be equated with
or considered an FDA approval,
endorsement, or recommendation of any
drug compounded using the substance.
Nor should it be assumed that a drug
compounded using the substances on
the proposed list has been proven to be
safe and effective under the standards
required for Agency approval. Any
person who represents that a
compounded drug made with a bulk
drug substance that appears on this list
is FDA approved, or otherwise endorsed
by FDA generally, or for a particular
indication, will cause the drug to be
misbranded under section 502(a) and/or
502(bb) of the FD&C Act.
On February 23 and 24, 2015, and on
June 17, 2015, FDA consulted with the
PCAC created under section 503A(c)(1)
VerDate Sep<11>2014
18:25 Dec 15, 2016
Jkt 241001
of the FD&C Act, about the criteria
proposed to evaluate substances
nominated for the list and about the 10
substances that are addressed in this
proposed rule (Refs. 2–4). The Agency
has considered all of the PCAC’s
recommendations in developing this
proposed rule, and the Agency intends
to continue to consult with the PCAC in
evaluating future candidates for the
503A Bulks List. The first 10 substances
evaluated are addressed in this
proposed rule. Going forward, FDA
intends to publish NPRMs proposing
additional substances be placed on the
list or not placed on the list on a rolling
basis as evaluations are completed.
Depending on the length of time it takes
to complete a rulemaking, multiple
rulemakings may be ongoing
simultaneously.
Section 503A of the FD&C Act
requires that FDA create the 503A Bulks
List by regulation, in consultation with
the USP. See section 503A(c)(2) of the
FD&C Act. To this end, FDA has been
periodically meeting with USP and
discussing the 503A Bulks List (Refs. 5
and 6). After publication of this NPRM,
the public will have an opportunity to
comment on the proposed rule. After
considering the comments on this
proposed rule submitted to the docket,
FDA will issue the 503A Bulks List as
a final rule, which will be codified in
the CFR. The final version of the rule
may include all, none, or only some of
the substances proposed here for
inclusion on the 503A Bulks List,
depending on the comments received,
and will also identify those substances
the Agency has determined should not
be placed on the list. The Agency may
amend the 503A Bulks List to add or
delete substances after further notice
and comment rulemaking.
Individuals and organizations may
petition FDA to amend the list (to add
or delete bulk drug substances) at any
time after the final rule is published (see
21 CFR 10.30). Individuals and
organizations may also nominate new
substances for the 503A Bulks List or
comment on nominated substances that
have not yet been addressed in an
NPRM via Docket No. FDA–2015–N–
3534 while that docket is open.
C. Substances Proposed for Inclusion on
the 503A Bulks List
Under section 503A(c)(2) of the FD&C
Act, FDA is proposing that the following
six bulk drug substances, which are
neither the subject of a current
applicable USP or NF monograph nor
components of FDA-approved drugs, be
included on the 503A Bulks List, and
the drug products compounded with
those substances may qualify for the
PO 00000
Frm 00028
Fmt 4702
Sfmt 4702
exemptions provided for in section
503A of the FD&C Act (i.e., from
sections 501(a)(2)(B), 502(f)(1), and 505
of the FD&C Act). When a salt or ester
of an active moiety is listed, only that
particular salt or ester may be used. The
base compound and other salts or esters
of the same active moiety must be
evaluated separately for eligibility for
the 503A Bulks List. Additionally, when
a bulk drug substance is included on the
503A Bulks List subject to certain
restrictions (for example, for a particular
route of administration (e.g., topical)),
only dosage forms for that route of
administration may be compounded
with that bulk drug substance.
The following bulk drug substances
are being proposed for the 503A Bulks
List, to appear in § 216.23(a) of Title 21
of the CFR:
1. Brilliant Blue G
Brilliant Blue G, also known as
Coomassie Brilliant Blue G-250,3 was
evaluated for use as a dye used in
staining for visualization during
ophthalmic procedures. It is well
characterized physically and
chemically. There are potential
mutagenic and carcinogenic concerns
associated with Brilliant Blue G;
however, those concerns are mitigated
in clinical use because the dye is
immediately washed out of the eye after
administration, and tissue that is
stained with the dye is removed as part
of the surgical procedure. Published
clinical trials provide some evidence for
efficacy of Brilliant Blue G in staining
the internal limiting membrane.
Brilliant Blue has had relatively
widespread use for staining the internal
limiting membrane during retinal
surgery for approximately 10 years.
There is one product that is FDAapproved for staining the internal
limiting membrane and the anterior
capsule.
FDA proposed to the PCAC that
Brilliant Blue G be included on the
503A Bulks List (Ref. 7), and at its
meeting on June 17, 2015, the PCAC
voted to include Brilliant Blue G on the
list (Ref. 4). The proposed rule would
place Brilliant Blue G on the 503A
Bulks List.
2. Cantharidin
Cantharidin, which is obtained from
various species of blister beetle, was
3 While there are other substances referred to by
the name ‘‘Brilliant Blue,’’ only Coomassie Brilliant
Blue G-250 (CAS RN 6104-58-1, UNII M1ZRX790SI)
was evaluated, and the Agency is proposing only
that substance for inclusion on the 503A Bulks List.
The other substances referred to as ‘‘Brilliant Blue’’
would have to be nominated and separately
evaluated for consideration for inclusion on the
503A Bulks List.
E:\FR\FM\16DEP1.SGM
16DEP1
Federal Register / Vol. 81, No. 242 / Friday, December 16, 2016 / Proposed Rules
asabaliauskas on DSK3SPTVN1PROD with PROPOSALS
evaluated for topical use 4 in the
treatment of warts and molluscum
contagiosum. It is well characterized
physically and chemically. Cantharidin
is extremely toxic, due to its potential
for severe irritation. However, clinical
data accumulated since 1958 indicate
that, with careful use under physician
direction, toxicities observed with
cantharidin, are no worse than and
sometimes less severe than those seen
with other destructive modalities in the
treatment of molluscum contagiosum
and warts. Evidence of some efficacy of
cantharidin in the treatment of warts
and molluscum contagiosum has been
reported in the literature. It appears to
have been widely used to treat
molluscum contagiosum and warts
since the 1950s. There are no approved
prescription or OTC monograph
products for molluscum contagiosum.
For warts, there are no prescription drug
products approved for use outside of the
genital area. A variety of OTC
monograph products containing
salicylic acid are available.
FDA proposed to the PCAC that
cantharidin be included on the 503A
Bulks List for topical use only (Ref. 8).
At the PCAC meeting on February 24,
2015, the PCAC voted to include
cantharidin on the list (Ref. 3). Because
the supported nominations and the
Agency’s review were limited to the
topical use of this substance, the
proposed rule would place cantharadin
on the 503A Bulks List for topical use
only.
3. Diphenylcyclopropenone (DPCP)
DPCP was evaluated for topical use in
the treatment of alopecia areata and
nongenital warts. It is well characterized
physically and chemically but degrades
readily by hydrolysis in an alcoholic
base or exposure to light. Known safety
concerns about the use of DPCP are
limited to reported adverse effects
primarily due to its action as a contact
sensitizer to elicit contact dermatitis.
Evidence of some efficacy of DPCP in
the treatment of alopecia areata and
recalcitrant nongenital warts has been
reported in the literature. DPCP has
been used to treat resistant non-genital
warts and alopecia areata for over 30
years. The only FDA-approved drug
product indicated for the treatment of
alopecia areata is intralesional injection
of corticosteroid suspensions. For warts,
there are no approved prescription drug
products outside of the genital area. A
variety of OTC monograph products are
available containing salicylic acid at
4 Except where specified otherwise, ‘‘topical use’’
means for application on the skin only and does not
include oral, intravaginal, or ophthalmic use.
VerDate Sep<11>2014
18:25 Dec 15, 2016
Jkt 241001
percentages varying from 17 to 40
percent.
FDA proposed to the PCAC that DPCP
be included on the 503A Bulks List (Ref.
8). At its meeting on February 24, 2015,
the PCAC voted to include DPCP on the
list (Ref. 3). Because the supported
nominations and the Agency’s review
were limited to the topical use of this
substance, the proposed rule would
place DPCP on the 503A Bulks List for
topical use only.
4. N-acetyl-D-glucosamine (NAG)
NAG, also known as acetyl-D
glucosamine or N-acetyl glucosamine,
was evaluated for topical use in the
treatment of hyperpigmentation and
other skin conditions. It is well
characterized physically and
chemically. Topical use of NAG has
been associated with relatively minor
and infrequent side effects. Studies have
indicated that NAG may be effective for
reducing diffuse and local facial
hyperpigmentation. NAG has been used
topically for the treatment of
hyperpigmentation since the mid-2000s.
There are FDA-approved drug products
indicated for the treatment of
hyperpigmentation and other skin
conditions, which are not serious or lifethreatening conditions.
FDA proposed to the PCAC that NAG
be included on the 503A Bulks List for
topical use only (Ref. 7). At the PCAC
meeting on June 17, 2015, the PCAC
voted to include NAG on the list (Ref.
4). Because the supported nominations
and the Agency’s review were limited to
the topical use of this substance, the
proposed rule would place NAG on the
503A Bulks List for topical use only.
5. Squaric Acid Dibutyl Ester (SADBE)
SADBE was evaluated for topical use
in the treatment of alopecia areata and
recalcitrant nongenital warts. It is well
characterized physically and chemically
but hydrolyzes readily in the presence
of water. The adverse effects from use of
SADBE are primarily related to its
action as contact sensitizer. Evidence of
some efficacy of SADBE in the treatment
of recalcitrant nongenital warts and
alopecia areata has been reported in the
literature. SADBE has been used in the
treatment of resistant nongenital warts
and alopecia areata for 30 to 40 years.
The only FDA-approved drug product
indicated for the treatment of alopecia
areata is intralesional injection of
corticosteroid suspensions. For warts,
there are no prescription drug products
approved for use outside of the genital
area. A variety of OTC monograph
products are available containing
salicylic acid at percentages varying
from 17 to 40 percent.
PO 00000
Frm 00029
Fmt 4702
Sfmt 4702
91077
FDA proposed to the PCAC that
SADBE be included on the 503A Bulks
List (Ref. 8). At its meeting on February
24, 2015, the PCAC voted to include
SADBE on the list (Ref. 3). Because the
supported nominations and the
Agency’s review were limited to the
topical use of this substance, the
proposed rule would place SADBE on
the 503A Bulks List for topical use only.
6. Thymol Iodide
Thymol iodide was evaluated for use
as a topical treatment for ulcerations
and skin infections, as well as an
intrapleural treatment for pleural
effusions. It is well characterized
physically and chemically. Reports
indicate that it has been used without
major complications. Literature reports
some efficacy of thymol iodide for
pleural effusions, which are serious and
can be life-threatening conditions. Data
regarding the effectiveness of thymol
iodide in compounding for topical use
on wounds or ulcers in various skin
conditions is limited; however, these
skin conditions generally are not serious
or life-threatening. Thymol iodide has
been in use for over 100 years.
Regarding use as an antiseptic in
surgery and use as an external
application to wounds or ulcers in
various skin conditions, approved and
OTC monograph products are available.
There are also FDA-approved products
available to treat malignant pleural
effusions.
FDA proposed to the PCAC that
thymol iodide be included on the 503A
Bulks List (Ref. 8). At its meeting on
February 23, 2015, the PCAC voted to
include thymol iodide on the list (Ref.
2). Because the supported nominations
were limited to the topical use of this
substance, and because pleural effusions
are serious and potentially lifethreatening conditions for which there
are approved products available, the
proposed rule would place thymol
iodide on the 503A Bulks List for
topical use only.
D. Substances Considered and Not
Proposed for Inclusion on the 503A
Bulks List
FDA is proposing that four of the bulk
drug substances that it has evaluated not
be included on the 503A Bulks List.
Bulk drug substances that are
considered for the 503A Bulks list but
not placed on the list cannot be used to
compound drug products that would
qualify for the exemptions in section
503A. If a prescribing practitioner
nevertheless believes that a patient
should be treated with a drug product
compounded from such a bulk drug
substance, it may be possible to obtain
E:\FR\FM\16DEP1.SGM
16DEP1
91078
Federal Register / Vol. 81, No. 242 / Friday, December 16, 2016 / Proposed Rules
asabaliauskas on DSK3SPTVN1PROD with PROPOSALS
the drug under an IND. For information
about the requirements for proceeding
under an IND, visit FDA’s Web site at
https://www.fda.gov/Drugs/Development
ApprovalProcess/HowDrugsare
DevelopedandApproved/Approval
Applications/InvestigationalNewDrug
INDApplication/default.htm.
The four bulk drug substances that
have been evaluated and that FDA is not
proposing to place on the list, and the
reasons for that proposal, are as follows:
1. Oxitriptan
Oxitriptan, also known as 5hydroxytryptophan (5-HTP), was
evaluated as a treatment for depression
and insomnia. It is a hydroxylated form
of a naturally occurring amino acid,
tryptophan. Oxitriptan is well
characterized physically and
chemically. However, there are
significant safety concerns related to its
use. Based upon its mechanism of
action, concomitant use of oxitriptan
with antidepressant drugs could result
in serotonin syndrome, a serious and
life-threatening drug interaction.
Additionally, medications used to treat
depression have been linked to an
increase in suicidal thinking and
behavior. There are no data to suggest
that oxitriptan would be free of similar
risks, and compounded drugs do not
include labeling that would adequately
warn physicians and patients of such
risks. Other potential adverse reactions
include moderate gastrointestinal
effects, which are common upon
administration of oxitriptan.
Data supporting the efficacy of
oxitriptan for depression are limited,
and there is no evidence to support
long-term efficacy of oxitriptan for the
treatment of this chronic disease.
Depression is a serious and potentially
life-threatening condition, and there are
multiple FDA-approved antidepressants
that have been shown to be safe and
effective in their approved forms that
are appropriately labeled. Regarding the
use of oxitriptan to treat insomnia, the
clinical trials examining insomnia were
too poorly designed and/or executed to
assess efficacy. There are multiple FDAapproved drug products available for
the treatment of insomnia. The length of
time oxitriptan has been used in
compounding is uncertain, although it
has been discussed in scientific journals
dating back approximately 40 years.
On balance, the physiochemical
characteristics, the safety concerns, lack
of evidence of effectiveness, and
historical use of oxitriptan weigh
against inclusion of this substance on
the 503A Bulks List. In particular, the
Agency’s proposal regarding this
substance is based on the seriousness of
VerDate Sep<11>2014
18:25 Dec 15, 2016
Jkt 241001
the safety concerns related to the use of
oxitriptan for depression in lieu of, or
causing a delay in the use of an
approved product, the lack of adequate
warnings that would inform patients
and prescribers of the risks associated
with taking an oxitriptan product, and
the availability of approved drug
products for the treatment of
depression, a potentially life-threatening
condition. FDA proposed to the PCAC
that this substance not be included on
the 503A Bulks List (Ref. 7). At its
meeting on June 17, 2015, the PCAC
voted not to include oxitriptan on the
list (Ref. 4). The proposed rule would
not place oxitriptan on the 503A Bulks
List.
2. Piracetam
Piracetam was evaluated as a
treatment for enhancing cognitive skills
in treating a variety of cognitive
disorders, including Alzheimer’s
disease. It has also been studied for
treatment of coagulation disorders and
vertigo. It is well characterized
physically and chemically. Piracetam is
approved in the United Kingdom (UK)
as a prescription drug for the adjunctive
treatment of cortical myoclonus. The
labeling of the UK product identifies
that the drug is renally excreted, that the
dosage should be adjusted in the
presence of renal disease, and that it is
contraindicated in end-stage renal
disease. Piracetam acts by multiple
mechanisms to prolong bleeding time
and is therefore not recommended for
use by individuals with medical
conditions that prolong bleeding time or
that are taking concomitant
anticoagulants or other medications that
prolong bleeding (Ref. 9). Piracetam is
not recommended for women who are
pregnant, planning to become pregnant,
or breastfeeding, because, according to
the UK product’s labeling, the drug has
been shown to cross the placenta and be
excreted in human milk. It is also
recommended that individuals required
to restrict their salt intake avoid
piracetam (id.).
Piracetam was assessed for the
treatment of mild cognitive impairment,
a potential component of Alzheimer’s
disease, in a large, well-conducted,
controlled clinical trial that failed to
demonstrate efficacy. Studies of the
efficacy of piracetam for other
indications have been inconclusive,
many of which were poorly designed or
executed, or used flawed statistical
methods to analyze the results.
Piracetam’s regulatory approval in the
UK for the treatment of cortical
myoclonus, which is not among the uses
for which piracetam was nominated,
was based on a single center,
PO 00000
Frm 00030
Fmt 4702
Sfmt 4702
retrospective review of 40 patients
treated with piracetam (id.). FDAapproved products are available for
treatment of the conditions, and
conditions related to, those for which
piracetam was nominated, for example,
for Alzheimer’s disease, which is
frequently preceded by mild cognitive
impairment. Regarding historical use,
piracetam has been available for
approximately 40 years.
On balance, the physiochemical
characteristics, safety concerns,
inconclusive evidence of effectiveness,
and historical use of piracetam weigh
against inclusion of this substance on
the list. In particular, the Agency’s
proposal regarding this substance is
based on the limited evidence of benefit
associated with piracetam, the
seriousness of the conditions for which
piracetam was nominated to be used,
and the availability of safe and effective
FDA-approved medications for many of
these uses. FDA proposed to the PCAC
that this substance not be included on
the 503A Bulks List (Ref. 8). At its
meeting on February 24, 2015, the PCAC
voted not to include piracetam on the
list (Ref. 3). The proposed rule would
not place piracetam on the 503A Bulks
List.
3. Silver Protein Mild
Silver protein mild, also known as
mild silver protein, was evaluated for
use as an anti-infective agent for
ophthalmic use. Silver protein mild is
not well characterized because the term
‘‘silver protein mild’’ is used to refer to
a variety of different drug products.
There are also safety concerns
associated with the use of silver protein
mild. It can cause argyria, which is a
permanent ashen-gray discoloration of
the skin, conjunctiva, and internal
organs. Regarding effectiveness, silver
protein mild has been found to be
inferior to another treatment in clinical
trials. A number of FDA-approved antiinfective agents for ophthalmic use are
available and have been shown to be
both safe and effective. While it has a
long history of use, dating back to the
early 1900s, the use of silver protein
mild declined dramatically after the
introduction of FDA-approved ocular
anti-infectives.
On balance, the physiochemical
characteristics, safety issues,
questionable effectiveness, and
historical use of silver protein mild
weigh against inclusion of this
substance on the 503A Bulks List. In
particular, the Agency’s proposal is
based on the facts that silver protein
mild is not well characterized, that in
clinical trials it has been found to be
inferior to another treatment and
E:\FR\FM\16DEP1.SGM
16DEP1
Federal Register / Vol. 81, No. 242 / Friday, December 16, 2016 / Proposed Rules
numerically inferior to no treatment at
all, and that chronic use may result in
permanent discoloration of the
conjunctiva, cornea, and/or lens. FDA
proposed to the PCAC that this
substance not be included on the 503A
Bulks List (Ref. 8). At its meeting on
February 23, 2015, the PCAC voted not
to include silver protein mild on the list
(Ref. 2). The proposed rule would not
place silver protein mild on the 503A
Bulks List.
asabaliauskas on DSK3SPTVN1PROD with PROPOSALS
4. Tranilast
Tranilast, an antiallergenic agent, was
evaluated for the treatment of allergic
disorders, arthritis, dry eye syndrome,
keloids, and hypertrophic scars. It is
approved in South Korea and Japan for
the treatment of asthma, keloids, and
hypertrophic scarring, and as an
ophthalmic solution for allergic
conjunctivitis. It is well characterized
physically and chemically. However,
there are significant safety concerns
associated with its systemic
administration. In a well-controlled
clinical trial with nearly 12,000
participants (the Prevention of
REStenosis with Tranilast and its
Outcomes (PRESTO) Trial) (Ref. 10),
tranilast was associated with
significantly elevated liver enzymes
(three times the upper limit of normal)
in 11 percent of patients within 1 to 3
months of drug initiation, as well as
anemia, renal failure, rash, and
dysuria.5 Liver toxicity is of particular
concern because many of the conditions
for which tranilast was nominated are
chronic conditions. While there is some
evidence that tranilast may be effective
for allergic disorders, evidence of
effectiveness for other uses is either not
available or inconclusive. For allergy,
arthritis, and ophthalmic indications,
there are numerous FDA-approved and
OTC monograph products. The length of
time tranilast has been used in
compounding is uncertain, although it
has been discussed in scientific journals
dating back approximately 40 years.
On balance, the physiochemical
characteristics, safety concerns, lack of
evidence of effectiveness, and historical
use of tranilast weigh against inclusion
of this substance on the 503A Bulks
List, particularly given the seriousness
of the safety concerns related to
hepatotoxicity of tranilast and
5 During the PCAC meeting on June 17, 2015, the
PRESTO trial was criticized by one of the tranilast
nominators as having insufficiently accounted for
the medical history of the subjects, among other
things (see Ref. 4). To the contrary, the five-arm trial
design appears to have been properly controlled for
the patients’ various medical conditions, and
signals of liver toxicity were consistent across arms
(see Ref. 10).
VerDate Sep<11>2014
18:25 Dec 15, 2016
Jkt 241001
contraindications in pregnant and
breastfeeding women, the availability of
approved products for most of the
proposed uses, and the lack of evidence
that tranilast is effective. FDA proposed
to the PCAC that this substance not be
included on the 503A Bulks List (Ref.
7). However, at its meeting on June 17,
2015, the PCAC voted to include
tranilast on the list for topical use only
(Ref. 4).
Subsequent to that meeting, FDA
reviewed the topical use of tranilast
further. It obtained the label of the
Japanese tranilast product, RIZABEN,
but found no information on the
transdermal absorption or other
pharmacokinetics of tranilast when
applied topically to healthy or diseased
human skin (Ref. 11). The labeling of
the Japanese product identifies a
number of safety concerns, including a
contraindication in pregnant women,
especially during the first trimester of
pregnancy, and in those who might be
pregnant, due to evidence of
teratogenicity in animal studies (id.).
The labeling also states that tranilast is
detected in breast milk and should be
avoided by breastfeeding women. In
addition, the RIZABEN label lists a drug
interaction with warfarin and identifies
a number of serious adverse events,
particularly those that are hematologic
in nature (leukopenia,
thrombocytopenia, anemia, hemolytic
anemia), associated with the oral use of
tranilast. Safety information regarding
other routes of administration is limited.
FDA also noted evidence that some
increases in some liver function tests
(bilirubin) are explained by tranilast
inhibition of uridine diphosphate
glucuronosyltransferase 1A1 (UGT1A1)
especially in patients with a genotype
for Gilbert’s Disease. Increases in liver
transaminases observed with tranilast
are not typically seen with inhibition of
UGT1A1. It is speculated that tranilast
impairs the metabolism of drugs that are
metabolized by UGT1A1. If these drugs
are associated with transaminase
elevations, inhibiting the drug’s
metabolism may lead to liver
transaminitis.
As was found in the Agency’s initial
review and presented to the PCAC, there
is no persuasive information available
regarding the safety or effectiveness of
topical tranilast. FDA has identified
only two reports in the literature
describing the efficacy and safety of
tranilast administered topically for the
treatment of keloids and hypertrophic
scars (Refs. 12 and 13). One of those
studies was an open-label trial, and the
other was a case series. Between the two
studies, only five patients were exposed
to topical tranilast.
PO 00000
Frm 00031
Fmt 4702
Sfmt 4702
91079
As stated previously, FDA has serious
concerns about the safety of tranilast
when administered orally. The Agency
has insufficient information about the
systemic absorption of topical tranilast
formulations to determine whether
topical administration of the drug
product would present the same safety
concerns. Given the lack of information
available about the safety and efficacy of
topical tranilast, and safety concerns
related to the oral use of this product,
the proposed rule would not place
tranilast on the 503A Bulks List.
VI. Proposed Effective Date
The Agency proposes that any final
rule based on this proposal will become
effective 30 days after the date of
publication of the final rule in the
Federal Register.
VII. Analysis of Environmental Impact
FDA has 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.
VIII. Economic Analysis of Impacts
We have examined the impacts of the
proposed rule under Executive Order
12866, Executive Order 13563, 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 and 13563
direct us to assess all costs and benefits
of available regulatory alternatives and,
when regulation is necessary, to select
regulatory approaches that maximize
net benefits (including potential
economic, environmental, public health
and safety, and other advantages;
distributive impacts; and equity). We
have developed a comprehensive
Economic Analysis of Impacts that
assesses the impacts of the proposed
rule. We believe that this proposed rule
is not a significant regulatory action as
defined by Executive Order 12866.
The Regulatory Flexibility Act
requires us to analyze regulatory options
that would minimize any significant
impact of a rule on small entities.
Because we find little evidence that a
substantial number of small entities
would be affected by the proposed rule
or that the economic impact on each
affected small entity would be
significant, we propose to certify that
the proposed rule will not have a
significant economic impact on a
substantial number of small entities.
The Unfunded Mandates Reform Act
of 1995 (section 202(a)) requires us to
E:\FR\FM\16DEP1.SGM
16DEP1
91080
Federal Register / Vol. 81, No. 242 / Friday, December 16, 2016 / Proposed Rules
prepare a written statement, which
includes an assessment of anticipated
costs and benefits, 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 $146 million,
using the most current (2015) Implicit
Price Deflator for the Gross Domestic
Product. This proposed rule would not
result in an expenditure in any year that
meets or exceeds this amount.
TABLE 1—ECONOMIC DATA: COSTS AND BENEFITS STATEMENT
Category
Primary estimate
Low estimate
High estimate
Units year dollars
Discount rate
(%)
Period
covered
(years)
Notes
Benefits
Annualized
Monetized $
mil/year.
Annualized
Monetized $
mil/year.
Annualized
Quantified.
Annualized
Quantified.
Qualitative .......
Not Estimated
(N.E.).
........................
........................
..............................
7
10
........................
N.E .......................
........................
........................
..............................
3
10
........................
N.E .......................
........................
........................
..............................
7
........................
........................
N.E .......................
........................
........................
..............................
3
........................
........................
Not including four
bulk drug substances from the
503A Bulks List
would limit the
use of potentially ineffective
or unsafe unapproved drugs.
........................
........................
..............................
........................
........................
........................
Costs
Annualized
Monetized $
mil/year.
Annualized
Monetized $
mil/year.
Annualized
Quantified.
N.E .......................
Qualitative .......
........................
..............................
7
10
........................
N.E .......................
Annualized
Quantified.
........................
........................
........................
..............................
3
10
........................
$118 to $235 onetime per firm
costs.
$118 to $235 onetime per firm
costs.
..............................
........................
........................
2014 .....................
7
........................
........................
........................
........................
2014 .....................
3
........................
........................
........................
........................
..............................
........................
........................
........................
asabaliauskas on DSK3SPTVN1PROD with PROPOSALS
Transfers
Federal
Annualized
Monetized $
mil/year.
Federal
Annualized
Monetized $
mil/year.
From/To ...........
Other
Annualized $
mil/year.
Other
Annualized
Monetized $
mil/year.
VerDate Sep<11>2014
..............................
........................
........................
..............................
7
........................
........................
..............................
........................
........................
..............................
3
........................
........................
From: ....................
N.E .......................
........................
........................
........................
........................
To: ........................
..............................
........................
7
........................
........................
........................
........................
N.E .......................
........................
........................
..............................
3
........................
........................
19:14 Dec 15, 2016
Jkt 241001
PO 00000
Frm 00032
Fmt 4702
Sfmt 4702
E:\FR\FM\16DEP1.SGM
16DEP1
Federal Register / Vol. 81, No. 242 / Friday, December 16, 2016 / Proposed Rules
91081
TABLE 1—ECONOMIC DATA: COSTS AND BENEFITS STATEMENT—Continued
Category
Primary estimate
Low estimate
High estimate
From/To ...........
From: Producers
of bulk drug
substances not
proposed for inclusion and
compounding
pharmacies
using these substances.
........................
........................
Units year dollars
Discount rate
(%)
To: Producers of
........................
alternative treatments, consumers, using
these treatments
and payers for
these treatments.
Period
covered
(years)
Notes
........................
........................
Effects
State, Local,
and/or Tribal
Government:
No effect.
Small Business:
Unknown effect.
Wages: No effect.
Growth: No effect.
The Economic Analysis of Impacts of
the proposed rule performed in
accordance with Executive Order 12866,
Executive Order 13563, the Regulatory
Flexibility Act, and the Unfunded
Mandates Reform Act is available at
https://www.regulations.gov under the
docket number for this proposed rule
(Ref. 14) and at https://www.fda.gov/
AboutFDA/ReportsManualsForms/
Reports/EconomicAnalyses/default.htm.
We invite comments on this analysis.
asabaliauskas on DSK3SPTVN1PROD with PROPOSALS
A. Summary of the Costs of the Rule
We lack data on the scope of the
current use of the affected bulk drug
substances and the number of firms that
would be affected by the rule. Without
this information, we cannot quantify the
total potential costs of the proposed
rule. Potential costs include
administrative costs, additional costs for
consumers and payers if alternative
therapies are more costly than the
affected compounded drug products,
and a potential loss of producer surplus
if producers use additional resources in
response to the rule. We estimate that
each affected firm would spend 1 to 2
hours on administrative costs to read
and understand the rule. The average
hourly wage for a pharmacist in 2014
equals about $57, or $114 including 100
percent overhead. Thus, each affected
firm would incur administrative costs
that range from $118 to $235. We
request comment on the potential costs
and number of firms affected by the
proposed rule.
VerDate Sep<11>2014
18:25 Dec 15, 2016
Jkt 241001
B. Summary of the Benefits of the Rule
The benefits of the rule are
unquantified. We include a qualitative
discussion of potential benefits. For
consumers who switch to more effective
treatments, there would be benefits as
consumers experience better health
outcomes than they do currently.
C. Summary of the Impact on Small
Entities
The Regulatory Flexibility Act
requires a Regulatory Flexibility
Analysis (RFA) unless the Agency can
certify that the proposed rule would
have no significant impact on a
substantial number of small entities.
The Small Business Administration
(SBA) establishes thresholds for small
entities by North American Industry
Classification System (NAICS); the SBA
considers small any entity below these
thresholds. Firms affected by the
proposed rule would fall into three
major industries, NAICS 325412
Pharmaceutical Preparation
Manufacturing, NAICS 424210 Drugs
and Druggists’ Sundries Merchant
Wholesalers, and NAICS 446110
Pharmacies and Drug Stores. The
thresholds for these industries are 750
employees for NAICS 325412, 100
employees for NAICS 424210, and
annual sales of $27.5 million for NAICS
446110.
We lack data on the number or size
of manufacturers, wholesalers, and
compounding pharmacies that would be
affected by the proposed rule. Moreover,
we find little evidence of widespread
PO 00000
Frm 00033
Fmt 4702
Sfmt 4702
use of four bulk drug substances not
proposed for inclusion on the 503A
Bulks List. This suggests that the impact
of the rule would likely not be
significant on small entities. Because we
find little evidence that a substantial
number of small entities would be
affected by the proposed rule or that the
economic impact on each affected small
entity would be significant, we believe
that the proposed rule would not have
a significant economic impact on a
substantial number of small entities, but
the impacts are uncertain. We request
detailed comments and data on the
number of small entities that would be
affected by the proposed rule, as well as
data on the economic impact of the
proposed rule on these small entities.
IX. Paperwork Reduction Act of 1995
The submission of comments on this
proposed rule would be submissions in
response to a Federal Register notice, in
the form of comments, which are
excluded from the definition of
‘‘information’’ under 5 CFR 1320.3(h)(4)
of Office of Management and Budget
regulations on the Paperwork Reduction
Act (i.e., facts or opinions submitted in
response to general solicitations of
comments from the public, published in
the Federal Register or other
publications, regardless of the form or
format thereof, provided that no person
is required to supply specific
information pertaining to the
commenter, other than that necessary
for self-identification, as a condition of
the Agency’s full consideration of the
E:\FR\FM\16DEP1.SGM
16DEP1
91082
Federal Register / Vol. 81, No. 242 / Friday, December 16, 2016 / Proposed Rules
comment). The proposed rule contains
no other collection of information.
X. Federalism
We have analyzed this proposed rule
in accordance with the principles set
forth in Executive Order 13132. We
have determined that the proposed rule,
if finalized, would not contain policies
that would 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.
asabaliauskas on DSK3SPTVN1PROD with PROPOSALS
XI. References
The following references are on
display in the Division of Dockets
Management (see ADDRESSES) and are
available for viewing by interested
persons between 9 a.m. and 4 p.m.,
Monday through Friday; they are also
available electronically at https://
www.regulations.gov. FDA has verified
the Web site addresses, as of the date
this document publishes in the Federal
Register, but Web sites are subject to
change over time.
1. FDA, ‘‘Guidance for Industry: Interim
Policy on Compounding Using Bulk Drug
Substances Under Section 503A of the
Federal Food, Drug, and Cosmetic Act,’’
(https://www.fda.gov/downloads/Drugs/
GuidanceComplianceRegulatoryInformation/
Guidances/UCM469120.pdf), 2016.
2. FDA, Transcript of the February 23,
2015, Meeting of the Pharmacy
Compounding Advisory Committee
(Afternoon Session), 2015, (https://
www.fda.gov/downloads/
AdvisoryCommittees/
CommitteesMeetingMaterials/Drugs/
PharmacyCompoundingAdvisoryCommittee/
UCM444500.pdf).
3. FDA, Transcript of the February 24,
2015, Meeting of the Pharmacy
Compounding Advisory Committee, 2015,
(https://www.fda.gov/downloads/
AdvisoryCommittees/
CommitteesMeetingMaterials/Drugs/
PharmacyCompoundingAdvisoryCommittee/
UCM444501.pdf).
4. Transcript of the June 17, 2015, Meeting
of the Pharmacy Compounding Advisory
Committee (Afternoon Session), 2015, (https://
www.fda.gov/downloads/
AdvisoryCommittees/
CommitteesMeetingMaterials/Drugs/
PharmacyCompoundingAdvisoryCommittee/
UCM458513.pdf).
5. Memorandum to File on FDA
Consultations with USP, September 26, 2016.
6. Letter from USP to FDA, October 7,
2016.
7. FDA Briefing Document for the June 17–
18, 2015, Meeting of the Pharmacy
VerDate Sep<11>2014
18:25 Dec 15, 2016
Jkt 241001
Compounding Advisory Committee, 2015,
(https://www.fda.gov/downloads/
AdvisoryCommittees/
CommitteesMeetingMaterials/Drugs/
PharmacyCompoundingAdvisoryCommittee/
UCM449535.pdf).
8. FDA Briefing Document for the February
23–24, 2015, Meeting of the Pharmacy
Compounding Advisory Committee, 2015,
(https://www.fda.gov/downloads/
AdvisoryCommittees/
CommitteesMeetingMaterials/Drugs/
PharmacyCompoundingAdvisoryCommittee/
UCM433804.pdf).
9. Obeso, J. A., et al., ‘‘Piracetam in the
Treatment of Different Types of Myoclonus,’’
Clinical Neuropharmacology, 11(6): 529–536,
1988.
10. Holmes, D.R., Jr., M. Savage, J.M.
LaBlanche, et al., ‘‘Results of Prevention of
REStenosis with Tranilast and its Outcomes
(PRESTO) Trial,’’ Circulation, 106(10): 1243–
1250, 2002.
11. FDA Supplemental Review of Topical
Tranilast, April 25, 2016.
12. Shigeki, S., T. Murakami, N. Yata, and
Y. Ikuta, ‘‘Treatment of Keloid and
Hypertrophic Scars by Iontophoretic
Transdermal Delivery of Tranilast,’’
Scandinavian Journal of Plastic and
Reconstructive Surgery and Hand Surgery,
31(2): 151–159, 1997.
13. Banov, D., F. Banov, and A.S. Bassani,
‘‘Case Series: The Effectiveness of Fatty
Acids From Pracaxi Oil in a Topical Silicone
Base for Scar and Wound Therapy,’’
Dermatology and Therapy, 4(2): 259–269,
2014.
14. Economic Analysis of Impacts.
List of Subjects in 21 CFR Part 216
Drugs, Prescription drugs.
Therefore, under the Federal Food,
Drug, and Cosmetic Act, and under
authority delegated to the Commissioner
of Food and Drugs, the Food and Drug
Administration proposes to amend 21
CFR part 216 as follows:
PART 216—HUMAN DRUG
COMPOUNDING
1. The authority citation for part 216
is revised to read as follows:
■
Authority: 21 U.S.C. 351, 352, 353a, 353b,
355, and 371.
2. The heading for part 216 is revised
to read as set forth above.
■ 3. Section 216.23 is added to read as
follows:
■
§ 216.23 Bulk drug substances that can be
used to compound drug products in
accordance with section 503A of the
Federal Food, Drug, and Cosmetic Act.
(a) The following bulk drug
substances can be used in compounding
under section 503A(b)(1)(A)(i)(III) of the
Federal Food, Drug, and Cosmetic Act.
Brilliant Blue G, also known as
Coomassie Brilliant Blue G–250.
Cantharidin (for topical use only).
Diphenylcyclopropenone (for topical
use only).
PO 00000
Frm 00034
Fmt 4702
Sfmt 9990
N-acetyl-D-glucosamine (for topical
use only).
Squaric acid dibutyl ester (for topical
use only).
Thymol iodide (for topical use only).
(b) After balancing the criteria set
forth in paragraph (c) of this section,
FDA has determined that the following
bulk drug substances will not be
included on the list of substances that
can be used in compounding set forth in
paragraph (a) of this section:
Oxitriptan.
Piracetam.
Silver Protein Mild.
Tranilast.
(c) FDA will use the following criteria
in evaluating substances considered for
inclusion on the list set forth in
paragraph (a) of this section:
(1) The physical and chemical
characterization of the substance;
(2) Any safety issues raised by the use
of the substance in compounded drug
products;
(3) The available evidence of the
effectiveness or lack of effectiveness of
a drug product compounded with the
substance, if any such evidence exists;
and
(4) Historical use of the substance in
compounded drug products, including
information about the medical
condition(s) the substance has been
used to treat and any references in peerreviewed medical literature.
(d) Based on evidence currently
available, there are inadequate data to
demonstrate the safety or efficacy of any
drug product compounded using any of
the drug substances listed in paragraph
(a) of this section, or to establish general
recognition of the safety or effectiveness
of any such drug product. Any person
who represents that a compounded drug
made with a bulk drug substance that
appears on this list is FDA approved, or
otherwise endorsed by FDA generally or
for a particular indication, will cause
the drug to be misbranded under section
502(a) and/or 502(bb) of the Federal
Food, Drug, and Cosmetic Act.
Dated: December 9, 2016.
Leslie Kux,
Associate Commissioner for Policy.
[FR Doc. 2016–30109 Filed 12–15–16; 8:45 am]
BILLING CODE 4164–01–P
E:\FR\FM\16DEP1.SGM
16DEP1
]]>Agencies
[Federal Register Volume 81, Number 242 (Friday, December 16, 2016)]
[Proposed Rules]
[Pages 91071-91082]
From the Federal Register Online via the Government Publishing Office [www.gpo.gov]
[FR Doc No: 2016-30109]
=======================================================================
-----------------------------------------------------------------------
DEPARTMENT OF HEALTH AND HUMAN SERVICES
Food and Drug Administration
21 CFR Part 216
[Docket No. FDA-2016-N-3464]
RIN 0910-AH29
List of Bulk Drug Substances That Can Be Used To Compound Drug
Products in Accordance With Section 503A of the Federal Food, Drug, and
Cosmetic Act
AGENCY: Food and Drug Administration, HHS.
ACTION: Proposed rule.
-----------------------------------------------------------------------
SUMMARY: The Food and Drug Administration (FDA or Agency) is proposing
a regulation to identify an initial list of bulk drug substances that
can be used to compound drug products in accordance with certain
compounding provisions of the Federal Food, Drug, and Cosmetic Act (the
FD&C Act), although they are neither the subject of an applicable
United States Pharmacopeia (USP) or National Formulary (NF) monograph
nor components of FDA-approved drugs. Specifically, the Agency proposes
to place six bulk drug substances on the list. This proposed rule also
identifies four bulk drug substances that FDA has considered and
proposes not to include on the list. Additional substances nominated by
the public for inclusion on this list are currently under consideration
and will be the subject of a future rulemaking.
DATES: Submit either electronic or written comments on the bulk drug
substances list by March 16, 2017. See section VI for the proposed
effective date of a final rule based on this proposed rule.
ADDRESSES: You may submit comments as follows:
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): Division of Dockets Management (HFA-305), Food and Drug
Administration, 5630 Fishers Lane, Rm. 1061, Rockville, MD 20852.
For written/paper comments submitted to the Division of
Dockets Management, 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-2016-N-3464 for ``List of Bulk Drug Substances That Can Be Used To
Compound Drug Products in Accordance With Section 503A of the Federal
Food, Drug, and Cosmetic Act.'' Received comments will be placed in the
docket and, except for those submitted as ``Confidential Submissions,''
publicly viewable at https://www.regulations.gov or at the Division of
Dockets Management between 9 a.m. and 4 p.m., Monday through Friday.
[[Page 91072]]
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 Division of Dockets Management. 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.fda.gov/regulatoryinformation/dockets/default.htm.
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 Division of Dockets Management, 5630 Fishers
Lane, Rm. 1061, Rockville, MD 20852.
FOR FURTHER INFORMATION CONTACT: James Flahive, Center for Drug
Evaluation and Research, Food and Drug Administration, 10903 New
Hampshire Ave., Bldg. 51, Rm. 5108, Silver Spring, MD 20993-0002, 301-
796-9293.
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 and Acronyms Commonly Used in This
Document
III. Background
A. Statutory and Regulatory Background
B. Regulatory History of the 503A Bulks List
C. Requests for Nominations
IV. Legal Authority
V. Description of the Proposed Rule
A. Criteria for Evaluating Bulk Drug Substances for the 503A
Bulks List
B. Methodology for Developing the 503A Bulks List
C. Substances Proposed for Inclusion on the 503A Bulks List
D. Substances Considered and Not Proposed for Inclusion on the
503A Bulks List
VI. Proposed Effective Date
VII. Analysis of Environmental Impact
VIII. Economic Analysis of Impacts
A. Summary of the Costs of the Rule
B. Summary of the Benefits of the Rule
C. Summary of the Impact on Small Entities
IX. Paperwork Reduction Act of 1995
X. Federalism
XI. References
I. Executive Summary
A. Purpose of the Proposed Rule
FDA is proposing to amend its regulations to add a list of bulk
drug substances that can be used in compounding under section 503A of
the FD&C Act (21 U.S.C. 353a) (referred to as ``the 503A Bulks List'').
Bulk drug substances that appear on the 503A Bulks List can be used to
compound drug products subject to the conditions of section 503A,
although those substances are not the subject of a USP or NF monograph
or components of approved drug products.
B. Summary of the Major Provisions of the Proposed Rule
FDA is proposing to establish the criteria by which bulk drug
substances will be evaluated for inclusion on the 503A Bulks List.
Based on the results of its evaluation of nominated bulk drug
substances to date, as well as consultation with the Pharmacy
Compounding Advisory Committee (PCAC), FDA is also proposing to include
six bulk drug substances on the list: Brilliant Blue G, also known as
Coomassie Brilliant Blue G-250; cantharidin (for topical use only);
diphenylcyclopropenone (for topical use only); N-acetyl-D-glucosamine
(for topical use only); squaric acid dibutyl ester (for topical use
only); and thymol iodide (for topical use only) and that four other
substances not be included on the list: Oxitriptan, piracetam, silver
protein mild, and tranilast.
C. Legal Authority
Section 503A of the FD&C Act, in conjunction with our general
rulemaking authority in section 701(a) of the FD&C Act (21 U.S.C.
371(a)), serves as our principal legal authority for this proposed
rule.
D. Costs and Benefits
FDA is proposing to place six bulk substances on the 503A Bulks
List and not to place four bulk substances on the 503A Bulks List.
Because we lack sufficient information to quantify the costs and
benefits of this proposed rule, we include a qualitative description of
potential benefits and potential costs. We expect that the rule would
affect compounding pharmacies and other entities that market the
affected substances or drug products made from the affected substances,
consumers of drug products containing the affected drug substances, and
payers that cover these drug products or alternative drug products.
II. Table of Abbreviations and Acronyms Commonly Used in This Document
5-HTP 5-hydroxytryptophan
BLA Biologics License Application
CFR Code of Federal Regulations
CSA Controlled Substances Act
DPCP Diphenylcyclopropenone
DQSA Drug Quality and Security Act
FD&C Act Federal Food, Drug, and Cosmetic Act
FDA Food and Drug Administration
IND Investigational New Drug
NAG N-acetyl-D-glucosamine
NAICS North American Industry Classification System
NF National Formulary
NPRM Notice of Proposed Rulemaking
OTC Over-The-Counter
PCAC Pharmacy Compounding Advisory Committee
PHS Act Public Health Service Act
PRESTO Prevention of REStenosis with Tranilast and its Outcomes
RFA Regulatory Flexibility Analysis
SADBE Squaric acid dibutyl ester
SBA Small Business Administration
UGT1A1 Uridine diphosphate glucuronosyltransferase 1A1
UK United Kingdom
USP United States Pharmacopeia
III. Background
A. Statutory and Regulatory Background
Section 503A of the FD&C Act (21 U.S.C. 353a) describes the
conditions under which a compounded drug product may qualify for an
exemption from certain sections of the FD&C Act. Those conditions
include that a licensed pharmacist in a State-licensed pharmacy or
Federal facility or a licensed physician compounds the drug product
using bulk drug substances that: (1) Comply with the standards of an
applicable USP or NF monograph,\1\ if a
[[Page 91073]]
monograph exists, and the USP chapter on pharmacy compounding; (2) if
such a monograph does not exist, are drug substances that are
components of drugs approved by the Secretary; or (3) if such a
monograph does not exist and the drug substance is not a component of a
drug approved by the Secretary, that appear on the 503A Bulks List. See
section 503A(b)(1)(A)(i) of the FD&C Act. This proposed rule proposes
criteria for evaluating substances for inclusion on the 503A Bulks List
and identifies six substances the Secretary proposes to place on the
list. The Agency considered four other substances and is proposing not
to include those substances on the 503A Bulks List. Additional
substances are under evaluation, and new substances may be added to the
list through subsequent rulemaking.
---------------------------------------------------------------------------
\1\ FDA has interpreted the statutory language ``applicable USP
or NF monographs'' to refer to official USP or NF drug substance
monographs. Therefore, a substance that is the subject of a dietary
supplement monograph, but not a USP or NF drug substance monograph,
does not satisfy the condition regarding bulk drug substances in
section 503A(b)(1)(A)(i)(I) of the Act. Such a substance may only be
used as a bulk drug substance under section 503A of the FD&C Act if
it is a component of an FDA-approved drug product or is on the 503A
Bulks List.
---------------------------------------------------------------------------
Section 503A adopts the definition of ``bulk drug substance'' in
FDA's drug establishment registration and listing regulations, which
was codified at Sec. 207.3(a)(4) (21 CFR 207.3(a)(4)) at the time
section 503A was enacted. See section 503A(b)(1)(A) of the FD&C Act.
Under the definition, bulk drug substance means any substance that is
represented for use in a drug and that, when used in the manufacturing,
processing, or packaging of a drug, becomes an active ingredient or a
finished dosage form of the drug, but the term does not include
intermediates used in the synthesis of such substances.
On August 31, 2016, FDA published a final rule in the Federal
Register to update its registration and listing regulations in part 207
(21 CFR part 207), which included minor changes to the definition of
bulk drug substance and moved the definition to Sec. 207.3 (see 81 FR
60170). This definition becomes effective on November 29, 2016. As set
forth in Sec. 207.3, ``bulk drug substance,'' as referenced in section
503A(b)(1)(A) of the FD&C Act, means the same as ``active
pharmaceutical ingredient'' as defined in Sec. 207.1(b). An ``active
pharmaceutical ingredient'' is any substance that is intended for
incorporation into a finished drug product and is intended to furnish
pharmacological activity or other direct effect in the diagnosis, cure,
mitigation, treatment, or prevention of disease, or to affect the
structure or any function of the body. Active pharmaceutical ingredient
does not include intermediates used in the synthesis of the substance
(Sec. 207.1).
Inactive ingredients used in compounded drug products, such as
flavorings, dyes, or diluents, need not appear on the 503A Bulks List
to be eligible for use in compounding drug products and will not be
included on the list.
B. Regulatory History of the 503A Bulks List
Section 503A of the FD&C Act was enacted in 1997. In the Federal
Register of April 7, 1998 (63 FR 17011), FDA invited all interested
persons to nominate bulk drug substances for inclusion on the 503A
Bulks List. In 1998, FDA received nominations for 41 different drug
substances. Ten of these drug substances were the subject of an
applicable USP or NF monograph or were components of FDA-approved drugs
and did not need to go on the list to be used in compounding. After
evaluating the nominated drug substances and consulting with the PCAC
as required by section 503A(c)(2), FDA published a proposed rule
listing 20 drug substances for potential inclusion on the initial
section 503A Bulks List (64 FR 996, January 7, 1999) (the 1999 Proposed
503A Bulks List). The proposed rule also described 10 nominated drug
substances that were still under consideration for the 503A Bulks List.
The PCAC reconvened in May 1999 to discuss bulk drug substances
included in the proposed rule, in addition to other bulk drug
substances (see 64 FR 19791, April 22, 1999).
In February 2001, the U.S. Court of Appeals for the Ninth Circuit
held that certain provisions of section 503A of the FD&C Act were
unconstitutional restrictions on commercial speech. (See Western States
Med. Ctr. v. Shalala, 238 F.3d 1090 (9th Cir. 2001).) Furthermore, the
Ninth Circuit held that the advertising and solicitation provisions
could not be severed from the rest of section 503A and, as a result,
found section 503A of the FD&C Act to be invalid in its entirety. In
April 2002, the U.S. Supreme Court affirmed the Ninth Circuit's
decision that the advertising and solicitation provisions were
unconstitutional; it did not, however, rule on the severability of
section 503A of the FD&C Act. (See Thompson v. Western States Med.
Ctr., 535 U.S. 357 (2002).) In 2008, the U.S. Court of Appeals for the
Fifth Circuit held that compounded drugs are subject to regulation by
FDA, and that the advertising and solicitation provisions are severable
from the rest of section 503A of the FD&C Act. (See Medical Ctr. Pharm.
v. Mukasey, 536 F.3d 383 (5th Cir. 2008).)
Following a fungal meningitis outbreak in September 2012, FDA
sought legislation to, among other things, resolve the split in the
Circuits to clarify that section 503A of the FD&C Act was valid
nationwide. On November 27, 2013, President Obama signed the Drug
Quality and Security Act (Pub. L. 113-54) (DQSA), which contains
important provisions relating to the oversight of human drug product
compounding. Among other things, the DQSA removed from section 503A of
the FD&C Act the provisions that had been held unconstitutional by the
U.S. Supreme Court in 2002. By removing these provisions, the DQSA
clarified that section 503A of the FD&C Act applies nationwide.
C. Requests for Nominations
Because of the amount of time that had passed between the
publication of the 1999 proposed rule and the enactment of the DQSA,
FDA felt it was necessary to begin again to develop the 503A Bulks
List. In the Federal Register of December 4, 2013 (78 FR 72841), FDA
published a notice withdrawing the 1999 proposed rule and inviting all
interested persons to nominate bulk drug substances for inclusion on
the 503A Bulks List.
Over 2,000 substances were nominated. However, many of those
nominations were for a substance that is the subject of an applicable
USP or NF monograph or a component of an FDA-approved drug, were not
for substances used in compounding as active ingredients, or did not
include sufficient information for FDA to evaluate whether the
substances should be proposed for inclusion on the 503A Bulks List. To
improve the efficiency of the process for developing the 503A Bulks
List, FDA reopened the nomination process in July 2014 (79 FR 37747,
July 2, 2014) and provided a more detailed description about what
information should be included in a nomination to support the Agency's
evaluation. FDA stated that bulk drug substances that were previously
nominated would not be further considered unless they were renominated
and the new nominations were adequately supported. Substances that were
already eligible for use in compounding or that were not adequately
supported would not be placed on the list.
In response to that solicitation, approximately 740 unique
substances were nominated. Of those substances, approximately 315 are
components of an FDA-approved drug product or the
[[Page 91074]]
subject of an applicable USP or NF monograph. Such substances can be
used in compounding under section 503A(b)(1)(A)(i)(I) and (II) of the
FD&C Act and, therefore, are not eligible for inclusion on the 503A
Bulks List.
At least one of the nominated substances is a finished drug product
that was nominated by its brand name. Finished drug products are not
eligible for the 503A Bulks List because they do not meet the
definition of a bulk drug substance in Sec. 207.3(4).
At least one of the nominated substances is a biological product
subject to approval in a biologics license application (BLA) under
section 351 of the Public Health Service (PHS) Act (42 U.S.C. 262) when
used for the indication proposed in the nomination. This substance is
not eligible for the 503A Bulks List because biological products
subject to approval in a BLA under section 351 of the PHS Act are not
eligible for the exemptions in section 503A of the FD&C Act. No
biological products subject to approval in a BLA will be considered for
the 503A Bulks List.
At least four of the nominated substances appear on the list
published by FDA of substances that have been withdrawn or removed from
the market because the drug products or components of the drug products
have been found to be unsafe or not effective (section 503A(b)(1)(C) of
the FD&C Act) (Withdrawn or Removed List). Such substances cannot be
used in compounding under section 503A of the FD&C Act, and therefore,
are not eligible for inclusion on the 503A Bulks List.
One of the nominated substances has no currently accepted medical
use and is included on Schedule I of the Controlled Substances Act
(CSA) (21 U.S.C. 812(c)). The CSA does not allow possession or
distribution of Schedule I substances (see 21 U.S.C. 841(a)(1) and
829), except for research purposes (see 21 U.S.C. 823(f)), and Schedule
I substances will not be considered for the 503A Bulks List. Those
desiring to do research on a Schedule I substance may apply to do so
under an investigational new drug (IND) application.
Of the substances that are not components of an approved drug
product or the subject of an applicable USP or NF monograph, finished
drug products, biological products subject to licensure in a BLA, and
do not appear on the Withdrawn or Removed List or Schedule I of the
CSA, about 350 substances were nominated with insufficient supporting
evidence for FDA to evaluate them.
The remaining substances may be eligible for inclusion on the 503A
Bulks List and were nominated with sufficient supporting information
for FDA to evaluate them. Ten of those substances have been evaluated
and are discussed in section V. The rest will be discussed in future
notices of proposed rulemaking (NPRMs) after they have been evaluated.
Once the Agency completes its review of the substances that were
nominated for the 503A Bulks List with adequate supporting information
under the July 2, 2014, request for nominations, FDA will consider
additional substances nominated for inclusion on the list if they are
eligible and adequate supporting information is submitted to permit FDA
to meaningfully evaluate them (see section III).
With regard to the substances nominated with sufficient supporting
information for FDA to evaluate them, including the 10 nominated
substances discussed in this proposed rule, FDA generally does not
intend to take regulatory action against a State-licensed pharmacy,
Federal facility, or licensed physician for compounding a drug product
using a bulk drug substance that is not the subject of an applicable
USP or NF monograph or a component of an FDA-approved drug product,
provided that the other conditions in section 503A and the FD&C Act are
met, until the substance is addressed in a final rule. FDA is not
applying this interim policy to a nominated substance however, if the
Agency has identified the substance as posing a significant safety
risk,\2\ or if the substance was nominated without adequate support.
For further information on this subject, see the guidance for industry
entitled ``Interim Policy on Compounding Using Bulk Drug Substances
Under Section 503A of the Federal Food, Drug, and Cosmetic Act'' (Ref.
1). As described in the guidance, the following categories of bulk drug
substances are identified on FDA's Web site at https://www.fda.gov/downloads/Drugs/GuidanceComplianceRegulatoryInformation/PharmacyCompounding/UCM467373.pdf: (1) The substances nominated with
sufficient supporting information that are under evaluation, (2) the
substances nominated with sufficient supporting information but with
which FDA has identified significant safety risks relating to the use
of these bulk drug substances in compounding, and (3) the substances
nominated with insufficient supporting evidence for FDA to evaluate
them.
---------------------------------------------------------------------------
\2\ This is not a determination regarding whether the substances
will be added to the 503A Bulks list. FDA intends to make that
determination after notice and comment rulemaking, as set forth in
this proposal.
---------------------------------------------------------------------------
IV. Legal Authority
As described in the Background section, section 503A of the FD&C
Act describes the conditions that must be satisfied for human drug
products compounded by a licensed pharmacist or licensed physician to
be exempt from three sections of the FD&C Act (sections 501(a)(2)(B),
502(f)(1), and 505 (21 U.S.C. 351(a)(2)(B), 352(f)(1), and 355)). One
of the conditions that must be satisfied for a compounded drug to
qualify for the exemptions under section 503A of the FD&C Act is that a
licensed pharmacist in a State-licensed pharmacy or Federal facility or
a licensed physician compounds the drug product using bulk drug
substances that: (1) Comply with the standards of an applicable USP or
NF monograph, if a monograph exists, and the USP chapter on pharmacy
compounding; (2) if such a monograph does not exist, are drug
substances that are components of drugs approved by the Secretary; or
(3) if such a monograph does not exist and the drug substance is not a
component of a drug approved by the Secretary, that appear on the 503A
Bulks List. See section 503A(b)(1)(A)(i) of the FD&C Act. Section
503A(c)(1) of the FD&C Act also states that the Secretary shall issue
regulations to implement section 503A, and that before issuing
regulations to implement section 503A(b)(1)(A)(i)(III) pertaining to
the 503A bulks list, among other sections, the Secretary shall convene
and consult an advisory committee on compounding unless the Secretary
determines that the issuance of such regulations before consultation is
necessary to protect the public health. Section 503A(c)(2) of the FD&C
Act requires the Secretary to issue the regulations in consultation
with the USP, and to include in the regulation the criteria for such
substances that shall include historical use, reports in peer reviewed
journals, and any other criteria the Secretary identifies. Thus,
section 503A of the FD&C Act, in conjunction with our general
rulemaking authority in section 701(a) of the FD&C Act, serves as our
principal legal authority for this proposed rule.
V. Description of the Proposed Rule
FDA is proposing to add Sec. 216.23 to title 21 of the Code of
Federal Regulations (CFR) to set forth criteria to evaluate bulk drug
substances for inclusion on the 503A Bulks List. Additionally, after
considering 10 bulk drug substances for the 503A Bulks List,
[[Page 91075]]
FDA proposes to codify the initial 503A Bulks List to include 6 of the
bulk drug substances that were considered and to identify 4 substances
that were considered and would not be placed on the list. The criteria
and the bulk drug substances considered for inclusion on the list are
described in the paragraphs that follow.
A. Criteria for Evaluating Bulk Drug Substances for the 503A Bulks List
Section 503A(c)(2) of the FD&C Act provides that the criteria for
determining which substances should appear on the 503A Bulks List shall
include historical use, reports in peer reviewed medical literature, or
other criteria the Secretary of Health and Human Services may identify.
Consistent with the July 2, 2014, Federal Register notice (79 FR 37747)
soliciting nominations for this list, and as presented to and discussed
with the PCAC in February 2015 (Ref. 2), FDA proposes that the
following criteria be used to evaluate the nominated substances:
The physical and chemical characterization of the
substance;
Any safety issues raised by the use of the substance in
compounded drug products;
The available evidence of effectiveness or lack of
effectiveness of a drug product compounded with the substance, if any
such evidence exists; and
Historical use of the substance in compounded drug
products, including information about the medical condition(s) the
substance has been used to treat and any references in peer-reviewed
medical literature.
In evaluating candidates for the 503A Bulks List under these
criteria, the Agency proposes to use a balancing test. Specifically,
the Agency proposes to consider each criterion in the context of the
others and balance them, on a substance-by-substance basis, to decide
whether a particular substance is appropriate for inclusion on the 503A
Bulks List.
Under the first criterion, the physical and chemical
characterization of the substance, FDA would consider each substance's
purity, identity, and quality. Based on attributes such as the
substance's molecular structure, stability, melting point, appearance,
likely impurities, and solubilities, FDA would determine whether the
substance can be identified consistently based on its physical and
chemical characteristics. If a substance cannot be well characterized
chemically and physically, the Agency proposes that this criterion
weigh against its inclusion on the 503A Bulks List because there can be
no assurance that its properties and toxicities, when used in
compounding, would be the same as the properties and toxicities
reported in the literature and considered by the Agency.
Under the second criterion, FDA would consider the safety issues
raised by the use of each substance in pharmacy compounding. Based on
FDA's review of the substances nominated to date, it is unlikely that
candidates for the 503A Bulks List will have been thoroughly
investigated in in vitro or in animal toxicology studies, or that there
will be well-controlled clinical trials to substantiate their safe use
in humans. Thus, in evaluating list candidates, the Agency is likely to
have at its disposal very limited information, or in some cases no
information, of the type and quality that is ordinarily required and
evaluated as part of the drug approval process.
To evaluate the safety of the substances then, the Agency proposes
to rely on available information, including reports in peer-reviewed
medical literature, about each substance's pharmacology, acute
toxicity, repeat dose toxicity, mutagenicity, developmental and
reproductive toxicity, and carcinogenicity. The Agency would also rely
on reports and abstracts in the literature about adverse reactions the
substances have caused in humans. In applying the safety criterion, FDA
also proposes to consider the availability of approved drug products or
drug products that follow an OTC monograph (OTC monograph products).
The existence of approved drug products or OTC monograph products would
likely weigh against inclusion on the proposed list when the toxicity
of a particular substance appears to be significant or where there are
other safety concerns associated with the use of the substance in
compounded drug products.
Under the third criterion, FDA proposes to consider the available
evidence of the substance's effectiveness or lack of effectiveness for
a particular use, including reports in peer-reviewed medical
literature, if any such evidence exists. In the new drug approval
process, applicants are required to demonstrate effectiveness under the
substantial evidence standard described in section 505(d) of the FD&C
Act. FDA recognizes that few, if any, of the candidates for the 503A
Bulks List will have been studied in adequate and well-controlled
investigations sufficient to satisfy this standard. Thus, in its
balancing of the relevant criteria, the Agency would take into account
whatever relevant evidence concerning effectiveness is available.
For example, for substances that have been widely used for a long
period of time, the literature may include anecdotal reports of
effectiveness for a particular use or reports of one or more trials
suggesting possible effectiveness. Conversely, the literature may
contain anecdotal or clinical evidence that a particular bulk drug
substance was not effective for a particular use (negative
effectiveness data). When evaluating a bulk drug substance that is
proposed for the treatment of a less serious illness, FDA would
generally be more concerned about the safety of the substance than
about its effectiveness. Thus, the availability of minimal
effectiveness data, or the existence of mere anecdotal reports, would
be less likely to preclude inclusion of the substance on the list.
However, for a bulk drug substance that is proposed to treat a more
serious or life-threatening disease, there may be more serious
consequences associated with ineffective therapy, particularly when
there are approved drug products or OTC monograph products. In those
cases, the existence of approved drug products or OTC monograph
products would likely weigh against inclusion on the proposed list, and
the availability of minimal effectiveness data, or the presence of
negative effectiveness data, would weigh more heavily against placement
on the list in FDA's balancing of the relevant criteria.
Under the fourth criterion, the historical use of the substance in
pharmacy compounding, FDA proposes to consider the length of time the
substance has been used in pharmacy compounding, the medical conditions
it has been used to treat, how widespread its use has been, including
use in other countries, and any references in peer-reviewed medical
literature. The Agency proposes that the longer a substance has been
used in pharmacy compounding and the broader its use, the more this
criterion will weigh in favor of inclusion of the substance on the
list.
B. Methodology for Developing the 503A Bulks List
FDA reviewed the substances addressed in this proposed rule in the
context of adequately supported nominated uses. In certain
circumstances, FDA also reviewed substances in the context of
unnominated or inadequately supported uses because, for example, such
uses appear to be widespread, are intended to treat serious conditions,
or pose serious risks to patients. The
[[Page 91076]]
information that FDA assessed to evaluate the substances addressed in
this proposed rule under each of the proposed evaluation criteria was
obtained from publicly available sources, including peer-reviewed
medical literature. Some of this information was referenced in the
nominations, and the remainder FDA gathered through independent
searches of medical and pharmaceutical databases. FDA did not review
raw data. The nature, quantity, and quality of the information FDA
assessed varied considerably from substance to substance. In some
cases, there were very little data. For other substances, reports in
the literature were more plentiful and sometimes comprised hundreds or
thousands of articles. In those cases, generally the Agency limited its
review to a sample of the best literature sources available (e.g.,
review articles in widely known, peer-reviewed journals; meta-analyses;
reports of randomized controlled trials).
FDA's evaluation of the nominated substances was, necessarily, far
less rigorous and less comprehensive than the Agency's review of drugs
as part of the new drug approval process. The new drug approval process
is conducted based on extensive data compiled and submitted with new
drug and abbreviated new drug applications, which are not available for
the nominated substances. Additionally, the Agency's review during the
drug approval process includes premarketing evaluation of a specific
drug formulation, the sponsor's chemistry and manufacturing controls,
and the establishments where approved drugs will be manufactured. In
contrast, these bulk drug substances will be evaluated only for
possible use in compounded drugs.
Therefore, the proposed inclusion of a drug substance on the 503A
Bulks List should not, in any way, be equated with or considered an FDA
approval, endorsement, or recommendation of any drug compounded using
the substance. Nor should it be assumed that a drug compounded using
the substances on the proposed list has been proven to be safe and
effective under the standards required for Agency approval. Any person
who represents that a compounded drug made with a bulk drug substance
that appears on this list is FDA approved, or otherwise endorsed by FDA
generally, or for a particular indication, will cause the drug to be
misbranded under section 502(a) and/or 502(bb) of the FD&C Act.
On February 23 and 24, 2015, and on June 17, 2015, FDA consulted
with the PCAC created under section 503A(c)(1) of the FD&C Act, about
the criteria proposed to evaluate substances nominated for the list and
about the 10 substances that are addressed in this proposed rule (Refs.
2-4). The Agency has considered all of the PCAC's recommendations in
developing this proposed rule, and the Agency intends to continue to
consult with the PCAC in evaluating future candidates for the 503A
Bulks List. The first 10 substances evaluated are addressed in this
proposed rule. Going forward, FDA intends to publish NPRMs proposing
additional substances be placed on the list or not placed on the list
on a rolling basis as evaluations are completed. Depending on the
length of time it takes to complete a rulemaking, multiple rulemakings
may be ongoing simultaneously.
Section 503A of the FD&C Act requires that FDA create the 503A
Bulks List by regulation, in consultation with the USP. See section
503A(c)(2) of the FD&C Act. To this end, FDA has been periodically
meeting with USP and discussing the 503A Bulks List (Refs. 5 and 6).
After publication of this NPRM, the public will have an opportunity to
comment on the proposed rule. After considering the comments on this
proposed rule submitted to the docket, FDA will issue the 503A Bulks
List as a final rule, which will be codified in the CFR. The final
version of the rule may include all, none, or only some of the
substances proposed here for inclusion on the 503A Bulks List,
depending on the comments received, and will also identify those
substances the Agency has determined should not be placed on the list.
The Agency may amend the 503A Bulks List to add or delete substances
after further notice and comment rulemaking.
Individuals and organizations may petition FDA to amend the list
(to add or delete bulk drug substances) at any time after the final
rule is published (see 21 CFR 10.30). Individuals and organizations may
also nominate new substances for the 503A Bulks List or comment on
nominated substances that have not yet been addressed in an NPRM via
Docket No. FDA-2015-N-3534 while that docket is open.
C. Substances Proposed for Inclusion on the 503A Bulks List
Under section 503A(c)(2) of the FD&C Act, FDA is proposing that the
following six bulk drug substances, which are neither the subject of a
current applicable USP or NF monograph nor components of FDA-approved
drugs, be included on the 503A Bulks List, and the drug products
compounded with those substances may qualify for the exemptions
provided for in section 503A of the FD&C Act (i.e., from sections
501(a)(2)(B), 502(f)(1), and 505 of the FD&C Act). When a salt or ester
of an active moiety is listed, only that particular salt or ester may
be used. The base compound and other salts or esters of the same active
moiety must be evaluated separately for eligibility for the 503A Bulks
List. Additionally, when a bulk drug substance is included on the 503A
Bulks List subject to certain restrictions (for example, for a
particular route of administration (e.g., topical)), only dosage forms
for that route of administration may be compounded with that bulk drug
substance.
The following bulk drug substances are being proposed for the 503A
Bulks List, to appear in Sec. 216.23(a) of Title 21 of the CFR:
1. Brilliant Blue G
Brilliant Blue G, also known as Coomassie Brilliant Blue G-250,\3\
was evaluated for use as a dye used in staining for visualization
during ophthalmic procedures. It is well characterized physically and
chemically. There are potential mutagenic and carcinogenic concerns
associated with Brilliant Blue G; however, those concerns are mitigated
in clinical use because the dye is immediately washed out of the eye
after administration, and tissue that is stained with the dye is
removed as part of the surgical procedure. Published clinical trials
provide some evidence for efficacy of Brilliant Blue G in staining the
internal limiting membrane. Brilliant Blue has had relatively
widespread use for staining the internal limiting membrane during
retinal surgery for approximately 10 years. There is one product that
is FDA-approved for staining the internal limiting membrane and the
anterior capsule.
---------------------------------------------------------------------------
\3\ While there are other substances referred to by the name
``Brilliant Blue,'' only Coomassie Brilliant Blue G-250 (CAS RN
6104-58-1, UNII M1ZRX790SI) was evaluated, and the Agency is
proposing only that substance for inclusion on the 503A Bulks List.
The other substances referred to as ``Brilliant Blue'' would have to
be nominated and separately evaluated for consideration for
inclusion on the 503A Bulks List.
---------------------------------------------------------------------------
FDA proposed to the PCAC that Brilliant Blue G be included on the
503A Bulks List (Ref. 7), and at its meeting on June 17, 2015, the PCAC
voted to include Brilliant Blue G on the list (Ref. 4). The proposed
rule would place Brilliant Blue G on the 503A Bulks List.
2. Cantharidin
Cantharidin, which is obtained from various species of blister
beetle, was
[[Page 91077]]
evaluated for topical use \4\ in the treatment of warts and molluscum
contagiosum. It is well characterized physically and chemically.
Cantharidin is extremely toxic, due to its potential for severe
irritation. However, clinical data accumulated since 1958 indicate
that, with careful use under physician direction, toxicities observed
with cantharidin, are no worse than and sometimes less severe than
those seen with other destructive modalities in the treatment of
molluscum contagiosum and warts. Evidence of some efficacy of
cantharidin in the treatment of warts and molluscum contagiosum has
been reported in the literature. It appears to have been widely used to
treat molluscum contagiosum and warts since the 1950s. There are no
approved prescription or OTC monograph products for molluscum
contagiosum. For warts, there are no prescription drug products
approved for use outside of the genital area. A variety of OTC
monograph products containing salicylic acid are available.
---------------------------------------------------------------------------
\4\ Except where specified otherwise, ``topical use'' means for
application on the skin only and does not include oral,
intravaginal, or ophthalmic use.
---------------------------------------------------------------------------
FDA proposed to the PCAC that cantharidin be included on the 503A
Bulks List for topical use only (Ref. 8). At the PCAC meeting on
February 24, 2015, the PCAC voted to include cantharidin on the list
(Ref. 3). Because the supported nominations and the Agency's review
were limited to the topical use of this substance, the proposed rule
would place cantharadin on the 503A Bulks List for topical use only.
3. Diphenylcyclopropenone (DPCP)
DPCP was evaluated for topical use in the treatment of alopecia
areata and nongenital warts. It is well characterized physically and
chemically but degrades readily by hydrolysis in an alcoholic base or
exposure to light. Known safety concerns about the use of DPCP are
limited to reported adverse effects primarily due to its action as a
contact sensitizer to elicit contact dermatitis. Evidence of some
efficacy of DPCP in the treatment of alopecia areata and recalcitrant
nongenital warts has been reported in the literature. DPCP has been
used to treat resistant non-genital warts and alopecia areata for over
30 years. The only FDA-approved drug product indicated for the
treatment of alopecia areata is intralesional injection of
corticosteroid suspensions. For warts, there are no approved
prescription drug products outside of the genital area. A variety of
OTC monograph products are available containing salicylic acid at
percentages varying from 17 to 40 percent.
FDA proposed to the PCAC that DPCP be included on the 503A Bulks
List (Ref. 8). At its meeting on February 24, 2015, the PCAC voted to
include DPCP on the list (Ref. 3). Because the supported nominations
and the Agency's review were limited to the topical use of this
substance, the proposed rule would place DPCP on the 503A Bulks List
for topical use only.
4. N-acetyl-D-glucosamine (NAG)
NAG, also known as acetyl-D glucosamine or N-acetyl glucosamine,
was evaluated for topical use in the treatment of hyperpigmentation and
other skin conditions. It is well characterized physically and
chemically. Topical use of NAG has been associated with relatively
minor and infrequent side effects. Studies have indicated that NAG may
be effective for reducing diffuse and local facial hyperpigmentation.
NAG has been used topically for the treatment of hyperpigmentation
since the mid-2000s. There are FDA-approved drug products indicated for
the treatment of hyperpigmentation and other skin conditions, which are
not serious or life-threatening conditions.
FDA proposed to the PCAC that NAG be included on the 503A Bulks
List for topical use only (Ref. 7). At the PCAC meeting on June 17,
2015, the PCAC voted to include NAG on the list (Ref. 4). Because the
supported nominations and the Agency's review were limited to the
topical use of this substance, the proposed rule would place NAG on the
503A Bulks List for topical use only.
5. Squaric Acid Dibutyl Ester (SADBE)
SADBE was evaluated for topical use in the treatment of alopecia
areata and recalcitrant nongenital warts. It is well characterized
physically and chemically but hydrolyzes readily in the presence of
water. The adverse effects from use of SADBE are primarily related to
its action as contact sensitizer. Evidence of some efficacy of SADBE in
the treatment of recalcitrant nongenital warts and alopecia areata has
been reported in the literature. SADBE has been used in the treatment
of resistant nongenital warts and alopecia areata for 30 to 40 years.
The only FDA-approved drug product indicated for the treatment of
alopecia areata is intralesional injection of corticosteroid
suspensions. For warts, there are no prescription drug products
approved for use outside of the genital area. A variety of OTC
monograph products are available containing salicylic acid at
percentages varying from 17 to 40 percent.
FDA proposed to the PCAC that SADBE be included on the 503A Bulks
List (Ref. 8). At its meeting on February 24, 2015, the PCAC voted to
include SADBE on the list (Ref. 3). Because the supported nominations
and the Agency's review were limited to the topical use of this
substance, the proposed rule would place SADBE on the 503A Bulks List
for topical use only.
6. Thymol Iodide
Thymol iodide was evaluated for use as a topical treatment for
ulcerations and skin infections, as well as an intrapleural treatment
for pleural effusions. It is well characterized physically and
chemically. Reports indicate that it has been used without major
complications. Literature reports some efficacy of thymol iodide for
pleural effusions, which are serious and can be life-threatening
conditions. Data regarding the effectiveness of thymol iodide in
compounding for topical use on wounds or ulcers in various skin
conditions is limited; however, these skin conditions generally are not
serious or life-threatening. Thymol iodide has been in use for over 100
years. Regarding use as an antiseptic in surgery and use as an external
application to wounds or ulcers in various skin conditions, approved
and OTC monograph products are available. There are also FDA-approved
products available to treat malignant pleural effusions.
FDA proposed to the PCAC that thymol iodide be included on the 503A
Bulks List (Ref. 8). At its meeting on February 23, 2015, the PCAC
voted to include thymol iodide on the list (Ref. 2). Because the
supported nominations were limited to the topical use of this
substance, and because pleural effusions are serious and potentially
life-threatening conditions for which there are approved products
available, the proposed rule would place thymol iodide on the 503A
Bulks List for topical use only.
D. Substances Considered and Not Proposed for Inclusion on the 503A
Bulks List
FDA is proposing that four of the bulk drug substances that it has
evaluated not be included on the 503A Bulks List. Bulk drug substances
that are considered for the 503A Bulks list but not placed on the list
cannot be used to compound drug products that would qualify for the
exemptions in section 503A. If a prescribing practitioner nevertheless
believes that a patient should be treated with a drug product
compounded from such a bulk drug substance, it may be possible to
obtain
[[Page 91078]]
the drug under an IND. For information about the requirements for
proceeding under an IND, visit FDA's Web site at https://www.fda.gov/Drugs/DevelopmentApprovalProcess/HowDrugsareDevelopedandApproved/ApprovalApplications/InvestigationalNewDrugINDApplication/default.htm.
The four bulk drug substances that have been evaluated and that FDA
is not proposing to place on the list, and the reasons for that
proposal, are as follows:
1. Oxitriptan
Oxitriptan, also known as 5-hydroxytryptophan (5-HTP), was
evaluated as a treatment for depression and insomnia. It is a
hydroxylated form of a naturally occurring amino acid, tryptophan.
Oxitriptan is well characterized physically and chemically. However,
there are significant safety concerns related to its use. Based upon
its mechanism of action, concomitant use of oxitriptan with
antidepressant drugs could result in serotonin syndrome, a serious and
life-threatening drug interaction. Additionally, medications used to
treat depression have been linked to an increase in suicidal thinking
and behavior. There are no data to suggest that oxitriptan would be
free of similar risks, and compounded drugs do not include labeling
that would adequately warn physicians and patients of such risks. Other
potential adverse reactions include moderate gastrointestinal effects,
which are common upon administration of oxitriptan.
Data supporting the efficacy of oxitriptan for depression are
limited, and there is no evidence to support long-term efficacy of
oxitriptan for the treatment of this chronic disease. Depression is a
serious and potentially life-threatening condition, and there are
multiple FDA-approved antidepressants that have been shown to be safe
and effective in their approved forms that are appropriately labeled.
Regarding the use of oxitriptan to treat insomnia, the clinical trials
examining insomnia were too poorly designed and/or executed to assess
efficacy. There are multiple FDA-approved drug products available for
the treatment of insomnia. The length of time oxitriptan has been used
in compounding is uncertain, although it has been discussed in
scientific journals dating back approximately 40 years.
On balance, the physiochemical characteristics, the safety
concerns, lack of evidence of effectiveness, and historical use of
oxitriptan weigh against inclusion of this substance on the 503A Bulks
List. In particular, the Agency's proposal regarding this substance is
based on the seriousness of the safety concerns related to the use of
oxitriptan for depression in lieu of, or causing a delay in the use of
an approved product, the lack of adequate warnings that would inform
patients and prescribers of the risks associated with taking an
oxitriptan product, and the availability of approved drug products for
the treatment of depression, a potentially life-threatening condition.
FDA proposed to the PCAC that this substance not be included on the
503A Bulks List (Ref. 7). At its meeting on June 17, 2015, the PCAC
voted not to include oxitriptan on the list (Ref. 4). The proposed rule
would not place oxitriptan on the 503A Bulks List.
2. Piracetam
Piracetam was evaluated as a treatment for enhancing cognitive
skills in treating a variety of cognitive disorders, including
Alzheimer's disease. It has also been studied for treatment of
coagulation disorders and vertigo. It is well characterized physically
and chemically. Piracetam is approved in the United Kingdom (UK) as a
prescription drug for the adjunctive treatment of cortical myoclonus.
The labeling of the UK product identifies that the drug is renally
excreted, that the dosage should be adjusted in the presence of renal
disease, and that it is contraindicated in end-stage renal disease.
Piracetam acts by multiple mechanisms to prolong bleeding time and is
therefore not recommended for use by individuals with medical
conditions that prolong bleeding time or that are taking concomitant
anticoagulants or other medications that prolong bleeding (Ref. 9).
Piracetam is not recommended for women who are pregnant, planning to
become pregnant, or breastfeeding, because, according to the UK
product's labeling, the drug has been shown to cross the placenta and
be excreted in human milk. It is also recommended that individuals
required to restrict their salt intake avoid piracetam (id.).
Piracetam was assessed for the treatment of mild cognitive
impairment, a potential component of Alzheimer's disease, in a large,
well-conducted, controlled clinical trial that failed to demonstrate
efficacy. Studies of the efficacy of piracetam for other indications
have been inconclusive, many of which were poorly designed or executed,
or used flawed statistical methods to analyze the results. Piracetam's
regulatory approval in the UK for the treatment of cortical myoclonus,
which is not among the uses for which piracetam was nominated, was
based on a single center, retrospective review of 40 patients treated
with piracetam (id.). FDA-approved products are available for treatment
of the conditions, and conditions related to, those for which piracetam
was nominated, for example, for Alzheimer's disease, which is
frequently preceded by mild cognitive impairment. Regarding historical
use, piracetam has been available for approximately 40 years.
On balance, the physiochemical characteristics, safety concerns,
inconclusive evidence of effectiveness, and historical use of piracetam
weigh against inclusion of this substance on the list. In particular,
the Agency's proposal regarding this substance is based on the limited
evidence of benefit associated with piracetam, the seriousness of the
conditions for which piracetam was nominated to be used, and the
availability of safe and effective FDA-approved medications for many of
these uses. FDA proposed to the PCAC that this substance not be
included on the 503A Bulks List (Ref. 8). At its meeting on February
24, 2015, the PCAC voted not to include piracetam on the list (Ref. 3).
The proposed rule would not place piracetam on the 503A Bulks List.
3. Silver Protein Mild
Silver protein mild, also known as mild silver protein, was
evaluated for use as an anti-infective agent for ophthalmic use. Silver
protein mild is not well characterized because the term ``silver
protein mild'' is used to refer to a variety of different drug
products. There are also safety concerns associated with the use of
silver protein mild. It can cause argyria, which is a permanent ashen-
gray discoloration of the skin, conjunctiva, and internal organs.
Regarding effectiveness, silver protein mild has been found to be
inferior to another treatment in clinical trials. A number of FDA-
approved anti-infective agents for ophthalmic use are available and
have been shown to be both safe and effective. While it has a long
history of use, dating back to the early 1900s, the use of silver
protein mild declined dramatically after the introduction of FDA-
approved ocular anti-infectives.
On balance, the physiochemical characteristics, safety issues,
questionable effectiveness, and historical use of silver protein mild
weigh against inclusion of this substance on the 503A Bulks List. In
particular, the Agency's proposal is based on the facts that silver
protein mild is not well characterized, that in clinical trials it has
been found to be inferior to another treatment and
[[Page 91079]]
numerically inferior to no treatment at all, and that chronic use may
result in permanent discoloration of the conjunctiva, cornea, and/or
lens. FDA proposed to the PCAC that this substance not be included on
the 503A Bulks List (Ref. 8). At its meeting on February 23, 2015, the
PCAC voted not to include silver protein mild on the list (Ref. 2). The
proposed rule would not place silver protein mild on the 503A Bulks
List.
4. Tranilast
Tranilast, an antiallergenic agent, was evaluated for the treatment
of allergic disorders, arthritis, dry eye syndrome, keloids, and
hypertrophic scars. It is approved in South Korea and Japan for the
treatment of asthma, keloids, and hypertrophic scarring, and as an
ophthalmic solution for allergic conjunctivitis. It is well
characterized physically and chemically. However, there are significant
safety concerns associated with its systemic administration. In a well-
controlled clinical trial with nearly 12,000 participants (the
Prevention of REStenosis with Tranilast and its Outcomes (PRESTO)
Trial) (Ref. 10), tranilast was associated with significantly elevated
liver enzymes (three times the upper limit of normal) in 11 percent of
patients within 1 to 3 months of drug initiation, as well as anemia,
renal failure, rash, and dysuria.\5\ Liver toxicity is of particular
concern because many of the conditions for which tranilast was
nominated are chronic conditions. While there is some evidence that
tranilast may be effective for allergic disorders, evidence of
effectiveness for other uses is either not available or inconclusive.
For allergy, arthritis, and ophthalmic indications, there are numerous
FDA-approved and OTC monograph products. The length of time tranilast
has been used in compounding is uncertain, although it has been
discussed in scientific journals dating back approximately 40 years.
---------------------------------------------------------------------------
\5\ During the PCAC meeting on June 17, 2015, the PRESTO trial
was criticized by one of the tranilast nominators as having
insufficiently accounted for the medical history of the subjects,
among other things (see Ref. 4). To the contrary, the five-arm trial
design appears to have been properly controlled for the patients'
various medical conditions, and signals of liver toxicity were
consistent across arms (see Ref. 10).
---------------------------------------------------------------------------
On balance, the physiochemical characteristics, safety concerns,
lack of evidence of effectiveness, and historical use of tranilast
weigh against inclusion of this substance on the 503A Bulks List,
particularly given the seriousness of the safety concerns related to
hepatotoxicity of tranilast and contraindications in pregnant and
breastfeeding women, the availability of approved products for most of
the proposed uses, and the lack of evidence that tranilast is
effective. FDA proposed to the PCAC that this substance not be included
on the 503A Bulks List (Ref. 7). However, at its meeting on June 17,
2015, the PCAC voted to include tranilast on the list for topical use
only (Ref. 4).
Subsequent to that meeting, FDA reviewed the topical use of
tranilast further. It obtained the label of the Japanese tranilast
product, RIZABEN, but found no information on the transdermal
absorption or other pharmacokinetics of tranilast when applied
topically to healthy or diseased human skin (Ref. 11). The labeling of
the Japanese product identifies a number of safety concerns, including
a contraindication in pregnant women, especially during the first
trimester of pregnancy, and in those who might be pregnant, due to
evidence of teratogenicity in animal studies (id.). The labeling also
states that tranilast is detected in breast milk and should be avoided
by breastfeeding women. In addition, the RIZABEN label lists a drug
interaction with warfarin and identifies a number of serious adverse
events, particularly those that are hematologic in nature (leukopenia,
thrombocytopenia, anemia, hemolytic anemia), associated with the oral
use of tranilast. Safety information regarding other routes of
administration is limited.
FDA also noted evidence that some increases in some liver function
tests (bilirubin) are explained by tranilast inhibition of uridine
diphosphate glucuronosyltransferase 1A1 (UGT1A1) especially in patients
with a genotype for Gilbert's Disease. Increases in liver transaminases
observed with tranilast are not typically seen with inhibition of
UGT1A1. It is speculated that tranilast impairs the metabolism of drugs
that are metabolized by UGT1A1. If these drugs are associated with
transaminase elevations, inhibiting the drug's metabolism may lead to
liver transaminitis.
As was found in the Agency's initial review and presented to the
PCAC, there is no persuasive information available regarding the safety
or effectiveness of topical tranilast. FDA has identified only two
reports in the literature describing the efficacy and safety of
tranilast administered topically for the treatment of keloids and
hypertrophic scars (Refs. 12 and 13). One of those studies was an open-
label trial, and the other was a case series. Between the two studies,
only five patients were exposed to topical tranilast.
As stated previously, FDA has serious concerns about the safety of
tranilast when administered orally. The Agency has insufficient
information about the systemic absorption of topical tranilast
formulations to determine whether topical administration of the drug
product would present the same safety concerns. Given the lack of
information available about the safety and efficacy of topical
tranilast, and safety concerns related to the oral use of this product,
the proposed rule would not place tranilast on the 503A Bulks List.
VI. Proposed Effective Date
The Agency proposes that any final rule based on this proposal will
become effective 30 days after the date of publication of the final
rule in the Federal Register.
VII. Analysis of Environmental Impact
FDA has 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.
VIII. Economic Analysis of Impacts
We have examined the impacts of the proposed rule under Executive
Order 12866, Executive Order 13563, 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 and 13563 direct us to assess all costs
and benefits of available regulatory alternatives and, when regulation
is necessary, to select regulatory approaches that maximize net
benefits (including potential economic, environmental, public health
and safety, and other advantages; distributive impacts; and equity). We
have developed a comprehensive Economic Analysis of Impacts that
assesses the impacts of the proposed rule. We believe that this
proposed rule is not a significant regulatory action as defined by
Executive Order 12866.
The Regulatory Flexibility Act requires us to analyze regulatory
options that would minimize any significant impact of a rule on small
entities. Because we find little evidence that a substantial number of
small entities would be affected by the proposed rule or that the
economic impact on each affected small entity would be significant, we
propose to certify that the proposed rule will not have a significant
economic impact on a substantial number of small entities.
The Unfunded Mandates Reform Act of 1995 (section 202(a)) requires
us to
[[Page 91080]]
prepare a written statement, which includes an assessment of
anticipated costs and benefits, 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 $146 million, using the most current (2015) Implicit
Price Deflator for the Gross Domestic Product. This proposed rule would
not result in an expenditure in any year that meets or exceeds this
amount.
Table 1--Economic Data: Costs and Benefits Statement
--------------------------------------------------------------------------------------------------------------------------------------------------------
Discount rate Period covered
Category Primary estimate Low estimate High estimate Units year dollars (%) (years) Notes
--------------------------------------------------------------------------------------------------------------------------------------------------------
Benefits
--------------------------------------------------------------------------------------------------------------------------------------------------------
Annualized Monetized $ mil/year. Not Estimated .............. .............. .................. 7 10 ..............
(N.E.).
Annualized Monetized $ mil/year. N.E............... .............. .............. .................. 3 10 ..............
Annualized Quantified........... N.E............... .............. .............. .................. 7 .............. ..............
Annualized Quantified........... N.E............... .............. .............. .................. 3 .............. ..............
Qualitative..................... Not including four .............. .............. .................. .............. .............. ..............
bulk drug
substances from
the 503A Bulks
List would limit
the use of
potentially
ineffective or
unsafe unapproved
drugs.
--------------------------------------------------------------------------------------------------------------------------------------------------------
Costs
--------------------------------------------------------------------------------------------------------------------------------------------------------
Annualized Monetized $ mil/year. N.E............... .............. .............. .................. 7 10 ..............
Annualized Monetized $ mil/year. N.E............... .............. .............. .................. 3 10 ..............
Annualized Quantified........... $118 to $235 one- .............. .............. 2014.............. 7 .............. ..............
time per firm
costs.
Annualized Quantified........... $118 to $235 one- .............. .............. 2014.............. 3 .............. ..............
time per firm
costs.
Qualitative..................... .................. .............. .............. .................. .............. .............. ..............
--------------------------------------------------------------------------------------------------------------------------------------------------------
Transfers
--------------------------------------------------------------------------------------------------------------------------------------------------------
Federal Annualized Monetized $ .................. .............. .............. .................. 7 .............. ..............
mil/year.
Federal Annualized Monetized $ .................. .............. .............. .................. 3 .............. ..............
mil/year.
From/To......................... From:............. .............. .............. To:............... .............. .............. ..............
Other Annualized $ mil/year..... N.E............... .............. .............. .................. 7 .............. ..............
Other Annualized Monetized $ mil/ N.E............... .............. .............. .................. 3 .............. ..............
year.
[[Page 91081]]
From/To......................... From: Producers of .............. .............. To: Producers of .............. .............. ..............
bulk drug alternative
substances not treatments,
proposed for consumers, using
inclusion and these treatments
compounding and payers for
pharmacies using these treatments.
these substances.
--------------------------------------------------------------------------------------------------------------------------------------------------------
Effects
--------------------------------------------------------------------------------------------------------------------------------------------------------
State, Local, and/or Tribal
Government: No effect.
Small Business: Unknown effect..
Wages: No effect................
Growth: No effect...............
--------------------------------------------------------------------------------------------------------------------------------------------------------
The Economic Analysis of Impacts of the proposed rule performed in
accordance with Executive Order 12866, Executive Order 13563, the
Regulatory Flexibility Act, and the Unfunded Mandates Reform Act is
available at https://www.regulations.gov under the docket number for
this proposed rule (Ref. 14) and at https://www.fda.gov/AboutFDA/ReportsManualsForms/Reports/EconomicAnalyses/default.htm. We invite
comments on this analysis.
A. Summary of the Costs of the Rule
We lack data on the scope of the current use of the affected bulk
drug substances and the number of firms that would be affected by the
rule. Without this information, we cannot quantify the total potential
costs of the proposed rule. Potential costs include administrative
costs, additional costs for consumers and payers if alternative
therapies are more costly than the affected compounded drug products,
and a potential loss of producer surplus if producers use additional
resources in response to the rule. We estimate that each affected firm
would spend 1 to 2 hours on administrative costs to read and understand
the rule. The average hourly wage for a pharmacist in 2014 equals about
$57, or $114 including 100 percent overhead. Thus, each affected firm
would incur administrative costs that range from $118 to $235. We
request comment on the potential costs and number of firms affected by
the proposed rule.
B. Summary of the Benefits of the Rule
The benefits of the rule are unquantified. We include a qualitative
discussion of potential benefits. For consumers who switch to more
effective treatments, there would be benefits as consumers experience
better health outcomes than they do currently.
C. Summary of the Impact on Small Entities
The Regulatory Flexibility Act requires a Regulatory Flexibility
Analysis (RFA) unless the Agency can certify that the proposed rule
would have no significant impact on a substantial number of small
entities. The Small Business Administration (SBA) establishes
thresholds for small entities by North American Industry Classification
System (NAICS); the SBA considers small any entity below these
thresholds. Firms affected by the proposed rule would fall into three
major industries, NAICS 325412 Pharmaceutical Preparation
Manufacturing, NAICS 424210 Drugs and Druggists' Sundries Merchant
Wholesalers, and NAICS 446110 Pharmacies and Drug Stores. The
thresholds for these industries are 750 employees for NAICS 325412, 100
employees for NAICS 424210, and annual sales of $27.5 million for NAICS
446110.
We lack data on the number or size of manufacturers, wholesalers,
and compounding pharmacies that would be affected by the proposed rule.
Moreover, we find little evidence of widespread use of four bulk drug
substances not proposed for inclusion on the 503A Bulks List. This
suggests that the impact of the rule would likely not be significant on
small entities. Because we find little evidence that a substantial
number of small entities would be affected by the proposed rule or that
the economic impact on each affected small entity would be significant,
we believe that the proposed rule would not have a significant economic
impact on a substantial number of small entities, but the impacts are
uncertain. We request detailed comments and data on the number of small
entities that would be affected by the proposed rule, as well as data
on the economic impact of the proposed rule on these small entities.
IX. Paperwork Reduction Act of 1995
The submission of comments on this proposed rule would be
submissions in response to a Federal Register notice, in the form of
comments, which are excluded from the definition of ``information''
under 5 CFR 1320.3(h)(4) of Office of Management and Budget regulations
on the Paperwork Reduction Act (i.e., facts or opinions submitted in
response to general solicitations of comments from the public,
published in the Federal Register or other publications, regardless of
the form or format thereof, provided that no person is required to
supply specific information pertaining to the commenter, other than
that necessary for self-identification, as a condition of the Agency's
full consideration of the
[[Page 91082]]
comment). The proposed rule contains no other collection of
information.
X. Federalism
We have analyzed this proposed rule in accordance with the
principles set forth in Executive Order 13132. We have determined that
the proposed rule, if finalized, would not contain policies that would
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.
XI. References
The following references are on display in the Division of Dockets
Management (see ADDRESSES) and are available for viewing by interested
persons between 9 a.m. and 4 p.m., Monday through Friday; they are also
available electronically at https://www.regulations.gov. FDA has
verified the Web site addresses, as of the date this document publishes
in the Federal Register, but Web sites are subject to change over time.
1. FDA, ``Guidance for Industry: Interim Policy on Compounding
Using Bulk Drug Substances Under Section 503A of the Federal Food,
Drug, and Cosmetic Act,'' (https://www.fda.gov/downloads/Drugs/GuidanceComplianceRegulatoryInformation/Guidances/UCM469120.pdf),
2016.
2. FDA, Transcript of the February 23, 2015, Meeting of the
Pharmacy Compounding Advisory Committee (Afternoon Session), 2015,
(https://www.fda.gov/downloads/AdvisoryCommittees/CommitteesMeetingMaterials/Drugs/PharmacyCompoundingAdvisoryCommittee/UCM444500.pdf).
3. FDA, Transcript of the February 24, 2015, Meeting of the
Pharmacy Compounding Advisory Committee, 2015, (https://www.fda.gov/downloads/AdvisoryCommittees/CommitteesMeetingMaterials/Drugs/PharmacyCompoundingAdvisoryCommittee/UCM444501.pdf).
4. Transcript of the June 17, 2015, Meeting of the Pharmacy
Compounding Advisory Committee (Afternoon Session), 2015, (https://www.fda.gov/downloads/AdvisoryCommittees/CommitteesMeetingMaterials/Drugs/PharmacyCompoundingAdvisoryCommittee/UCM458513.pdf).
5. Memorandum to File on FDA Consultations with USP, September
26, 2016.
6. Letter from USP to FDA, October 7, 2016.
7. FDA Briefing Document for the June 17-18, 2015, Meeting of
the Pharmacy Compounding Advisory Committee, 2015, (https://www.fda.gov/downloads/AdvisoryCommittees/CommitteesMeetingMaterials/Drugs/PharmacyCompoundingAdvisoryCommittee/UCM449535.pdf).
8. FDA Briefing Document for the February 23-24, 2015, Meeting
of the Pharmacy Compounding Advisory Committee, 2015, (https://www.fda.gov/downloads/AdvisoryCommittees/CommitteesMeetingMaterials/Drugs/PharmacyCompoundingAdvisoryCommittee/UCM433804.pdf).
9. Obeso, J. A., et al., ``Piracetam in the Treatment of
Different Types of Myoclonus,'' Clinical Neuropharmacology, 11(6):
529-536, 1988.
10. Holmes, D.R., Jr., M. Savage, J.M. LaBlanche, et al.,
``Results of Prevention of REStenosis with Tranilast and its
Outcomes (PRESTO) Trial,'' Circulation, 106(10): 1243-1250, 2002.
11. FDA Supplemental Review of Topical Tranilast, April 25,
2016.
12. Shigeki, S., T. Murakami, N. Yata, and Y. Ikuta, ``Treatment
of Keloid and Hypertrophic Scars by Iontophoretic Transdermal
Delivery of Tranilast,'' Scandinavian Journal of Plastic and
Reconstructive Surgery and Hand Surgery, 31(2): 151-159, 1997.
13. Banov, D., F. Banov, and A.S. Bassani, ``Case Series: The
Effectiveness of Fatty Acids From Pracaxi Oil in a Topical Silicone
Base for Scar and Wound Therapy,'' Dermatology and Therapy, 4(2):
259-269, 2014.
14. Economic Analysis of Impacts.
List of Subjects in 21 CFR Part 216
Drugs, Prescription drugs.
Therefore, under the Federal Food, Drug, and Cosmetic Act, and
under authority delegated to the Commissioner of Food and Drugs, the
Food and Drug Administration proposes to amend 21 CFR part 216 as
follows:
PART 216--HUMAN DRUG COMPOUNDING
0
1. The authority citation for part 216 is revised to read as follows:
Authority: 21 U.S.C. 351, 352, 353a, 353b, 355, and 371.
0
2. The heading for part 216 is revised to read as set forth above.
0
3. Section 216.23 is added to read as follows:
Sec. 216.23 Bulk drug substances that can be used to compound drug
products in accordance with section 503A of the Federal Food, Drug, and
Cosmetic Act.
(a) The following bulk drug substances can be used in compounding
under section 503A(b)(1)(A)(i)(III) of the Federal Food, Drug, and
Cosmetic Act.
Brilliant Blue G, also known as Coomassie Brilliant Blue G-250.
Cantharidin (for topical use only).
Diphenylcyclopropenone (for topical use only).
N-acetyl-D-glucosamine (for topical use only).
Squaric acid dibutyl ester (for topical use only).
Thymol iodide (for topical use only).
(b) After balancing the criteria set forth in paragraph (c) of this
section, FDA has determined that the following bulk drug substances
will not be included on the list of substances that can be used in
compounding set forth in paragraph (a) of this section:
Oxitriptan.
Piracetam.
Silver Protein Mild.
Tranilast.
(c) FDA will use the following criteria in evaluating substances
considered for inclusion on the list set forth in paragraph (a) of this
section:
(1) The physical and chemical characterization of the substance;
(2) Any safety issues raised by the use of the substance in
compounded drug products;
(3) The available evidence of the effectiveness or lack of
effectiveness of a drug product compounded with the substance, if any
such evidence exists; and
(4) Historical use of the substance in compounded drug products,
including information about the medical condition(s) the substance has
been used to treat and any references in peer-reviewed medical
literature.
(d) Based on evidence currently available, there are inadequate
data to demonstrate the safety or efficacy of any drug product
compounded using any of the drug substances listed in paragraph (a) of
this section, or to establish general recognition of the safety or
effectiveness of any such drug product. Any person who represents that
a compounded drug made with a bulk drug substance that appears on this
list is FDA approved, or otherwise endorsed by FDA generally or for a
particular indication, will cause the drug to be misbranded under
section 502(a) and/or 502(bb) of the Federal Food, Drug, and Cosmetic
Act.
Dated: December 9, 2016.
Leslie Kux,
Associate Commissioner for Policy.
[FR Doc. 2016-30109 Filed 12-15-16; 8:45 am]
BILLING CODE 4164-01-P
