List of Bulk Drug Substances for Which There is a Clinical Need Under Section 503B of the Federal Food, Drug, and Cosmetic Act, 71642-71652 [2022-25549]
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[FR Doc. 2022–25538 Filed 11–22–22; 8:45 am]
BILLING CODE 4163–18–P
DEPARTMENT OF HEALTH AND
HUMAN SERVICES
Food and Drug Administration
[Docket No. FDA–2018–N–3240]
List of Bulk Drug Substances for
Which There is a Clinical Need Under
Section 503B of the Federal Food,
Drug, and Cosmetic Act
AGENCY:
Food and Drug Administration,
HHS.
ACTION:
Notice.
The Food and Drug
Administration (FDA or Agency) is
developing a list of bulk drug
substances (active pharmaceutical
ingredients) for which there is a clinical
need (the 503B Bulks List). Drug
products that outsourcing facilities
compound using bulk drug substances
on the 503B Bulks List can qualify for
certain exemptions from the Federal
Food, Drug, and Cosmetic Act (FD&C
Act) provided certain conditions are
met. This notice identifies two bulk
drug substances that FDA has
considered and proposes to include on
the 503B Bulks List to compound three
categories of compounded drug
products: arginine hydrochloride (HCl)
for oral use, lysine HCl for oral use, and
lysine HCl for intravenous use in
SUMMARY:
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combination with FDA-approved,
single-ingredient arginine HCl for
intravenous use. This notice identifies
three bulk drug substances that FDA has
considered and proposes not to include
on the 503B Bulks List: etomidate,
furosemide, and rocuronium bromide.
Additional bulk drug substances
nominated for inclusion on this list are
under consideration and may be the
subject of future notices.
DATES: Either electronic or written
comments on the notice must be
submitted by January 23, 2023.
ADDRESSES: You may submit comments
as follows. Please note that late,
untimely filed comments will not be
considered. The https://
www.regulations.gov electronic filing
system will accept comments until
11:59 p.m. Eastern Time at the end of
January 23, 2023. Comments received by
mail/hand delivery/courier (for written/
paper submissions) will be considered
timely if they are postmarked or the
delivery service acceptance receipt is on
or before that date.
Electronic Submissions
Submit electronic comments in the
following way:
• Federal eRulemaking Portal:
https://www.regulations.gov. Follow the
instructions for submitting comments.
Comments submitted electronically,
including attachments, to https://
www.regulations.gov will be posted to
the docket unchanged. Because your
comment will be made public, you are
solely responsible for ensuring that your
comment does not include any
confidential information that you or a
third party may not wish to be posted,
such as medical information, your or
anyone else’s Social Security number, or
confidential business information, such
as a manufacturing process. Please note
that if you include your name, contact
information, or other information that
identifies you in the body of your
comments, that information will be
posted on https://www.regulations.gov.
• If you want to submit a comment
with confidential information that you
do not wish to be made available to the
public, submit the comment as a
written/paper submission and in the
manner detailed (see ‘‘Written/Paper
Submissions’’ and ‘‘Instructions’’).
Written/Paper Submissions
Submit written/paper submissions as
follows:
• Mail/Hand Delivery/Courier (for
written/paper submissions): Dockets
Management Staff (HFA–305), Food and
Drug Administration, 5630 Fishers
Lane, Rm. 1061, Rockville, MD 20852.
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Federal Register / Vol. 87, No. 225 / Wednesday, November 23, 2022 / Notices
• For written/paper comments
submitted to the Dockets Management
Staff, FDA will post your comment, as
well as any attachments, except for
information submitted, marked and
identified, as confidential, if submitted
as detailed in ‘‘Instructions.’’
Instructions: All submissions received
must include the Docket No. FDA–
2018–N–3240 for ‘‘List of Bulk Drug
Substances for Which There is a Clinical
Need Under Section 503B of the Federal
Food, Drug, and Cosmetic Act.’’
Received comments, those filed in a
timely manner (see ADDRESSES), will be
placed in the docket and, except for
those submitted as ‘‘Confidential
Submissions,’’ publicly viewable at
https://www.regulations.gov or at the
Dockets Management Staff between 9
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Friday, 240–402–7500.
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submission. You should submit two
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with a heading or cover note that states
‘‘THIS DOCUMENT CONTAINS
CONFIDENTIAL INFORMATION.’’ The
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www.govinfo.gov/content/pkg/FR-201509-18/pdf/2015-23389.pdf.
Docket: For access to the docket to
read background documents or the
electronic and written/paper comments
received, go to https://
www.regulations.gov and insert the
docket number, found in brackets in the
heading of this document, into the
‘‘Search’’ box and follow the prompts
and/or go to the Dockets Management
Staff, 5630 Fishers Lane, Rm. 1061,
Rockville, MD 20852, 240–402–7500.
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FOR FURTHER INFORMATION CONTACT:
Tracy Rupp, Center for Drug Evaluation
and Research, Food and Drug
Administration, 10903 New Hampshire
Ave., Bldg. 51, Silver Spring, MD 20993,
301–796–3100.
SUPPLEMENTARY INFORMATION:
I. Background
Section 503B of the FD&C Act (21
U.S.C. 353b) describes the conditions
that must be satisfied for drug products
compounded by an outsourcing facility
to be exempt from section 505 of the
FD&C Act (21 U.S.C. 355) (concerning
the approval of drugs under new drug
applications (NDAs) or abbreviated new
drug applications (ANDAs)), section
502(f)(1) (21 U.S.C. 352(f)(1))
(concerning the labeling of drugs with
adequate directions for use), and section
582 of the FD&C Act (21 U.S.C. 360eee–
1) (concerning drug supply chain
security requirements).1
Compounded drug products that meet
the conditions in section 503B are not
exempt from current good
manufacturing practice (CGMP)
requirements in section 501(a)(2)(B) of
the FD&C Act (21 U.S.C. 351(a)(2)(B)).2
Outsourcing facilities are also subject to
FDA inspections according to a riskbased schedule, specific adverse event
reporting requirements, and other
conditions that help to mitigate the risks
of the drug products they compound.3
Outsourcing facilities may or may not
obtain prescriptions for identified
individual patients and can, therefore,
distribute compounded drugs to
healthcare practitioners for ‘‘office
stock,’’ to hold in their offices in
advance of patient need.4
One of the conditions that must be
met for a drug product compounded by
an outsourcing facility to qualify for the
exemptions under section 503B of the
FD&C Act is that the outsourcing facility
may not compound a drug using a bulk
drug substance unless: (1) the bulk drug
substance appears on a list established
by the Secretary of Health and Human
Services identifying bulk drug
substances for which there is a clinical
need (the 503B Bulks List) or (2) the
drug compounded from the bulk drug
substance appears on the drug shortage
list in effect under section 506E of the
FD&C Act (21 U.S.C. 356e) at the time
1 Section
503B(a) of the FD&C Act.
section 503A(a) of the FD&C Act (21
U.S.C. 353a(a)) (exempting drugs compounded in
accordance with that section from CGMP
requirements) with section 503B(a) of the FD&C Act
(not providing an exemption from CGMP
requirements).
3 Section 503B(b)(4) and (5) of the FD&C Act.
4 Section 503B(d)(4)(C) of the FD&C Act.
2 Compare
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of compounding, distribution, and
dispensing.5
Section 503B of the FD&C Act directs
FDA to establish the 503B Bulks List by:
(1) publishing a notice in the Federal
Register proposing bulk drug substances
to be included on the list, including the
rationale for such proposal; (2)
providing a period of not less than 60
calendar days for comment on the
notice; and (3) publishing a notice in the
Federal Register designating bulk drug
substances for inclusion on the list.6
FDA has published a series of Federal
Register notices addressing bulk drug
substances nominated for inclusion on
the 503B Bulks List.7 This notice
identifies two bulk drug substances that
FDA has considered and proposes to
include on the 503B Bulks List and
three bulk drug substances that FDA has
considered and proposes not to include
on the 503B Bulks List.
For purposes of section 503B of the
FD&C Act, bulk drug substance means
an active pharmaceutical ingredient as
defined in § 207.1 (21 CFR
207.1).8 Active pharmaceutical
ingredient means 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, but the term does
not include intermediates used in the
synthesis of the substance.9 10
5 Section
6 Section
503B(a)(2)(A) of the FD&C Act.
503B(a)(2)(A)(i)(I) to (III) of the FD&C
Act.
7 See Federal Register of August 28, 2018 (83 FR
43877), March 4, 2019 (84 FR 7383), September 3,
2019 (84 FR 46014), July 31, 2020 (85 FR 46126),
and March 24, 2021 (86 FR 15673). The comment
period for the July 2020 notice was reopened for 30
days on January 8, 2021 (86 FR 1515), to allow
interested parties an additional opportunity to
comment. FDA has not yet reached a final
determination on whether the substances evaluated
in the September 2019, July 2020, or March 2021
notices will be added to the 503B Bulks List. In
addition, bumetanide, which was considered in the
August 2018 notice, remains under consideration
by the Agency.
8 See section 503B(a)(2) of the FD&C Act, which
defines bulk drug substances used in compounding
under section 503B according to 21 CFR 207.3(a)(4)
‘‘or any successor regulation.’’ Section 207.1 is the
successor regulation.
9 Section 503B(a)(2) of the FD&C Act and § 207.1.
10 Inactive ingredients are not subject to section
503B(a)(2) of the FD&C Act and will not be
included in the 503B Bulks List because they are
not included within the definition of a bulk drug
substance. Pursuant to section 503B(a)(3) of the
FD&C Act, inactive ingredients used in
compounding must comply with the standards of
an applicable U.S. Pharmacopeia or National
Formulary monograph, if a monograph exists.
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Federal Register / Vol. 87, No. 225 / Wednesday, November 23, 2022 / Notices
II. Methodology for Developing the
503B Bulks List
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A. Process for Developing the List
In the Federal Register of December 4,
2013 (78 FR 72838), FDA requested
nominations for specific bulk drug
substances for the Agency to consider
for inclusion on the 503B Bulks List.
FDA reopened the nomination process
in the Federal Register of July 2, 2014
(79 FR 37747) and provided more
detailed information on what FDA
needs to evaluate nominations for the
list. In the Federal Register of October
27, 2015 (80 FR 65770), the Agency
opened a new docket, FDA–2015–N–
3469, to provide an opportunity for
interested persons to submit new
nominations of bulk drug substances or
to renominate substances with sufficient
information or submit comments on
nominated substances.
As FDA evaluates bulk drug
substances, it intends to publish notices
for public comment in the Federal
Register that describe the FDA’s
proposed position on each substance
along with the rationale for that
position.11 After considering any
comments on FDA’s proposals regarding
whether to include nominated
substances on the 503B Bulks List, FDA
intends to consider whether input from
the Pharmacy Compounding Advisory
Committee (PCAC) on the nominations
would be helpful to the Agency in
making its determination, and if so, it
will seek PCAC input.12 Depending on
its review of the docket comments and
other relevant information before the
Agency, FDA may finalize its proposed
determination without change, or it may
finalize a modification to its proposal to
reflect new evidence or analysis
regarding clinical need. FDA will then
publish in the Federal Register a list
identifying the bulk drug substances for
which it has determined there is a
clinical need and FDA’s rationale in
making that final determination. FDA
will also publish in the Federal Register
a list of those substances it considered
but found that there is no clinical need
to use in compounding and FDA’s
rationale in making this decision.
FDA intends to maintain a list of all
bulk drug substances it has evaluated on
11 This is consistent with procedure set forth in
section 503B(a)(2)(A)(i) of the FD&C Act. Although
the statute only directs FDA to issue a Federal
Register notice and seek public comment when it
proposes to include bulk drug substances on the
503B Bulks List, we intend to seek comment when
the Agency has evaluated a nominated substance
and proposes either to include or not to include the
substance on the list.
12 Section 503B of the FD&C Act does not require
FDA to consult the PCAC before developing a 503B
Bulks List.
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its website, and separately identify bulk
drug substances it has placed on the
503B Bulks List and those it has decided
not to place on the 503B Bulks List. This
list is available at https://www.fda.gov/
media/120692/download. FDA will only
place a bulk drug substance on the 503B
Bulks List when it has determined there
is a clinical need for outsourcing
facilities to compound drug products
using the bulk drug substance. If a
clinical need to compound drug
products using the bulk drug substance
has not been demonstrated, based on the
information submitted by the nominator
and any other information considered
by the Agency, FDA will not place a
bulk drug substance on the 503B Bulks
List.
FDA is evaluating bulk drug
substances nominated for the 503B
Bulks List on a rolling basis. FDA
intends to evaluate and publish in the
Federal Register its proposed and final
determinations in groups of bulk drug
substances until all nominated
substances that were sufficiently
supported have been evaluated and
either placed on the 503B Bulks List or
identified as bulk drug substances that
were considered, but determined not to
be appropriate for inclusion on the 503B
Bulks List (Ref. 1).
B. Analysis of Substances Nominated
for the List
As noted above, the 503B Bulks List
includes bulk drug substances for which
the Agency has determined there is a
clinical need. The Agency is evaluating
bulk drug substances that were
nominated for inclusion on the 503B
Bulks List, proceeding case by case,
under the clinical need standard
provided by the statute (Ref. 2).13 In
applying this standard to develop the
proposals in this notice, FDA interprets
the phrase ‘‘bulk drug substances for
which there is a clinical need’’ to mean
that the 503B Bulks List may include a
bulk drug substance if: (1) there is a
clinical need for an outsourcing facility
to compound the drug product and (2)
the drug product must be compounded
using the bulk drug substance. FDA
does not interpret supply issues, such as
13 On March 4, 2019, FDA announced the
availability of a final guidance entitled ‘‘Evaluation
of Bulk Drug Substances Nominated for Use in
Compounding Under Section 503B of the Federal
Food, Drug, and Cosmetic Act’’ (84 FR 7390);
available at https://www.fda.gov/media/121315/
download. This guidance describes FDA policies for
developing the 503B Bulks List and the Agency’s
interpretation of the phrase ‘‘bulk drug substances
for which there is a clinical need’’ as it is used in
section 503B of the FD&C Act. The analysis under
the statutory ‘‘clinical need’’ standard described in
this notice is consistent with the approach
described in FDA’s guidance.
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backorders, to be within the meaning of
‘‘clinical need’’ for compounding with a
bulk drug substance. Section 503B of
the FD&C Act separately provides for
compounding from a bulk drug
substance under the exemptions
discussed above if the drug product
compounded from the bulk drug
substance is on the FDA drug shortage
list at the time of compounding,
distribution, and dispensing.
Additionally, FDA does not consider
convenience in administering a
particular drug product (e.g., a ready-touse form) or the cost of the compounded
drug product as compared with an FDAapproved drug product when assessing
‘‘clinical need.’’
All of the bulk drug substances that
we are addressing in this notice are
components of FDA-approved drug
products,14 and we therefore began our
evaluation of the bulk drug substances
by asking one or both, as applicable, of
the following questions:
(1) Is there a basis to conclude, for
each FDA-approved product that
includes the nominated bulk drug
substance, that: (a) an attribute of the
FDA-approved drug product makes it
medically unsuitable to treat certain
patients for a condition that FDA has
identified for evaluation and (b) the
drug product proposed to be
compounded is intended to address that
attribute?
(2) Is there a basis to conclude that the
drug product proposed to be
compounded must be produced from a
bulk drug substance rather than from an
FDA-approved drug product?
The reason for question 1 is that
unless an attribute of the FDA-approved
drug is medically unsuitable for certain
patients, and a drug product
compounded using a bulk drug
substance that is a component of the
approved drug is intended to address
that attribute, there is no clinical need
to compound a drug product using that
bulk drug substance. Rather, such
compounding would unnecessarily
expose patients to the risks associated
with drug products that do not meet the
standards applicable to FDA-approved
drug products for safety, effectiveness,
quality, and labeling and would
undermine the drug approval process.
The reason for question 2 is that to place
a bulk drug substance on the 503B Bulks
List, FDA must determine that there is
a clinical need for outsourcing facilities
to compound a drug product using the
bulk drug substance rather than starting
with an FDA-approved drug product.
When it is feasible to compound a drug
14 Specifically, arginine HCl, etomidate,
furosemide, lysine HCl, and rocuronium bromide.
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product by starting with an approved
drug product, there are certain benefits
of doing so over starting with a bulk
drug substance, including that approved
drugs have undergone premarket review
for safety, effectiveness, and quality,
and are manufactured by a facility that
is subject to premarket assessment,
including site inspection, as well as
routine post-approval risk-based
inspections. In contrast, FDA does not
conduct a premarket review of the
quality standards, specifications, and
controls for bulk drug substances used
in compounding and does not conduct
a premarket assessment of the
manufacturer of the bulk drug
substance.
If the answer to both of these
questions is ‘‘yes,’’ there may be a
clinical need for outsourcing facilities to
compound using the bulk drug
substance, and we would evaluate the
substance further, applying the factors
described below. If the answer to either
of these questions is ‘‘no,’’ we generally
would not include the bulk drug
substance on the 503B Bulks List,
because there would not be a basis to
conclude that there may be a clinical
need to compound drug products using
the bulk drug substance instead of
administering an approved drug or
compounding starting with an approved
drug product. FDA answered ‘‘yes’’ to
both of the threshold questions for two
of the bulk drug substances that are
components of approved drug products
that we are addressing in this notice.
Accordingly, as explained further
below, we proceeded further in our
evaluation of these substances by
conducting a balancing test and are
proposing to include those substances
on the 503B Bulks List.
We are conducting a balancing test
using four factors. Specifically, on a
substance-by-substance basis, we
consider available data relevant to each
factor in the context of the other factors
and balance all four factors to determine
whether the statutory ‘‘clinical need’’
standard has been met. The balancing
test includes the following factors:
• The physical and chemical
characterization of the substance;
• Any safety issues raised by the use
of the substance in compounding;
• The available evidence of
effectiveness or lack of effectiveness of
a drug product compounded with the
substance, if any such evidence exists;
and
• Current and historical use of the
substance in compounded drug
products, including information about
the medical condition(s) that the
substance has been used to treat and any
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references in peer-reviewed medical
literature.
The discussion below reflects FDA’s
consideration of these four factors
where they are applicable and describes
how they were applied to develop
FDA’s proposal to include three entries
addressing two bulk drug substances on
the 503B Bulks List.
In this notice, FDA evaluated certain
nominated bulk drug substances for
potential inclusion on the 503B Bulks
List either alone or in combination with
other bulk drug substances. FDA will
not consider comments raising different
combinations of bulk drug substances
than those evaluated by FDA in this
notice to be within the scope of this
notice. New nominations may be
submitted to docket FDA–2015–N–3469
for combinations of bulk drug
substances that were not previously
nominated and included for evaluation
in this notice. The docket is available on
https://www.regulations.gov.
To assess whether there is a clinical
need for outsourcing facilities to use a
bulk drug substance in compounding,
FDA must evaluate the drug products
that have been proposed to be made
from the nominated bulk drug
substances. Therefore, FDA’s evaluation
of a bulk drug substance includes
detailed consideration of the drug
products that are proposed to be
compounded, including the conditions
justifying clinical need under the
applicable statutory standard.
Comments on FDA’s preliminary
evaluation of a bulk drug substance
should include adequate support for the
commenter’s position. For example, a
commenter writing to support inclusion
of a nominated bulk drug substance on
the 503B Bulks List should include
sufficient information to permit a
meaningful clinical need evaluation by
FDA of the proposed product.
Commenters writing in favor of or in
opposition to a proposal to include or
not to include an entry on the 503B
Bulks List should address, for each
proposed compounded drug product,
the factors FDA evaluated in making its
proposal.15 After FDA publishes a
Federal Register notice making a final
determination regarding whether a bulk
drug substance will be placed on the
503B Bulks List, FDA will no longer
consider comments submitted to the
docket regarding that bulk drug
substance, but interested parties may
submit a citizen petition to FDA
15 See also FDA’s guidance for industry,
‘‘Evaluation of Bulk Drug Substances Nominated for
Use in Compounding Under Section 503B of the
Federal Food, Drug, and Cosmetic Act’’ (March
2019), and our Federal Register notice of October
27, 2015.
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71645
requesting specific action or relief (see
21 CFR 10.30).
C. Inclusion of Bulk Drug Substances on
the 503B Bulks List
In preparing its proposal to include
two bulk drug substances on the 503B
Bulks List, FDA considered whether the
clinical need for the bulk drug
substance in the proposed compounded
drug product is limited by, for example,
route of administration or dosage form.
As appropriate, and as explained further
below, the Agency has tailored its
proposed entries on the 503B Bulks List
to reflect its findings related to clinical
need for the bulk substances proposed
for inclusion on the list. FDA requested
comments on the proposal to limit
listings in this manner in our Federal
Register notice of July 31, 2020 (85 FR
46126). The comment period for the July
2020 notice was reopened for 30 days
on January 8, 2021 (86 FR 1515), to
provide interested parties an additional
opportunity to comment before FDA
began to develop its final
determinations. After considering the
comments submitted regarding the
proposal, in the Federal Register notice
of January 27, 2022 (87 FR 4240), FDA
listed three bulk drug substances to
compound drug products for topical use
only.
Consistent with the approach
described in the 2020 notice, and as
reflected in the entries that appear on
the 503B Bulks List to date, the entries
proposed in this notice would authorize
use of two bulk drug substances.
Arginine HCl would be authorized for
use to compound single-ingredient drug
products for oral use only; lysine HCl
would be authorized for use to
compound single-ingredient drug
products for oral use; and lysine HCl
would also be authorized for use in
combination with FDA-approved,
single-ingredient arginine HCl injection,
U.S. Pharmacoepia (USP) to compound
drug products for intravenous (IV) use
only.16 As discussed further in this
notice, FDA’s proposals with respect to
inclusion of lysine HCl and arginine
HCl on the 503B Bulks List pertain to
the L- forms of lysine HCl and arginine
HCl exclusively.17
III. Substances Considered and
Proposed for Inclusion on the 503B
Bulks List
Because the substances in this section
are components of FDA-approved drug
products, we considered whether: (1)
16 In this notice, ‘‘single-ingredient’’ refers to a
drug product containing one active ingredient. The
drug product may also contain excipients.
17 See footnote 18 below.
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there is a basis to conclude that an
attribute of each FDA-approved drug
product that includes the nominated
bulk drug substance makes each one
medically unsuitable to treat certain
patients for a condition that FDA has
identified for evaluation, and the drug
products proposed to be compounded
are intended to address that attribute in
each FDA-approved drug product and
(2) whether the drug products proposed
to be compounded must be
compounded using a bulk drug
substance. In addition, because we
answered these two questions in the
affirmative for certain drug products
proposed to be compounded from the
nominated bulk drug substances, we
applied the four-factor balancing test
described above. The bulk drug
substances that were evaluated and that
FDA is proposing to place on the 503B
Bulks List are arginine HCl for oral use
only, lysine HCl for oral use only, and
lysine HCl for use in combination with
FDA-approved, arginine HCl injection
for intravenous use only. The reasons
for FDA’s proposals are included below.
lotter on DSK11XQN23PROD with NOTICES1
A. Arginine HCl
Arginine HCl was nominated as a
bulk drug substance for the 503B Bulks
List to compound drug products that are
used for acute hyperammonemia in urea
cycle disorders (UCDs) and refractory
metabolic alkalosis, among other
conditions.18 19 The proposed routes of
18 See Docket No. FDA–2015–N–3469, document
nos. FDA–2015–N–3469–0244, FDA–2015–N–
3469–0169, FDA–2015–N–3469–0156-attachment
10, FDA–2015–N–3469–0202, and FDA–2015–N–
3469–0320. The nomination in Docket No. FDA–
2015–N–3469–0156-attachment 10 was for
‘‘Arginine HCL’’ and stated that the common name
of the substance is ‘‘L-arginine hydrochloride; Darginine hydrochloride.’’ However, the nominator
also stated that the chemical grade of the bulk drug
substance is USP. The USP monograph for arginine
HCl does not include D-arginine HCl. Therefore,
this review focuses on L-arginine HCl, not the
mixture of D- and L-arginine HCl. Arginine HCl
USP grade consists of L-arginine
monohydrochloride. The nomination discussed in
this Federal Register notice nominated L-arginine
HCl USP grade. ‘‘Arginine HCl’’ and ‘‘L-arginine
HCl’’ are used interchangeably throughout this
Federal Register notice. L-arginine HCl and Llysine HCl were also nominated (Docket No. FDA–
2015–N–3469–0073-attachment 10) to be used in
combination for intravenous administration with
LUTATHERA (lutetium Lu 177 dotatate injection)
treatment. That nomination is the subject of another
evaluation.
19 The following uses will not be considered in
this evaluation because the nominations did not
provide sufficient information, including citations
to relevant literature, supporting a clinical need for
the proposed uses: thyroid cysts; arginine
deficiency/supplementation; orgasmic dysfunction
in women; prevention or treatment of heart and
circulatory disease; combat fatigue; stimulation of
wound healing; boosting production of nitric oxide,
relaxing blood vessels, and treating circulatory and
other cardiovascular problems; and reducing waist
circumference, visceral fat, weight, and body mass
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administration are oral and intravenous,
among others,20 and the proposed
dosage forms are an oral solution or
suspension, capsule, powder for
dispersion, and injectable, among
others.21 The nominators proposed a
range of concentrations (12.5 to 40
percent) and 200 and 500 milligrams/
milliliters (mg/mL). They also proposed
strengths of 250 mg-500 mg unspecified
oral dosage forms and 700 mg-750 mg
oral capsules. This nominated bulk drug
substance is a component of an FDAapproved drug product (NDA 016931).
FDA has approved arginine HCl (R-Gene
10) as a 10 gram (GM)/100 mL (100 mg/
mL; 10 percent) injection for
intravenous administration 22 (Ref. 3).
index. In addition, the following labeled uses will
not be considered in this evaluation because the
nominations did not provide sufficient information,
including citations to relevant literature, supporting
a clinical need for a more concentrated IV product
or for a product to be administered via the oral or
topical route of administration: diagnostic aid in
conditions such as panhypopituitarism, pituitary
dwarfism, chromophobe adenoma, postsurgical
craniopharyngioma, hypophysectomy, pituitary
trauma, acromegaly, gigantism, and problems of
growth and stature.
20 The topical and IV routes of administration for
use of arginine HCl to treat hyperammonemia
associated with urea cycle disorder will not be
considered further because the nominations did not
provide sufficient evidence to support a clinical
need for drug products with these routes of
administration. Although some of the nominations
included articles that describe the use of
intravenous arginine HCl for treating patients with
hyperammonemia in urea cycle disorder, the
articles do not provide support for the nominator’s
proposal to make a more concentrated product than
the approved IV drug product containing the same
active ingredient. Therefore, the IV route of
administration will not be considered further for
treating hyperammonemia in urea cycle disorder
because the nominations did not provide
information supporting a clinical need for a more
concentrated product. Similarly, the oral route of
administration will not be considered further for
the use of arginine HCl to treat refractory metabolic
alkalosis because the nomination did not provide
any evidence to support a clinical need for drug
products with this route of administration. As
explained in section II.B of this notice, if a member
of the public would like FDA to evaluate arginine
HCl based on a clinical need for a drug product to
be compounded containing arginine HCl for
administration by a route that was not evaluated in
this notice, then that person should submit a
nomination to Docket No. FDA–2015–N–3469,
which is available on https://www.regulations.gov.
21 The proposed dosage forms (cream, ointment,
and gel) are associated with uses or routes of
administration that will not be considered in this
evaluation.
22 See, e.g., NDA 016931 labeling available as of
the date of this notice at https://
www.accessdata.fda.gov/drugsatfda_docs/label/
2010/016931s031lbl.pdf. Arginine (not HCl salt) is
available as a component of several approved drug
products that contain multiple amino acids (e.g., for
parenteral nutrition) (e.g., AMINOSYN II; NDA
020015). NDA 020015 labeling is available as of the
date of this notice at https://dailymed.nlm.nih.gov/
dailymed/fda/fdaDrugXsl.cfm?setid=5b426208f090-4650-86c3-89040ba45c2d&type=display. The
arginine in these approved drug products is not the
same bulk drug substance as arginine HCl, which
is the subject of this evaluation.
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Because arginine HCl is a component
of an FDA-approved drug product, we
considered whether: (1) there is a basis
to conclude that an attribute of the FDAapproved drug product that contains
arginine HCl makes it medically
unsuitable to treat certain patients for a
condition that FDA has identified for
evaluation, and the arginine HCl drug
product proposed to be compounded is
intended to address that attribute in the
FDA-approved drug product and (2)
whether the drug product proposed to
be compounded must be compounded
using a bulk drug substance. In
addition, because we answered these
two questions in the affirmative for an
oral arginine HCl compounded drug
product, we also conducted a balancing
test to further evaluate this bulk drug
substance by considering and applying
the four factors described above.
1. Suitability of FDA-Approved Drug
Products
A nominator proposes that there is a
clinical need for an oral, singleingredient arginine HCl compounded
drug product to treat patients with
certain UCDs. The references submitted
with the nomination describe the use of
arginine HCl orally for long-term
maintenance therapy in patients with
UCDs. There is a basis to conclude that
the FDA-approved drug product that
contains only arginine HCl (R-Gene 10)
is medically unsuitable to treat patients
who require long-term oral maintenance
therapy because the approved drug
product is only available for intravenous
administration and would not be
suitable for the use proposed in the
nomination, which would involve daily
oral administration.23 The drug product
proposed to be compounded is intended
to address the attribute of the approved
drug product that makes it medically
unsuitable for some patients because the
nominator proposes to compound oral
formulations (capsules, powder for
dispersion, and oral solution/
suspension) of arginine HCl.
Accordingly, FDA finds that the drug
product proposed to be compounded is
intended to address the attribute of the
approved drug product that makes it
medically unsuitable for some patients.
A nominator also proposes that there
is a clinical need for an intravenous
single-ingredient arginine HCl
23 Empower Pharmacy proposed to make several
different dosage forms, including ‘‘oral capsules,
powder for dispersion, oral solutions/suspensions.’’
We are not commenting on the potential suitability
of these various proposed dosage forms due to the
lack of data available on the various dosage forms.
Furthermore, none of the scientific literature
reviewed by FDA referred to off-label use of the
approved intravenous arginine HCL drug product in
patients with urea cycle disorder.
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lotter on DSK11XQN23PROD with NOTICES1
compounded drug product to treat
patients with refractory metabolic
alkalosis. The nomination does not
identify an attribute of the FDAapproved arginine HCl (R-Gene 10) 10
GM/100 mL (100 mg/mL; 10 percent)
injection for intravenous administration
that makes it medically unsuitable for
certain patients or indicate that the
compounded drug product is intended
to address any such attribute. FDA finds
no basis to conclude that an attribute of
the FDA-approved product makes it
medically unsuitable to treat certain
patients for a condition that FDA has
identified for evaluation and that a
proposed compounded product is
intended to address.
2. Whether the Drug Product Must Be
Compounded From a Bulk Drug
Substance
FDA finds that there is a basis to
conclude that the oral drug products
proposed to be compounded must be
made from a bulk drug substance rather
than from FDA-approved R-Gene 10
because of the difficulties and
complexities associated with starting
with the approved solution for
intravenous administration and
converting it either to capsules or to a
powder for dispersion that would be
administered orally. The nominator also
proposed to compound an oral solution
of arginine HCl that is at a higher
concentration than the approved
intravenous product (100 mg/mL).
There is a basis to conclude that the
proposed oral liquid drug product must
also be compounded starting from the
bulk drug substance because of the
difficulties and complexities associated
with compounding a more concentrated
solution beginning with the approved
product.
With regard to an intravenous, singleingredient arginine HCl compounded
drug product proposed to treat patients
with refractory metabolic alkalosis, the
nominator has not identified patients for
whom the approved products are
medically unsuitable or identified an
attribute of the approved drug product
that the proposed compounded drug
product is intended to address. Because
the nominations do not identify specific
differences between drug products that
would be compounded using arginine
HCl and the approved drug product
containing arginine HCl, there is
nothing for FDA to evaluate under
question 2 for intravenous singleingredient arginine HCl.
3. Balancing Test
Because FDA answered ‘‘yes’’ to both
of the threshold questions for arginine
HCl for oral administration, we next
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conducted the following balancing
testing to determine whether the
statutory ‘‘clinical need’’ standard has
been met. We considered data and
information regarding the physical and
chemical characterization of arginine
HCl, safety issues raised by use of this
substance in compounding, available
evidence of effectiveness or lack of
effectiveness, and historical and current
use in compounding.
Arginine HCl is a well-characterized
amino acid and is stable under ordinary
storage conditions. Provided the quality
of arginine HCl meets the standards in
its USP drug substance monograph,
arginine HCl is well characterized
physically and chemically.24
Oral administration of arginine HCl
does not raise serious safety issues. The
available literature and general clinical
practice guidelines for the treatment of
UCDs indicate that the oral formulation
of arginine HCl may be effective in
treating UCDs. There is evidence of the
historical and current use of arginine
HCl in compounding as an oral
formulation for the treatment of UCDs
(except those with arginase deficiency)
in the United States, Belgium, and the
United Kingdom. There are no FDAapproved oral arginine HCl drug
products in the United States.
Arginine HCl is a well-characterized
amino acid, does not raise serious safety
concerns, may be effective in treating
UCDs, and there is evidence of
historical and current use of arginine
HCl in compounding. Therefore, on
balance, the physical and chemical
characterization, safety, effectiveness,
and historical and current use of
arginine HCl for oral use weigh in favor
of including this substance on the 503B
Bulks List. Accordingly, we propose
adding arginine HCl to the 503B Bulks
List for oral use only.
B. Lysine HCl
Lysine HCl was nominated as a bulk
drug substance for the 503B Bulks List
to compound drug products that are
used to correct lysine deficiency with
lysinuric protein intolerance (LPI) and
for prophylaxis and acute treatment of
herpes simplex outbreak, among other
conditions.25 26 The proposed route of
24 See
section 503B(a)(2)(B) of the FD&C Act.
Docket No. FDA–2015–N–3469, document
nos. FDA–2015–N–3469–0200 and FDA–2015–N–
3469–0245. All of the nominations included in this
evaluation nominated lysine HCl USP grade. Lysine
HCl USP grade consists of L-lysine hydrochloride.
A nominator submitted duplicate nominations for
L-lysine HCl to the docket: FDA–2015–N–3469–
0199 (submitted on August 31, 2018) and FDA–
2015–N–3469–0200 (submitted on September 4,
2018). For the purposes of this evaluation, FDA
referred to the information in the most recent
nomination submitted to the docket (FDA–2015–N–
25 See
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71647
administration is oral, among others; the
proposed dosage forms are capsules and
solutions, among others.27 The
nominations proposed a strength range
of 100 to 500 mg. This nominated bulk
drug substance is a component of many
approved drug products as part of a
combination with multiple other amino
acids for intravenous administration
(e.g., NDA 018931).28 Lysine HCl is not
approved as a single-ingredient drug
product in any dosage form (Ref. 4).
Because lysine HCl is a component of
FDA-approved drug products, we
considered whether: (1) there is a basis
to conclude that an attribute of each
FDA-approved drug product that
contains lysine HCl makes each one
medically unsuitable to treat certain
patients for a condition that FDA has
identified for evaluation, and the lysine
HCl drug product proposed to be
3469–0200). On February 26, 2021, this nominator
provided additional information regarding their
nomination for lysine HCl to the University of
Maryland Center of Excellence in Regulatory
Science and Innovation (M–CERSI). The updated
information is also considered in this evaluation.
Another nominator nominated ‘‘L-lysine;’’ M–
CERSI clarified with this nominator that they
intended to nominate L-lysine HCl. L-arginine HCl
and L-lysine HCl were also nominated by a different
nominator (FDA–2015–N–3469–0074) to be used in
combination for intravenous administration with
LUTATHERA (lutetium Lu 177 dotatate injection)
treatment, which is the subject of another
evaluation.
26 The following uses will not be considered in
this evaluation because the nominations did not
provide any information, including citations to
relevant literature, supporting a clinical need for
the proposed use: correcting lysine deficiency
without LPI, rehydration and immune support,
osteoporosis, muscle recovery, prevention of
mucositis. The use of lysine HCl during peptide
receptor radionuclide therapy to reduce the
radiation dose to the kidneys is discussed in a
separate evaluation. In the updated nomination
information provided to M–CERSI, a nominator
proposed an additional use of ‘‘rehydration and
immune support’’ as an intramuscular injection.
27 The proposed topical, intravenous, and
intramuscular routes of administration will not be
considered in this evaluation because the
nominations do not provide any evidence to
support a clinical need for drug products with these
routes of administration for use of lysine HCL to
correct lysine deficiency with LPI or for the use of
lysine HCL for prophylaxis and acute treatment of
herpes simplex outbreak. Accordingly, the
proposed dosage forms associated with these routes
of administration (cream, ointment, and solutions
for injection) will not be considered in this
evaluation. A nominator cited one article that
studied the use of the topical product
‘‘SuperLysinePlus+’’ every 2 hours during waking
hours in patients with symptoms of a cold sore
consistent with a herpes simplex virus infection of
≤24 hours duration (Ref. 5). ‘‘[L]ysine’’ is included
in ‘‘SuperLysinePlus+’’ as an inactive ingredient.
Thus, this study does not provide evidence that
there is a need for topical lysine HCl in patients
with herpes simplex virus.
28 See, e.g., NDA 018931 labeling is available as
of the date of this notice at https://dailymed.nlm.
nih.gov/dailymed/fda/fdaDrugXsl.
cfm?setid=8543b5be-0f43-4891-9e56d7c39fe839b5&type=display.
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compounded is intended to address that
attribute in each FDA-approved drug
product and (2) whether the drug
product proposed to be compounded
must be compounded using a bulk drug
substance. In addition, because we
answered these two questions in the
affirmative for an oral lysine HCl
compounded drug product, we also
conducted a balancing test to further
evaluate this bulk drug substance by
considering and applying the four
factors described above.
lotter on DSK11XQN23PROD with NOTICES1
1. Suitability of FDA-Approved Drug
Products
A nominator proposes that there is a
clinical need for an oral, singleingredient lysine HCl compounded drug
product to treat patients with lysine
deficiency with LPI and for prophylaxis
and treatment of acute herpes simplex
outbreak. We find there is a basis to
conclude that the FDA-approved drug
products that contain lysine HCl are
medically unsuitable for the proposed
uses. The approved drug products all
contain lysine HCl in combination with
multiple other amino acids and are for
intravenous administration. The
nominators did not provide, and FDA
did not otherwise identify, evidence
that these additional active ingredients
are needed to treat the conditions
proposed by the nominators. In
addition, the approved products are
only available for intravenous
administration and would not be
suitable for the uses proposed in the
nominations, which would involve
daily oral administration. Accordingly,
FDA finds that the drug products
proposed to be compounded, oral
formulations of single-ingredient lysine
HCl, are intended to address the
attribute of the approved drugs that
makes them medically unsuitable for
some patients.
2. Whether the Drug Product Must Be
Compounded From a Bulk Drug
Substance
FDA finds that there is a basis to
conclude that the oral drug products
containing lysine as the single
ingredient proposed to treat patients
with lysine deficiency with LPI and for
prophylaxis and treatment of acute
herpes simplex outbreak must be
produced from a bulk drug substance
because of the difficulties and
complexities associated with removing
lysine HCl from the approved products,
which are all multiple amino acid
solutions.
3. Balancing Test
Because FDA answered ‘‘yes’’ to both
of the threshold questions for lysine
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HCl, we next conducted the following
balancing testing to determine whether
the statutory ‘‘clinical need’’ standard
has been met. We considered data and
information regarding the physical and
chemical characterization of lysine HCl,
safety issues raised by use of this
substance in compounding, available
evidence of effectiveness or lack of
effectiveness, and historical and current
use in compounding.
Lysine HCl is well-characterized
chemically and physically and is
expected to be stable under ordinary
storage conditions. Provided the quality
of lysine HCl meets the standards in its
USP drug substance monograph, lysine
HCl is well characterized physically and
chemically.29
The available data do not provide
evidence to support the effectiveness of
oral lysine in the prophylaxis or
treatment of herpes simplex, and a
number of FDA-approved therapies are
available for acute treatment and
prophylaxis of herpes simplex. Oral
lysine is also nominated for use in LPI,
an extremely rare disease, the exact
prevalence of which in the United
States is unknown. Oral lysine is used
in the treatment of LPI patients in small
doses established and prescribed on a
per patient basis to avoid
gastrointestinal intolerance. Published
data show that oral lysine normalizes
plasma concentration of lysine in
patients with LPI. While the long-term
results are inconclusive as to whether
chronic supplementation or intermittent
supplementation is consistently helpful
(or needed), they do suggest a positive
impact on growth in some patients. In
addition, there are no FDA-approved
products indicated for the treatment of
LPI and no FDA-approved, singleingredient lysine drug products for
lysine supplementation. Oral use of
lysine HCl does not raise serious safety
issues. The most commonly reported
adverse events of abdominal pain and
diarrhea are associated with high doses
of lysine HCl and are usually prevented
by titrating the dose to a lower
acceptable level. There is evidence
regarding the current and historical use
of lysine HCl in pharmacy
compounding, commonly in an
injectable dosage form, within the
United States. We found no evidence of
current or historical use of a
compounded lysine HCl product for oral
administration.
Lysine HCl is well-characterized
chemically; does not raise serious safety
issues; and although the data do not
support the effectiveness of lysine HCl
in the prophylaxis or treatment of
29 See
PO 00000
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Sfmt 4703
herpes simplex, published data show
that oral lysine normalizes plasma
concentration of lysine in patients with
LPI. There is evidence of historical and
current use of lysine HCl in
compounding. Therefore, on balance,
the physical and chemical
characterization, safety, effectiveness,
and historical and current use of lysine
HCl weigh in favor of including this
substance for oral use on the 503B Bulks
List. Accordingly, we propose adding
lysine HCl to the 503B Bulks List for
oral use only.
C. Lysine HCl as a Single Ingredient and
in Combination With Single-Ingredient
Arginine HCl
Lysine HCl was also nominated for
the 503B Bulks List both as a singleingredient and in combination with
arginine HCl.30 31 Lysine HCl was
nominated to compound singleingredient drug products that are used
for reduction of radiolabeled peptides
during peptide receptor radionuclide
therapy (PRRT).32 Lysine HCl in
combination with arginine HCl was
nominated for post-LUTATHERA 33
treatment. LUTATHERA is indicated to
treat somatostatin receptor-positive
gastroenteropancreatic neuroendocrine
tumors, including foregut, midgut, and
hindgut neuroendocrine tumors in
adults. The proposed route of
administration for lysine HCl used in a
compounded drug product in
combination with arginine HCl, is
intravenous and the proposed dosage
form is injection. For lysine HCl as a
30 See Docket No. FDA–2015–N–3469, document
nos. FDA–2015–N–3469–0073 attachment 10, FDA–
2015–N–3469–0074 attachment 4, and FDA–2015–
N–3469–0245. A nominator nominated ‘‘L-lysine.’’
M–CERSI clarified with the nominator that they
intended to nominate L-lysine HCl. L-arginine HCl
as a single ingredient product was nominated by
other parties for different uses and in different
formulations. Those nominations are the subject of
another evaluation. In addition, L-lysine HCl was
nominated as a single ingredient product for the
following uses: to correct lysine deficiency with or
without lysinuric protein intolerance, prophylaxis
and treatment of herpes simplex outbreak,
osteoporosis, muscle recovery, and prevention of
mucositis. These nominated uses are the subject of
another evaluation.
31 Lysine HCl USP grade consists of L-lysine
hydrochloride. All the nominations discussed in
this Federal Register notice nominated lysine HCl
USP grade. ‘‘lysine HCl’’ and ‘‘L-lysine HCl’’ are
used interchangeably throughout this Federal
Register notice. Arginine HCl USP grade consists of
L-arginine monohydrochloride. The nomination
discussed in this Federal Register notice nominated
L-arginine HCl USP grade. ‘‘Arginine HCl’’ and ‘‘Larginine HCl’’ are used interchangeably throughout
this Federal Register notice.
32 FDA interprets the nominator’s proposed use to
be to reduce the radiation dose to the kidneys
during PRRT.
33 Lutetium Lu-177 dotatate (LUTATHERA) was
approved by FDA on January 26, 2018. It is a PRRT
used to treat patients with neuroendocrine tumors.
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single-ingredient drug product, the
proposed route of administration is
intravenous, among others, and the
proposed dosage form is injection.34
The nominations proposed a strength
range of 25 to 100 mg/mL. The
nominated bulk drug substances
arginine HCl 35 and lysine HCl 36 are
components of FDA-approved drug
products labeled for intravenous
administration. Lysine HCl is not a
component of any single-ingredient,
approved drug product in any dosage
form, but arginine HCl is a component
of one single-ingredient, approved drug
product for intravenous administration
(Ref. 6).
Because lysine HCl and arginine HCl
are components of FDA-approved drug
products, we considered whether: (1)
there is a basis to conclude that an
attribute of each FDA-approved drug
product that contains lysine HCl or
arginine HCl makes each one medically
unsuitable to treat certain patients for a
condition that FDA has identified for
evaluation, and the lysine HCl and
arginine HCl drug products proposed to
be compounded are intended to address
that attribute in each FDA-approved
drug product and (2) whether the drug
product proposed to be compounded
must be compounded using a bulk drug
substance. In addition, because we
answered these two questions in the
affirmative for lysine HCl for the
intravenous route of administration, we
also conducted a balancing test to
further evaluate both the proposed
lysine HCl single-ingredient product
and the use of lysine HCl to compound
a drug product containing both lysine
HCl and FDA-approved arginine HCl by
considering and applying the four
factors described above.
1. Suitability of FDA-Approved Drug
Products
lotter on DSK11XQN23PROD with NOTICES1
A nominator proposes that there is a
clinical need for an intravenous product
containing a unique combination of
lysine HCl and arginine HCl to be used
in patients receiving LUTATHERA
34 The oral and topical routes of administration
will not be considered in this evaluation because
the nomination does not provide any evidence to
support FDA’s evaluation of these routes of
administration for use of lysine HCl to reduce the
radiation dose to the kidneys during PRRT.
35 See NDA 016931 labeling is available as of the
date of this notice at https://
www.accessdata.fda.gov/drugsatfda_docs/label/
2010/016931s031lbl.pdf.
36 See, e.g., NDA 018931 labeling is available as
of the date of this notice at https://
www.accessdata.fda.gov/drugsatfda_docs/label/
2020/018931s055,020849s025lbl.pdf. TRAVASOL
contains essential (including lysine as the HCl salt)
and nonessential amino acids (including arginine
base, not HCl salt).
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16:45 Nov 22, 2022
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treatment.37 According to the
LUTATHERA labeling, a dual
combination of arginine HCl and lysine
HCl is recommended for renal
protection during LUTATHERA
treatment.38 FDA-approved drug
products that contain lysine HCl are
medically unsuitable for the proposed
use for patients. Although approved
drug products that contain lysine HCl in
combination with multiple other amino
acids are used off-label for this
indication, the nominators did not
provide, and FDA did not otherwise
identify, evidence that these additional
active ingredients are needed for
radiation protection. Furthermore, there
is evidence that suggests that
combination L-lysine HCl/L-arginine
HCl compounded intravenous infusions
produce less nausea in patients
receiving them for this indication than
the FDA-approved amino acid solutions,
and therefore would lead to fewer
episodes of vomiting. The FDAapproved product containing arginine
HCl, R-Gene 10 10 GM/100 mL injection
for intravenous administration, is
medically unsuitable for patients
receiving LUTATHERA treatment
because LUTATHERA’s labeling
recommends administering an amino
acid solution containing L-lysine and Larginine before administering
LUTATHERA, rather than administering
arginine HCl as a single-ingredient.
The drug product proposed to be
compounded is intended to address the
attributes of the approved drugs that
make them medically unsuitable for
some patients because the nominator
proposes to compound an intravenous
formulation containing both lysine HCl
and arginine HCl without additional
active ingredients.
A nominator also proposes that there
is a clinical need for an intravenous
product containing lysine HCl as a
single ingredient (i.e., not in
combination with arginine-HCl) to
reduce radiolabeled peptides during
PRRT. The FDA-approved drug
products that contain lysine HCl all
contain lysine HCl in combination with
multiple other amino acids. The FDAapproved drug products that contain
37 In addition, a letter from the Society of Nuclear
Medicine and Molecular Imaging (SNMMI)
provided support for the proposed compounded
drug product, stating that ‘‘patients receiving lysine
and arginine solution suffered from much less
vomiting incidents in comparison with patients
infused with commercial solutions’’ and ‘‘lysine
and arginine solution is also more effective in
inhibiting renal uptake of radioactivity during
peptide receptor radionuclide therapy.’’ (Ref. 7).
38 See NDA 208700 labeling is available as of the
date of this notice at https://
www.accessdata.fda.gov/drugsatfda_docs/label/
2018/208700s000lbl.pdf.
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71649
lysine HCl are medically unsuitable for
the proposed use for some patients.
Although FDA-approved drug products
that contain lysine HCl in combination
with multiple other amino acids are
used off-label for this indication, the
nominators did not provide, and FDA
did not otherwise identify, evidence
that these additional active ingredients
are needed for radiation protection.
The drug product proposed to be
compounded is intended to address the
attribute of the approved drug that
makes it medically unsuitable for some
patients because the nominator
proposes to compound an intravenous
product containing lysine HCl as the
single ingredient, without the other
amino acids that are present in the
approved drug product.
2. Whether the Drug Product Must Be
Compounded From a Bulk Drug
Substance
In order to compound the proposed
drug product containing a combination
of lysine HCl and arginine HCl, FDA has
a basis to conclude that lysine HCl must
be compounded from bulk drug
substance rather than from the FDAapproved drug products. The bulk drug
substance lysine HCl must be used
because of the difficulties and
complexities associated with removing
lysine HCl from the approved drug
products that contain multiple other
amino acids (e.g., TRAVASOL).39
FDA does not have a basis to
conclude that, in order to compound the
proposed drug product, arginine HCl
must be compounded from a bulk drug
substance rather than from the FDAapproved drug product. There is one
FDA-approved drug product containing
arginine HCl as the single ingredient (RGene 10). R-Gene 10 is a solution of 10
g/100 mL of arginine HCl, USP in water
for injection, USP. We do not anticipate
compatibility or stability issues if this
approved drug product is used as the
starting material to be combined with
the bulk drug substance lysine HCl to
produce a combined solution of lysine
HCl and arginine HCl at the
concentration proposed in the
nomination. The pH of the compounded
drug product must be adjusted to the
target pH irrespective of the source of
arginine HCl (R-Gene 10 or bulk drug
substance). In addition, the desired
osmolarity of <1050 mOsmol is
attainable irrespective of the source of
arginine (R-Gene 10 or bulk drug
substance) used for compounding the
39 See, e.g., NDA 018931 labeling available as of
the date of this notice at https://
www.accessdata.fda.gov/drugsatfda_docs/label/
2020/018931s055,020849s025lbl.pdf.
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lysine HCl and arginine HCl drug
product for injection. The nomination
does not provide any support for the
proposition that the proposed product
must be compounded from a bulk drug
substance rather than by starting with
the FDA-approved drug product R-Gene
10. Because the nomination does not
provide support for the proposition that
the arginine HCl component of the drug
product must be compounded from a
bulk drug substance rather than by
starting with the FDA-approved drug
product R-Gene 10, as explained further
below, FDA is proposing not to add
arginine HCl to the 503B Bulks List for
use in combination with lysine HCl
(bulk drug substance).
For the same reason that there is a
basis to conclude that lysine HCl for
combination with arginine HCl must be
compounded from a bulk drug
substance, there is also a basis to
conclude that lysine HCl as a singleingredient compounded drug product
for the intravenous route of
administration must be produced from a
bulk drug substance. As with the
preceding analysis, this is because of the
difficulties and complexities associated
with removing lysine HCl from the
approved multiple amino acid
solutions.
3. Balancing Test
Because FDA answered ‘‘yes’’ to both
of the threshold questions for lysine HCl
as a single ingredient for reducing the
radiation dose to the kidneys during
PRRT and for use in combination with
FDA-approved arginine HCl, we next
conducted the following balancing test
to determine whether the statutory
‘‘clinical need’’ standard has been met.
We considered data and information
regarding the physical and chemical
characterization of lysine HCl as a single
ingredient and in combination with
arginine HCl, safety issues raised by use
of these substances in compounding,
available evidence of effectiveness or
lack of effectiveness, and historical and
current use in compounding.
Arginine HCl and lysine HCl are well
characterized physically and
chemically. Each of these amino acids
has a USP drug substance monograph.
In addition, lysine HCl and arginine HCl
are stable under ordinary storage
conditions. The FDA-approved arginine
HCl drug product, R-Gene 10, is stable
at room temperature. Therefore,
provided the quality of lysine HCl meets
the standards in its USP drug substance
monograph and L-arginine HCl is used
starting from the FDA-approved drug
product, R-Gene 10, both these
components are physically and
chemically well characterized.
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Safety risks associated with the
combination of lysine HCl and arginine
HCl for intravenous infusion are not
such that they outweigh the benefits,
and can be managed. The most common
adverse events associated with its use
are nausea and vomiting. Although
there are hyperkalemia concerns
associated with lysine HCl/arginine HCl
infusion, this risk could be monitored
and managed, if necessary. There is
evidence of effectiveness of lysine HCl
as a single ingredient during PRRT;
however, lysine HCl as a single
ingredient for intravenous
administration is associated with a
higher risk of and more severe
hyperkalemia and a higher incidence of
vomiting than the lysine HCl/arginine
HCl combination for intravenous
administration. There is evidence of
effectiveness of combination lysine HCl
and arginine HCl infusions for reducing
the radiation dose to the kidneys during
PRRT in the published literature and as
described in the approved labeling of
LUTATHERA. There is also evidence in
the published literature that suggests
that combination lysine HCl/arginine
HCl compounded intravenous infusions
produce less nausea than FDA-approved
amino acid solutions when used to
reduce the radiation dose to the kidneys
during PRRT, and therefore would lead
to fewer episodes of vomiting. There is
current and historical evidence that
lysine HCl and arginine HCl are used in
combination to compound injectable
drug products within the United States
for nephroprotection during PRRT.
There also appears to be current and
historical evidence that lysine HCl and
arginine HCl are used in combination to
compound injectable drug products
outside the United States.
On balance, consideration of the
physical and chemical characterization,
safety, effectiveness, and historical and
current use weighs against lysine HCl as
a single ingredient (bulk drug substance)
for intravenous use, but weighs in favor
of placement on the 503B Bulks List of
lysine HCl (bulk drug substance) in
combination with FDA-approved, single
ingredient arginine HCl injection for
intravenous use only. Accordingly, we
propose adding lysine HCl for use in
combination with FDA-approved,
single-ingredient arginine HCl injection
to the 503B Bulks List for intravenous
use only. FDA encourages public
comment on any particular
considerations related to compounding
a drug product using FDA-approved,
single-ingredient arginine HCl injection
in combination with lysine HCl (bulk
drug substance).
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4. Additional Comments
Due to the safety risks referred to
above, if the lysine HCl in combination
with FDA-approved, single-ingredient
arginine HCl injection is placed on the
503B Bulks List, FDA intends to make
safety information about the use of
lysine HCl/arginine HCl available to
prescribers, pharmacists, outsourcing
facilities, and the public through
information on FDA’s website, in a
safety guide, or through other
mechanisms, as appropriate.
IV. Substances Evaluated and Not
Proposed for Inclusion on the 503B
Bulks List
The three bulk drug substances that
have been evaluated and that FDA is
proposing not to place on the list are as
follows: etomidate, furosemide, and
rocuronium bromide. The reasons for
FDA’s proposals are included below.40
Because the substances in this section
are components of FDA-approved drug
products, we considered, as applicable,
one or both of the following questions:
(1) is there a basis to conclude that an
attribute of each FDA-approved drug
product containing the bulk drug
substance makes each one medically
unsuitable to treat certain patients for a
condition that FDA has identified for
evaluation, and the drug product
proposed to be compounded is intended
to address that attribute and (2) is there
a basis to conclude that the drug
product proposed to be compounded
must be compounded using a bulk drug
substance.
A. Etomidate
Etomidate has been nominated for
inclusion on the 503B Bulks List to
compound drug products for the
40 We note that furosemide injection currently
appears on FDA’s drug shortage list. Under section
503B(a)(2)(A)(ii of the FD&C Act), outsourcing
facilities may compound using a bulk drug
substance if the drug compounded from such bulk
drug substance appears on FDA’s drug shortage list
at the time of compounding, distribution, and
dispensing, provided all of the conditions in section
503B are met. See also FDA’s Guidance for
Industry, ‘‘Interim Policy on Compounding Using
Bulk Drug Substances Under Section 503B of the
Federal Food, Drug, and Cosmetic Act,’’ which
describes an enforcement policy for compounding
a drug product that appeared on FDA’s drug
shortage list using a bulk drug substance that is not
on the 503B Bulks List provided certain conditions
are met. We further note that both furosemide and
rocuronium bromide appear on the list maintained
by FDA of drugs used for hospitalized patients with
COVID–19. FDA’s Guidance for Industry,
‘‘Temporary Policy for Compounding of Certain
Drugs for Hospitalized Patients by Outsourcing
Facilities During the COVID–19 Public Health
Emergency’’ describes an enforcement policy,
subject to certain conditions, for compounding a
drug product using a bulk drug substance that is not
on the 503B Bulks List during the COVID public
health emergency.
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Federal Register / Vol. 87, No. 225 / Wednesday, November 23, 2022 / Notices
induction of general anesthesia and as
an adjunct in maintenance of general
anesthesia.41 The proposed route of
administration is intravenous, the
proposed dosage form is a preservativefree solution, and the proposed
concentration is 2 mg/mL. The
nominations propose to compound a
preservative-free solution. However,
they fail to acknowledge that there is a
preservative-free formulation of
etomidate that is FDA-approved or
explain why that formulation would be
medically unsuitable for certain
patients. The nominations state that
etomidate might also be used to
compound other drug products, but do
not identify those products. The
nominated bulk drug substance is a
component of FDA-approved drug
products (e.g., NDA 018227). FDAapproved etomidate is available as a
single dose, preservative-free 20 mg/10
mL (2 mg/mL) solution to be
administered by intravenous
injection.42 43
1. Suitability of FDA-Approved Drug
Product(s)
The nominations do not explain why
an attribute of each of the FDAapproved single dose, preservative-free
2 mg/mL solution products for
intravenous injection is medically
unsuitable for certain patients or
identify an attribute of the approved
drug products that the proposed
compounded drug product is intended
to address. FDA finds no basis to
conclude that an attribute of the FDAapproved products makes them
medically unsuitable to treat certain
patients for a condition that FDA has
identified for evaluation and that a
proposed compounded product is
intended to address.
2. Whether the Drug Product Must Be
Compounded From a Bulk Drug
Substance
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Because the nominations do not
identify specific differences between
drug products that would be
compounded using etomidate and
approved drug products containing
etomidate, there is nothing for FDA to
evaluate under question 2.
41 See Docket No. FDA–2013–N–1524, document
nos. FDA–2013–N–1524–2292 and FDA–2013–N–
1524–2298.
42 See, e.g., NDA 018227 labeling available as of
the date of this notice at https://
www.accessdata.fda.gov/spl/data/41253af6-deac43de-9af3-3b727ea351d8/41253af6-deac-43de-9af33b727ea351d8.xml.
43 According to the label for NDA 018227, each
mL contains etomidate, 2 mg, propylene glycol 35%
v/v.
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B. Furosemide
Furosemide has been nominated for
inclusion on the 503B Bulks List to
compound drug products that treat
congestive heart failure, edema, renal
failure, and hypertension, among other
conditions.44 The proposed routes of
administration are intravenous and
intramuscular, the proposed dosage
forms are both a preservative-free and a
preserved solution, and the proposed
concentration is 10 mg/mL. The
nominations propose to compound both
preservative-free and preserved
solutions. However, they fail to
acknowledge that there is a
preservative-free formulation of
furosemide that is FDA-approved or
explain why that formulation would be
medically unsuitable for certain
patients. The nominations state that
furosemide might also be used to
compound other drug products, but do
not identify those products. The
nominated bulk drug substance is a
component of FDA-approved drug
products (e.g., ANDA 212174). FDAapproved furosemide is available as a
preservative-free 40 mg per 4 mL (10
mg/mL) solution for intravenous or
intramuscular administration.45 46 47
1. Suitability of FDA-Approved Drug
Product(s)
71651
proposed compounded product is
intended to address.
2. Whether the Drug Product Must Be
Compounded From a Bulk Drug
Substance
Because the nominations have not
identified a population for whom the
approved products would be medically
unsuitable, FDA has not evaluated
whether the proposed preserved drug
products containing furosemide must be
compounded from bulk drug substances
rather than using the approved drug
product.
C. Rocuronium Bromide
Rocuronium bromide has been
nominated for inclusion on the 503B
Bulks List to compound drug products
that serve as an adjunct to general
anesthesia to facilitate both rapid
sequence and routine tracheal
intubation and to provide skeletal
muscle relaxation during surgery or
mechanical ventilation.48 The proposed
route of administration is intravenous,
the proposed dosage form is a
preservative-free solution for injection,
and the proposed concentration is 10
mg/mL. The nominations propose to
compound a preservative-free solution.
However, they fail to acknowledge that
there is a preservative-free formulation
of rocuronium bromide that is FDAapproved or explain why that
formulation would be medically
unsuitable for certain patients. The
nominations state that rocuronium
bromide might also be used to
compound other drug products, but do
not identify those products. The
nominated bulk drug substance is a
component of FDA-approved drug
products (e.g., ANDA 079195). FDAapproved rocuronium bromide is
available as a preservative-free 10 mg/
mL solution for intravenous
administration.49 50
The nominations do not explain why
an attribute of each of the FDAapproved preservative-free 40 mg per 4
mL (10 mg/mL) solution products for
intravenous or intramuscular
administration is medically unsuitable
for certain patients or identify an
attribute of the approved drug products
that the proposed compounded drug
products are intended to address. For
example, the nominations propose to
compound a preserved solution because
the available FDA-approved products
are preservative-free, but the
nominations do not identify specific
data or information supporting the need
for a preserved product. FDA finds no
basis to conclude that an attribute of the
FDA-approved products makes them
medically unsuitable to treat certain
patients for a condition that FDA has
identified for evaluation and that a
1. Suitability of FDA-Approved Drug
Product(s)
The nominations do not explain why
an attribute of each of the FDAapproved 10 mg/mL preservative-free
solution products is medically
unsuitable for certain patients or
44 See Docket No. FDA–2013–N–1524, document
nos. FDA–2013–N–1524–2292 and FDA–2013–N–
1524–2298.
45 See, e.g., ANDA 212174 labeling available as of
the date of this notice at https://
www.accessdata.fda.gov/spl/data/421aa6d5-623b4dc2-abd5-bb9e7765bf37/421aa6d5-623b-4dc2abd5-bb9e7765bf37.xml.
46 Per the label for ANDA 212174, the solution is
preservative-free and is intended for intravenous or
intramuscular administration.
47 Furosemide is also approved as an oral solution
and as a tablet.
48 See Docket No. FDA–2013–N–1524, document
nos. FDA–2013–N–1524–2292 and FDA–2013–N–
1524–2298.
49 See, e.g., ANDA 079195 labeling available as of
the date of this notice at https://
www.accessdata.fda.gov/spl/data/e21db7bf-3cab4000-94dd-15c6d2a213de/e21db7bf-3cab-400094dd-15c6d2a213de.xml.
50 Per the label for ANDA 079195 each mL
contains 10 mg rocuronium bromide and 2 mg
sodium acetate. The aqueous solution is adjusted to
isotonicity with sodium chloride and to a pH of 4
with acetic acid and/or sodium hydroxide.
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Federal Register / Vol. 87, No. 225 / Wednesday, November 23, 2022 / Notices
identify an attribute of the approved
drug products that the proposed
compounded drug product is intended
to address. FDA finds no basis to
conclude that an attribute of the FDAapproved products makes them
medically unsuitable to treat certain
patients for a condition that FDA has
identified for evaluation and that a
proposed compounded product is
intended to address.
2. Whether the Drug Product Must Be
Compounded from a Bulk Drug
Substance
Because the nominations do not
identify specific differences between
drug products that would be
compounded using rocuronium bromide
and approved drug products containing
rocuronium bromide, there is nothing
for FDA to evaluate under question 2.
lotter on DSK11XQN23PROD with NOTICES1
VI. Conclusion
For the reasons stated above, we
tentatively conclude that there is a
clinical need for outsourcing facilities to
compound drug products using the bulk
drug substances arginine HCl for oral
use only, lysine HCl for oral use only,
and lysine HCl in combination with
FDA-approved single-ingredient
arginine HCl for injection for
intravenous use only. We therefore
propose to include those bulk drug
substances on the 503B Bulks List as
described in this notice.
At this time, we find no basis to
conclude that there is a clinical need for
outsourcing facilities to compound drug
products using the bulk drug substances
etomidate, furosemide, and rocuronium
bromide. Therefore, we propose not to
include these bulk drug substances on
the 503B Bulks List.
VII. References
The following references marked with
an asterisk (*) are on display at the
Dockets Management Staff (see
ADDRESSES) and are available for
viewing by interested persons between
9 a.m. and 4 p.m., Monday through
Friday; they are also available
electronically at https://
www.regulations.gov. References
without asterisks are not on public
display at https://www.regulations.gov
because they have copyright restriction.
Some may be available at the website
address, if listed. References without
asterisks are available for viewing only
at the Dockets Management Staff. FDA
has verified the website addresses, as of
the date this document publishes in the
Federal Register, but websites are
subject to change over time.
*1. FDA, Guidance for Industry, ‘‘Interim
Policy on Compounding Using Bulk
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Drug Substances Under Section 503B of
the Federal Food, Drug, and Cosmetic
Act,’’ January 2017 (available at https://
www.fda.gov/media/94402/download).
*2. FDA, Guidance for Industry, ‘‘Evaluation
of Bulk Drug Substances Nominated for
Use in Compounding Under Section
503B of the Federal Food, Drug, and
Cosmetic Act,’’ March 2019 (available at
https://www.fda.gov/media/121315/
download).
*3. FDA Memorandum to File, ‘‘Clinical
Need for Arginine Hydrochloride in
Compounding Under Section 503B of the
FD&C Act,’’ October 2022.
*4. FDA Memorandum to File, ‘‘Clinical
Need for Lysine Hydrochloride in
Compounding Under Section 503B of the
FD&C Act,’’ October 2022.
5. Singh, B.B., J. Udani, S.P, Vinjamury, C,
Der-Martirosian, et al, 2005, ‘‘Safety and
Effectiveness of an L-lysine, Zinc, and
Herbal-Based Product on the Treatment
of Facial and Circumoral Herpes,’’
Alternative Medicine Review, 10: 123–7
*6. FDA Memorandum to File, ‘‘Clinical
Need for Lysine Hydrochloride (HCl)
Alone and in Combination With
Arginine HCl in Compounding Under
Section 503B of the FD&C Act,’’ October
2022.
*7. Letter from SNMMI to FDA dated May 25,
2018, requesting FDA place arginine and
lysine on the 503B Bulks List.
Dated: November 17, 2022.
Lauren K. Roth,
Associate Commissioner for Policy.
[FR Doc. 2022–25549 Filed 11–22–22; 8:45 am]
BILLING CODE 4164–01–P
DEPARTMENT OF HEALTH AND
HUMAN SERVICES
Food and Drug Administration
[Docket No. FDA–2022–N–2796]
Bristol Myers Products Inc.; Proposal
To Withdraw Approval of a New Drug
Application for Bufferin (Aspirin)
Tablets; Opportunity for a Hearing
AGENCY:
Food and Drug Administration,
HHS.
ACTION:
Notice.
The Food and Drug
Administration’s (FDA or Agency)
Center for Drug Evaluation and Research
(CDER) is proposing to withdraw
approval of a new drug application
(NDA) for Bufferin (aspirin) tablets, for
which Bristol Myers Products Inc., 1350
Liberty Ave., Hillside, NJ 07205 is the
last holder of record, and is announcing
an opportunity for the holder of the
NDA to request a hearing on this
proposal. The basis for the proposal is
that the holder of the NDA has
repeatedly failed to file required annual
reports for this NDA.
SUMMARY:
PO 00000
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The holder of the NDA may
submit a request for a hearing by
December 23, 2022. Submit all data,
information, and analyses upon which
the request for a hearing relies by
January 23, 2023. Submit electronic or
written comments by January 23, 2023.
ADDRESSES: The request for a hearing
may be submitted by the holder of the
NDA by either of the following methods:
DATES:
Electronic Submissions
Submit electronic comments in the
following way:
• Federal eRulemaking Portal:
https://www.regulations.gov. Follow the
instructions for submitting comments to
submit your request for a hearing.
Comments submitted electronically to
https://www.regulations.gov, including
any attachments to the request for a
hearing, will be posted to the docket
unchanged.
Written/Paper Submissions
Submit written/paper submissions as
follows:
• Mail/Hand Delivery/Courier (for
written/paper submissions): Dockets
Management Staff (HFA–305), Food and
Drug Administration, 5630 Fishers
Lane, Rm. 1061, Rockville, MD 20852.
• Because your request for a hearing
will be made public, you are solely
responsible for ensuring that your
request 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. The request
for a hearing must include the Docket
No. FDA–2022–N–2796 for ‘‘Bristol
Myers Products Inc.; Proposal To
Withdraw Approval of a New Drug
Application for Bufferin (Aspirin)
Tablets; Opportunity for a Hearing.’’
The request for a hearing will be placed
in the docket and publicly viewable at
https://www.regulations.gov or at the
Dockets Management Staff between 9
a.m. and 4 p.m., Monday through
Friday. The holder of the NDA may
submit all data and analyses upon
which the request for a hearing relies in
the same manner as the request for a
hearing except as follows:
• Confidential Submissions—To
submit any data analyses with
confidential information that you do not
wish to be made publicly available,
submit your data and analyses only as
a written/paper submission. You should
submit two copies total of all data and
analyses. One copy will include the
information you claim to be confidential
with a heading or cover note that states
‘‘THIS DOCUMENT CONTAINS
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]]>Agencies
[Federal Register Volume 87, Number 225 (Wednesday, November 23, 2022)]
[Notices]
[Pages 71642-71652]
From the Federal Register Online via the Government Publishing Office [www.gpo.gov]
[FR Doc No: 2022-25549]
-----------------------------------------------------------------------
DEPARTMENT OF HEALTH AND HUMAN SERVICES
Food and Drug Administration
[Docket No. FDA-2018-N-3240]
List of Bulk Drug Substances for Which There is a Clinical Need
Under Section 503B of the Federal Food, Drug, and Cosmetic Act
AGENCY: Food and Drug Administration, HHS.
ACTION: Notice.
-----------------------------------------------------------------------
SUMMARY: The Food and Drug Administration (FDA or Agency) is developing
a list of bulk drug substances (active pharmaceutical ingredients) for
which there is a clinical need (the 503B Bulks List). Drug products
that outsourcing facilities compound using bulk drug substances on the
503B Bulks List can qualify for certain exemptions from the Federal
Food, Drug, and Cosmetic Act (FD&C Act) provided certain conditions are
met. This notice identifies two bulk drug substances that FDA has
considered and proposes to include on the 503B Bulks List to compound
three categories of compounded drug products: arginine hydrochloride
(HCl) for oral use, lysine HCl for oral use, and lysine HCl for
intravenous use in combination with FDA-approved, single-ingredient
arginine HCl for intravenous use. This notice identifies three bulk
drug substances that FDA has considered and proposes not to include on
the 503B Bulks List: etomidate, furosemide, and rocuronium bromide.
Additional bulk drug substances nominated for inclusion on this list
are under consideration and may be the subject of future notices.
DATES: Either electronic or written comments on the notice must be
submitted by January 23, 2023.
ADDRESSES: You may submit comments as follows. Please note that late,
untimely filed comments will not be considered. The https://www.regulations.gov electronic filing system will accept comments until
11:59 p.m. Eastern Time at the end of January 23, 2023. Comments
received by mail/hand delivery/courier (for written/paper submissions)
will be considered timely if they are postmarked or the delivery
service acceptance receipt is on or before that date.
Electronic Submissions
Submit electronic comments in the following way:
Federal eRulemaking Portal: https://www.regulations.gov.
Follow the instructions for submitting comments. Comments submitted
electronically, including attachments, to https://www.regulations.gov
will be posted to the docket unchanged. Because your comment will be
made public, you are solely responsible for ensuring that your comment
does not include any confidential information that you or a third party
may not wish to be posted, such as medical information, your or anyone
else's Social Security number, or confidential business information,
such as a manufacturing process. Please note that if you include your
name, contact information, or other information that identifies you in
the body of your comments, that information will be posted on https://www.regulations.gov.
If you want to submit a comment with confidential
information that you do not wish to be made available to the public,
submit the comment as a written/paper submission and in the manner
detailed (see ``Written/Paper Submissions'' and ``Instructions'').
Written/Paper Submissions
Submit written/paper submissions as follows:
Mail/Hand Delivery/Courier (for written/paper
submissions): Dockets Management Staff (HFA-305), Food and Drug
Administration, 5630 Fishers Lane, Rm. 1061, Rockville, MD 20852.
[[Page 71643]]
For written/paper comments submitted to the Dockets
Management Staff, FDA will post your comment, as well as any
attachments, except for information submitted, marked and identified,
as confidential, if submitted as detailed in ``Instructions.''
Instructions: All submissions received must include the Docket No.
FDA-2018-N-3240 for ``List of Bulk Drug Substances for Which There is a
Clinical Need Under Section 503B of the Federal Food, Drug, and
Cosmetic Act.'' Received comments, those filed in a timely manner (see
ADDRESSES), will be placed in the docket and, except for those
submitted as ``Confidential Submissions,'' publicly viewable at https://www.regulations.gov or at the Dockets Management Staff between 9 a.m.
and 4 p.m., Monday through Friday, 240-402-7500.
Confidential Submissions--To submit a comment with
confidential information that you do not wish to be made publicly
available, submit your comments only as a written/paper submission. You
should submit two copies total. One copy will include the information
you claim to be confidential with a heading or cover note that states
``THIS DOCUMENT CONTAINS CONFIDENTIAL INFORMATION.'' The Agency will
review this copy, including the claimed confidential information, in
its consideration of comments. The second copy, which will have the
claimed confidential information redacted/blacked out, will be
available for public viewing and posted on https://www.regulations.gov.
Submit both copies to the Dockets Management Staff. If you do not wish
your name and contact information to be made publicly available, you
can provide this information on the cover sheet and not in the body of
your comments and you must identify this information as
``confidential.'' Any information marked as ``confidential'' will not
be disclosed except in accordance with 21 CFR 10.20 and other
applicable disclosure law. For more information about FDA's posting of
comments to public dockets, see 80 FR 56469, September 18, 2015, or
access the information at: https://www.govinfo.gov/content/pkg/FR-2015-09-18/pdf/2015-23389.pdf.
Docket: For access to the docket to read background documents or
the electronic and written/paper comments received, go to https://www.regulations.gov and insert the docket number, found in brackets in
the heading of this document, into the ``Search'' box and follow the
prompts and/or go to the Dockets Management Staff, 5630 Fishers Lane,
Rm. 1061, Rockville, MD 20852, 240-402-7500.
FOR FURTHER INFORMATION CONTACT: Tracy Rupp, Center for Drug Evaluation
and Research, Food and Drug Administration, 10903 New Hampshire Ave.,
Bldg. 51, Silver Spring, MD 20993, 301-796-3100.
SUPPLEMENTARY INFORMATION:
I. Background
Section 503B of the FD&C Act (21 U.S.C. 353b) describes the
conditions that must be satisfied for drug products compounded by an
outsourcing facility to be exempt from section 505 of the FD&C Act (21
U.S.C. 355) (concerning the approval of drugs under new drug
applications (NDAs) or abbreviated new drug applications (ANDAs)),
section 502(f)(1) (21 U.S.C. 352(f)(1)) (concerning the labeling of
drugs with adequate directions for use), and section 582 of the FD&C
Act (21 U.S.C. 360eee-1) (concerning drug supply chain security
requirements).\1\
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\1\ Section 503B(a) of the FD&C Act.
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Compounded drug products that meet the conditions in section 503B
are not exempt from current good manufacturing practice (CGMP)
requirements in section 501(a)(2)(B) of the FD&C Act (21 U.S.C.
351(a)(2)(B)).\2\ Outsourcing facilities are also subject to FDA
inspections according to a risk-based schedule, specific adverse event
reporting requirements, and other conditions that help to mitigate the
risks of the drug products they compound.\3\ Outsourcing facilities may
or may not obtain prescriptions for identified individual patients and
can, therefore, distribute compounded drugs to healthcare practitioners
for ``office stock,'' to hold in their offices in advance of patient
need.\4\
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\2\ Compare section 503A(a) of the FD&C Act (21 U.S.C. 353a(a))
(exempting drugs compounded in accordance with that section from
CGMP requirements) with section 503B(a) of the FD&C Act (not
providing an exemption from CGMP requirements).
\3\ Section 503B(b)(4) and (5) of the FD&C Act.
\4\ Section 503B(d)(4)(C) of the FD&C Act.
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One of the conditions that must be met for a drug product
compounded by an outsourcing facility to qualify for the exemptions
under section 503B of the FD&C Act is that the outsourcing facility may
not compound a drug using a bulk drug substance unless: (1) the bulk
drug substance appears on a list established by the Secretary of Health
and Human Services identifying bulk drug substances for which there is
a clinical need (the 503B Bulks List) or (2) the drug compounded from
the bulk drug substance appears on the drug shortage list in effect
under section 506E of the FD&C Act (21 U.S.C. 356e) at the time of
compounding, distribution, and dispensing.\5\
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\5\ Section 503B(a)(2)(A) of the FD&C Act.
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Section 503B of the FD&C Act directs FDA to establish the 503B
Bulks List by: (1) publishing a notice in the Federal Register
proposing bulk drug substances to be included on the list, including
the rationale for such proposal; (2) providing a period of not less
than 60 calendar days for comment on the notice; and (3) publishing a
notice in the Federal Register designating bulk drug substances for
inclusion on the list.\6\
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\6\ Section 503B(a)(2)(A)(i)(I) to (III) of the FD&C Act.
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FDA has published a series of Federal Register notices addressing
bulk drug substances nominated for inclusion on the 503B Bulks List.\7\
This notice identifies two bulk drug substances that FDA has considered
and proposes to include on the 503B Bulks List and three bulk drug
substances that FDA has considered and proposes not to include on the
503B Bulks List.
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\7\ See Federal Register of August 28, 2018 (83 FR 43877), March
4, 2019 (84 FR 7383), September 3, 2019 (84 FR 46014), July 31, 2020
(85 FR 46126), and March 24, 2021 (86 FR 15673). The comment period
for the July 2020 notice was reopened for 30 days on January 8, 2021
(86 FR 1515), to allow interested parties an additional opportunity
to comment. FDA has not yet reached a final determination on whether
the substances evaluated in the September 2019, July 2020, or March
2021 notices will be added to the 503B Bulks List. In addition,
bumetanide, which was considered in the August 2018 notice, remains
under consideration by the Agency.
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For purposes of section 503B of the FD&C Act, bulk drug substance
means an active pharmaceutical ingredient as defined in Sec. 207.1 (21
CFR 207.1).\8\ Active pharmaceutical ingredient means 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, but the term
does not include intermediates used in the synthesis of the
substance.9 10
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\8\ See section 503B(a)(2) of the FD&C Act, which defines bulk
drug substances used in compounding under section 503B according to
21 CFR 207.3(a)(4) ``or any successor regulation.'' Section 207.1 is
the successor regulation.
\9\ Section 503B(a)(2) of the FD&C Act and Sec. 207.1.
\10\ Inactive ingredients are not subject to section 503B(a)(2)
of the FD&C Act and will not be included in the 503B Bulks List
because they are not included within the definition of a bulk drug
substance. Pursuant to section 503B(a)(3) of the FD&C Act, inactive
ingredients used in compounding must comply with the standards of an
applicable U.S. Pharmacopeia or National Formulary monograph, if a
monograph exists.
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[[Page 71644]]
II. Methodology for Developing the 503B Bulks List
A. Process for Developing the List
In the Federal Register of December 4, 2013 (78 FR 72838), FDA
requested nominations for specific bulk drug substances for the Agency
to consider for inclusion on the 503B Bulks List. FDA reopened the
nomination process in the Federal Register of July 2, 2014 (79 FR
37747) and provided more detailed information on what FDA needs to
evaluate nominations for the list. In the Federal Register of October
27, 2015 (80 FR 65770), the Agency opened a new docket, FDA-2015-N-
3469, to provide an opportunity for interested persons to submit new
nominations of bulk drug substances or to renominate substances with
sufficient information or submit comments on nominated substances.
As FDA evaluates bulk drug substances, it intends to publish
notices for public comment in the Federal Register that describe the
FDA's proposed position on each substance along with the rationale for
that position.\11\ After considering any comments on FDA's proposals
regarding whether to include nominated substances on the 503B Bulks
List, FDA intends to consider whether input from the Pharmacy
Compounding Advisory Committee (PCAC) on the nominations would be
helpful to the Agency in making its determination, and if so, it will
seek PCAC input.\12\ Depending on its review of the docket comments and
other relevant information before the Agency, FDA may finalize its
proposed determination without change, or it may finalize a
modification to its proposal to reflect new evidence or analysis
regarding clinical need. FDA will then publish in the Federal Register
a list identifying the bulk drug substances for which it has determined
there is a clinical need and FDA's rationale in making that final
determination. FDA will also publish in the Federal Register a list of
those substances it considered but found that there is no clinical need
to use in compounding and FDA's rationale in making this decision.
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\11\ This is consistent with procedure set forth in section
503B(a)(2)(A)(i) of the FD&C Act. Although the statute only directs
FDA to issue a Federal Register notice and seek public comment when
it proposes to include bulk drug substances on the 503B Bulks List,
we intend to seek comment when the Agency has evaluated a nominated
substance and proposes either to include or not to include the
substance on the list.
\12\ Section 503B of the FD&C Act does not require FDA to
consult the PCAC before developing a 503B Bulks List.
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FDA intends to maintain a list of all bulk drug substances it has
evaluated on its website, and separately identify bulk drug substances
it has placed on the 503B Bulks List and those it has decided not to
place on the 503B Bulks List. This list is available at https://www.fda.gov/media/120692/download. FDA will only place a bulk drug
substance on the 503B Bulks List when it has determined there is a
clinical need for outsourcing facilities to compound drug products
using the bulk drug substance. If a clinical need to compound drug
products using the bulk drug substance has not been demonstrated, based
on the information submitted by the nominator and any other information
considered by the Agency, FDA will not place a bulk drug substance on
the 503B Bulks List.
FDA is evaluating bulk drug substances nominated for the 503B Bulks
List on a rolling basis. FDA intends to evaluate and publish in the
Federal Register its proposed and final determinations in groups of
bulk drug substances until all nominated substances that were
sufficiently supported have been evaluated and either placed on the
503B Bulks List or identified as bulk drug substances that were
considered, but determined not to be appropriate for inclusion on the
503B Bulks List (Ref. 1).
B. Analysis of Substances Nominated for the List
As noted above, the 503B Bulks List includes bulk drug substances
for which the Agency has determined there is a clinical need. The
Agency is evaluating bulk drug substances that were nominated for
inclusion on the 503B Bulks List, proceeding case by case, under the
clinical need standard provided by the statute (Ref. 2).\13\ In
applying this standard to develop the proposals in this notice, FDA
interprets the phrase ``bulk drug substances for which there is a
clinical need'' to mean that the 503B Bulks List may include a bulk
drug substance if: (1) there is a clinical need for an outsourcing
facility to compound the drug product and (2) the drug product must be
compounded using the bulk drug substance. FDA does not interpret supply
issues, such as backorders, to be within the meaning of ``clinical
need'' for compounding with a bulk drug substance. Section 503B of the
FD&C Act separately provides for compounding from a bulk drug substance
under the exemptions discussed above if the drug product compounded
from the bulk drug substance is on the FDA drug shortage list at the
time of compounding, distribution, and dispensing. Additionally, FDA
does not consider convenience in administering a particular drug
product (e.g., a ready-to-use form) or the cost of the compounded drug
product as compared with an FDA-approved drug product when assessing
``clinical need.''
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\13\ On March 4, 2019, FDA announced the availability of a final
guidance entitled ``Evaluation of Bulk Drug Substances Nominated for
Use in Compounding Under Section 503B of the Federal Food, Drug, and
Cosmetic Act'' (84 FR 7390); available at https://www.fda.gov/media/121315/download. This guidance describes FDA policies for developing
the 503B Bulks List and the Agency's interpretation of the phrase
``bulk drug substances for which there is a clinical need'' as it is
used in section 503B of the FD&C Act. The analysis under the
statutory ``clinical need'' standard described in this notice is
consistent with the approach described in FDA's guidance.
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All of the bulk drug substances that we are addressing in this
notice are components of FDA-approved drug products,\14\ and we
therefore began our evaluation of the bulk drug substances by asking
one or both, as applicable, of the following questions:
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\14\ Specifically, arginine HCl, etomidate, furosemide, lysine
HCl, and rocuronium bromide.
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(1) Is there a basis to conclude, for each FDA-approved product
that includes the nominated bulk drug substance, that: (a) an attribute
of the FDA-approved drug product makes it medically unsuitable to treat
certain patients for a condition that FDA has identified for evaluation
and (b) the drug product proposed to be compounded is intended to
address that attribute?
(2) Is there a basis to conclude that the drug product proposed to
be compounded must be produced from a bulk drug substance rather than
from an FDA-approved drug product?
The reason for question 1 is that unless an attribute of the FDA-
approved drug is medically unsuitable for certain patients, and a drug
product compounded using a bulk drug substance that is a component of
the approved drug is intended to address that attribute, there is no
clinical need to compound a drug product using that bulk drug
substance. Rather, such compounding would unnecessarily expose patients
to the risks associated with drug products that do not meet the
standards applicable to FDA-approved drug products for safety,
effectiveness, quality, and labeling and would undermine the drug
approval process. The reason for question 2 is that to place a bulk
drug substance on the 503B Bulks List, FDA must determine that there is
a clinical need for outsourcing facilities to compound a drug product
using the bulk drug substance rather than starting with an FDA-approved
drug product. When it is feasible to compound a drug
[[Page 71645]]
product by starting with an approved drug product, there are certain
benefits of doing so over starting with a bulk drug substance,
including that approved drugs have undergone premarket review for
safety, effectiveness, and quality, and are manufactured by a facility
that is subject to premarket assessment, including site inspection, as
well as routine post-approval risk-based inspections. In contrast, FDA
does not conduct a premarket review of the quality standards,
specifications, and controls for bulk drug substances used in
compounding and does not conduct a premarket assessment of the
manufacturer of the bulk drug substance.
If the answer to both of these questions is ``yes,'' there may be a
clinical need for outsourcing facilities to compound using the bulk
drug substance, and we would evaluate the substance further, applying
the factors described below. If the answer to either of these questions
is ``no,'' we generally would not include the bulk drug substance on
the 503B Bulks List, because there would not be a basis to conclude
that there may be a clinical need to compound drug products using the
bulk drug substance instead of administering an approved drug or
compounding starting with an approved drug product. FDA answered
``yes'' to both of the threshold questions for two of the bulk drug
substances that are components of approved drug products that we are
addressing in this notice. Accordingly, as explained further below, we
proceeded further in our evaluation of these substances by conducting a
balancing test and are proposing to include those substances on the
503B Bulks List.
We are conducting a balancing test using four factors.
Specifically, on a substance-by-substance basis, we consider available
data relevant to each factor in the context of the other factors and
balance all four factors to determine whether the statutory ``clinical
need'' standard has been met. The balancing test includes the following
factors:
The physical and chemical characterization of the
substance;
Any safety issues raised by the use of the substance in
compounding;
The available evidence of effectiveness or lack of
effectiveness of a drug product compounded with the substance, if any
such evidence exists; and
Current and historical use of the substance in compounded
drug products, including information about the medical condition(s)
that the substance has been used to treat and any references in peer-
reviewed medical literature.
The discussion below reflects FDA's consideration of these four
factors where they are applicable and describes how they were applied
to develop FDA's proposal to include three entries addressing two bulk
drug substances on the 503B Bulks List.
In this notice, FDA evaluated certain nominated bulk drug
substances for potential inclusion on the 503B Bulks List either alone
or in combination with other bulk drug substances. FDA will not
consider comments raising different combinations of bulk drug
substances than those evaluated by FDA in this notice to be within the
scope of this notice. New nominations may be submitted to docket FDA-
2015-N-3469 for combinations of bulk drug substances that were not
previously nominated and included for evaluation in this notice. The
docket is available on https://www.regulations.gov.
To assess whether there is a clinical need for outsourcing
facilities to use a bulk drug substance in compounding, FDA must
evaluate the drug products that have been proposed to be made from the
nominated bulk drug substances. Therefore, FDA's evaluation of a bulk
drug substance includes detailed consideration of the drug products
that are proposed to be compounded, including the conditions justifying
clinical need under the applicable statutory standard. Comments on
FDA's preliminary evaluation of a bulk drug substance should include
adequate support for the commenter's position. For example, a commenter
writing to support inclusion of a nominated bulk drug substance on the
503B Bulks List should include sufficient information to permit a
meaningful clinical need evaluation by FDA of the proposed product.
Commenters writing in favor of or in opposition to a proposal to
include or not to include an entry on the 503B Bulks List should
address, for each proposed compounded drug product, the factors FDA
evaluated in making its proposal.\15\ After FDA publishes a Federal
Register notice making a final determination regarding whether a bulk
drug substance will be placed on the 503B Bulks List, FDA will no
longer consider comments submitted to the docket regarding that bulk
drug substance, but interested parties may submit a citizen petition to
FDA requesting specific action or relief (see 21 CFR 10.30).
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\15\ See also FDA's guidance for industry, ``Evaluation of Bulk
Drug Substances Nominated for Use in Compounding Under Section 503B
of the Federal Food, Drug, and Cosmetic Act'' (March 2019), and our
Federal Register notice of October 27, 2015.
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C. Inclusion of Bulk Drug Substances on the 503B Bulks List
In preparing its proposal to include two bulk drug substances on
the 503B Bulks List, FDA considered whether the clinical need for the
bulk drug substance in the proposed compounded drug product is limited
by, for example, route of administration or dosage form. As
appropriate, and as explained further below, the Agency has tailored
its proposed entries on the 503B Bulks List to reflect its findings
related to clinical need for the bulk substances proposed for inclusion
on the list. FDA requested comments on the proposal to limit listings
in this manner in our Federal Register notice of July 31, 2020 (85 FR
46126). The comment period for the July 2020 notice was reopened for 30
days on January 8, 2021 (86 FR 1515), to provide interested parties an
additional opportunity to comment before FDA began to develop its final
determinations. After considering the comments submitted regarding the
proposal, in the Federal Register notice of January 27, 2022 (87 FR
4240), FDA listed three bulk drug substances to compound drug products
for topical use only.
Consistent with the approach described in the 2020 notice, and as
reflected in the entries that appear on the 503B Bulks List to date,
the entries proposed in this notice would authorize use of two bulk
drug substances. Arginine HCl would be authorized for use to compound
single-ingredient drug products for oral use only; lysine HCl would be
authorized for use to compound single-ingredient drug products for oral
use; and lysine HCl would also be authorized for use in combination
with FDA-approved, single-ingredient arginine HCl injection, U.S.
Pharmacoepia (USP) to compound drug products for intravenous (IV) use
only.\16\ As discussed further in this notice, FDA's proposals with
respect to inclusion of lysine HCl and arginine HCl on the 503B Bulks
List pertain to the L- forms of lysine HCl and arginine HCl
exclusively.\17\
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\16\ In this notice, ``single-ingredient'' refers to a drug
product containing one active ingredient. The drug product may also
contain excipients.
\17\ See footnote 18 below.
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III. Substances Considered and Proposed for Inclusion on the 503B Bulks
List
Because the substances in this section are components of FDA-
approved drug products, we considered whether: (1)
[[Page 71646]]
there is a basis to conclude that an attribute of each FDA-approved
drug product that includes the nominated bulk drug substance makes each
one medically unsuitable to treat certain patients for a condition that
FDA has identified for evaluation, and the drug products proposed to be
compounded are intended to address that attribute in each FDA-approved
drug product and (2) whether the drug products proposed to be
compounded must be compounded using a bulk drug substance. In addition,
because we answered these two questions in the affirmative for certain
drug products proposed to be compounded from the nominated bulk drug
substances, we applied the four-factor balancing test described above.
The bulk drug substances that were evaluated and that FDA is proposing
to place on the 503B Bulks List are arginine HCl for oral use only,
lysine HCl for oral use only, and lysine HCl for use in combination
with FDA-approved, arginine HCl injection for intravenous use only. The
reasons for FDA's proposals are included below.
A. Arginine HCl
Arginine HCl was nominated as a bulk drug substance for the 503B
Bulks List to compound drug products that are used for acute
hyperammonemia in urea cycle disorders (UCDs) and refractory metabolic
alkalosis, among other conditions.18 19 The proposed routes
of administration are oral and intravenous, among others,\20\ and the
proposed dosage forms are an oral solution or suspension, capsule,
powder for dispersion, and injectable, among others.\21\ The nominators
proposed a range of concentrations (12.5 to 40 percent) and 200 and 500
milligrams/milliliters (mg/mL). They also proposed strengths of 250 mg-
500 mg unspecified oral dosage forms and 700 mg-750 mg oral capsules.
This nominated bulk drug substance is a component of an FDA-approved
drug product (NDA 016931). FDA has approved arginine HCl (R-Gene 10) as
a 10 gram (GM)/100 mL (100 mg/mL; 10 percent) injection for intravenous
administration \22\ (Ref. 3).
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\18\ See Docket No. FDA-2015-N-3469, document nos. FDA-2015-N-
3469-0244, FDA-2015-N-3469-0169, FDA-2015-N-3469-0156-attachment 10,
FDA-2015-N-3469-0202, and FDA-2015-N-3469-0320. The nomination in
Docket No. FDA-2015-N-3469-0156-attachment 10 was for ``Arginine
HCL'' and stated that the common name of the substance is ``L-
arginine hydrochloride; D-arginine hydrochloride.'' However, the
nominator also stated that the chemical grade of the bulk drug
substance is USP. The USP monograph for arginine HCl does not
include D-arginine HCl. Therefore, this review focuses on L-arginine
HCl, not the mixture of D- and L-arginine HCl. Arginine HCl USP
grade consists of L-arginine monohydrochloride. The nomination
discussed in this Federal Register notice nominated L-arginine HCl
USP grade. ``Arginine HCl'' and ``L-arginine HCl'' are used
interchangeably throughout this Federal Register notice. L-arginine
HCl and L-lysine HCl were also nominated (Docket No. FDA-2015-N-
3469-0073-attachment 10) to be used in combination for intravenous
administration with LUTATHERA (lutetium Lu 177 dotatate injection)
treatment. That nomination is the subject of another evaluation.
\19\ The following uses will not be considered in this
evaluation because the nominations did not provide sufficient
information, including citations to relevant literature, supporting
a clinical need for the proposed uses: thyroid cysts; arginine
deficiency/supplementation; orgasmic dysfunction in women;
prevention or treatment of heart and circulatory disease; combat
fatigue; stimulation of wound healing; boosting production of nitric
oxide, relaxing blood vessels, and treating circulatory and other
cardiovascular problems; and reducing waist circumference, visceral
fat, weight, and body mass index. In addition, the following labeled
uses will not be considered in this evaluation because the
nominations did not provide sufficient information, including
citations to relevant literature, supporting a clinical need for a
more concentrated IV product or for a product to be administered via
the oral or topical route of administration: diagnostic aid in
conditions such as panhypopituitarism, pituitary dwarfism,
chromophobe adenoma, postsurgical craniopharyngioma, hypophysectomy,
pituitary trauma, acromegaly, gigantism, and problems of growth and
stature.
\20\ The topical and IV routes of administration for use of
arginine HCl to treat hyperammonemia associated with urea cycle
disorder will not be considered further because the nominations did
not provide sufficient evidence to support a clinical need for drug
products with these routes of administration. Although some of the
nominations included articles that describe the use of intravenous
arginine HCl for treating patients with hyperammonemia in urea cycle
disorder, the articles do not provide support for the nominator's
proposal to make a more concentrated product than the approved IV
drug product containing the same active ingredient. Therefore, the
IV route of administration will not be considered further for
treating hyperammonemia in urea cycle disorder because the
nominations did not provide information supporting a clinical need
for a more concentrated product. Similarly, the oral route of
administration will not be considered further for the use of
arginine HCl to treat refractory metabolic alkalosis because the
nomination did not provide any evidence to support a clinical need
for drug products with this route of administration. As explained in
section II.B of this notice, if a member of the public would like
FDA to evaluate arginine HCl based on a clinical need for a drug
product to be compounded containing arginine HCl for administration
by a route that was not evaluated in this notice, then that person
should submit a nomination to Docket No. FDA-2015-N-3469, which is
available on https://www.regulations.gov.
\21\ The proposed dosage forms (cream, ointment, and gel) are
associated with uses or routes of administration that will not be
considered in this evaluation.
\22\ See, e.g., NDA 016931 labeling available as of the date of
this notice at https://www.accessdata.fda.gov/drugsatfda_docs/label/2010/016931s031lbl.pdf. Arginine (not HCl salt) is available as a
component of several approved drug products that contain multiple
amino acids (e.g., for parenteral nutrition) (e.g., AMINOSYN II; NDA
020015). NDA 020015 labeling is available as of the date of this
notice at https://dailymed.nlm.nih.gov/dailymed/fda/fdaDrugXsl.cfm?setid=5b426208-f090-4650-86c3-89040ba45c2d&type=display. The arginine in these approved drug
products is not the same bulk drug substance as arginine HCl, which
is the subject of this evaluation.
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Because arginine HCl is a component of an FDA-approved drug
product, we considered whether: (1) there is a basis to conclude that
an attribute of the FDA-approved drug product that contains arginine
HCl makes it medically unsuitable to treat certain patients for a
condition that FDA has identified for evaluation, and the arginine HCl
drug product proposed to be compounded is intended to address that
attribute in the FDA-approved drug product and (2) whether the drug
product proposed to be compounded must be compounded using a bulk drug
substance. In addition, because we answered these two questions in the
affirmative for an oral arginine HCl compounded drug product, we also
conducted a balancing test to further evaluate this bulk drug substance
by considering and applying the four factors described above.
1. Suitability of FDA-Approved Drug Products
A nominator proposes that there is a clinical need for an oral,
single-ingredient arginine HCl compounded drug product to treat
patients with certain UCDs. The references submitted with the
nomination describe the use of arginine HCl orally for long-term
maintenance therapy in patients with UCDs. There is a basis to conclude
that the FDA-approved drug product that contains only arginine HCl (R-
Gene 10) is medically unsuitable to treat patients who require long-
term oral maintenance therapy because the approved drug product is only
available for intravenous administration and would not be suitable for
the use proposed in the nomination, which would involve daily oral
administration.\23\ The drug product proposed to be compounded is
intended to address the attribute of the approved drug product that
makes it medically unsuitable for some patients because the nominator
proposes to compound oral formulations (capsules, powder for
dispersion, and oral solution/suspension) of arginine HCl. Accordingly,
FDA finds that the drug product proposed to be compounded is intended
to address the attribute of the approved drug product that makes it
medically unsuitable for some patients.
---------------------------------------------------------------------------
\23\ Empower Pharmacy proposed to make several different dosage
forms, including ``oral capsules, powder for dispersion, oral
solutions/suspensions.'' We are not commenting on the potential
suitability of these various proposed dosage forms due to the lack
of data available on the various dosage forms. Furthermore, none of
the scientific literature reviewed by FDA referred to off-label use
of the approved intravenous arginine HCL drug product in patients
with urea cycle disorder.
---------------------------------------------------------------------------
A nominator also proposes that there is a clinical need for an
intravenous single-ingredient arginine HCl
[[Page 71647]]
compounded drug product to treat patients with refractory metabolic
alkalosis. The nomination does not identify an attribute of the FDA-
approved arginine HCl (R-Gene 10) 10 GM/100 mL (100 mg/mL; 10 percent)
injection for intravenous administration that makes it medically
unsuitable for certain patients or indicate that the compounded drug
product is intended to address any such attribute. FDA finds no basis
to conclude that an attribute of the FDA-approved product makes it
medically unsuitable to treat certain patients for a condition that FDA
has identified for evaluation and that a proposed compounded product is
intended to address.
2. Whether the Drug Product Must Be Compounded From a Bulk Drug
Substance
FDA finds that there is a basis to conclude that the oral drug
products proposed to be compounded must be made from a bulk drug
substance rather than from FDA-approved R-Gene 10 because of the
difficulties and complexities associated with starting with the
approved solution for intravenous administration and converting it
either to capsules or to a powder for dispersion that would be
administered orally. The nominator also proposed to compound an oral
solution of arginine HCl that is at a higher concentration than the
approved intravenous product (100 mg/mL). There is a basis to conclude
that the proposed oral liquid drug product must also be compounded
starting from the bulk drug substance because of the difficulties and
complexities associated with compounding a more concentrated solution
beginning with the approved product.
With regard to an intravenous, single-ingredient arginine HCl
compounded drug product proposed to treat patients with refractory
metabolic alkalosis, the nominator has not identified patients for whom
the approved products are medically unsuitable or identified an
attribute of the approved drug product that the proposed compounded
drug product is intended to address. Because the nominations do not
identify specific differences between drug products that would be
compounded using arginine HCl and the approved drug product containing
arginine HCl, there is nothing for FDA to evaluate under question 2 for
intravenous single-ingredient arginine HCl.
3. Balancing Test
Because FDA answered ``yes'' to both of the threshold questions for
arginine HCl for oral administration, we next conducted the following
balancing testing to determine whether the statutory ``clinical need''
standard has been met. We considered data and information regarding the
physical and chemical characterization of arginine HCl, safety issues
raised by use of this substance in compounding, available evidence of
effectiveness or lack of effectiveness, and historical and current use
in compounding.
Arginine HCl is a well-characterized amino acid and is stable under
ordinary storage conditions. Provided the quality of arginine HCl meets
the standards in its USP drug substance monograph, arginine HCl is well
characterized physically and chemically.\24\
---------------------------------------------------------------------------
\24\ See section 503B(a)(2)(B) of the FD&C Act.
---------------------------------------------------------------------------
Oral administration of arginine HCl does not raise serious safety
issues. The available literature and general clinical practice
guidelines for the treatment of UCDs indicate that the oral formulation
of arginine HCl may be effective in treating UCDs. There is evidence of
the historical and current use of arginine HCl in compounding as an
oral formulation for the treatment of UCDs (except those with arginase
deficiency) in the United States, Belgium, and the United Kingdom.
There are no FDA-approved oral arginine HCl drug products in the United
States.
Arginine HCl is a well-characterized amino acid, does not raise
serious safety concerns, may be effective in treating UCDs, and there
is evidence of historical and current use of arginine HCl in
compounding. Therefore, on balance, the physical and chemical
characterization, safety, effectiveness, and historical and current use
of arginine HCl for oral use weigh in favor of including this substance
on the 503B Bulks List. Accordingly, we propose adding arginine HCl to
the 503B Bulks List for oral use only.
B. Lysine HCl
Lysine HCl was nominated as a bulk drug substance for the 503B
Bulks List to compound drug products that are used to correct lysine
deficiency with lysinuric protein intolerance (LPI) and for prophylaxis
and acute treatment of herpes simplex outbreak, among other
conditions.25 26 The proposed route of administration is
oral, among others; the proposed dosage forms are capsules and
solutions, among others.\27\ The nominations proposed a strength range
of 100 to 500 mg. This nominated bulk drug substance is a component of
many approved drug products as part of a combination with multiple
other amino acids for intravenous administration (e.g., NDA
018931).\28\ Lysine HCl is not approved as a single-ingredient drug
product in any dosage form (Ref. 4).
---------------------------------------------------------------------------
\25\ See Docket No. FDA-2015-N-3469, document nos. FDA-2015-N-
3469-0200 and FDA-2015-N-3469-0245. All of the nominations included
in this evaluation nominated lysine HCl USP grade. Lysine HCl USP
grade consists of L-lysine hydrochloride. A nominator submitted
duplicate nominations for L-lysine HCl to the docket: FDA-2015-N-
3469-0199 (submitted on August 31, 2018) and FDA-2015-N-3469-0200
(submitted on September 4, 2018). For the purposes of this
evaluation, FDA referred to the information in the most recent
nomination submitted to the docket (FDA-2015-N-3469-0200). On
February 26, 2021, this nominator provided additional information
regarding their nomination for lysine HCl to the University of
Maryland Center of Excellence in Regulatory Science and Innovation
(M-CERSI). The updated information is also considered in this
evaluation. Another nominator nominated ``L-lysine;'' M-CERSI
clarified with this nominator that they intended to nominate L-
lysine HCl. L-arginine HCl and L-lysine HCl were also nominated by a
different nominator (FDA-2015-N-3469-0074) to be used in combination
for intravenous administration with LUTATHERA (lutetium Lu 177
dotatate injection) treatment, which is the subject of another
evaluation.
\26\ The following uses will not be considered in this
evaluation because the nominations did not provide any information,
including citations to relevant literature, supporting a clinical
need for the proposed use: correcting lysine deficiency without LPI,
rehydration and immune support, osteoporosis, muscle recovery,
prevention of mucositis. The use of lysine HCl during peptide
receptor radionuclide therapy to reduce the radiation dose to the
kidneys is discussed in a separate evaluation. In the updated
nomination information provided to M-CERSI, a nominator proposed an
additional use of ``rehydration and immune support'' as an
intramuscular injection.
\27\ The proposed topical, intravenous, and intramuscular routes
of administration will not be considered in this evaluation because
the nominations do not provide any evidence to support a clinical
need for drug products with these routes of administration for use
of lysine HCL to correct lysine deficiency with LPI or for the use
of lysine HCL for prophylaxis and acute treatment of herpes simplex
outbreak. Accordingly, the proposed dosage forms associated with
these routes of administration (cream, ointment, and solutions for
injection) will not be considered in this evaluation. A nominator
cited one article that studied the use of the topical product
``SuperLysinePlus+'' every 2 hours during waking hours in patients
with symptoms of a cold sore consistent with a herpes simplex virus
infection of <=24 hours duration (Ref. 5). ``[L]ysine'' is included
in ``SuperLysinePlus+'' as an inactive ingredient. Thus, this study
does not provide evidence that there is a need for topical lysine
HCl in patients with herpes simplex virus.
\28\ See, e.g., NDA 018931 labeling is available as of the date
of this notice at https://dailymed.nlm.nih.gov/dailymed/fda/fdaDrugXsl.cfm?setid=8543b5be-0f43-4891-9e56-d7c39fe839b5&type=display.
---------------------------------------------------------------------------
Because lysine HCl is a component of FDA-approved drug products, we
considered whether: (1) there is a basis to conclude that an attribute
of each FDA-approved drug product that contains lysine HCl makes each
one medically unsuitable to treat certain patients for a condition that
FDA has identified for evaluation, and the lysine HCl drug product
proposed to be
[[Page 71648]]
compounded is intended to address that attribute in each FDA-approved
drug product and (2) whether the drug product proposed to be compounded
must be compounded using a bulk drug substance. In addition, because we
answered these two questions in the affirmative for an oral lysine HCl
compounded drug product, we also conducted a balancing test to further
evaluate this bulk drug substance by considering and applying the four
factors described above.
1. Suitability of FDA-Approved Drug Products
A nominator proposes that there is a clinical need for an oral,
single-ingredient lysine HCl compounded drug product to treat patients
with lysine deficiency with LPI and for prophylaxis and treatment of
acute herpes simplex outbreak. We find there is a basis to conclude
that the FDA-approved drug products that contain lysine HCl are
medically unsuitable for the proposed uses. The approved drug products
all contain lysine HCl in combination with multiple other amino acids
and are for intravenous administration. The nominators did not provide,
and FDA did not otherwise identify, evidence that these additional
active ingredients are needed to treat the conditions proposed by the
nominators. In addition, the approved products are only available for
intravenous administration and would not be suitable for the uses
proposed in the nominations, which would involve daily oral
administration. Accordingly, FDA finds that the drug products proposed
to be compounded, oral formulations of single-ingredient lysine HCl,
are intended to address the attribute of the approved drugs that makes
them medically unsuitable for some patients.
2. Whether the Drug Product Must Be Compounded From a Bulk Drug
Substance
FDA finds that there is a basis to conclude that the oral drug
products containing lysine as the single ingredient proposed to treat
patients with lysine deficiency with LPI and for prophylaxis and
treatment of acute herpes simplex outbreak must be produced from a bulk
drug substance because of the difficulties and complexities associated
with removing lysine HCl from the approved products, which are all
multiple amino acid solutions.
3. Balancing Test
Because FDA answered ``yes'' to both of the threshold questions for
lysine HCl, we next conducted the following balancing testing to
determine whether the statutory ``clinical need'' standard has been
met. We considered data and information regarding the physical and
chemical characterization of lysine HCl, safety issues raised by use of
this substance in compounding, available evidence of effectiveness or
lack of effectiveness, and historical and current use in compounding.
Lysine HCl is well-characterized chemically and physically and is
expected to be stable under ordinary storage conditions. Provided the
quality of lysine HCl meets the standards in its USP drug substance
monograph, lysine HCl is well characterized physically and
chemically.\29\
---------------------------------------------------------------------------
\29\ See section 503B(a)(2)(B) of the FD&C Act.
---------------------------------------------------------------------------
The available data do not provide evidence to support the
effectiveness of oral lysine in the prophylaxis or treatment of herpes
simplex, and a number of FDA-approved therapies are available for acute
treatment and prophylaxis of herpes simplex. Oral lysine is also
nominated for use in LPI, an extremely rare disease, the exact
prevalence of which in the United States is unknown. Oral lysine is
used in the treatment of LPI patients in small doses established and
prescribed on a per patient basis to avoid gastrointestinal
intolerance. Published data show that oral lysine normalizes plasma
concentration of lysine in patients with LPI. While the long-term
results are inconclusive as to whether chronic supplementation or
intermittent supplementation is consistently helpful (or needed), they
do suggest a positive impact on growth in some patients. In addition,
there are no FDA-approved products indicated for the treatment of LPI
and no FDA-approved, single-ingredient lysine drug products for lysine
supplementation. Oral use of lysine HCl does not raise serious safety
issues. The most commonly reported adverse events of abdominal pain and
diarrhea are associated with high doses of lysine HCl and are usually
prevented by titrating the dose to a lower acceptable level. There is
evidence regarding the current and historical use of lysine HCl in
pharmacy compounding, commonly in an injectable dosage form, within the
United States. We found no evidence of current or historical use of a
compounded lysine HCl product for oral administration.
Lysine HCl is well-characterized chemically; does not raise serious
safety issues; and although the data do not support the effectiveness
of lysine HCl in the prophylaxis or treatment of herpes simplex,
published data show that oral lysine normalizes plasma concentration of
lysine in patients with LPI. There is evidence of historical and
current use of lysine HCl in compounding. Therefore, on balance, the
physical and chemical characterization, safety, effectiveness, and
historical and current use of lysine HCl weigh in favor of including
this substance for oral use on the 503B Bulks List. Accordingly, we
propose adding lysine HCl to the 503B Bulks List for oral use only.
C. Lysine HCl as a Single Ingredient and in Combination With Single-
Ingredient Arginine HCl
Lysine HCl was also nominated for the 503B Bulks List both as a
single-ingredient and in combination with arginine HCl.30 31
Lysine HCl was nominated to compound single-ingredient drug products
that are used for reduction of radiolabeled peptides during peptide
receptor radionuclide therapy (PRRT).\32\ Lysine HCl in combination
with arginine HCl was nominated for post-LUTATHERA \33\ treatment.
LUTATHERA is indicated to treat somatostatin receptor-positive
gastroenteropancreatic neuroendocrine tumors, including foregut,
midgut, and hindgut neuroendocrine tumors in adults. The proposed route
of administration for lysine HCl used in a compounded drug product in
combination with arginine HCl, is intravenous and the proposed dosage
form is injection. For lysine HCl as a
[[Page 71649]]
single-ingredient drug product, the proposed route of administration is
intravenous, among others, and the proposed dosage form is
injection.\34\ The nominations proposed a strength range of 25 to 100
mg/mL. The nominated bulk drug substances arginine HCl \35\ and lysine
HCl \36\ are components of FDA-approved drug products labeled for
intravenous administration. Lysine HCl is not a component of any
single-ingredient, approved drug product in any dosage form, but
arginine HCl is a component of one single-ingredient, approved drug
product for intravenous administration (Ref. 6).
---------------------------------------------------------------------------
\30\ See Docket No. FDA-2015-N-3469, document nos. FDA-2015-N-
3469-0073 attachment 10, FDA-2015-N-3469-0074 attachment 4, and FDA-
2015-N-3469-0245. A nominator nominated ``L-lysine.'' M-CERSI
clarified with the nominator that they intended to nominate L-lysine
HCl. L-arginine HCl as a single ingredient product was nominated by
other parties for different uses and in different formulations.
Those nominations are the subject of another evaluation. In
addition, L-lysine HCl was nominated as a single ingredient product
for the following uses: to correct lysine deficiency with or without
lysinuric protein intolerance, prophylaxis and treatment of herpes
simplex outbreak, osteoporosis, muscle recovery, and prevention of
mucositis. These nominated uses are the subject of another
evaluation.
\31\ Lysine HCl USP grade consists of L-lysine hydrochloride.
All the nominations discussed in this Federal Register notice
nominated lysine HCl USP grade. ``lysine HCl'' and ``L-lysine HCl''
are used interchangeably throughout this Federal Register notice.
Arginine HCl USP grade consists of L-arginine monohydrochloride. The
nomination discussed in this Federal Register notice nominated L-
arginine HCl USP grade. ``Arginine HCl'' and ``L-arginine HCl'' are
used interchangeably throughout this Federal Register notice.
\32\ FDA interprets the nominator's proposed use to be to reduce
the radiation dose to the kidneys during PRRT.
\33\ Lutetium Lu-177 dotatate (LUTATHERA) was approved by FDA on
January 26, 2018. It is a PRRT used to treat patients with
neuroendocrine tumors.
\34\ The oral and topical routes of administration will not be
considered in this evaluation because the nomination does not
provide any evidence to support FDA's evaluation of these routes of
administration for use of lysine HCl to reduce the radiation dose to
the kidneys during PRRT.
\35\ See NDA 016931 labeling is available as of the date of this
notice at https://www.accessdata.fda.gov/drugsatfda_docs/label/2010/016931s031lbl.pdf.
\36\ See, e.g., NDA 018931 labeling is available as of the date
of this notice at https://www.accessdata.fda.gov/drugsatfda_docs/label/2020/018931s055,020849s025lbl.pdf. TRAVASOL contains essential
(including lysine as the HCl salt) and nonessential amino acids
(including arginine base, not HCl salt).
---------------------------------------------------------------------------
Because lysine HCl and arginine HCl are components of FDA-approved
drug products, we considered whether: (1) there is a basis to conclude
that an attribute of each FDA-approved drug product that contains
lysine HCl or arginine HCl makes each one medically unsuitable to treat
certain patients for a condition that FDA has identified for
evaluation, and the lysine HCl and arginine HCl drug products proposed
to be compounded are intended to address that attribute in each FDA-
approved drug product and (2) whether the drug product proposed to be
compounded must be compounded using a bulk drug substance. In addition,
because we answered these two questions in the affirmative for lysine
HCl for the intravenous route of administration, we also conducted a
balancing test to further evaluate both the proposed lysine HCl single-
ingredient product and the use of lysine HCl to compound a drug product
containing both lysine HCl and FDA-approved arginine HCl by considering
and applying the four factors described above.
1. Suitability of FDA-Approved Drug Products
A nominator proposes that there is a clinical need for an
intravenous product containing a unique combination of lysine HCl and
arginine HCl to be used in patients receiving LUTATHERA treatment.\37\
According to the LUTATHERA labeling, a dual combination of arginine HCl
and lysine HCl is recommended for renal protection during LUTATHERA
treatment.\38\ FDA-approved drug products that contain lysine HCl are
medically unsuitable for the proposed use for patients. Although
approved drug products that contain lysine HCl in combination with
multiple other amino acids are used off-label for this indication, the
nominators did not provide, and FDA did not otherwise identify,
evidence that these additional active ingredients are needed for
radiation protection. Furthermore, there is evidence that suggests that
combination L-lysine HCl/L-arginine HCl compounded intravenous
infusions produce less nausea in patients receiving them for this
indication than the FDA-approved amino acid solutions, and therefore
would lead to fewer episodes of vomiting. The FDA-approved product
containing arginine HCl, R-Gene 10 10 GM/100 mL injection for
intravenous administration, is medically unsuitable for patients
receiving LUTATHERA treatment because LUTATHERA's labeling recommends
administering an amino acid solution containing L-lysine and L-arginine
before administering LUTATHERA, rather than administering arginine HCl
as a single-ingredient.
---------------------------------------------------------------------------
\37\ In addition, a letter from the Society of Nuclear Medicine
and Molecular Imaging (SNMMI) provided support for the proposed
compounded drug product, stating that ``patients receiving lysine
and arginine solution suffered from much less vomiting incidents in
comparison with patients infused with commercial solutions'' and
``lysine and arginine solution is also more effective in inhibiting
renal uptake of radioactivity during peptide receptor radionuclide
therapy.'' (Ref. 7).
\38\ See NDA 208700 labeling is available as of the date of this
notice at https://www.accessdata.fda.gov/drugsatfda_docs/label/2018/208700s000lbl.pdf.
---------------------------------------------------------------------------
The drug product proposed to be compounded is intended to address
the attributes of the approved drugs that make them medically
unsuitable for some patients because the nominator proposes to compound
an intravenous formulation containing both lysine HCl and arginine HCl
without additional active ingredients.
A nominator also proposes that there is a clinical need for an
intravenous product containing lysine HCl as a single ingredient (i.e.,
not in combination with arginine-HCl) to reduce radiolabeled peptides
during PRRT. The FDA-approved drug products that contain lysine HCl all
contain lysine HCl in combination with multiple other amino acids. The
FDA-approved drug products that contain lysine HCl are medically
unsuitable for the proposed use for some patients. Although FDA-
approved drug products that contain lysine HCl in combination with
multiple other amino acids are used off-label for this indication, the
nominators did not provide, and FDA did not otherwise identify,
evidence that these additional active ingredients are needed for
radiation protection.
The drug product proposed to be compounded is intended to address
the attribute of the approved drug that makes it medically unsuitable
for some patients because the nominator proposes to compound an
intravenous product containing lysine HCl as the single ingredient,
without the other amino acids that are present in the approved drug
product.
2. Whether the Drug Product Must Be Compounded From a Bulk Drug
Substance
In order to compound the proposed drug product containing a
combination of lysine HCl and arginine HCl, FDA has a basis to conclude
that lysine HCl must be compounded from bulk drug substance rather than
from the FDA-approved drug products. The bulk drug substance lysine HCl
must be used because of the difficulties and complexities associated
with removing lysine HCl from the approved drug products that contain
multiple other amino acids (e.g., TRAVASOL).\39\
---------------------------------------------------------------------------
\39\ See, e.g., NDA 018931 labeling available as of the date of
this notice at https://www.accessdata.fda.gov/drugsatfda_docs/label/2020/018931s055,020849s025lbl.pdf.
---------------------------------------------------------------------------
FDA does not have a basis to conclude that, in order to compound
the proposed drug product, arginine HCl must be compounded from a bulk
drug substance rather than from the FDA-approved drug product. There is
one FDA-approved drug product containing arginine HCl as the single
ingredient (R-Gene 10). R-Gene 10 is a solution of 10 g/100 mL of
arginine HCl, USP in water for injection, USP. We do not anticipate
compatibility or stability issues if this approved drug product is used
as the starting material to be combined with the bulk drug substance
lysine HCl to produce a combined solution of lysine HCl and arginine
HCl at the concentration proposed in the nomination. The pH of the
compounded drug product must be adjusted to the target pH irrespective
of the source of arginine HCl (R-Gene 10 or bulk drug substance). In
addition, the desired osmolarity of <1050 mOsmol is attainable
irrespective of the source of arginine (R-Gene 10 or bulk drug
substance) used for compounding the
[[Page 71650]]
lysine HCl and arginine HCl drug product for injection. The nomination
does not provide any support for the proposition that the proposed
product must be compounded from a bulk drug substance rather than by
starting with the FDA-approved drug product R-Gene 10. Because the
nomination does not provide support for the proposition that the
arginine HCl component of the drug product must be compounded from a
bulk drug substance rather than by starting with the FDA-approved drug
product R-Gene 10, as explained further below, FDA is proposing not to
add arginine HCl to the 503B Bulks List for use in combination with
lysine HCl (bulk drug substance).
For the same reason that there is a basis to conclude that lysine
HCl for combination with arginine HCl must be compounded from a bulk
drug substance, there is also a basis to conclude that lysine HCl as a
single-ingredient compounded drug product for the intravenous route of
administration must be produced from a bulk drug substance. As with the
preceding analysis, this is because of the difficulties and
complexities associated with removing lysine HCl from the approved
multiple amino acid solutions.
3. Balancing Test
Because FDA answered ``yes'' to both of the threshold questions for
lysine HCl as a single ingredient for reducing the radiation dose to
the kidneys during PRRT and for use in combination with FDA-approved
arginine HCl, we next conducted the following balancing test to
determine whether the statutory ``clinical need'' standard has been
met. We considered data and information regarding the physical and
chemical characterization of lysine HCl as a single ingredient and in
combination with arginine HCl, safety issues raised by use of these
substances in compounding, available evidence of effectiveness or lack
of effectiveness, and historical and current use in compounding.
Arginine HCl and lysine HCl are well characterized physically and
chemically. Each of these amino acids has a USP drug substance
monograph. In addition, lysine HCl and arginine HCl are stable under
ordinary storage conditions. The FDA-approved arginine HCl drug
product, R-Gene 10, is stable at room temperature. Therefore, provided
the quality of lysine HCl meets the standards in its USP drug substance
monograph and L-arginine HCl is used starting from the FDA-approved
drug product, R-Gene 10, both these components are physically and
chemically well characterized.
Safety risks associated with the combination of lysine HCl and
arginine HCl for intravenous infusion are not such that they outweigh
the benefits, and can be managed. The most common adverse events
associated with its use are nausea and vomiting. Although there are
hyperkalemia concerns associated with lysine HCl/arginine HCl infusion,
this risk could be monitored and managed, if necessary. There is
evidence of effectiveness of lysine HCl as a single ingredient during
PRRT; however, lysine HCl as a single ingredient for intravenous
administration is associated with a higher risk of and more severe
hyperkalemia and a higher incidence of vomiting than the lysine HCl/
arginine HCl combination for intravenous administration. There is
evidence of effectiveness of combination lysine HCl and arginine HCl
infusions for reducing the radiation dose to the kidneys during PRRT in
the published literature and as described in the approved labeling of
LUTATHERA. There is also evidence in the published literature that
suggests that combination lysine HCl/arginine HCl compounded
intravenous infusions produce less nausea than FDA-approved amino acid
solutions when used to reduce the radiation dose to the kidneys during
PRRT, and therefore would lead to fewer episodes of vomiting. There is
current and historical evidence that lysine HCl and arginine HCl are
used in combination to compound injectable drug products within the
United States for nephroprotection during PRRT. There also appears to
be current and historical evidence that lysine HCl and arginine HCl are
used in combination to compound injectable drug products outside the
United States.
On balance, consideration of the physical and chemical
characterization, safety, effectiveness, and historical and current use
weighs against lysine HCl as a single ingredient (bulk drug substance)
for intravenous use, but weighs in favor of placement on the 503B Bulks
List of lysine HCl (bulk drug substance) in combination with FDA-
approved, single ingredient arginine HCl injection for intravenous use
only. Accordingly, we propose adding lysine HCl for use in combination
with FDA-approved, single-ingredient arginine HCl injection to the 503B
Bulks List for intravenous use only. FDA encourages public comment on
any particular considerations related to compounding a drug product
using FDA-approved, single-ingredient arginine HCl injection in
combination with lysine HCl (bulk drug substance).
4. Additional Comments
Due to the safety risks referred to above, if the lysine HCl in
combination with FDA-approved, single-ingredient arginine HCl injection
is placed on the 503B Bulks List, FDA intends to make safety
information about the use of lysine HCl/arginine HCl available to
prescribers, pharmacists, outsourcing facilities, and the public
through information on FDA's website, in a safety guide, or through
other mechanisms, as appropriate.
IV. Substances Evaluated and Not Proposed for Inclusion on the 503B
Bulks List
The three bulk drug substances that have been evaluated and that
FDA is proposing not to place on the list are as follows: etomidate,
furosemide, and rocuronium bromide. The reasons for FDA's proposals are
included below.\40\
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\40\ We note that furosemide injection currently appears on
FDA's drug shortage list. Under section 503B(a)(2)(A)(ii of the FD&C
Act), outsourcing facilities may compound using a bulk drug
substance if the drug compounded from such bulk drug substance
appears on FDA's drug shortage list at the time of compounding,
distribution, and dispensing, provided all of the conditions in
section 503B are met. See also FDA's Guidance for Industry,
``Interim Policy on Compounding Using Bulk Drug Substances Under
Section 503B of the Federal Food, Drug, and Cosmetic Act,'' which
describes an enforcement policy for compounding a drug product that
appeared on FDA's drug shortage list using a bulk drug substance
that is not on the 503B Bulks List provided certain conditions are
met. We further note that both furosemide and rocuronium bromide
appear on the list maintained by FDA of drugs used for hospitalized
patients with COVID-19. FDA's Guidance for Industry, ``Temporary
Policy for Compounding of Certain Drugs for Hospitalized Patients by
Outsourcing Facilities During the COVID-19 Public Health Emergency''
describes an enforcement policy, subject to certain conditions, for
compounding a drug product using a bulk drug substance that is not
on the 503B Bulks List during the COVID public health emergency.
---------------------------------------------------------------------------
Because the substances in this section are components of FDA-
approved drug products, we considered, as applicable, one or both of
the following questions: (1) is there a basis to conclude that an
attribute of each FDA-approved drug product containing the bulk drug
substance makes each one medically unsuitable to treat certain patients
for a condition that FDA has identified for evaluation, and the drug
product proposed to be compounded is intended to address that attribute
and (2) is there a basis to conclude that the drug product proposed to
be compounded must be compounded using a bulk drug substance.
A. Etomidate
Etomidate has been nominated for inclusion on the 503B Bulks List
to compound drug products for the
[[Page 71651]]
induction of general anesthesia and as an adjunct in maintenance of
general anesthesia.\41\ The proposed route of administration is
intravenous, the proposed dosage form is a preservative-free solution,
and the proposed concentration is 2 mg/mL. The nominations propose to
compound a preservative-free solution. However, they fail to
acknowledge that there is a preservative-free formulation of etomidate
that is FDA-approved or explain why that formulation would be medically
unsuitable for certain patients. The nominations state that etomidate
might also be used to compound other drug products, but do not identify
those products. The nominated bulk drug substance is a component of
FDA-approved drug products (e.g., NDA 018227). FDA-approved etomidate
is available as a single dose, preservative-free 20 mg/10 mL (2 mg/mL)
solution to be administered by intravenous injection.42 43
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\41\ See Docket No. FDA-2013-N-1524, document nos. FDA-2013-N-
1524-2292 and FDA-2013-N-1524-2298.
\42\ See, e.g., NDA 018227 labeling available as of the date of
this notice at https://www.accessdata.fda.gov/spl/data/41253af6-deac-43de-9af3-3b727ea351d8/41253af6-deac-43de-9af3-3b727ea351d8.xml.
\43\ According to the label for NDA 018227, each mL contains
etomidate, 2 mg, propylene glycol 35% v/v.
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1. Suitability of FDA-Approved Drug Product(s)
The nominations do not explain why an attribute of each of the FDA-
approved single dose, preservative-free 2 mg/mL solution products for
intravenous injection is medically unsuitable for certain patients or
identify an attribute of the approved drug products that the proposed
compounded drug product is intended to address. FDA finds no basis to
conclude that an attribute of the FDA-approved products makes them
medically unsuitable to treat certain patients for a condition that FDA
has identified for evaluation and that a proposed compounded product is
intended to address.
2. Whether the Drug Product Must Be Compounded From a Bulk Drug
Substance
Because the nominations do not identify specific differences
between drug products that would be compounded using etomidate and
approved drug products containing etomidate, there is nothing for FDA
to evaluate under question 2.
B. Furosemide
Furosemide has been nominated for inclusion on the 503B Bulks List
to compound drug products that treat congestive heart failure, edema,
renal failure, and hypertension, among other conditions.\44\ The
proposed routes of administration are intravenous and intramuscular,
the proposed dosage forms are both a preservative-free and a preserved
solution, and the proposed concentration is 10 mg/mL. The nominations
propose to compound both preservative-free and preserved solutions.
However, they fail to acknowledge that there is a preservative-free
formulation of furosemide that is FDA-approved or explain why that
formulation would be medically unsuitable for certain patients. The
nominations state that furosemide might also be used to compound other
drug products, but do not identify those products. The nominated bulk
drug substance is a component of FDA-approved drug products (e.g., ANDA
212174). FDA-approved furosemide is available as a preservative-free 40
mg per 4 mL (10 mg/mL) solution for intravenous or intramuscular
administration.45 46 47
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\44\ See Docket No. FDA-2013-N-1524, document nos. FDA-2013-N-
1524-2292 and FDA-2013-N-1524-2298.
\45\ See, e.g., ANDA 212174 labeling available as of the date of
this notice at https://www.accessdata.fda.gov/spl/data/421aa6d5-623b-4dc2-abd5-bb9e7765bf37/421aa6d5-623b-4dc2-abd5-bb9e7765bf37.xml.
\46\ Per the label for ANDA 212174, the solution is
preservative-free and is intended for intravenous or intramuscular
administration.
\47\ Furosemide is also approved as an oral solution and as a
tablet.
---------------------------------------------------------------------------
1. Suitability of FDA-Approved Drug Product(s)
The nominations do not explain why an attribute of each of the FDA-
approved preservative-free 40 mg per 4 mL (10 mg/mL) solution products
for intravenous or intramuscular administration is medically unsuitable
for certain patients or identify an attribute of the approved drug
products that the proposed compounded drug products are intended to
address. For example, the nominations propose to compound a preserved
solution because the available FDA-approved products are preservative-
free, but the nominations do not identify specific data or information
supporting the need for a preserved product. FDA finds no basis to
conclude that an attribute of the FDA-approved products makes them
medically unsuitable to treat certain patients for a condition that FDA
has identified for evaluation and that a proposed compounded product is
intended to address.
2. Whether the Drug Product Must Be Compounded From a Bulk Drug
Substance
Because the nominations have not identified a population for whom
the approved products would be medically unsuitable, FDA has not
evaluated whether the proposed preserved drug products containing
furosemide must be compounded from bulk drug substances rather than
using the approved drug product.
C. Rocuronium Bromide
Rocuronium bromide has been nominated for inclusion on the 503B
Bulks List to compound drug products that serve as an adjunct to
general anesthesia to facilitate both rapid sequence and routine
tracheal intubation and to provide skeletal muscle relaxation during
surgery or mechanical ventilation.\48\ The proposed route of
administration is intravenous, the proposed dosage form is a
preservative-free solution for injection, and the proposed
concentration is 10 mg/mL. The nominations propose to compound a
preservative-free solution. However, they fail to acknowledge that
there is a preservative-free formulation of rocuronium bromide that is
FDA-approved or explain why that formulation would be medically
unsuitable for certain patients. The nominations state that rocuronium
bromide might also be used to compound other drug products, but do not
identify those products. The nominated bulk drug substance is a
component of FDA-approved drug products (e.g., ANDA 079195). FDA-
approved rocuronium bromide is available as a preservative-free 10 mg/
mL solution for intravenous administration.49 50
---------------------------------------------------------------------------
\48\ See Docket No. FDA-2013-N-1524, document nos. FDA-2013-N-
1524-2292 and FDA-2013-N-1524-2298.
\49\ See, e.g., ANDA 079195 labeling available as of the date of
this notice at https://www.accessdata.fda.gov/spl/data/e21db7bf-3cab-4000-94dd-15c6d2a213de/e21db7bf-3cab-4000-94dd-15c6d2a213de.xml.
\50\ Per the label for ANDA 079195 each mL contains 10 mg
rocuronium bromide and 2 mg sodium acetate. The aqueous solution is
adjusted to isotonicity with sodium chloride and to a pH of 4 with
acetic acid and/or sodium hydroxide.
---------------------------------------------------------------------------
1. Suitability of FDA-Approved Drug Product(s)
The nominations do not explain why an attribute of each of the FDA-
approved 10 mg/mL preservative-free solution products is medically
unsuitable for certain patients or
[[Page 71652]]
identify an attribute of the approved drug products that the proposed
compounded drug product is intended to address. FDA finds no basis to
conclude that an attribute of the FDA-approved products makes them
medically unsuitable to treat certain patients for a condition that FDA
has identified for evaluation and that a proposed compounded product is
intended to address.
2. Whether the Drug Product Must Be Compounded from a Bulk Drug
Substance
Because the nominations do not identify specific differences
between drug products that would be compounded using rocuronium bromide
and approved drug products containing rocuronium bromide, there is
nothing for FDA to evaluate under question 2.
VI. Conclusion
For the reasons stated above, we tentatively conclude that there is
a clinical need for outsourcing facilities to compound drug products
using the bulk drug substances arginine HCl for oral use only, lysine
HCl for oral use only, and lysine HCl in combination with FDA-approved
single-ingredient arginine HCl for injection for intravenous use only.
We therefore propose to include those bulk drug substances on the 503B
Bulks List as described in this notice.
At this time, we find no basis to conclude that there is a clinical
need for outsourcing facilities to compound drug products using the
bulk drug substances etomidate, furosemide, and rocuronium bromide.
Therefore, we propose not to include these bulk drug substances on the
503B Bulks List.
VII. References
The following references marked with an asterisk (*) are on display
at the Dockets Management Staff (see ADDRESSES) and are available for
viewing by interested persons between 9 a.m. and 4 p.m., Monday through
Friday; they are also available electronically at https://www.regulations.gov. References without asterisks are not on public
display at https://www.regulations.gov because they have copyright
restriction. Some may be available at the website address, if listed.
References without asterisks are available for viewing only at the
Dockets Management Staff. FDA has verified the website addresses, as of
the date this document publishes in the Federal Register, but websites
are subject to change over time.
*1. FDA, Guidance for Industry, ``Interim Policy on Compounding
Using Bulk Drug Substances Under Section 503B of the Federal Food,
Drug, and Cosmetic Act,'' January 2017 (available at https://www.fda.gov/media/94402/download).
*2. FDA, Guidance for Industry, ``Evaluation of Bulk Drug Substances
Nominated for Use in Compounding Under Section 503B of the Federal
Food, Drug, and Cosmetic Act,'' March 2019 (available at https://www.fda.gov/media/121315/download).
*3. FDA Memorandum to File, ``Clinical Need for Arginine
Hydrochloride in Compounding Under Section 503B of the FD&C Act,''
October 2022.
*4. FDA Memorandum to File, ``Clinical Need for Lysine Hydrochloride
in Compounding Under Section 503B of the FD&C Act,'' October 2022.
5. Singh, B.B., J. Udani, S.P, Vinjamury, C, Der-Martirosian, et al,
2005, ``Safety and Effectiveness of an L-lysine, Zinc, and Herbal-
Based Product on the Treatment of Facial and Circumoral Herpes,''
Alternative Medicine Review, 10: 123-7
*6. FDA Memorandum to File, ``Clinical Need for Lysine Hydrochloride
(HCl) Alone and in Combination With Arginine HCl in Compounding
Under Section 503B of the FD&C Act,'' October 2022.
*7. Letter from SNMMI to FDA dated May 25, 2018, requesting FDA
place arginine and lysine on the 503B Bulks List.
Dated: November 17, 2022.
Lauren K. Roth,
Associate Commissioner for Policy.
[FR Doc. 2022-25549 Filed 11-22-22; 8:45 am]
BILLING CODE 4164-01-P
