Biowaiver request: powder oral dosage form, same formulation/manufacturing process approach

Abbreviated New Animal Drug Applications

GFI171

Biowaiver request: powder oral dosage form, same formulation/manufacturing process approach

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#171
Demonstrating Bioequivalence for Soluble
Powder Oral Dosage Form Products and
Type A Medicated Articles Containing Active
Pharmaceutical Ingredients Considered to Be
Soluble in Aqueous Media

Guidance for Industry
This guidance document makes revisions to the draft guidance withdrawn in March 2017.
Among the revisions, we revised the method for defining drug solubility, provided information on how to
conduct the solubility assessment, provided instructions on how to calculate the maximum dose for testing
drug solubility, and provided recommendations for handling situations where there are multiple species
on the label.

Submit comments on this guidance at any time. Submit electronic comments to
https://www.regulations.gov. Submit written comments to the Dockets Management Staff
(HFA-305), Food and Drug Administration, 5630 Fishers Lane, Rm. 1061, Rockville, MD
20852. All comments should be identified with the docket number FDA-2019-D-3764.
For further information regarding this document, contact [email protected].
Additional copies of this guidance document may be requested from the Policy and Regulations
Staff (HFV-6), Center for Veterinary Medicine, Food and Drug Administration, 7500 Standish
Place, Rockville MD 20855, and may be viewed on the Internet at either
https://www.fda.gov/animal-veterinary or https://www.regulations.gov.

U.S. Department of Health and Human Services
Food and Drug Administration
Center for Veterinary Medicine (CVM)
May 2021

Contains Nonbinding Recommendations

Table of Contents

I.

Introduction .......................................................................................................................... 3

II.

Background ........................................................................................................................... 4

III. Human Food Safety Considerations ................................................................................... 5
IV. Biowaivers for Soluble Powder Oral Dosage Form Products .......................................... 5
A. Qualifying for a waiver from the requirements for performing an in vivo
bioequivalence study (biowaiver) ................................................................................. 5
B. Data to support a waiver from the requirement to perform an in vivo
bioequivalence study (biowaiver) request.................................................................... 5
1. Information about the API(s): ................................................................................ 6
2. Information about the formulation: ....................................................................... 6
V.

Biowaivers for Type A Medicated Articles Manufactured from Water-Soluble Active
Pharmaceutical Ingredients ................................................................................................. 6
A. Qualifying for a waiver from the requirements for conducting an in vivo
bioequivalence study (biowaiver) ................................................................................. 6
B. Data to support a waiver from the requirement to perform an in vivo
bioequivalence study (biowaiver) request.................................................................... 7
1. Information about the API(s): ................................................................................ 7
2. Information about the formulation: ....................................................................... 8
3. Solubility Data:......................................................................................................... 8
C. Manufacturing Process .................................................................................................. 8
D. CVM evaluation of solubility data................................................................................ 8
1. Calculation based on the Maximum Daily Dose: .................................................. 9
2. Calculations based on the Dosage Adjusted Approach:....................................... 9
E. Solubility determination .............................................................................................. 10
F. Technical parameters to consider include: ................................................................ 11
1. Use of the Shaker flask: ......................................................................................... 11
2. Media composition and pH considerations: ........................................................ 11
3. Other considerations: ............................................................................................ 12

VI. GLOSSARY ........................................................................................................................ 13

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Demonstrating Bioequivalence for Soluble Powder Oral Dosage
Form Products and Type A Medicated Articles Containing Active
Pharmaceutical Ingredients Considered to Be Soluble in Aqueous
Media
Guidance for Industry
This guidance represents the current thinking of the Food and Drug Administration (FDA or
Agency) on this topic. It does not establish any rights for any person and is not binding on FDA
or the public. You can use an alternative approach if it satisfies the requirements of the
applicable statutes and regulations. To discuss an alternative approach, contact the FDA staff
responsible for this guidance as listed on the title page.
I.

Introduction

This document describes how the Center for Veterinary Medicine (CVM) intends to evaluate
requests for waiving the requirement for performing in vivo bioequivalence studies (biowaivers)
for animal drugs administered orally as soluble powders or as Type A medicated articles
manufactured from active pharmaceutical ingredients (APIs) considered to be soluble in aqueous
media (water-soluble APIs). This document expands upon CVM’s Guidance for Industry (GFI)
#35, “Bioequivalence Guidance,” 1 to include biowaivers for soluble powder oral dosage form
products as well as Type A medicated articles manufactured from APIs considered to be soluble
in aqueous media, and it offers particular focus on criteria for the waiver of the requirements for
submitting in vivo bioequivalence study data. This guidance does not address Type A medicated
articles manufactured from APIs considered to be insoluble in aqueous media.
This guidance is applicable to generic investigational new animal drug (JINAD) files and to
abbreviated new animal drug applications (ANADAs). Although the recommendations in this
guidance refer to ANADAs, the general principles described may also be applicable to new
animal drug applications (NADAs), supplemental NADAs, and investigational new animal drug
(INAD) files.
The recommendations in this guidance are premised on the assumption that a sponsor will be
bridging between identical dosage forms (e.g., their Type A medicated article for use in complete
feed to the approved reference Type A medicated article for use in complete feed). Therefore,
you should not use the recommendations in this guidance to compare the solubility of two drug
products where the API will be administered in differing manners (e.g., drinking water versus
complete feed; complete feed for administration throughout the day versus top dress). CVM
encourages sponsors to contact the Center to discuss that type of comparison.
The granting of a waiver from the requirement to perform an in vivo bioequivalence study does
not imply that a drug product is approvable. For drug product approval, all applicable legal

1

https://www.fda.gov/media/70115/download

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Contains Nonbinding Recommendations
requirements must be met (see, e.g., sections 512(c)(2) and 512(n) of the Federal Food, Drug,
and Cosmetic Act (FD&C Act)).
The contents of this document do not have the force and effect of law and are not meant to bind
the public in any way, unless specifically incorporated into a contract. This document is
intended only to provide clarity to the public regarding existing requirements under the law.
FDA’s guidance documents should be viewed only as recommendations, unless specific
regulatory or statutory requirements are cited. The use of the word should in Agency guidances
means that something is suggested or recommended, but not required.
II.

Background

An ANADA must include information to show that the proposed generic new animal drug and
reference listed new animal drug (RLNAD) are bioequivalent. 2 This requirement is patterned
very closely on the approval requirements for human generic drugs. 3
The Center for Drug Evaluation and Research’s (CDER) regulations implementing the
bioequivalence requirement for human generic drugs can be found in 21 CFR part 320. In most
cases, there must be an in vivo demonstration of no significant differences in the rate and extent
of drug availability associated with the proposed generic and reference drug products when
administered at the same molar dose under similar conditions. 4 In certain circumstances,
however, the demonstration of bioequivalence does not need to be established on the basis of in
vivo studies. 5 For several categories of human drug products, including oral solutions,
bioequivalence is considered self-evident under specified conditions. 6 In other circumstances, a
large body of research on human intestinal physiology has been used to support a determination
of product bioequivalence of solid oral dosage forms based on the use of in vitro approaches. In
this regard, the human Biopharmaceutics Classification System (BCS) criteria have been applied
to support the use of an in vitro approach to document product bioequivalence for highly soluble,
rapidly dissolving, and orally administered drug products. 7 However, because of the
physiological differences between the gastrointestinal (GI) tract of humans and that of veterinary
species, and because of the additional complexities associated with drugs that are administered as
medicated feeds, the human BCS criteria cannot be applied to support the use of an in vitro
approach for demonstrating product bioequivalence for orally administered veterinary drug
products.
CVM has issued guidance on in vivo bioequivalence studies, which includes a list of some of the
product categories, including oral solutions and other solubilized forms, that may be eligible for
a waiver from the requirement to perform in vivo bioequivalence studies.2 This guidance
2

Section 512(n)(1)(E) of the FD&C Act.

3

Section 505(j)(2)(A)(iv) of the FD&C Act.

4

21 CFR 320.1(e) and 320.21(b).

5

21 CFR 320.21(b) and (f), and 320.22.

6

21 CFR 320.22(b)(3).

7

See CDER Guidance for Industry, “Waiver of In Vivo Bioavailability and Bioequivalence Studies for ImmediateRelease Solid Oral Dosage Forms Based on a Biopharmaceutics Classification System,” December 2017, Pages 2
and 11-12. (https://www.fda.gov/media/70963/download)

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Contains Nonbinding Recommendations
provides additional information and recommendations regarding bioequivalence waivers for
soluble powder oral dosage form products intended for use in animal drinking water, and Type A
medicated articles manufactured from APIs considered to be soluble in aqueous media and
intended for use in animal feed.
III. Human Food Safety Considerations
The granting of a waiver from the requirement to perform an in vivo bioequivalence study
(biowaiver) does not imply that a drug product is approvable. For drug product approval, all
applicable legal requirements must be met, which includes addressing the tissue residue portion
of the Human Food Safety (HFS) technical section of the application (sections
512(c)(2)(A)(viii), 512(c)(2)(B), and 512(n)(1)(A) of the FD&C Act). For products that receive
a biowaiver using the concepts of this guidance, the sponsor should contact the Division of
Human Food Safety (HFV-150) directly to discuss what, if any, additional information may be
needed to satisfy the requirements for approval.
IV. Biowaivers for Soluble Powder Oral Dosage Form Products
A. Qualifying for a waiver from the requirements for performing an in vivo
bioequivalence study (biowaiver)
CVM believes it is appropriate to grant biowaivers for oral dosage forms known as “soluble
powders” that meet the solubility requirements discussed in this guidance. Such products are
intended for administration to animals via the drinking water that is provided on an ad libitum
basis under most husbandry systems.
The conceptual basis for granting biowaivers for “soluble powders” is that if an API is in
solution before administration, the drug product’s formulation will usually not influence the
bioavailability of the active ingredient. If the test and reference formulations contain essentially
the same inactive ingredients, then from a mechanistic perspective, the rate-limiting step in
systemic API absorption will be either: (a) the rate of gastric transit; or (b) the permeability of
the API across the gastrointestinal (GI) mucosal membranes. Typically, both these variables are
formulation independent, relying solely on the API and the characteristics of the GI tract of that
animal species. Similarly, because the rate-limiting step is the API movement down the GI tract
and its lateral diffusion across the viscous intestinal contents, if an API acts locally within the GI
tract (i.e., not systemically absorbed), the local exposure to the dissolved API in the proposed
and reference drug product formulations will be equivalent if the API is already in solution. The
only exceptions of which CVM is aware are when the formulation of the drug product contains
substances other than the API that could cause a direct pharmacologic effect (e.g., altered GI
transit time, membrane permeability, or drug metabolism) or when there is inactivation of the
API.
B. Data to support a waiver from the requirement to perform an in vivo
bioequivalence study (biowaiver) request
For soluble powder oral dosage form products, CVM recommends that justification of requests
for biowaivers be made by a demonstration of solubility. CVM recommends that sponsors make

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these biowaiver requests before submitting an ANADA. The following should be provided in
the biowaiver request:
1. Information about the API(s):
CVM recommends that the API(s) used to support a biowaiver request for soluble
powder oral dosage forms be provided from the same supplier of the API(s) that
will be used to formulate the proposed drug product during production. CVM
recommends that the applicant identify the source of the API(s) and provide a
certificate of analysis (COA) for the API(s). If the API has a United States
Pharmacopeia (USP) monograph, the API should at a minimum comply with the
monograph specifications. The acceptability of the API(s) will be determined upon
review of the Chemistry, Manufacturing, and Controls (CMC) Technical Section.
2. Information about the formulation:
The formulation of the proposed drug product should be submitted. The formulation
should be such that there are no differences between the RLNAD and the proposed
drug product that would have an effect on the bioavailability of the API. There
should be no inactive ingredients in the proposed drug product’s formulation likely
to cause adverse pharmacologic effects. The API should be qualitatively (Q1) and
quantitatively (Q2) the same as the API used in the RLNAD. 8 The solubility of the
drug product should be determined under the range of physical conditions that a
user of the product would typically encounter when reconstituting the soluble
powder with animal drinking water (i.e., well or municipal water) in the field. This
study is the same as the reconstitution study outlined in GFI #5, “Drug Stability
Guidelines,” section IV.F. Soluble Powders and Drinking Water. 9 The
reconstitution data for soluble powder oral dosage form products should be
submitted in the Chemistry, Manufacturing, and Controls (CMC) Technical
Section.
V.

Biowaivers for Type A Medicated Articles Manufactured from Water-Soluble Active
Pharmaceutical Ingredients
A. Qualifying for a waiver from the requirements for conducting an in vivo
bioequivalence study (biowaiver)

Type A medicated articles that contain APIs that are not classified as water soluble are not the
subject of this guidance. The determination of the water solubility of APIs is discussed in section
V.E. Solubility Determination.
With respect to eligibility for a biowaiver, CVM believes there is no reasonable basis for
drawing a distinction between APIs intended for administration to animals via drinking water
and APIs intended to be administered via feed, provided these APIs have similar solubility
8

Current Standards & Emerging Issues of Pharmaceutical Equivalence. AAPS/EUFEPS/FIP Workshop. Mei-Ling
Chen, Ph.D. November 13–14, 2010.
9

See CVM GFI #5, “Drug Stability Guidelines,” December 2008. (https://www.fda.gov/media/69957/download)

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Contains Nonbinding Recommendations
characteristics. A water-soluble API present in a Type A medicated article and mixed into a feed
matrix rapidly dissolves when exposed to the fluids of the GI tract. If such an API readily goes
into solution across the range of physiological pH values, it will also readily go into solution
when exposed to the fluids in the GI tract. Accordingly, such medicated feeds will effectively
behave as oral solutions immediately after consumption by the animal. Therefore, CVM intends
to review biowaiver requests for Type A medicated articles containing water soluble APIs based
on a demonstration of solubility of the API, as well as an evaluation of the drug product
formulation, to ensure that there are no ingredients in the proposed formulation likely to cause
pharmacologic or pharmacodynamic differences from the RLNAD.
The criteria detailed in this guidance assume that the in vivo dissolution of the test and reference
products represents the only factor influencing the relative bioavailability of both
products. However, for compounds that are fully soluble and systemically absorbed, there is the
potential for certain excipients to alter drug absorption and or pre-systemic metabolism (liver or
intestinal), and hence affect the relative bioavailability of the products. Therefore, for Type A
medicated articles containing water-soluble APIs that are systemically absorbed, the formulation
of the proposed product should be such that there are no differences in the formulations of the
proposed drug product and the RLNAD that would have an effect on the bioavailability of the
API. Further, there should be no inactive ingredients in the proposed drug product’s formulation
likely to cause adverse pharmacologic effects.
Type A medicated articles may contain biomass drug substances, which are APIs produced
through fermentation that are not subjected to extensive post-fermentation purification. Biomass
drug substances may contain the active molecule(s), microorganisms used for production, other
metabolites produced by the microorganisms used for production, and media components.
Biomass drug substances are only used as the drug substance in Type A medicated article
formulations. Because certain biomass drug substances are well-accepted and routinely used
components of Type A medicated articles, CVM will consider the potential for the biomass drug
substance component of a Type A medicated article to cause adverse pharmacologic effects or
effects on API bioavailability in the same manner that it considers these effects with respect to
other excipients.
B. Data to support a waiver from the requirement to perform an in vivo
bioequivalence study (biowaiver) request
For Type A medicated articles containing water-soluble APIs, CVM recommends that requests
for biowaivers be made by a demonstration of solubility. CVM recommends that sponsors make
these biowaiver requests before submitting an ANADA. The following should be provided in the
biowaiver request:
1. Information about the API(s):
CVM recommends that the API(s) used to support a biowaiver request be provided
from the same supplier of the API(s) that will be used to formulate the proposed
drug product during production. CVM recommends that the applicant identify the
source of the API(s), indicate if the API(s) is a biomass drug substance (if
applicable), and provide a COA for the API(s). If the API has a USP monograph,
the API should at a minimum comply with the monograph specifications. The
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Contains Nonbinding Recommendations
acceptability of the API(s) will be determined upon review of the Chemistry,
Manufacturing and Controls (CMC) Technical Section.
2. Information about the formulation:
The formulation of the proposed drug product should be submitted. The
formulation should be such that there are no differences between the RLNAD and
the proposed drug product that would have an effect on the bioavailability of the
API. There should be no inactive ingredients in the proposed drug product’s
formulation likely to cause adverse pharmacologic effects. The API should be
qualitatively (Q1) and quantitatively (Q2) the same as the API used in the RLNAD.
Sponsors should address the inactive ingredients in their formulation and any
potential impact they may have on the bioavailability of the API(s) or the
likelihood to cause adverse pharmacologic effects. If supporting data or
information regarding any potential impact of the inactive ingredients on the
bioavailability of the API(s) or their likelihood to cause adverse pharmacologic
effects is available, it should be submitted.
3. Solubility Data:
Solubility data including method validations, and chromatograms as appropriate,
should be submitted with each biowaiver request for Type A medicated articles.
The solubility of the API should be determined in aqueous media. The inherent
ability of the API to dissolve in aqueous media is critical to using the solubility data
in support of any request for granting a biowaiver. Solubility data should represent
a pH range that is inclusive of all the pH values expected in the gastric/ruminal
environment for all the major species on the RLNAD label.
CVM recommends that the Shaker flask method be used for solubility
determinations, employing an appropriate dissolution time and temperature,
relevant to the labeled species. CVM-recommended times and temperatures for
major species are documented in Table 1 of section V.E. Solubility Determination.
C. Manufacturing process
If the process used to manufacture the Type A medicated article has the potential to alter the
solubility of the API, thereby potentially impacting bioequivalence of the generic product to the
RLNAD, then CVM may request additional data regarding solubility of the API in the final
formulation.
D. CVM evaluation of solubility data
Sponsors should submit solubility data, analytical method validations, and additional
documentation such as chromatograms in support of their biowaiver request. CVM will evaluate
the acceptability of the solubility data for the purposes of a biowaiver based on the criteria as
documented below. If a sponsor wishes to propose an alternative to meeting the bioequivalence
requirements, the sponsor may request a meeting with CVM to discuss their approach prior to

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requesting a biowaiver. In general, CVM will evaluate data submitted with a biowaiver request
using the following criteria:
1. Calculation based on the Maximum Daily Dose:
In this scenario, the entire daily dose is administered in a single feeding event.
Therefore, a demonstration that the maximum administered dose, as indicated on
the RLNAD label, is soluble in the minimum fluid volume, in the specified time, for
the indicated species (Table 1) will suffice as evidence for granting a biowaiver.
2. Calculations based on the Dosage Adjusted Approach:
In this scenario, the dose is administered as multiple feeding events through the
day. The number of feeding events by which the dose is divided is species
dependent (Table 1). Therefore, the aqueous solubility is to be evaluated based on
the highest expected mg of API per mL of gastric fluid at any point in time. This
assessment is determined based on the API concentration in the feed and
characteristics of the gastric physiology of the target animal species.
a. API concentration:
The API concentration should be calculated by using the amount of API in the
Type A medicated article likely to be consumed per feeding event, e.g.,
dividing the daily dose into the number of feeding events that the target animal
species typically takes to consume their daily ration (Table 1). This scenario is
typically applicable to situations where the animals do not consume their
rations on a continual basis through the day. An exception to this approach is
seen in poultry, where due to their continuous feeding behavior, the solubility
assessments of Type A medicated articles intended for use in poultry is to be
based upon the highest approved (undivided) mg/kg/day dose.
b. Gastric physiology:
The animal physiology is critical as it determines the gastric residence time
(how long it takes for the consumed medicated feed to exit the stomach or
rumen), the gastric fluid volume of the target animal species (Table 1), the pH
range over which solubility measurements must be made, and the temperature
at which solubility should be determined.
The solubility of the API, when tested based on the API concentration, is
defined by the highest expected daily dose (mg of API) that will go into
solution when tested in a manner consistent with the most conservative
conditions associated with the approved product label (e.g., the largest dose to
fluid volume ratio, minimum time of dissolution, and the broadest pH range
over which solubility is demonstrated). When this level of solubility of the API
is demonstrated, CVM will consider the API to be eligible for a biowaiver.

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Contains Nonbinding Recommendations
If there are multiple species on the labeling, solubility should be based on the
most conservative mg/mL scenario (i.e., use the species that produces the
highest dose to gastric fluid volume ratio).
This method of defining API solubility is similar to that described for
categorizing compounds when using the BCS and to the BCS-based approach
described in CDER guidance 10. In this case, the appropriate fluid volume for
testing API solubility depends on the target animal species/class for which the
medicated feed is intended. For example, a conservative estimate of ruminal
fluid volume (fluid volume available for drug solubilization) for steers is 47 L.
The sponsor should provide the estimated daily drug intake (mg/kg body
weight) based on the labeled drug concentration (grams of drug per ton) in the
feed administered to the animal (e.g., the Type C medicated feed) and the
highest amount of medicated feed (kg/day) expected to be consumed by an
individual animal. When using this approach, CVM recommends using the
species-specific animal data estimates summarized in Table 1.
E. Solubility determination
For the purposes of granting a biowaiver under this guidance, CVM is interested in the
physiologically relevant solubility of the API in aqueous solutions. As such, the addition of
compounds, such as surfactants used to increase the solubility of the API in aqueous media, is
not considered acceptable. If the use of surfactants is required to achieve acceptable solubility
data, then the API is not considered to be fully soluble in water, and therefore is no longer
covered under the scope of this guidance. If the use of a buffer results in any effect that may
increase the solubility of the API or drug product, that waiver request will also be denied.
The preferred method for determination of solubility is by use of the Shaker flask method 11
containing an aqueous media for the indicated time and temperature relevant to the labeled
species (Table 1). Solubility should be confirmed using a validated assay procedure that can
distinguish the API from its degradation products. The media used for testing should represent a
pH range that is inclusive of all the pH values expected in the gastric environment for all the
major species on the RLNAD label and as described in section V.F.2. Media composition and pH
considerations below. When the conditions within the GI tract are markedly different across
labeled species, appropriate media composition for testing API solubility should be discussed
with CVM.

10

See CDER Guidance for Industry, “Waiver of In Vivo Bioavailability and Bioequivalence Studies for Immediate-Release
Solid Oral Dosage Forms Based on a Biopharmaceutics Classification System,” December 2017.

11

USP 1236.

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Table 1. Standard Conditions for Use in Determining Experimental Conditions
Species *

Gastric Fluid
Volume in Liters

Gastric resident
times (hours)

Temperature
(⁰C)

Feeding events per
day

Cattle 1, 3
Swine 3
Horse 2, 3
Chicken 3
Turkey 4

47 #
0.5
1.5
0.01 ‡
0.04 ‡

8
1
0.25
2
2

36.7 – 39.3
38.7 – 39.8
37.2 – 38.2
40.6 – 43.0
40.6 – 41.5

2
2
2
N/A
N/A

* CVM

acknowledges that the estimates for the indicated species are very conservative. If alternate data points are
used, that use must be adequately justified. CVM notes that in certain instances the appropriate variable may be less
than that indicated in the table, as is the case when dealing with younger animals.
# Fluid volume of the rumen.
‡ Includes the fluid volumes of both the proventriculus and the ventriculus.
1 Martinez, M. N., Apley, M. D. Drug solubility classification in the bovine. J. vet. Pharmacol. Therap. 35 (Suppl. 1),
93–97, 2012.
2 The Equine Hospital Manual first edition, ed. Kevin Corley and Jennifer Stephen, Chapter 5, page 282. Wiley
Blackwell, 2008.
3 The Merck Veterinary Manual: http://www.merckvetmanual.com/appendixes/reference-guides/normal-rectaltemperature-ranges .
4 Some Factors Affecting Body Temperature of Turkeys: Poultry Science, Volume 34, Issue 2, 1 March 1955, Pages
369–371, https://doi.org/10.3382/ps.0340369

F. Technical parameters to consider include:
1. Use of the Shaker flask:
•

The temperature of the solution within the flask should be within the
physiological range of the healthy animal for the major indicated species on the
label. Temperatures should be maintained within ± 0.5°C of the indicated
temperature throughout the study to ensure solubility is not affected by
variation in temperature.

•

After the appropriate period of shaking (based on Gastric residence time as
described in Table 1), prior to sampling, there should be an excess of API
apparent on the bottom of the flask.

•

The supernatant (liquid above the solid) should be filtered to remove
undissolved particles not apparent to the naked eye.

•

Samples for analysis should be taken from the filtered supernatant. The
supernatant solution may need to be diluted before analysis to be within the
linear range of the analytical method and to avoid possible precipitation.

2. Media composition and pH considerations:
•

For monogastric animals: pH 1.2, 4.6 (acetate buffer), and 7.5 phosphate buffer.

•

For ruminants: For the purposes of generating data for a biowaiver request, the
media should be buffered at a pH of 4.5 (acetate buffer) and 7.5 (lactate buffer).
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•

For poultry: The sponsor should justify the sets of conditions under which
solubility will be tested. Without agreed upon justification, the default
conditions would be the same conditions as those described for monogastric
animals.

•

Solution pH should be verified after addition of the API to the buffer solution.
If the pH changes significantly after addition of the API, we would conclude
that the buffers selected are inadequate to control fluctuations in pH.

•

The pH of the solution should be verified to be consistent throughout the
assessment of the API solubility. At a minimum the pH should be verified at the
time the sample is taken for analysis.

Note that the buffers used may need to be modified if there are concerns that the
buffer itself may alter the inherent solubility of the API or drug product (e.g.,
common ion effect). However, the inclusion of organic compound-containing
buffer systems is not considered to be acceptable.
3. Other considerations:

12

•

CVM recommends a minimum of three replicate determinations of solubility
under each pH condition. Depending on study variability, additional replication
may be necessary to provide a reliable estimate of solubility.

•

A visual determination of solubility alone is insufficient. For the determination
of solubility, the concentration of the API in the selected media must be
determined using a validated quantitative assay method. 12

21 CFR 514.1(b)(5)(vii)(a)

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VI. GLOSSARY
For purposes of this guidance document, the following definitions apply:
Active Pharmaceutical Ingredient (API): A substance used in a finished pharmaceutical
product, intended to furnish pharmacological activity or to otherwise have direct effects in
the diagnosis, cure, mitigation, treatment, or prevention of disease or to have direct effect in
restoring, correcting, or modifying physiological functions of the body.
Bioavailability: The rate and extent to which the active ingredient or active moiety is
absorbed from a drug product and becomes available at the site of action. For drug products
that are not intended to be absorbed into the bloodstream, bioavailability may be assessed
by measurements intended to reflect the rate and extent to which the active ingredient or
active moiety becomes available at the site of action.
Bioequivalence: The absence of a significant difference in the rate and extent to which the
active ingredient or active moiety in pharmaceutical equivalents or pharmaceutical
alternatives becomes available at the site of drug action when administered at the same
molar dose under similar conditions in an appropriately designed study.
Biomass Drug Substance: An active ingredient, which is an unpurified fermentation
product derived from the cultivation of microorganisms, that is intended to furnish
pharmacological activity or other direct effects in the diagnosis, cure, mitigation, treatment,
or prevention of disease or to affect the structure or any function of the animal.
Biowaiver: A waiver from the requirement to perform an in vivo bioequivalence study
(21 USC 360b(n)(1)(E)).
Qualitative (Q1), Quantitative (Q2) and Structural Similarity (Q3):
Q1 means qualitative similarity between generic and reference listed products, while Q2
represents quantitative similarity of composition. Q3 describes structural similarity and
refers to the arrangement of matter and state of aggregation of the product.

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File TitleCVM GFI 171 Demonstrating Bioequivalence for Soluble Powder Oral Dosage Form Products and Type A Medicated Articles Containing A
Subjectoral dosage form, bioequivalence, guidance for industry
AuthorFDA CVM
File Modified2021-05-20
File Created2021-05-20

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