Waiver of in Vivo Bioavailability

Waiver of In Vivo
Bioavailability and
Bioequivalence Studies for
Immediate-Release Solid Oral
Dosage Forms Based on a
Biopharmaceutics Classification
System
Guidance for Industry
DRAFT GUIDANCE
This guidance document is being distributed for comment purposes only.
Comments and suggestions regarding this draft document should be submitted within 60 days of
publication in the Federal Register of the notice announcing the availability of the draft
guidance. Submit electronic comments to http://www.regulations.gov. Submit written
comments to the Division of Dockets Management (HFA-305), Food and Drug Administration,
5630 Fishers Lane, rm. 1061, Rockville, MD 20852. All comments should be identified with
the docket number listed in the notice of availability that publishes in the Federal Register.
For questions regarding this draft document contact (CDER) Mehul Mehta 301-796-1573.
U.S. Department of Health and Human Services

Food and Drug Administration
Center for Drug Evaluation and Research (CDER)
May 2015
Biopharmaceutics
Revision 1
Draft Guidance Temp

05/04/15
Waiver of In Vivo
Bioavailability and
Bioequivalence Studies for
Immediate-Release Solid Oral
Dosage Forms Based on a
Biopharmaceutics Classification
System
Guidance for Industry
Additional copies are available from:
Office of Communications, Division of Drug Information
Center for Drug Evaluation and Research
10001 New Hampshire Ave., Hillandale Bldg., 4th Floor
Silver Spring, MD 20993-0002
Phone: 855-543-3784 or 301-796-3400; Fax: 301-431-6353
Email: druginfo@fda.hhs.gov
http://www.fda.gov/Drugs/GuidanceComplianceRegulatoryInformation/Guidances/default.htm
U.S. Department of Health and Human Services

Center for Drug Evaluation and Research (CDER)
May 2015
Biopharmaceutics
Revision 1
Draft Guidance Temp

05/04/15
Contains Nonbinding Recommendations
Draft — Not for Implementation
TABLE OF CONTENTS
I. INTRODUCTION............................................................................................................. 1
II. THE BIOPHARMACEUTICS CLASSIFICATION SYSTEM ................................... 2
A. Solubility ......................................................................................................................................... 3
B. Permeability ................................................................................................................................... 3
C. Dissolution ...................................................................................................................................... 3
III. RECOMMENDED METHODOLOGY FOR CLASSIFYING A DRUG
SUBSTANCE AND FOR DETERMINING THE DISSOLUTION
CHARACTERISTICS OF A DRUG
PRODUCT ......................................................................................................................... 3
A. Determining Drug Substance Solubility Class ............................................................................ 3
B. Determining Drug Substance Permeability Class ....................................................................... 4
1. Pharmacokinetic Studies in Humans .................................................................................. 4
2. Intestinal Permeability Methods ......................................................................................... 5
3. Instability in the Gastrointestinal Tract.............................................................................. 7
C. Determining Drug Product Dissolution Characteristics and Dissolution Profile Similarity .. 7
IV. BIOWAIVERS BASED ON BCS .................................................................................... 8
V. ADDITIONAL CONSIDERATIONS FOR REQUESTING A BIOWAIVER ........... 9
A. Excipients ........................................................................................................................................ 9
B. Prodrugs ......................................................................................................................................... 9
C. Fixed Dose Combinations ............................................................................................................ 10
D. Exceptions ..................................................................................................................................... 10
1. Narrow Therapeutic Range Drugs.................................................................................... 10
2. Products Designed to be Absorbed in the Oral Cavity ..................................................... 10
VI. REGULATORY APPLICATIONS OF THE BCS ...................................................... 11
A. INDs/NDASs ................................................................................................................................. 11
B. ANDAs .......................................................................................................................................... 11
C. Supplemental NDAs/ANDAs (Postapproval Changes) ............................................................. 11
VII. DATA TO SUPPORT A REQUEST FOR BIOWAIVERS ........................................ 12
A. Data Supporting High Solubility ................................................................................................ 12
B. Data Supporting High Permeability........................................................................................... 12
C. Data Supporting Rapid, Very Rapid, and Similar Dissolution................................................ 13
D. Additional Information ............................................................................................................... 13
ATTACHMENT A ............................................................................................................................... 14
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1 Waiver of In Vivo Bioavailability and Bioequivalence Studies for

2 Immediate-Release Solid Oral Dosage Forms Based on a
3 Biopharmaceutics Classification System
4 Guidance for Industry 1
5
6
7 This draft guidance, when finalized, will represent the Food and Drug Administration’s (FDA’s) current
8 thinking on this topic. It does not create or confer any rights for or on any person and does not operate to
9 bind FDA or the public. You can use an alternative approach if the approach satisfies the requirements of
10 the applicable statutes and regulations. If you want to discuss an alternative approach, contact the FDA
11 staff responsible for implementing this guidance. If you cannot identify the appropriate FDA staff, call
12 the appropriate number listed on the title page of this guidance.
13
14
15
16
17 I. INTRODUCTION
18
19 This guidance provides recommendations for sponsors of investigational new drug applications
20 (INDs), and applicants that submit new drug applications (NDAs), abbreviated new drug applications
21 (ANDAs), and supplements to these applications for immediate-release (IR) solid oral dosage forms,
22 and who wish to request a waiver of in vivo bioavailability (BA) and/or bioequivalence (BE) studies.
23 These waivers are intended to apply to: (1) subsequent in vivo BA or BE studies of formulations
24 after the initial establishment of the in vivo BA of IR dosage forms during the IND period, and (2) in
25 vivo BE studies of IR dosage forms in ANDAs.
26
27 Regulations at 21 CFR part 320 address the requirements for BA and BE data for approval of drug
28 applications and supplemental applications. Provision for waivers of in vivo BA/BE studies
29 (biowaivers) under certain conditions is provided at 21 CFR 320.22. 2 This guidance updates the
30 guidance for industry on Waiver of In Vivo Bioavailability and Bioequivalence Studies for
31 Immediate-Release Solid Oral Dosage Forms Based on a Biopharmaceutics Classification System, 3
32 published in August 2000, and explains when biowaivers can be requested for IR solid oral dosage
33 forms based on an approach termed the Biopharmaceutics Classification System (BCS). This
1
This guidance has been prepared by the Office of Pharmaceutical Quality and the Office of Translational Sciences
in the Center for Drug Evaluation and Research (CDER) at the Food and Drug Administration.
2
In addition to waiver of an in vivo BE requirement under 21 CFR 320.22, there are certain circumstances in which
BE can be evaluated using in vitro approaches under 21 CFR 320.24(b)(6). The scientific principles described in
this guidance regarding waiver of an in vivo requirement also apply to consideration of in vitro data under that
regulation. In such circumstances, an in vivo data requirement is not waived, but rather, FDA has determined that in
vitro data is the most accurate, sensitive, and reproducible for a product, as required under 21 CFR 320.24(a).
Nonetheless, for ease of the reader, in this guidance we will refer to either the decision to waive an in vivo BE
requirement under 21 CFR 320.22 or the decision to accept in vitro BE data in accordance with 21 CFR 320.24(a)
as a “biowaiver.”
3
We update guidances periodically. To make sure you have the most recent version of a guidance, check the FDA
Drugs guidance Web page at
http://www.fda.gov/Drugs/GuidanceComplianceRegulatoryInformation/Guidances/default.htm.
Draft Guidance Temp 1

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34 guidance includes biowaiver extension to BCS class 3 drug products, and additional modifications,
35 such as criteria for high permeability and high solubility.
36
37 In general, FDA’s guidance documents do not establish legally enforceable responsibilities.
38 Instead, guidances describe the Agency’s current thinking on a topic and should be viewed only
39 as recommendations, unless specific regulatory or statutory requirements are cited. The use of
40 the word should in Agency guidances means that something is suggested or recommended, but
41 not required.
42
43
44 II. THE BIOPHARMACEUTICS CLASSIFICATION SYSTEM
45
46 The BCS is a scientific framework for classifying drug substances based on their aqueous solubility
47 and intestinal permeability. When combined with the dissolution of the drug product, the BCS takes
48 into account three major factors that govern the rate and extent of drug absorption from IR solid oral
49 dosage forms: (1) dissolution, (2) solubility, and (3) intestinal permeability. 4 According to the BCS,
50 drug substances are classified as follows:
51
52 Class 1: High Solubility – High Permeability
53 Class 2: Low Solubility – High Permeability
54 Class 3: High Solubility – Low Permeability
55 Class 4: Low Solubility – Low Permeability
56
57 In addition, some IR solid oral dosage forms are categorized as having rapid or very rapid 5
58 dissolution. Within this framework, when certain criteria are met, the BCS can be used as a drug
59 development tool to help sponsors/applicants justify requests for biowaivers.
60
61 Observed in vivo differences in the rate and extent of absorption of a drug from two
62 pharmaceutically equivalent solid oral products may be due to differences in drug dissolution in
63 vivo. 6 However, when the in vivo dissolution of an IR solid oral dosage form is rapid or very rapid
64 in relation to gastric emptying and the drug has high solubility, the rate and extent of drug absorption
65 is unlikely to be dependent on drug dissolution and/or gastrointestinal (GI) transit time. Under such
66 circumstances, demonstration of in vivo BA or BE may not be necessary for drug products
67 containing class 1 and class 3 drug substances, as long as the inactive ingredients used in the dosage
68 form do not significantly affect absorption of the active ingredients.
69
70 The BCS approach outlined in this guidance can be used to justify biowaivers for highly soluble and
71 highly permeable drug substances (i.e., class 1) as well as highly soluble and low permeable drug
72 substances (i.e., class 3) in IR solid oral dosage forms that exhibit rapid or very rapid in vitro
73 dissolution using the recommended test methods. The recommended methods for determining
74 solubility, permeability, and in vitro dissolution are discussed below.
75
4
Amidon GL, Lennernäs H, Shah VP, and Crison JR, 1995, A Theoretical Basis For a Biopharmaceutics Drug
Classification: The Correlation of In Vitro Drug Product Dissolution and In Vivo Bioavailability, Pharm Res, 12:
413-420.
5
Yu LX, Amidon GL, Polli JE, Zhao H, Mehta MU, Conner DP, et al, 2002, Biopharmaceutics classification
system: The scientific basis for biowaiver extensions, Pharm Res, 19(7):921-5.
6
See footnote 4.

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76 A. Solubility
77
78 The solubility class boundary is based on the highest strength of an IR product that is the subject of a
79 biowaiver request. A drug substance is considered highly soluble when the highest strength is
80 soluble in 250 mL or less of aqueous media over the pH range of 1-6.8. The volume estimate of 250
81 mL is derived from typical BE study protocols that prescribe administration of a drug product to
82 fasting human volunteers with a glass (about 8 ounces) of water.
83
84 B. Permeability
85
86 The permeability class boundary is based indirectly on the extent of absorption (fraction of dose
87 absorbed, not systemic BA) of a drug substance in humans, and directly on measurements of the rate
88 of mass transfer across human intestinal membrane. Alternatively, other systems capable of
89 predicting the extent of drug absorption in humans can be used (e.g., in situ animal, in vitro epithelial
90 cell culture methods). A drug substance is considered to be highly permeable when the extent of
91 absorption in humans is determined to be 85 percent or more of an administered dose based on a
92 mass balance determination (along with evidence showing stability of the drug in the GI tract) or in
93 comparison to an intravenous reference dose.
94
95 C. Dissolution
96
97 An IR drug product is considered rapidly dissolving when 85 percent or more of the labeled amount
98 of the drug substance dissolves within 30 minutes, using United States Pharmacopeia (USP)
99 Apparatus I at 100 rpm (or Apparatus II at 50 rpm or at 75 rpm when appropriately justified (see
100 section III.C.)) in a volume of 500 mL or less in each of the following media: (1) 0.1 N HCl or
101 Simulated Gastric Fluid USP without enzymes; (2) a pH 4.5 buffer; and (3) a pH 6.8 buffer or
102 Simulated Intestinal Fluid USP without enzymes.
103
104 An IR product is considered very rapidly dissolving when 85 percent or more of the labeled amount
105 of the drug substance dissolves within 15 minutes using the above mentioned conditions.
106
107
108 III. RECOMMENDED METHODOLOGY FOR CLASSIFYING A DRUG
109 SUBSTANCE AND FOR DETERMINING THE DISSOLUTION
110 CHARACTERISTICS OF A DRUG PRODUCT
111
112 The following approaches are recommended for classifying a drug substance and determining the
113 dissolution characteristics of an IR drug product according to the BCS.
114
115 A. Determining Drug Substance Solubility Class
116
117 An objective of the BCS approach is to determine the equilibrium solubility of a drug substance
118 under physiological pH conditions. The pH-solubility profile of the test drug substance should be
119 determined at 37 ± 1oC in aqueous media with a pH in the range of 1-6.8. A sufficient number of pH
120 conditions should be evaluated to accurately define the pH-solubility profile within the pH range of
121 1-6.8. The number of pH conditions for a solubility determination can be based on the ionization
122 characteristics of the test drug substance to include pH = pKa, pH = pKa +1, pH = pKa-1, and at pH
123 = 1 and 6.8. A minimum of three replicate determinations of solubility in each pH condition is

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124 recommended. Depending on study variability, additional replication may be necessary to provide a
125 reliable estimate of solubility. Standard buffer solutions described in the USP are considered
126 appropriate for use in solubility studies. If these buffers are not suitable for physical or chemical
127 reasons, other buffer solutions can be used. Solution pH should be verified after addition of the drug
128 substance to a buffer. Methods other than the traditional shake-flask method, such as acid or base
129 titration methods, can also be used with justification to support the ability of such methods to predict
130 equilibrium solubility of the test drug substance. Concentration of the drug substance in selected
131 buffers (or pH conditions) should be determined using a validated stability-indicating assay that can
132 distinguish the drug substance from its degradation products. 7 If degradation of the drug substance
133 is observed as a function of buffer composition and/or pH, it should be reported. The solubility class
134 should be determined by calculating the volume of an aqueous medium sufficient to dissolve the
135 highest strength in the pH range of 1-6.8. A drug substance should be classified as highly soluble
136 when the highest strength is soluble in < 250 mL of aqueous media over the pH range of 1-6.8. In
137 other words, the maximum dose divided by 250 should be greater than or equal to the lowest
138 solubility observed over the entire pH range of 1-6.8.
139
140 B. Determining Drug Substance Permeability Class
141
142 The permeability class of a drug substance can be determined in human subjects using mass balance,
143 or absolute BA, which are the preferred methods, or intestinal perfusion approaches. Recommended
144 methods not involving human subjects include in vivo or in situ intestinal perfusion in a suitable
145 animal model (e.g., rats), or in vitro permeability methods using excised intestinal tissues, or
146 monolayers of suitable epithelial cells. In many cases, a single method may be sufficient: (i) when
147 the absolute BA is 85 percent or more, or (ii) when 85 percent or more of the administered drug is
148 excreted unchanged in urine, or (iii) when 85 percent or more of the administered drug is recovered
149 in urine as parent and metabolites with evidence indicating stability in the GI tract. When a single
150 method fails to conclusively demonstrate a permeability classification, two different methods may be
151 advisable. In case of conflicting information from different types of studies, it is important to note
152 that human data supersede in vitro or animal data.
153
154 1. Pharmacokinetic Studies in Humans
155
156 • Mass Balance Studies
157
158 Pharmacokinetic (PK) mass balance studies using unlabeled, stable isotopes or a
159 radiolabeled drug substance can be used to document the extent of absorption of a
160 drug. A sufficient number of subjects should be enrolled to provide a reliable
161 estimate of extent of absorption.
162
163 When mass balance studies are used to demonstrate high permeability, additional data
164 to document the drug’s stability in the GI tract is required, unless 85 percent or more
165 of the drug is excreted unchanged in urine. Please see method details in section
166 III.B.3.
167
7
Refer to the FDA guidance for industry on Submitting Documentation for the Stability of Human Drugs and
Biologics (February 1987), posted at http://www.fda.gov/downloads/Drugs/Guidances/UCM070632.pdf.

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168 • Absolute Bioavailability Studies

169
170 Oral BA determination using intravenous administration as a reference can be used.
171 Depending on the variability of the studies, a sufficient number of subjects should be
172 enrolled in a study to provide a reliable estimate of the extent of absorption. When
173 the absolute BA of a drug is shown to be 85 percent or more, additional data to
174 document drug stability in the GI fluid is not necessary.
175
176 2. Intestinal Permeability Methods
177
178 The following methods can be used to determine the permeability of a drug substance from
179 the GI tract: (1) in vivo intestinal perfusion studies in humans; (2) in vivo or in situ intestinal
180 perfusion studies using suitable animal models; (3) in vitro permeation studies using excised
181 human or animal intestinal tissues; or (4) in vitro permeation studies across a monolayer of
182 cultured epithelial cells.
183
184 In vivo or in situ animal models and in vitro methods, such as those using cultured
185 monolayers of animal or human epithelial cells, are considered appropriate for passively
186 transported drugs. The observed low permeability of some drug substances in humans could
187 be caused by efflux of drugs via membrane efflux transporters such as P-glycoprotein (P-gp).
188 When the efflux transporters are absent in these models, or their degree of expression is low
189 compared to that in humans, there may be a greater likelihood of misclassification of
190 permeability class for a drug subject to efflux compared to a drug transported passively.
191 Expression of known transporters in selected study systems should be characterized.
192 Functional expression of efflux systems (e.g., P-gp) can be demonstrated with techniques
193 such as bidirectional transport studies, demonstrating a higher rate of transport in the
194 basolateral-to-apical direction as compared to apical-to-basolateral direction (efflux ratio
195 >2) 8,9, using selected model drugs or chemicals at concentrations that do not saturate the
196 efflux system (e.g., digoxin, vinblastine, rhodamine 123). We recommend limiting the use of
197 animal or in vitro permeability test methods for drug substances that are transported by
198 passive mechanisms (efflux ratio of the test drug should be <2). PK studies on dose linearity
199 or proportionality may provide useful information for evaluating the relevance of observed in
200 vitro efflux of a drug. For example, there may be fewer concerns associated with the use of
201 in vitro methods for a drug that has a higher rate of transport in the basolateral-to-apical
202 direction at low drug concentrations but exhibits linear PK in humans.
203
204 For BCS-based permeability determination, an apparent passive transport mechanism can be
205 assumed when one of the following conditions is satisfied:
206
207 • A linear (pharmacokinetic) relationship between the dose (e.g., relevant clinical
208 dose range) and measures of BA (area under the concentration-time curve) of a
209 drug is demonstrated in humans.
210
8
KM Giacomini, SM Huang, DJ Tweedie, LZ Benet, KLR Brouwer, X Chu, A Dahlin, R Evers, V Fischer, et al.
March 2010, The International Transporter Consortium, Membrane transporters in drug development, Nature
Reviews Drug Discovery, 9:215-236.
9
See the FDA draft guidance for industry on Drug Interaction Studies--Study Design, Data Analysis, Implications
for Dosing, and Labeling Recommendations, (Feb 2012).

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211 • Lack of dependence of the measured in vivo or in situ permeability is
212 demonstrated in an animal model on initial drug concentration (e.g., 0.01, 0.1,
213 and 1 times the highest strength dissolved in 250 mL) in the perfusion fluid.
214
215 • Lack of dependence of the measured in vitro permeability on initial drug
216 concentration (e.g., 0.01, 0.1, and 1 times the highest strength dissolved in 250
217 ml) is demonstrated, or on transport direction (e.g., no statistically significant
218 difference in the rate of transport between the apical-to-basolateral and
219 basolateral-to-apical direction for the drug concentrations selected) using a
220 suitable in vitro cell culture method that has been shown to express known efflux
221 transporters (e.g., P-gp).
222
223 METHOD SUITABILITY: One of the critical steps in using in vitro permeability
224 methods for permeability classification is to demonstrate the suitability of the
225 method. To demonstrate suitability of a permeability method intended for BCS-
226 based permeability determination, a rank-order relationship between experimental
227 permeability values and the extent of drug absorption data in human subjects should
228 be established using a sufficient number of model drugs. For in vivo intestinal
229 perfusion studies in humans, six model drugs are recommended. For in vivo or in
230 situ intestinal perfusion studies in animals, and for in vitro cell culture methods,
231 twenty model drugs are recommended. Depending on study variability, a sufficient
232 number of subjects, animals, excised tissue samples, or cell monolayers should be
233 used in a study to provide a reliable estimate of drug permeability. This relationship
234 should allow precise differentiation between drug substances of low and high
235 intestinal permeability attributes.
236
237 To demonstrate the suitability of a method, model drugs should represent a range of
238 zero, low (e.g., < 50 percent), moderate (e.g., 50 – 84 percent), and high (≥ 85
239 percent) absorption. Sponsors/applicants may select compounds from the list of
240 drugs and/or chemicals provided in Attachment A, or they may select other drugs for
241 which there is information available on mechanism of absorption and reliable
242 estimates of the extent of drug absorption in humans.
243
244 After demonstrating suitability of a method and maintaining the same study protocol,
245 it is not necessary to retest all selected model drugs for subsequent studies intended to
246 classify a drug substance. Instead, a low and a high permeability model drug should
247 be used as internal standards (i.e., included in the perfusion fluid or donor fluid along
248 with the test drug substance). These two internal standards are in addition to the fluid
249 volume marker (or a zero permeability compound such as PEG 4000) that is included
250 in certain types of perfusion techniques (e.g., closed loop techniques). The choice of
251 internal standards should be based on compatibility with the test drug substance (i.e.,
252 they should not exhibit any significant physical, chemical, or permeation
253 interactions). When it is not feasible to follow this protocol, the permeability of
254 internal standards should be determined in the same subjects, animals, tissues, or
255 monolayers, following evaluation of the test drug substance. The permeability values
256 of the two internal standards should not differ significantly between different tests,
257 including those conducted to demonstrate suitability of the method. For example, the
258 laboratory may set acceptance criteria for the permeability values of its high, low, and

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259 zero permeability standard compounds. At the end of an in situ or in vitro test, the
260 amount of drug in the membrane should be determined to assist in calculation of
261 mass balance.
262
263 For a given test method with set conditions, selection of a high permeability internal
264 standard with permeability in close proximity to the low/high permeability class
265 boundary may be used to facilitate classification of a test drug substance. For
266 instance, a test drug substance may be determined to be highly permeable when its
267 permeability value is equal to or greater than that of the selected internal standard
268 with high permeability.
269
270 When intestinal permeability methods are used to demonstrate high permeability,
271 additional data to document the drug’s stability in the GI tract is required. Please see
272 method details in section III.B.3.
273
274 3. Instability in the Gastrointestinal Tract
275
276 Determining the extent of absorption in humans based on mass balance studies using total
277 radioactivity in urine does not take into consideration the extent of degradation of a drug in
278 the GI fluid prior to intestinal membrane permeation. In addition, some methods for
279 determining permeability could be based on loss or clearance of a drug from fluids perfused
280 into the human and/or animal GI tract either in vivo or in situ. Documenting the fact that
281 drug loss from the GI tract arises from intestinal membrane permeation, rather than a
282 degradation process, will help establish permeability. Stability in the GI tract may be
283 documented using simulated gastric and intestinal fluids. Obtaining GI fluids from human
284 subjects requires intubation and may be difficult. Therefore, use of simulated fluids such as
285 Gastric and Intestinal Fluids USP may be reasonable.
286
287 Drug solutions in these fluids should be incubated at 37oC for a period that is representative
288 of in vivo drug contact with these fluids; for example, 1 hour in gastric fluid and 3 hours in
289 intestinal fluid. Drug concentrations should then be determined using a validated stability-
290 indicating assay method. Significant degradation (>5 percent) of a drug in this study could
291 suggest potential instability.
292
293 C. Determining Drug Product Dissolution Characteristics and Dissolution Profile
294 Similarity 10
295
296 Dissolution testing should be carried out in USP Apparatus I at 100 rpm or Apparatus II at 50
297 rpm (or at 75 rpm when appropriately justified) using 500 mL of the following dissolution
298 media: (1) 0.1 N HCl or Simulated Gastric Fluid USP without enzymes; (2) a pH 4.5 buffer;
299 and (3) a pH 6.8 buffer or Simulated Intestinal Fluid USP without enzymes. For capsules and
300 tablets with gelatin coating, Simulated Gastric and Intestinal Fluids USP (with enzymes) can
301 be used.
302
10
See the FDA guidance for industry on Dissolution Testing of Immediate Release Solid Oral Dosage Forms
(August 1997).

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303 The dissolution testing apparatus used in this evaluation should conform to the requirements
304 in USP (<711> Dissolution). Selection of the dissolution testing apparatus (USP Apparatus I
305 or II) during drug development should be based on a comparison of in vitro dissolution and in
306 vivo PK data available for the product. The USP Apparatus I (basket method) is generally
307 preferred for capsules and products that tend to float, and USP Apparatus II (paddle method)
308 is generally preferred for tablets. For some tablet dosage forms, in vitro (but not in vivo)
309 dissolution may be slow due to the manner in which the disintegrated product settles at the
310 bottom of a dissolution vessel. In such situations, USP Apparatus I may be preferred over
311 Apparatus II. If the testing conditions need to be modified to better reflect rapid in vivo
312 dissolution (e.g., use of a different rotating speed), such modifications can be justified by
313 comparing in vitro dissolution with in vivo absorption data (e.g., a relative BA study using a
314 simple aqueous solution as the reference product).
315
316 A minimum of 12 dosage units of a drug product should be evaluated to support a biowaiver
317 request. Samples should be collected at a sufficient number of intervals to characterize the
318 dissolution profile of the drug product (e.g., 5, 10, 15, 20, and 30 minutes).
319
320 When comparing the test and reference products, dissolution profiles should be compared
321 using a similarity factor (f2).
322
n 2 -0.5
323 f2 = 50 • log {[1 + (1/n)Σt=1 (Rt - Tt) ] • 100}
324
325 The similarity factor is a logarithmic reciprocal square root transformation of the sum of
326 squared error and is a measurement of the similarity in the percent (%) of dissolution
327 between the two curves; where n is the number of time points, Rt is the dissolution value of
328 the reference batch at time t, and Tt is the dissolution value of the test batch at time t.
329
330 Two dissolution profiles are considered similar when the f2 value is ≥50. To allow the use of
331 mean data, the coefficient of variation should not be more than 20 percent at the earlier time
332 points (e.g., 10 minutes), and should not be more than 10 percent at other time points. Note
333 that when both test and reference products dissolve 85 percent or more of the label amount of
334 the drug in 15 minutes using all three dissolution media recommended above, the profile
335 comparison with an f2 test is unnecessary.
336
337
338 IV. BIOWAIVERS BASED ON BCS
339
340 This guidance is applicable for BA/BE waivers (biowaivers) based on BCS, for BCS class 1 and
341 class 3 immediate-release solid oral dosage forms.
342
343 For BCS class 1 drug products, the following should be demonstrated:
344
345 • the drug substance is highly soluble
346 • the drug substance is highly permeable
347 • the drug product (test and reference) is rapidly dissolving, and

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348 • the product does not contain any excipients that will affect the rate or extent of absorption of
349 the drug (see section V.A.)
350
351 For BCS class 3 drug products, the following should be demonstrated:
352
353 • the drug substance is highly soluble
354 • the drug product (test and reference) is very rapidly dissolving (see section II.C.), and
355 • the test product formulation is qualitatively the same and quantitatively very similar, e.g.,
356 falls within scale-up and post-approval changes (SUPAC) IR level 1 and 2 changes, in
357 composition to the reference (see section V.A.)
358
359
360 V. ADDITIONAL CONSIDERATIONS FOR REQUESTING A BIOWAIVER
361
362 When requesting a BCS-based biowaiver for in vivo BA/BE studies for IR solid oral dosage forms,
363 sponsors/applicants should note that the following factors can affect their request or the
364 documentation of their request.
365
366 A. Excipients
367
368 (i) BCS class 1 drug products: Excipients can sometimes affect the rate and extent of
369 drug absorption. In general, using excipients that are currently in FDA-approved IR
370 solid oral dosage forms will not affect the rate or extent of absorption of a highly
371 soluble and highly permeable drug substance that is formulated in a rapidly
372 dissolving IR product. To support a biowaiver request, the quantity of excipients in
373 the IR drug product should be consistent with the intended function (e.g., lubricant).
374 When new excipients or atypically large amounts of commonly used excipients are
375 included in an IR solid dosage form, additional information documenting the absence
376 of an impact on BA of the drug may be requested by the Agency. Such information
377 can be provided with a relative BA study using a simple aqueous solution as the
378 reference product. Large quantities of certain excipients, such as surfactants (e.g.,
379 polysorbate 80) and sweeteners (e.g., mannitol or sorbitol) may be problematic, and
380 sponsors are encouraged to contact the review division when this is a factor.
381
382 (ii) BCS class 3 drug products: Unlike for BCS class 1 products, for a biowaiver to
383 be scientifically justified, BCS class 3 test drug product must contain the same
384 excipients as the reference product. This is due to the concern that excipients can
385 have a greater impact on absorption of low permeability drugs. The composition of
386 the test product must be qualitatively the same and should be quantitatively very
387 similar to the reference product.
388
389 B. Prodrugs
390
391 Permeability of prodrugs will generally depend on the mechanism and (anatomical) site of
392 conversion to the drug substance. When the prodrug-to-drug conversion is shown to occur
393 predominantly after intestinal membrane permeation, the permeability of the prodrug should
394 be measured. When this conversion occurs prior to intestinal permeation, the permeability of
395 the drug should be determined. Dissolution and pH-solubility data on both prodrug and drug

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396 can be relevant. Sponsors may wish to consult with appropriate review staff before applying
397 the BCS approach to IR products containing prodrugs.
398
399 C. Fixed Dose Combinations
400
401 a. If all active components belong to BCS class 1: BCS-based biowaivers are
402 applicable for IR fixed dose combination products if all the drugs in the combination
403 belong to BCS class 1; provided there is no PK interaction between the components,
404 and the excipients fulfill the considerations outlined in section V.A. (i). If there is a
405 PK interaction, the excipients should fulfill the considerations outlined in section
406 V.A. (ii). Otherwise, in vivo bioequivalence testing is required.
407
408 b. If all components of the combination belong to BCS class 3 or a combination of
409 class 1 and 3: BCS-based biowaivers are applicable for IR fixed dose combination
410 products in this situation provided the excipients fulfill the considerations outlined in
411 section V.A. (ii). Otherwise, in vivo bioequivalence testing is required.
412
413 D. Exceptions
414
415 BCS-based biowaivers are not applicable for the following:
416
417 1. Narrow Therapeutic Range Drugs 11
418
419 This guidance defines narrow therapeutic range drug products as those containing
420 certain drug substances that are subject to therapeutic drug concentration or
421 pharmacodynamic (PD) monitoring, and/or where product labeling indicates a narrow
422 therapeutic range designation. Examples include digoxin, lithium, phenytoin,
423 theophylline, and warfarin. Because not all drugs subject to therapeutic drug
424 concentration or PD monitoring are narrow therapeutic range drugs, sponsors should
425 contact the appropriate review division to determine whether a drug should be
426 considered to have a narrow therapeutic range.
427
428 2. Products Designed to be Absorbed in the Oral Cavity
429
430 A request for a waiver of in vivo BA/BE studies based on the BCS is not appropriate
431 for dosage forms intended for absorption in the oral cavity (e.g., sublingual or buccal
432 tablets). Similarly, a biowaiver for an orally disintegrating tablet can be considered,
433 based on BCS, only if the absorption from the oral cavity is ruled out.
434
435
11
This guidance uses the term narrow therapeutic range instead of narrow therapeutic index, although the latter is
more commonly used.

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436 VI. REGULATORY APPLICATIONS OF THE BCS
437
438 A. INDs/NDAs
439
440 Evidence demonstrating in vivo BA or information to permit FDA to waive this evidence must be
441 included in NDAs (21 CFR 320.21(a)). A specific objective of such BA information is to establish in
442 vivo performance of the dosage form used in the clinical studies that provided primary evidence of
443 efficacy and safety. The sponsors may wish to determine the relative BA of an IR solid oral dosage
444 form by comparison with an oral solution, suspension, or intravenous injection (21 CFR 320.25
445 (d)(2) and 320.25 (d)(3)). The BA of the clinical trial dosage form should be optimized during the
446 IND period.
447
448 Once the in vivo BA of a formulation is established during the IND period, waivers of subsequent in
449 vivo BE studies, following major changes in components, composition, and/or method of
450 manufacture (e.g., similar to SUPAC-IR Level 3 changes 12) may be possible using the BCS. BCS-
451 based biowaivers are applicable to the to-be-marketed formulation when changes in components,
452 composition, and/or method of manufacture occur to the clinical trial formulation, as long as the
453 dosage forms have rapid, very rapid and similar in vitro dissolution profiles (see sections II and III).
454 This approach is useful only when the drug substance belongs to BCS class 1 or 3, and the
455 formulations pre- and post-change are pharmaceutical equivalents (under the definition at 21 CFR
456 320.1 (c)). BCS-based biowaivers are intended only for BE studies. They do not apply to food effect
457 BA studies or other PK studies. BCS-based biowaivers may be applicable for pharmaceutical
458 alternatives, if appropriately justified. The sponsor should contact the appropriate review division in
459 such situations.
460
461 B. ANDAs
462
463 BCS-based biowaivers are appropriate for IR test products that meet the criteria for BCS class 1 or 3
464 as discussed above, provided that the reference listed drug product also meets those criteria and the
465 test product exhibits similar dissolution profiles to the reference listed drug product (see sections II
466 and III). This approach is useful when the test and reference dosage forms are pharmaceutical
467 equivalents. The choice of dissolution apparatus (USP Apparatus I or II) should be the same as that
468 established for the reference listed drug product.
469
470 C. Supplemental NDAs/ANDAs (Postapproval Changes)
471
472 BCS-based biowaivers are appropriate for significant postapproval changes (e.g., Level 3 changes in
473 components and composition) to an IR test product that meets the criteria for BCS class 1 or 3 as
474 discussed above, and both pre- and post-change products exhibit similar dissolution profiles (see
475 sections II and III). This approach is useful only when the drug products pre- and post-change are
476 pharmaceutical equivalents.
477
478
12
See the FDA guidance for industry on Immediate Release Solid Oral Dosage Forms: Scale-Up and Post-Approval
Changes (November 1995).

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479 VII. DATA TO SUPPORT A BIOWAIVER REQUEST
480
481 The drug product for which a biowaiver is being requested should include a drug substance that is
482 highly soluble (BCS class 1 and BCS class 3) and highly permeable (BCS class 1), and the drug
483 product should be rapidly dissolving (BCS class 1) or very rapidly dissolving (BCS class 3).
484 Sponsors/applicants requesting biowaivers based on the BCS should submit the following
485 information to the Agency for review.
486
487 A. Data Supporting High Solubility
488
489 Data supporting high solubility of the test drug substance should be developed (see section III.A).
490 The following information should be included in the application:
491
492 • A description of test methods, including information on analytical method(s) and
493 composition of the buffer solutions.
494
495 • Information on chemical structure, molecular weight, nature of the drug substance (acid,
496 base, amphoteric, or neutral), and dissociation constants (pKa(s)).
497
498 • Test results (mean, standard deviation, and coefficient of variation) summarized in a table
499 under solution pH, drug solubility (e.g., mg/mL), and volume of media required to
500 dissolve the highest strength.
501
502 • A graphic representation of mean pH-solubility profile.
503
504 B. Data Supporting High Permeability
505
506 Data supporting high permeability of the test drug substance should be developed (see section III.B).
507 The following information should be included in the application:
508
511
512 • For human PK studies, information on study design and methods used along with the PK
513 data.
514
515 • For direct permeability methods, information supporting the suitability of a selected
516 method that encompasses a description of the study method, criteria for selection of
517 human subjects, animals, or epithelial cell line, drug concentrations in the donor fluid,
518 description of the analytical method, method used to calculate extent of absorption or
519 permeability, and where appropriate, information on efflux potential (e.g., bidirectional
520 transport data).
521
522 • A list of selected model drugs along with data on extent of absorption in humans (mean,
523 standard deviation, coefficient of variation) used to establish suitability of a method,
524 permeability values for each model drug (mean, standard deviation, coefficient of
525 variation), permeability class of each model drug, and a plot of the extent of absorption as

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526 a function of permeability (mean ± standard deviation or 95 percent confidence interval)
527 with identification of the low/high permeability class boundary and selected internal
528 standard. Information to support high permeability of a test drug substance (mean,
529 standard deviation, coefficient of variation) should include permeability data on the test
530 drug substance, the internal standards, GI stability information, data supporting passive
531 transport mechanism where appropriate, and methods used to establish high permeability
532 of the test drug substance.
533
534 C. Data Supporting Rapid, Very Rapid, and Similar Dissolution
535
536 For submission of a biowaiver request, an IR product should be rapidly dissolving (BCS class 1) or
537 very rapidly dissolving (BCS class 3). Data supporting rapid dissolution attributes of the test and
538 reference products should be developed (see section III.C). The following information should be
539 included in the application:
540
543
544 • A brief description of the IR products used for dissolution testing, including information
545 on batch or lot number, expiry date, dimensions, strength, and weight.
546
547 • Dissolution data obtained with 12 individual units of the test and reference products using
548 recommended test methods in section III.C. The percentage of labeled claim dissolved at
549 each specified testing interval should be reported for each individual dosage unit. The
550 mean percent dissolved, range (highest and lowest) of dissolution, and coefficient of
551 variation (relative standard deviation), should be tabulated. A graphic representation of
552 the mean dissolution profiles for the test and reference products in the three media should
553 also be included.
554
555 • Data supporting similarity in dissolution profiles between the test and reference products
556 in each of the three media (see section IIIC).
557
558 D. Additional Information
559
560 The manufacturing process used to make the test product should be described briefly to provide
561 information on the method of manufacture (e.g., wet granulation versus direct compression).
562
563 A list of excipients used, the amount used, and their intended functions should be provided.
564 Excipients used in the test product should have been used previously in FDA-approved IR solid oral
565 dosage forms. In addition, it is important to provide quantitative comparison of excipients between
566 the test and reference product, for BCS class 3 drug products.
567
568

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569 ATTACHMENT A
570
571 This attachment includes model drugs suggested for use in establishing suitability of a permeability
572 method as described in section III. Zero permeability markers and efflux substrates are also
573 identified.
574
Group Drug
High Permeability Antipyrine
(fa ≥ 85 percent) Caffeine
Ketoprofen
Naproxen
Theophylline
Metoprolol
Propranolol
Carbamazepine
Phenytoin
Disopyramide
Minoxidil
Moderate Permeability Chlorpheniramine
(fa = 50-84 percent) Creatinine
Terbutaline
Hydrochlorothiazide
Enalapril
Furosemide
Metformin
Amiloride
Atenolol
Ranitidine
Low Permeability Famotidine
(fa < 50 percent) Nadolol
Sulpiride
Lisinopril
Acyclovir
Foscarnet
Mannitol
Chlorothiazide
Polyethylene glycol 400
Enalaprilat
Zero Permeability FITC-Dextran
Polyethylene glycol 4000
Lucifer yellow
Inulin
Lactulose
Efflux Substrates Digoxin
Paclitaxel
Quinidine
Vinblastine
575

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Waiver of in Vivo Bioavailability

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1 Waiver of In Vivo Bioavailability and Bioequivalence Studies for

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168 • Absolute Bioavailability Studies

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