PhRMA Perspective on Population and Individual Bioequivalence

Barrett, Jeffrey S.; Batra, Vishal; Chow, Andrew; Cook, Jack; Gould, A. Lawrence; Heller, Allen H.; Lo, Mimi; Patterson, Scott D.; Smith, Brian P.; Stritar, Jeffrey A.; Vega, José M.; Zariffa, Névine

doi:10.1002/j.1552-4604.2000.tb05980.x

Cited by 30 publications

(17 citation statements)

References 21 publications

(4 reference statements)

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“…It is then accepted that, when used as alternatives, the products ⁄ routes can be expected to provide sufficiently similar efficacy and safety to guarantee therapeutic equivalence. The differences between and procedures required to establish average, individual and population bioequivalences are not considered here (see reviews by Barrett et al, 2000 andGould, 2000), as all regulatory authorities require that data satisfy only the criteria for average bioequivalence. Also not reviewed are the arguments for and against the use of chiral ⁄ nonchiral methods for drug residue studies in food-producing species, except to note that residue depletion profiles depend on rate of depletion in the terminal elimination phase.…”

Section: Decision Trees On Choice Of Analytical Methodsmentioning

confidence: 99%

Pharmacokinetics and pharmacodynamics of stereoisomeric drugs with particular reference to bioequivalence determination

Lees

Hunter

Reeves

et al. 2012

Vet Pharm & Therapeutics

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Drugs containing one or more chiral centres exist in stereoisomeric molecular forms. Most commonly, drugs containing a single asymmetric carbon atom exist in two enantiomeric forms, designated as eutomer (the more potent) and distomer (the less potent). As well as differences in potency and other pharmacodynamic properties, most members of enantiomeric pairs commonly differ also in their pharmacokinetic profiles. This article reviews factors underlying differences in pharmacological properties of enantiomers. The relevance of such differences for studies designed to evaluate the bioequivalence of products containing chiral drugs is also reviewed.

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Section: Decision Trees On Choice Of Analytical Methodsmentioning

confidence: 99%

Pharmacokinetics and pharmacodynamics of stereoisomeric drugs with particular reference to bioequivalence determination

Lees

Hunter

Reeves

et al. 2012

Vet Pharm & Therapeutics

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“…It has been noted that while there is little evidence to suggest that the ABE criterion has failed, consumers may find these specific questions above related to PBE and IBE more relevant. [8][9][10] There is some level of intuitive appeal for both PBE and IBE, although it is expected that the IBE criterion will be more relevant to consumers as they "switch" to generic formulations of chronically administered medications. The key motivation behind the proposed change lies in answering more appropriate questions regarding bioequivalence.…”

confidence: 99%

Population and Individual Bioequivalence: Lessons from Real Data and Simulation Studies

Zariffa

Patterson

2001

The Journal of Clinical Pharma

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The Food and Drug Administration (FDA) has proposed replacing the 1992 average bioequivalence (ABE) with population and individual bioequivalence (PBE & IBE), as outlined in the preliminary draft guidance of December 1997, which was subsequently replaced by the draft guidances of August 1999 and resolved in the final guidance of October 2000. This has led to considerable public debate among regulatory, academic, and industry experts at numerous conferences (e.g., FDA/AAPS March 1998, FDA/AAPS August-September 1999, FDA Pharmaceutical Sciences Advisory Committee September 1999) and in the literature. The final guidance calls for ABE to remain as the primary criterion by which new formulations may be judged ready for access to the marketplace. In addition, the FDA recommends the use of replicate study designs for the specific drug classes of controlled-release formulations and highly variable drugs. The final guidance also alludes to the possibility of a sponsor requesting alternative criteria such as PBE and IBE following consultation with the FDA. This procedure amounts to a data collection period during which data suitable to evaluate the operating characteristics of PBE and IBE would be generated, analyzed, and discussed among interested parties. A comprehensive review of currently available databases is useful in determining the ultimate value of this data collection period. This report provides an update to the previous publication by the authors. In all, 28 data sets from 20 replicate cross-over bioequivalence studies have been analyzed (n = 12-96) using the statistical methodology in the most recent FDA draft guidance. The results are presented below. ABE Pass: ABE Fail: Total: AUC/Cmax AUC/Cmax AUC/Cmax AUC/Cmax Pass PBE & IBE 20/14 1/3 21/17 Pass IBE only 1/0 0/0 1/0 Fail PBE and IBE 0/2 0/1 0/3 Fail IBE only 2/3 4/5 6/8 Total 23/19 5/9 28/28 Review of the database reveals many interesting features, most notably the lack of consistent results within a given data set across all three criteria. The sensitivity of subject-by-formulation interaction to sample size and inherent variability of the compounds is further explored through simulation studies. It is concluded that additional simulation assessments must be considered when evaluating the value of a data collection period for PBE and IBE assessment. It will be shown that definitive conclusions regarding some of the operating characteristics of PBE and IBE can be achieved through a combination of data-driven hypotheses followed by simulation studies to further evaluate the hypotheses. Some recommendations for further data collection will be made.

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“…The use of bioequivalence trials is recommended to evaluate the interchangeability of two or more formulations. A brief summary of these trials (after 1970) is presented by Barrett et al [1].…”

Section: Introductionmentioning

confidence: 99%

The use of asymmetric distributions in average bioequivalence

Souza

Achcar

Martinez

et al. 2016

Statistics in Medicine

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Generic drugs have been commercialized in numerous countries. Most of these countries approve the commercialization of a generic drug when there is evidence of bioequivalence between the generic drug and the reference drug. Generally, the pharmaceutical industry is responsible for the bioequivalence test under the supervision of a regulatory agency. This procedure is concluded after a statistical data analysis. Several agencies adopt a standard statistical analysis based on procedures that were previously established. In practice, we face situations in which this standard model does not fit to some sets of bioequivalence data. In this study, we propose an evaluation of bioequivalence using univariate and bivariate models based on an extended generalized gamma distribution and a skew-t distribution, under a Bayesian perspective. We introduce a study of the empirical power of hypothesis tests for univariate models, showing advantages in the use of an extended generalized gamma distribution. Three sets of bioequivalence data were analyzed under these new procedures and compared with the standard model proposed by the majority of regulatory agencies. In order to verify that the asymmetrical distributions are usually better fitted for the data, when compared with the standard model, model discrimination methods were used, such as the Deviance Information Criterion (DIC) and quantile-quantile plots. The research concluded that, in general, the use of the extended generalized gamma distribution may be more appropriate to model bioequivalence data in the original scale. Copyright © 2016 John Wiley & Sons, Ltd.

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PhRMA Perspective on Population and Individual Bioequivalence

Cited by 30 publications

References 21 publications

Pharmacokinetics and pharmacodynamics of stereoisomeric drugs with particular reference to bioequivalence determination

Pharmacokinetics and pharmacodynamics of stereoisomeric drugs with particular reference to bioequivalence determination

Population and Individual Bioequivalence: Lessons from Real Data and Simulation Studies

The use of asymmetric distributions in average bioequivalence

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