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Bioequivalence for highly variable drugs: regulatory agreements, disagreements, and harmonization

Journal of Pharmacokinetics and Pharmacodynamics volume 46pages 117–126 (2019)Cite this article

Abstract

Regulatory authorities introduced procedures in the last decade for evaluating the bioequivalence (BE) for highly variable drugs. These approaches are similar in principle but differ in details. For example, the Food and Drug Administration (FDA) and the European Medicines Agency (EMA) recommend differing regulatory constants. The constant suggested by FDA results in discontinuity of the BE limits around the switching variation at 30% observed within-subject variation of the reference product. The regulatory constant of EMA does not have these problems. The Type I error reaches 6–7% around the switching variation with the EMA constant but 16–17% with the FDA constant. Various procedures were recently suggested, especially for the EMA approach, to eliminate the inflation of the Type I error. Notably, the so-called Exact algorithms try to amalgamate the positive features of both EMA and FDA procedures without their negative sides. The computational procedure for the EMA approach is simple and has a straightforward interpretation. The procedure for the FDA approach is based on an approximation, has a bias at small degrees of freedom, and requires a suitable computer program. All regulatory agencies impose a second requirement constraining the point estimate of the ratio of geometric means. In addition, EMA and Health Canada impose an upper limit for applying the recommended procedures. These expectations have psychological motivation and political rationale but no scientific foundations. Their inclusion results in incorrect and misleading interpretation of the principal criterion which involves confidence intervals. Different regulatory authorities expect to apply their approaches either to both AUC and Cmax or only to AUC or only to Cmax. Rational resolution of the disharmonization is needed.

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Acknowledgement

We appreciate the very careful and thoughtful review of the original manuscript by two referees.

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Affiliations

  1. Department of Pharmacology and Toxicology, University of Toronto, Toronto, ON, M5S 1A8, Canada

    Laszlo Endrenyi

  2. Semmelweis University, Budapest, Hungary

    Laszlo Tothfalusi

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  1. Laszlo Endrenyi
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  2. Laszlo Tothfalusi
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Correspondence to Laszlo Endrenyi.

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Endrenyi, L., Tothfalusi, L. Bioequivalence for highly variable drugs: regulatory agreements, disagreements, and harmonization. J Pharmacokinet Pharmacodyn 46, 117–126 (2019). https://doi.org/10.1007/s10928-019-09623-w

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  • DOI: https://doi.org/10.1007/s10928-019-09623-w

Keywords

  • Bioequivalence
  • Highly variable drugs
  • Reference-scaled average bioequivalence
  • Regulatory constants
  • Type I error