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Open Access 01-07-2019 | Mannitol | Current Opinion

Levothyrox^® New and Old Formulations: Are they Switchable for Millions of Patients?

Authors: Didier Concordet, Peggy Gandia, Jean-Louis Montastruc, Alain Bousquet-Mélou, Peter Lees, Aude Ferran, Pierre-Louis Toutain

Published in: Clinical Pharmacokinetics | Issue 7/2019

Abstract

In France, more than 2.5 million patients are currently treated with levothyroxine, mainly as the marketed product Levothyrox^®. In March 2017, at the request of French authorities, a new formulation of Levothyrox^® was licensed, with the objective of avoiding stability deficiencies of the old formulation. Before launching this new formulation, an average bioequivalence trial, based on European Union recommended guidelines, was performed. The implicit rationale was the assumption that the two products, being bioequivalent, would also be switchable, allowing substitution of the new for the old formulation, thus avoiding the need for individual calibration of the dosage regimen of thyroxine, using the thyroid-stimulating hormone level as the endpoint, as required for a new patient on initiating treatment. Despite the fact that both formulations were shown to be bioequivalent, adverse drug reactions were reported in several thousands of patients after taking the new formulation. In this opinion paper, we report that more than 50% of healthy volunteers enrolled in a successful regulatory average bioequivalence trial were actually outside the a priori bioequivalence range. Therefore, we question the ability of an average bioequivalence trial to guarantee the switchability within patients of the new and old levothyroxine formulations. We further propose an analysis of this problem using the conceptual framework of individual bioequivalence. This involves investigating the bioavailability of the two formulations within a subject, by comparing not only the population means (as established by average bioequivalence) but also by assessing two variance terms, namely the within-subject variance and the variance estimating subject-by-formulation interaction. A higher within individual variability for the new formulation would lead to reconsideration of the appropriateness of the new formulation. Alternatively, a possible subject-by-formulation interaction would allow a judgement on the ability, or not, of doctors to manage patients effectively during transition from the old to the new formulation.

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Title: Levothyrox® New and Old Formulations: Are they Switchable for Millions of Patients?
Authors: Didier Concordet
Peggy Gandia
Jean-Louis Montastruc
Alain Bousquet-Mélou
Peter Lees
Aude Ferran
Pierre-Louis Toutain
Publication date: 01-07-2019
Publisher: Springer International Publishing
Keywords: Mannitol
Levothyroxine
Published in: Clinical Pharmacokinetics / Issue 7/2019
Print ISSN: 0312-5963
Electronic ISSN: 1179-1926
DOI: https://doi.org/10.1007/s40262-019-00747-3

ACC 2024 Congress

Springer Medicine

Levothyrox^® New and Old Formulations: Are they Switchable for Millions of Patients?

Abstract

ACC 2024 Congress

Springer Medicine

Abstract

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Author’s Reply to Trechot: “Comment on Levothyrox® New and Old Formulations: Are they Switchable for Millions of Patients?”

Authors’ Reply to Nicolas: “Levothyrox® New and Old Formulations: Are they Switchable for Millions of Patients?”