Alternative Pharmacokinetic Metrics in Single-Dose Studies to Ensure Bioequivalence of Prolonged-Release Products at Steady State—A Case Study

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Alternative Pharmacokinetic Metrics in Single-Dose Studies to Ensure Bioequivalence of Prolonged-Release Products at Steady State—A Case Study

Publicated to:Pharmaceutics. 15 (2): - 2023-02-01 15(2), DOI: 10.3390/pharmaceutics15020409

Authors: Mangas-Sanjuán, V; Simón, M; González-Rojano, E; Ochoa, D; Abad-Santos, F; Román, M; Ramos, M; Govantes, C; Garcfa-Arieta, A

Affiliations

Agencia Espanola Medicamentos & Prod Sanitarios, Dept Medicamentos Uso Humano, Div Farmacol & Evaluac Clin, Madrid 28022, Spain - Author

División de Farmacología y Evaluación Clínica - Author

Hosp Univ Clin San Carlos, Inst Invest Sanitaria Hosp Clin San Carlos IdISSC, Clin Pharmacol Dept, Madrid 28040, Spain - Author

Hosp Univ La Princesa, Inst Teofilo Hernando, Inst Invest Sanitaria Princesa IIS IP, Clin Pharmacol Dept, Madrid 28006, Spain - Author

Hospital Clínico San Carlos - Author

Instituto de Investigación Sanitaria Hospital Universitario de La Princesa - Author

Instituto de Investigación Sanitaria Hospital Universitario de La Princesa , Facultad de Medicina de la Universidad Autónoma de Madrid - Author

Laboratorios Normon - Author

Labs Normon, Madrid 28760, Spain - Author

Univ Autonoma Madrid, Fac Med, Pharmacol Dept, Madrid 28029, Spain - Author

Univ Valencia, Dept Pharm & Pharmaceut Technol & Parasitol, Valencia 46100, Spain - Author

Univ Valencia, Polytech Univ Valencia, Interuniv Res Inst Mol Recognit & Technol Dev, Valencia 46100, Spain - Author

Universitat Politècnica de València , Universitat de València - Author

Abstract

(1) Background: this article investigates which PK metrics in a single-dose study (concentration at the end of posology interval, Cτ, partial areas under the curve, pAUCs, or half-value duration, HVD) are more sensitive and less variable for predicting the failure of a prolonged-release product at steady-state that was the bioequivalent for Cmax, AUC0-t and AUC0-inf, in the single-dose study; (2) Methods: a cross-over study was performed in 36 subjects receiving desvenlafaxine 100 mg prolonged-release tablets. Conventional (Cmax, AUC0-t and AUC0-inf) and additional (Cτ, pAUCs and HVD) PK metrics were considered after single-dose conditions. Predicted PK metrics at steady state (AUC0-τ, Cmax,ss, and Cτ,ss) were derived using a population PK model approach; (3) Results: the existing differences in the shape of the concentration–time curves precluded to show equivalence for Cτ,ss in the simulated study at steady state. This failure to show equivalence at steady state was predicted by Cτ, pAUCs and HVD in the single-dose study. Cτ was the most sensitive metric for detecting the different shape, with a lower intra-subject variability than HVD; (4) Conclusions: conventional PK metrics for single-dose studies (Cmax, AUC0-t and AUC0-inf) are not enough to guarantee bioequivalence at steady state for prolonged-release products.

Keywords

absorptionanalytebcs drugsbioequivalencecomputer-simulationsmetabolismparameterpaucpredictionprolonged releasesingle dosesteady statetrials selectionvalidationBioequivalencePaucProlonged releaseSemi-physiological modelSingle doseSteady state

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The work has been published in the journal Pharmaceutics due to its progression and the good impact it has achieved in recent years, according to the agency WoS (JCR), it has become a reference in its field. In the year of publication of the work, 2023, it was in position 46/354, thus managing to position itself as a Q1 (Primer Cuartil), in the category Pharmacology & Pharmacy.

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