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Physiologically Based Pharmacokinetic Modeling Approach to Predict Drug-Drug Interactions With Ethionamide Involving Impact of Genetic Polymorphism on FMO3.

J Clin Pharmacol. 2019-01; 
NguyenPhuong Thi Thu, ParvezMd Masud, KimMin Jung, YooSung Eun, AhnSangzin, GhimJong-Lyul, ShinJae-
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Gene Synthesis … Material and Methods. Construction of Recombinant Baculoviruses of Wild‐Type and Mutant FMO3. Human FMO3 cDNA (wild‐type) cloned into pFastBac vector was purchased from GenScript Biotech Corp. (Piscataway, New … Get A Quote

摘要

The widely used second-line antituberculosis drug ethionamide shows wide interindividual variability in its disposition; however, the relevant factors affecting this phenomenon have not been characterized. We previously reported the major contribution of flavin-containing monooxygenase 3 (FMO3) in the reductive elimination pathway of ethionamide. In this study, ethionamide metabolism was potentially inhibited by methimazole in vitro. The drug-drug interaction leading to methimazole affecting the disposition of ethionamide mediated by FMO3 was then quantitated using a bottom-up approach with a physiologically based pharmacokinetic framework. The maximum concentration (C ) and area under the curve (AUC) of et... More

关键词

FMO3,PBPK,drug-drug interactions,ethionamide,genetic polymorp