Cytochrome P450 3A4 Induction: Lumacaftor versus Ivacaftor Potentially Resulting in Significantly Reduced Plasma Concentration of Ivacaftor.

Drug metabolism letters Pub Date : 2018-01-01 DOI:10.2174/1872312812666180328105259

Elena K Schneider

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引用次数: 37

Abstract

Background & objective: Since the release of ivacaftor-lumacaftor, several red-flags have been raised that highlight the clinical efficacy of this combination strategy that may be limited due to antagonistic drug-drug interactions.

Method: The effect of ivacaftor, its major metabolites M1 and M6, lumacaftor and the novel cystic fibrosis transmembrane conductance regulator (CFTR) modulator tezacaftor at 10 µg/mL on the enzymatic activity of the major xenobiotic metabolizing enzymes CYP1A2 and CYP3A4 as well as the minor enzymes CYP2B6 and CYP2C9 was assayed.

Results: Lumacaftor (3.74 x 105 ± 3.11 x 104 RLU), and ivacaftor-M6 (3.43 x 105 ± 7.61 x 103 RLU) markedly induced the activity of CYP3A4. Ivacaftor (2.22 x 105 ± 3.94 x 104 RLU) showed a lower relative ratio of luminescence units compared to chloramphenicol (3.17 x 105 ± 1.55 x 104 RLU). Interestingly, ivacaftor-M1 (6.74 x 104 ± 3.09 x 104 RLU) and the novel CFTR modulator tezacaftor (2.40 x 104 ± 8.14 x 104 RLU) did not show CYP3A4 induction. In the CYP1A2 and CYP2C9 assay, all metabolites showed a decrease in the ratio of luminescence units compared to the controls. Ivacaftor, its major metabolites, lumacaftor and tezacaftor all showed a slight increase in the ratio of luminescence units compared to the control rifampin with CYP2B6.

Conclusion: All in all, present findings would suggest that lumacaftor and ivacaftor-M6 are strong inducers of CYP3A4, potentially reducing ivacaftor concentrations; ivacaftor itself induces CYP3A4 to some extent.

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细胞色素P450 3A4诱导:Lumacaftor与Ivacaftor可能导致Ivacaftor血浆浓度显著降低。

背景与目的:自ivacaftor-lumacaftor上市以来，已经出现了一些危险信号，强调这种联合策略的临床疗效可能由于药物-药物相互作用而受到限制。方法:测定ivacaftor及其主要代谢产物M1、M6、lumacaftor和新型囊性纤维化跨膜传导调节剂tezacaftor在10µg/mL浓度下对主要外生代谢酶CYP1A2、CYP3A4及次要代谢酶CYP2B6、CYP2C9酶活性的影响。结果:Lumacaftor (3.74 × 105±3.11 × 104 RLU)和ivacaftor-M6 (3.43 × 105±7.61 × 103 RLU)显著诱导CYP3A4活性。Ivacaftor (2.22 × 105±3.94 × 104 RLU)的相对发光单位比低于氯霉素(3.17 × 105±1.55 × 104 RLU)。有趣的是，ivacaftor-M1 (6.74 × 104±3.09 × 104 RLU)和新型CFTR调制器tezacaftor (2.40 × 104±8.14 × 104 RLU)没有表现出CYP3A4诱导。在CYP1A2和CYP2C9实验中，与对照组相比，所有代谢物的发光单位比例都有所下降。与对照利福平和CYP2B6相比，Ivacaftor及其主要代谢产物lumacaftor和tezacaftor的发光单位比例均略有增加。结论:总而言之，本研究结果表明，lumacaftor和ivacaftor- m6是CYP3A4的强诱导剂，可能降低ivacaftor的浓度;ivacaftor本身在一定程度上诱导CYP3A4。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Drug metabolism letters Pharmacology, Toxicology and Pharmaceutics-Pharmaceutical Science

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期刊介绍： Drug Metabolism Letters publishes letters and research articles on major advances in all areas of drug metabolism and disposition. The emphasis is on publishing quality papers very rapidly by taking full advantage of the Internet technology both for the submission and review of manuscripts. The journal covers the following areas: In vitro systems including CYP-450; enzyme induction and inhibition; drug-drug interactions and enzyme kinetics; pharmacokinetics, toxicokinetics, species scaling and extrapolations; P-glycoprotein and transport carriers; target organ toxicity and interindividual variability; drug metabolism and disposition studies; extrahepatic metabolism; phase I and phase II metabolism; recent developments for the identification of drug metabolites.