Metabolism of repaglinide by CYP2C8 and CYP3A4 in vitro: effect of fibrates and rifampicin.

Kajosaari LI; Laitila J; Neuvonen PJ; Backman JT

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Metabolism of repaglinide by CYP2C8 and CYP3A4 in vitro: effect of fibrates and rifampicin.

机译：CYP2C8和CYP3A4在体外对瑞格列奈的代谢：贝特类药物和利福平的作用。

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Repaglinide is an antidiabetic drug metabolised by cytochrome P450 (CYP) 2C8 and CYP3A4 enzymes. To clarify the mechanisms of observed repaglinide drug interactions, we determined the contribution of the two enzymes to repaglinide metabolism at different substrate concentrations, and examined the effect of fibrates and rifampicin on CYP2C8, CYP3A4 and repaglinide metabolism in vitro. We studied repaglinide metabolism using pooled human liver microsomes, recombinant CYP2C8 and recombinant CYP3A4 enzymes. The effect of quercetin and itraconazole on repaglinide metabolism, and of gemfibrozil, bezafibrate, fenofibrate and rifampicin on CYP2C8 (paclitaxel 6alpha-hydroxylation) and CYP3A4 (midazolam 1-hydroxylation) activities and repaglinide metabolism were studied using human liver microsomes. At therapeutic repaglinide concentrations (<0.4 microM), CYP2C8 and CYP3A4 metabolised repaglinide at similar rates. Quercetin (25 microM) and itraconazole (3 microM) inhibited the metabolism of 0.2 microM repaglinide by 58% and 71%, and that of 2 microM repaglinide by 56% and 59%, respectively. The three fibrates inhibited CYP2C8 (Ki: bezafibrate 9.7 microM, gemfibrozil 30.4 microM and fenofibrate 92.6 microM) and repaglinide metabolism (IC50: bezafibrate 37.7 microM, gemfibrozil 111 microM and fenofibrate 164 microM), but had no effect on CYP3A4. Rifampicin inhibited CYP2C8 (Ki 30.2 microM), CYP3A4 (Ki 18.5 microM) and repaglinide metabolism (IC50 13.7 microM). In conclusion, both CYP2C8 and CYP3A4 are important in the metabolism of therapeutic concentrations of repaglinide in vitro, but their predicted contributions in vivo are highly dependent on the scaling factor used. Gemfibrozil is only a moderate inhibitor of CYP2C8 and does not inhibit CYP3A4; inhibition of CYP-enzymes by parent gemfibrozil alone does not explain its interaction with repaglinide in vivo. Rifampicin competitively inhibits both CYP2C8 and CYP3A4, which can counteract its inducing effect in humans.

机译：瑞格列奈是一种通过细胞色素P450（CYP）2C8和CYP3A4酶代谢的抗糖尿病药物。为了阐明观察到的瑞格列奈药物相互作用的机制，我们确定了两种酶在不同底物浓度下对瑞格列奈代谢的贡献，并研究了贝特和利福平对CYP2C8，CYP3A4和瑞格列奈体外代谢的影响。我们使用合并的人肝微粒体，重组CYP2C8和重组CYP3A4酶研究了瑞格列奈的代谢。使用人肝微粒体研究了槲皮素和伊曲康唑对瑞格列奈代谢的影响，以及吉非贝齐，苯扎贝特，非诺贝特和利福平对CYP2C8（紫杉醇6α-羟基化）和CYP3A4（咪达唑仑1-羟基化）活性和瑞格列奈代谢的影响。在治疗性瑞格列奈浓度（<0.4 microM）下，CYP2C8和CYP3A4代谢瑞格列奈的速率相似。槲皮素（25 microM）和伊曲康唑（3 microM）分别抑制0.2 microM瑞格列奈的代谢58％和71％，以及2 microM瑞格列奈的代谢56％和59％。这三种贝特类药物抑制CYP2C8（Ki：苯扎贝特9.7 microM，吉非贝齐30.4 microM和非诺贝特92.6 microM）和瑞格列奈代谢（IC50：苯扎贝特37.7 microM，吉非贝齐111 microM和非诺贝特164 microM），但对CYP3没有影响。利福平抑制CYP2C8（Ki 30.2 microM），CYP3A4（Ki 18.5 microM）和瑞格列奈代谢（IC50 13.7 microM）。总之，CYP2C8和CYP3A4在体外瑞格列奈治疗浓度的代谢中均很重要，但它们在体内的预测作用高度依赖于所用的比例因子。 Gemfibrozil只是CYP2C8的中度抑制剂，不抑制CYP3A4。单独的母体吉非贝齐抑制CYP酶不能解释其与瑞格列奈在体内的相互作用。利福平竞争性地抑制CYP2C8和CYP3A4，这可以抵消其对人的诱导作用。

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《Basic & clinical pharmacology & toxicology.》 |2005年第4期|共8页
作者
Kajosaari LI; Laitila J; Neuvonen PJ; Backman JT;
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正文语种 eng
中图分类药学;
关键词
Aryl Hydrocarbon Hydroxylases; Carbamates; Cytochrome P-450 Enzyme System; 芳基烃羟化酶类; 氨甲酸酯类; 降血糖药; 微粒体; 肝; 哌啶类;

机译：Aryl Hydrocarbon Hydroxylases;Carbamates;Cytochrome P-450 Enzyme System;芳基烃羟化酶类;氨甲酸酯类;降血糖药;微粒体;肝;哌啶类;
入库时间 2022-08-18 09:30:48

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1. Metabolism of repaglinide by CYP2C8 and CYP3A4 in vitro: effect of fibrates and rifampicin. [J] . Kajosaari LI, Laitila J, Neuvonen PJ, Basic & clinical pharmacology & toxicology. . 2005,第4期

机译：CYP2C8和CYP3A4在体外对瑞格列奈的代谢：贝特类药物和利福平的作用。
2. Pioglitazone, an in vitro inhibitor of CYP2C8 and CYP3A4, does not increase the plasma concentrations of the CYP2C8 and CYP3A4 substrate repaglinide [J] . Lauri I. Kajosaari, Tiina Jaakkola, Pertti J. Neuvonen, European Journal of Clinical Pharmacology . 2006,第3期

机译：吡格列酮是CYP2C8和CYP3A4的体外抑制剂，不会增加CYP2C8和CYP3A4底物瑞格列奈的血浆浓度
3. CYP2C8 and CYP3A4 are the principal enzymes involved in the human in vitro biotransformation of the insulin secretagogue repaglinide. [J] . Bidstrup TB, Bjornsdottir I, Sidelmann UG, British Journal of Clinical Pharmacology . 2003,第3期

机译：CYP2C8和CYP3A4是参与人胰岛素促分泌素瑞格列奈体外生物转化的主要酶。
4. CHARACTERIZATION OF IN VITRO METABOLITES OF TROLEANDOMYCIN, A METABOLISM-DEPENDENT INHIBITOR OF CYP3A4, BY UPLC~(TM) QTOF MASS SPECTROMETRY [C] . Joanna E. Barbara, David Buckley, Phyllis Yerino, American Society for Mass Spectrometry Conference on Mass Spectrometry and Allied Topics . 2009

机译：Troleandomcin体外代谢物，CYPOM3A4的代谢依赖性抑制剂的表征，UPLC〜（TM）质谱法
5. In Vitro-In Vivo Assessment of Repaglinide Metabolism and Drug-Drug Interactions: Towards a Physiologically-Based Pharmacokinetic Model [D] . Thule S?ll, Carolina Maria. 2013

机译：瑞格列奈代谢和药物-药物相互作用的体外评估：建立基于生理学的药代动力学模型
6. CYP2C8 and CYP3A4 are the principal enzymes involved in the human in vitro biotransformation of the insulin secretagogue repaglinide [O] . Tanja Busk Bidstrup, Inga Bjørnsdottir, Ulla Grove Sidelmann, 2003

机译：CYP2C8和CYP3A4是参与人胰岛素促分泌素瑞格列奈体外生物转化的主要酶
7. Estimation of the Contribution of CYP2C8 and CYP3A4 in Repaglinide Metabolism by Human Liver Microsomes Under Various Buffer Conditions [O] . Toshiyuki Kudo, Hitomi Goda, Yuki Yokosuka, 2017

机译：在各种缓冲条件下，人肝微粒体估算CYP2C8和CYP3A4在regaglinide代谢的贡献
8. Metabolism of Endosulfan-Alpha by Human Liver Microsomes and its Utility as a Simultaneous In Vitro Probe for CYP2B6 and CYP3A4 [R] . Casabar, R. C. , Wallace, A. D. , Hodgson, E. , 2006

机译：人肝微粒体对硫丹-α的代谢及其作为CYp2B6和CYp3a4同时体外探针的应用

Metabolism of repaglinide by CYP2C8 and CYP3A4 in vitro: effect of fibrates and rifampicin.

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