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细胞色素P450 2C9蛋白与细胞色素b5的相互作用:对催化偶联的影响

CYP2C9 protein interactions with cytochrome b(5): effects on the coupling of catalysis.

作者信息

Locuson Charles W, Wienkers Larry C, Jones Jeffrey P, Tracy Timothy S

机构信息

Department of Experimental and Clinical Pharmacology, College of Pharmacy, University of Minnesota, Minneapolis, MN 55455, USA.

出版信息

Drug Metab Dispos. 2007 Jul;35(7):1174-81. doi: 10.1124/dmd.107.014910. Epub 2007 Apr 19.

Abstract

The hemoprotein cytochrome b(5) (cyt b5) has been demonstrated to affect the kinetics of drug oxidation by the microsomal cytochromes P450 (P450s). However, the mechanisms through which cyt b5 exerts these effects are variable and P450 isoform-dependent. Whereas the effects of cyt b5 on the major drug-metabolizing enzymes CYP2D6, CYP2E1, and CYP3A4 are well studied, fewer studies conducted over limited ranges of cyt b5 concentrations have been performed on CYP2C9. In the present study with CYP2C9, cyt b5 exerted complex actions upon P450 oxidative reactions by affecting the rate of metabolite formation, the consumption of NADPH by cytochrome P450 reductase, and uncoupling of the reaction cycle to hydrogen peroxide and water. Cytochrome b(5) devoid of the heme moiety (apo-b5) exhibited effects similar to those of native cyt b5. All rates were highly dependent on the cyt b5 to CYP2C9 enzyme ratio, suggesting that the amount of cyt b5 present in an in vitro incubation is an important factor that can have an impact on the reliability of extrapolating in vitro generated data to predict the in vivo condition. The major effects of cyt b5 are hypothesized to result from a cyt b5-induced conformational change in CYP2C9 that results in an increased collision frequency between the iron-oxygen species (Cpd I) and the substrate, and a decrease in the oxidase activity. Together, these findings suggest that cyt b5 can alter multiple steps in the P450 catalytic cycle via complex interactions with P450 and P450 reductase.

摘要

血红蛋白细胞色素b5(cyt b5)已被证明会影响微粒体细胞色素P450(P450s)对药物氧化的动力学。然而,cyt b5发挥这些作用的机制是可变的,且依赖于P450同工酶。虽然cyt b5对主要药物代谢酶CYP2D6、CYP2E1和CYP3A4的影响已得到充分研究,但在有限的cyt b5浓度范围内对CYP2C9进行的研究较少。在本项关于CYP2C9的研究中,cyt b5通过影响代谢物形成速率、细胞色素P450还原酶对NADPH的消耗以及反应循环与过氧化氢和水的解偶联,对P450氧化反应产生复杂作用。不含血红素部分的细胞色素b5(脱辅基b5)表现出与天然cyt b5相似的作用。所有速率都高度依赖于cyt b5与CYP2C9酶的比例,这表明体外孵育中cyt b5的含量是一个重要因素,可能会影响将体外生成的数据外推以预测体内情况的可靠性。据推测,cyt b5的主要作用是由其诱导的CYP2C9构象变化导致的,这种变化会使铁氧物种(化合物I)与底物之间的碰撞频率增加,同时氧化酶活性降低。总之,这些发现表明cyt b5可通过与P450和P450还原酶的复杂相互作用改变P450催化循环中的多个步骤。

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