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甲萘醌对全细胞、微粒体及重组系统中苯并(a)芘代谢的抑制作用。

Menadione inhibition of benzo(a)pyrene metabolism in whole cells, microsomes and reconstituted systems.

作者信息

Sadowski I J, Wright J A, Ollmann D, Israels L G

出版信息

Int J Biochem. 1986;18(6):565-8. doi: 10.1016/0020-711x(86)90169-2.

Abstract

Menadione is known to decrease the mixed function oxidase mediated metabolism of a number of substrates in microsomal systems. The present study examines the effect of menadione on benzo(a)pyrene metabolism in whole cells, microsomes and a semi-purified reconstituted mixed function oxidase system. Menadione has a high affinity for the NADPH dependent cytochrome P-450 reductase and acts as a competitive inhibitor of cytochrome P-450 reductase in the metabolism of benzo(a)pyrene. This is the mechanism of inhibition of aryl hydrocarbon hydroxylase by menadione in reconstituted systems. In a whole cell system and at low concentrations of menadione, depletion of reduced pyridine nucleotides is the initial inhibitory event.

摘要

已知甲萘醌可降低微粒体系统中多种底物的混合功能氧化酶介导的代谢。本研究考察了甲萘醌对全细胞、微粒体及半纯化重组混合功能氧化酶系统中苯并(a)芘代谢的影响。甲萘醌对依赖烟酰胺腺嘌呤二核苷酸磷酸(NADPH)的细胞色素P - 450还原酶具有高亲和力,并在苯并(a)芘代谢中作为细胞色素P - 450还原酶的竞争性抑制剂。这是重组系统中甲萘醌抑制芳烃羟化酶的机制。在全细胞系统中以及低浓度甲萘醌情况下,还原型吡啶核苷酸的耗竭是初始抑制事件。

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