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乙醇氧化与毒性:乙醇P-450加氧酶的作用

Ethanol oxidation and toxicity: role of alcohol P-450 oxygenase.

作者信息

Koop D R, Coon M J

出版信息

Alcohol Clin Exp Res. 1986;10(6 Suppl):44S-49S. doi: 10.1111/j.1530-0277.1986.tb05179.x.

Abstract

The isolation and characterization of ethanol-inducible rabbit liver microsomal cytochrome P-450, termed P-450 3a or P-450ALC, has provided definitive evidence for the role of this enzyme in alcohol oxidation. From findings on the distribution, substrate specificity, and mechanism of action of P-450ALC we have suggested "alcohol P-450 oxygenase" as a more biochemically accurate name than "microsomal ethanol-oxidizing system." The present review is concerned with studies in this and other laboratories on activities and inducers associated with this versatile enzyme. Numerous xenobiotics, including alcohols and ketones, nitrosamines, aromatic compounds, and halogenated alkanes, alkenes, and ethers, are known to undergo increased microsomal metabolism after chronic exposure of various species to ethanol. Diverse compounds and treatments may induce P-450ALC, including the administration of ten or more chemically different compounds, fasting, or the diabetic state. Whether a common mechanism of induction is involved is unknown at this time. As direct evidence that P-450ALC catalyzes numerous metabolic reactions, the purified rabbit enzyme has been used in a reconstituted system to demonstrate various metabolic transformations, including the oxidation of various alcohols, acetone, acetol, p-nitrophenol, and aniline, the dealkylation of substituted nitrosamines, the reductive dechlorination of carbon tetrachloride, carbon tetrachloride-induced lipid peroxidation, and acetaminophen activation to form the glutathione conjugate.

摘要

乙醇诱导的兔肝微粒体细胞色素P-450(称为P-450 3a或P-450ALC)的分离与特性鉴定,为该酶在酒精氧化中的作用提供了确凿证据。根据P-450ALC的分布、底物特异性及作用机制的研究结果,我们提出“酒精P-450加氧酶”作为比“微粒体乙醇氧化系统”在生物化学上更准确的名称。本综述关注的是本实验室及其他实验室关于这种多功能酶的活性和诱导剂的研究。已知在各种物种长期接触乙醇后,许多外源性物质,包括醇类、酮类、亚硝胺类、芳香族化合物以及卤代烷烃、烯烃和醚类,其微粒体代谢会增强。多种化合物和处理方式可诱导P-450ALC,包括给予十种或更多化学性质不同的化合物、禁食或处于糖尿病状态。目前尚不清楚是否涉及共同的诱导机制。作为P-450ALC催化众多代谢反应的直接证据,纯化的兔酶已用于重组系统中以证明各种代谢转化,包括各种醇类、丙酮、乙酰醇、对硝基苯酚和苯胺的氧化,取代亚硝胺的脱烷基化,四氯化碳的还原脱氯,四氯化碳诱导的脂质过氧化,以及对乙酰氨基酚活化形成谷胱甘肽共轭物。

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