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使用多种底物对人肝脏乙醇脱氢酶变体进行的体外研究。

In vitro studies of human liver alcohol dehydrogenase variants using a variety of substrates.

作者信息

Kassam J P, Tang B K, Kadar D, Kalow W

机构信息

Department of Pharmacology, University of Toronto, Ontario, Canada.

出版信息

Drug Metab Dispos. 1989 Sep-Oct;17(5):567-72.

PMID:2573502
Abstract

Alcohol dehydrogenase (ADH) is genetically polymorphic, and large differences in allele frequencies exist between the major human races. Genetic variants at the ADH2 gene locus include the beta 2-ADH ("atypical" ADH) present in 85% of Orientals and the beta 1-ADH ("normal" ADH) present in 85 to 95% of whites. Although the presence of one or the other of these ADH variants does not significantly affect the rate of ethanol oxidation in the living subject, it may affect that of other substrates. The overall objective of this work was to screen in vitro for ADH substrates which might be differentially metabolized by these ADH2variants in living subjects. In an in vitro screening method using autopsy livers at pH 8.5, the formation or disappearance of NADH at 340 nm was measured before and after exposure to 4-methylpyrazole, an ADH-specific competitive inhibitor. The screening test revealed three new substrates and suggested that alcohol substrates fall into two groups. The majority of substrates belonged to a group which was oxidized at a significantly lower rate by the beta 2-ADH as compared to the beta 1-ADH, but this was not the case for a small group which included ethanol. Subsequent kinetic studies of selected alcohols tended to indicate a uniqueness of ethanol kinetics in that both KM and Vmax favored its oxidation by beta 2-ADH rather than by the beta 1 variant. None of the other seven tested alcohols showed a similar differential. Also, reduction of aldehydes and ketones tended to be moderately slower by beta 2- than by beta 1-ADH.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

乙醇脱氢酶(ADH)具有遗传多态性,主要人类种族之间的等位基因频率存在很大差异。ADH2基因位点的遗传变异包括85%的东方人所具有的β2-ADH(“非典型”ADH)和85%至95%的白人所具有的β1-ADH(“正常”ADH)。虽然这些ADH变体中的一种或另一种的存在不会显著影响活体受试者中乙醇的氧化速率,但它可能会影响其他底物的氧化速率。这项工作的总体目标是在体外筛选可能在活体受试者中被这些ADH2变体差异代谢的ADH底物。在一种使用尸检肝脏、pH值为8.5的体外筛选方法中,在暴露于ADH特异性竞争性抑制剂4-甲基吡唑之前和之后,测量340nm处NADH的形成或消失。筛选试验揭示了三种新底物,并表明酒精底物可分为两组。大多数底物属于一组,与β1-ADH相比,β2-ADH氧化该组底物的速率明显较低,但包括乙醇在内的一小组底物并非如此。随后对选定醇类的动力学研究倾向于表明乙醇动力学具有独特性,因为Km和Vmax都有利于其被β2-ADH而非β1变体氧化。其他七种测试醇类均未显示出类似的差异。此外,β2-ADH还原醛和酮的速度往往比β1-ADH略慢。(摘要截断于250字)

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