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大肠杆菌厌氧核糖核苷酸还原酶底物特异性的别构调控。

Allosteric control of the substrate specificity of the anaerobic ribonucleotide reductase from Escherichia coli.

作者信息

Eliasson R, Pontis E, Sun X, Reichard P

机构信息

Department of Biochemistry 1, Medical Nobel Institute, Karolinska Institutet, Stockholm, Sweden.

出版信息

J Biol Chem. 1994 Oct 21;269(42):26052-7.

PMID:7929317
Abstract

The reduction of ribonucleotides is catalyzed by different enzymes in aerobic and anaerobic Escherichia coli, each with a different primary and quaternary structure. Here, we describe the allosteric regulation of the substrate specificity of the anaerobic ribonucleoside triphosphate reductase. The enzyme reduced ribonucleotides at a low basal rate. Reduction was stimulated up to 10-fold by an appropriate modulator (dGTP for ATP reduction, ATP for CTP and UTP reduction, and dTTP for GTP reduction). dGTP and dTTP inhibited the reduction of the "incorrect" substrate; dATP inhibited reduction of all four. From kinetic, effector binding, and competition experiments we conclude that the enzyme has two classes of sites, one that binds ATP and dATP and regulates pyrimidine ribonucleotide reduction ("pyrimidine site"), the other that binds dATP, dGTP, and dTTP and regulates purine ribonucleotide reduction ("purine site"). This model differs slightly from the model for the aerobic reductase, but the physiological consequences remain the same and explain how a single enzyme can provide a balanced supply of the four dNTPs. The similarity of a highly sophisticated control mechanism for the aerobic and anaerobic enzymes suggests that both arose by divergent evolution from a common ancestor, in spite of their different structures.

摘要

在需氧和厌氧的大肠杆菌中,核糖核苷酸的还原由不同的酶催化,每种酶具有不同的一级和四级结构。在此,我们描述了厌氧核糖核苷三磷酸还原酶底物特异性的变构调节。该酶以低基础速率还原核糖核苷酸。通过适当的调节剂(用于还原ATP的dGTP、用于还原CTP和UTP的ATP以及用于还原GTP的dTTP),还原作用可被刺激高达10倍。dGTP和dTTP抑制“错误”底物的还原;dATP抑制所有四种底物的还原。从动力学、效应物结合和竞争实验中我们得出结论,该酶有两类位点,一类结合ATP和dATP并调节嘧啶核糖核苷酸的还原(“嘧啶位点”),另一类结合dATP、dGTP和dTTP并调节嘌呤核糖核苷酸的还原(“嘌呤位点”)。该模型与需氧还原酶的模型略有不同,但生理后果是相同的,并解释了单一酶如何能提供四种脱氧核苷酸三磷酸的平衡供应。需氧和厌氧酶高度复杂的控制机制的相似性表明,尽管它们结构不同,但两者都是由共同祖先通过趋异进化产生的。

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