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组氨酸操纵子的去阻遏与阻遏:第一种酶反馈位点的作用

Derepression and repression of the histidine operon: role of the feedback site of the first enzyme.

作者信息

Fernández V M, Martíndelrío R, Tébar A R, Guisán J M, Ballesteros A O

出版信息

J Bacteriol. 1975 Dec;124(3):1366-73. doi: 10.1128/jb.124.3.1366-1373.1975.

Abstract

Thiazolealanine, a false feedback inhibitor, causes transient repression of the his operon previously derepressed by a severe histidine limitation in strains with a wild-type or feedback-hypersensitive first enzyme but not in feedback-resistant mutants. Since experiments reported here clearly demonstrate that thiazolealanine is not transferred to tRNAHis, it is proposed that this "transient repression" is effected through the interaction of thiazolealanine with the feedback site of the enzyme. Experiments in the presence of rifampin indicate that this thiazolealanine-mediated effect is exerted at the level of translation. We conclude that histidine (free), in addition to forming co-repressor, also represses the operon at the level of translation through feedback interaction with the first enzyme of the pathway (adenosine 5'-triphosphate phosphoribosyltransferase). Rates of derepression in feedback-resistant strains are roughly half of those observed in controls, suggesting a positive role played by a first enzyme with a normal but unoccupied feedback site. Some feedback-resistant mutants, in contrast to the wild type, were unable to exhibit derepression under histidine limitation caused by aminotriazole.

摘要

噻唑丙氨酸是一种错误反馈抑制剂,它会导致组氨酸操纵子出现短暂的阻遏现象。在具有野生型或反馈超敏的第一种酶的菌株中,先前由于严重的组氨酸限制而解除阻遏的组氨酸操纵子,在这种情况下会受到短暂阻遏,但在反馈抗性突变体中则不会。由于此处报道的实验清楚地表明噻唑丙氨酸不会转移到tRNAHis上,因此有人提出这种“短暂阻遏”是通过噻唑丙氨酸与该酶的反馈位点相互作用实现的。在利福平存在的情况下进行的实验表明,这种由噻唑丙氨酸介导的效应是在翻译水平上发挥作用的。我们得出结论,组氨酸(游离的)除了形成共阻遏物外,还通过与该途径的第一种酶(腺苷5'-三磷酸磷酸核糖基转移酶)的反馈相互作用在翻译水平上阻遏操纵子。反馈抗性菌株中的去阻遏速率大约是对照中观察到的速率的一半,这表明具有正常但未被占据的反馈位点的第一种酶发挥了积极作用。与野生型相比,一些反馈抗性突变体在氨基三唑引起的组氨酸限制下无法表现出去阻遏现象。

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Derepression and repression of the histidine operon: role of the feedback site of the first enzyme.
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