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色氨酸阻遏物的DNA结合结构域识别不同操纵基因序列时所需的灵活性。

Flexibility of DNA binding domain of trp repressor required for recognition of different operator sequences.

作者信息

Gryk M R, Jardetzky O, Klig L S, Yanofsky C

机构信息

Stanford Magnetic Resonance Laboratory, Stanford University, California 94305-5055, USA.

出版信息

Protein Sci. 1996 Jun;5(6):1195-7. doi: 10.1002/pro.5560050624.

Abstract

Trp repressor (25 kDa) is a regulatory protein that controls transcription initiation in the tryptophan biosynthetic operon and at least four other operons in Escherichia coli. An alanine to valine mutation (AV77) in the DNA binding domain is known to increase repressor activity at the trp operator in vivo, but not in vitro. We report here the amide proton exchange rates for the DNA-binding domains of both the wild-type and AV77 proteins. We find that the alanine to valine change stabilizes the flexible DNA-binding domain of the repressor. We present in vivo data showing that, although the AV77 repressor is more inhibitory at the trp operator than the wild-type repressor, it does not have increased activity at the aroH or trpR operator; repression at the aroH operator is, in fact, reduced. Our results suggest that the flexibility exhibited by the wild-type repressor allows a broader range of repressor/DNA interactions, whereas the increased rigidity resulting from the AV77 change limits the repressor's effectiveness at some operators.

摘要

色氨酸阻遏蛋白(25 kDa)是一种调控蛋白,可控制大肠杆菌中色氨酸生物合成操纵子以及至少其他四个操纵子的转录起始。已知DNA结合结构域中的丙氨酸到缬氨酸突变(AV77)会在体内而非体外增加色氨酸操纵基因处的阻遏蛋白活性。我们在此报告野生型和AV77蛋白DNA结合结构域的酰胺质子交换率。我们发现丙氨酸到缬氨酸的变化稳定了阻遏蛋白的柔性DNA结合结构域。我们提供的体内数据表明,尽管AV77阻遏蛋白在色氨酸操纵基因处比野生型阻遏蛋白更具抑制性,但它在aroH或trpR操纵基因处并未表现出增强的活性;事实上,aroH操纵基因处的阻遏作用有所降低。我们的结果表明,野生型阻遏蛋白表现出的灵活性允许更广泛的阻遏蛋白/DNA相互作用,而AV77变化导致的刚性增加限制了阻遏蛋白在某些操纵基因处的有效性。

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