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全局调控因子H-NS与Tn10转座体中的两类不同位点结合,以促进转座。

The global regulator H-NS binds to two distinct classes of sites within the Tn10 transpososome to promote transposition.

作者信息

Ward Chris M, Wardle Simon J, Singh Randeep K, Haniford David B

机构信息

Department of Biochemistry, University of Western Ontario, London, Ontario, Canada N6A 5C1.

出版信息

Mol Microbiol. 2007 May;64(4):1000-13. doi: 10.1111/j.1365-2958.2007.05708.x.

Abstract

The histone-like nucleoid structuring protein (H-NS) is a global transcriptional regulator that influences stress response and virulence pathways in Gram-negative bacteria. H-NS also promotes Tn10 transposition by binding directly to the transpososome and inducing a conformational change in the transpososome that favours intermolecular transposition events. H-NS binds preferentially to curved DNA and can bend non-curved DNA, it self-oligomerizes and can interact with other proteins. To determine what functions of H-NS are important in promoting Tn10 transposition, we have examined the ability of two mutant forms of H-NS, P116S and 1-64, to act in Tn10 transposition. We provide evidence that the initial interaction of H-NS with the transpososome is dependent on H-NS binding to a specific structure in DNA flanking the transposon end. Additional molecules of H-NS then bind within the transposon end. This latter event appears to be directed by H-NS binding to the Tn10 transposase protein, and is important in maintaining the transpososome in a conformation that promotes intermolecular transposition. The binding of H-NS to a transposase protein is a novel function for this important regulatory molecule.

摘要

类组蛋白核仁结构蛋白(H-NS)是一种全局转录调节因子,可影响革兰氏阴性菌的应激反应和毒力途径。H-NS还通过直接结合转座体并诱导转座体发生构象变化来促进Tn10转座,这种构象变化有利于分子间转座事件。H-NS优先结合弯曲的DNA,也能使非弯曲的DNA弯曲,它能自我寡聚化,并能与其他蛋白质相互作用。为了确定H-NS的哪些功能在促进Tn10转座中起重要作用,我们研究了H-NS的两种突变形式P116S和1-64在Tn10转座中的作用能力。我们提供的证据表明,H-NS与转座体的初始相互作用取决于H-NS与转座子末端侧翼DNA中特定结构的结合。然后,额外的H-NS分子在转座子末端内结合。后一事件似乎是由H-NS与Tn10转座酶蛋白的结合所引导的,并且在将转座体维持在促进分子间转座的构象中起重要作用。H-NS与转座酶蛋白的结合是这种重要调节分子的一种新功能。

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