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肠致病性大肠杆菌 Rns 调节子的突变揭示了一个连接序列和两个螺旋-转角-螺旋基序的作用。

Mutagenesis of the Rns regulator of enterotoxigenic Escherichia coli reveals roles for a linker sequence and two helix-turn-helix motifs.

机构信息

Department of Clinical Microbiology, School of Medicine, Trinity College Dublin, St James's Hospital, Dublin 8, Ireland.

Institute of Molecular Medicine, Trinity Centre, Trinity College Dublin, St James's Hospital, Dublin 8, Ireland.

出版信息

Microbiology (Reading). 2010 Sep;156(Pt 9):2796-2806. doi: 10.1099/mic.0.038521-0. Epub 2010 May 27.

Abstract

The pathogenesis of diarrhoeal disease due to human enterotoxigenic Escherichia coli absolutely requires the expression of fimbriae. The expression of CS1 fimbriae is positively regulated by the AraC-like protein Rns. AraC-like proteins are DNA-binding proteins that typically contain two helix-turn-helix (HTH) motifs. A program of pentapeptide insertion mutagenesis of the Rns protein was performed, and this revealed that both HTH motifs are required by Rns to positively regulate CS1 fimbrial gene expression. Intriguingly, a pentapeptide insertion after amino acid C102 reduced the ability of Rns to transactivate CS1 fimbrial expression. The structure of Rns in this vicinity (NACRS) was predicted to be disordered and thus might act as a flexible linker. This hypothesis was confirmed by deletion of this amino acid sequence from the Rns protein; a truncated protein that lacked this sequence was no longer functional. Strikingly, this sequence could be functionally substituted in vivo and in vitro by a flexible seven amino acid sequence from another E. coli AraC-like protein RhaS. Our data indicate that HTH motifs and a flexible sequence are required by Rns for maximal activation of fimbrial gene expression.

摘要

人肠致病性大肠杆菌引起的腹泻病的发病机制绝对需要菌毛的表达。CS1 菌毛的表达受 AraC 样蛋白 Rns 的正调控。AraC 样蛋白是 DNA 结合蛋白,通常包含两个螺旋-转角-螺旋 (HTH) 基序。对 Rns 蛋白进行五肽插入诱变的方案,结果表明 Rns 正向调控 CS1 菌毛基因表达需要两个 HTH 基序。有趣的是,在氨基酸 C102 后插入五肽降低了 Rns 激活 CS1 菌毛表达的能力。该附近区域(NACRS)的 Rns 结构被预测为无序,因此可能充当柔性接头。通过从 Rns 蛋白中删除该氨基酸序列证实了这一假设;缺乏该序列的截断蛋白不再具有功能。引人注目的是,该序列可以在体内和体外通过另一种大肠杆菌 AraC 样蛋白 RhaS 的灵活的七个氨基酸序列进行功能替代。我们的数据表明,HTH 基序和柔性序列是 Rns 激活菌毛基因表达所必需的。

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