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霍乱弧菌原核转录因子 HigA2 的模糊识别。

Fuzzy recognition by the prokaryotic transcription factor HigA2 from Vibrio cholerae.

机构信息

Structural Biology Brussels, Department of Biotechnology, Vrije Universiteit Brussel, Pleinlaan 2, 1050, Brussels, Belgium.

Centre for Structural Biology, VIB, Pleinlaan 2, 1050, Brussels, Belgium.

出版信息

Nat Commun. 2024 Apr 10;15(1):3105. doi: 10.1038/s41467-024-47296-3.

Abstract

Disordered protein sequences can exhibit different binding modes, ranging from well-ordered folding-upon-binding to highly dynamic fuzzy binding. The primary function of the intrinsically disordered region of the antitoxin HigA2 from Vibrio cholerae is to neutralize HigB2 toxin through ultra-high-affinity folding-upon-binding interaction. Here, we show that the same intrinsically disordered region can also mediate fuzzy interactions with its operator DNA and, through interplay with the folded helix-turn-helix domain, regulates transcription from the higBA2 operon. NMR, SAXS, ITC and in vivo experiments converge towards a consistent picture where a specific set of residues in the intrinsically disordered region mediate electrostatic and hydrophobic interactions while "hovering" over the DNA operator. Sensitivity of the intrinsically disordered region to scrambling the sequence, position-specific contacts and absence of redundant, multivalent interactions, point towards a more specific type of fuzzy binding. Our work demonstrates how a bacterial regulator achieves dual functionality by utilizing two distinct interaction modes within the same disordered sequence.

摘要

无序蛋白质序列可能表现出不同的结合模式,从有序的折叠结合到高度动态的模糊结合。霍乱弧菌抗毒素 HigA2 的无规卷曲区的主要功能是通过超高亲和力的折叠结合相互作用来中和 HigB2 毒素。在这里,我们表明,同一个无规卷曲区也可以与它的操纵子 DNA 介导模糊相互作用,并通过与折叠的螺旋-转角-螺旋结构域相互作用,调节 higBA2 操纵子的转录。NMR、SAXS、ITC 和体内实验得出了一致的结论,即无规卷曲区的一组特定残基介导静电和疏水相互作用,同时“盘旋”在 DNA 操纵子上。无规卷曲区对序列混乱、位置特异性接触和缺乏冗余、多价相互作用的敏感性表明了一种更特定类型的模糊结合。我们的工作表明,细菌调节剂如何通过在同一无序序列中利用两种不同的相互作用模式来实现双重功能。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/7ced/11006873/671a9c80429b/41467_2024_47296_Fig1_HTML.jpg

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