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RNA聚合酶诱导的NusA重塑产生一个暂停增强复合物。

RNA polymerase-induced remodelling of NusA produces a pause enhancement complex.

作者信息

Ma Cong, Mobli Mehdi, Yang Xiao, Keller Andrew N, King Glenn F, Lewis Peter J

机构信息

School of Environmental and Life Sciences, University of Newcastle, Callaghan, NSW 2308, Australia.

Centre for Advanced Imaging, The University of Queensland, St Lucia, QLD 4072, Australia.

出版信息

Nucleic Acids Res. 2015 Mar 11;43(5):2829-40. doi: 10.1093/nar/gkv108. Epub 2015 Feb 17.

Abstract

Pausing during transcription elongation is a fundamental activity in all kingdoms of life. In bacteria, the essential protein NusA modulates transcriptional pausing, but its mechanism of action has remained enigmatic. By combining structural and functional studies we show that a helical rearrangement induced in NusA upon interaction with RNA polymerase is the key to its modulatory function. This conformational change leads to an allosteric re-positioning of conserved basic residues that could enable their interaction with an RNA pause hairpin that forms in the exit channel of the polymerase. This weak interaction would stabilize the paused complex and increases the duration of the transcriptional pause. Allosteric spatial re-positioning of regulatory elements may represent a general approach used across all taxa for modulation of transcription and protein-RNA interactions.

摘要

转录延伸过程中的暂停是所有生命王国中的一项基本活动。在细菌中,必需蛋白NusA调节转录暂停,但其作用机制一直成谜。通过结合结构和功能研究,我们表明,NusA与RNA聚合酶相互作用时诱导的螺旋重排是其调节功能的关键。这种构象变化导致保守碱性残基的变构重新定位,这可能使其与在聚合酶出口通道中形成的RNA暂停发夹相互作用。这种弱相互作用将稳定暂停复合物并增加转录暂停的持续时间。调节元件的变构空间重新定位可能代表了所有生物分类群用于调节转录和蛋白质-RNA相互作用的一种通用方法。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/38a5/4357713/d54be73fe432/gkv108fig1.jpg

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