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DsrA RNA上Hfq结合位点的鉴定:Hfq结合时不会改变DsrA的二级结构。

Identification of the Hfq-binding site on DsrA RNA: Hfq binds without altering DsrA secondary structure.

作者信息

Brescia Cristin C, Mikulecky Peter J, Feig Andrew L, Sledjeski Darren D

机构信息

Department of Microbiology and Immunology, Medical College of Ohio, Toledo 43614, USA.

出版信息

RNA. 2003 Jan;9(1):33-43. doi: 10.1261/rna.2570803.

Abstract

DsrA RNA regulates the translation of two global regulatory proteins in Escherichia coli. DsrA activates the translation of RpoS while repressing the translation of H-NS. The RNA-binding protein Hfq is necessary for DsrA to function in vivo. Although Hfq binds to DsrA in vitro, the role of Hfq in DsrA-mediated regulation is not known. One hypothesis was that Hfq acts as an RNA chaperone by unfolding DsrA, thereby facilitating interactions with target RNAs. To test this hypothesis, we have examined the structure of DsrA bound to Hfq in vitro. Comparison of free DsrA to DsrA bound to Hfq by RNase footprinting, circular dichroism, and thermal melt profiles shows that Hfq does not alter DsrA secondary structures, but might affect its tertiary conformation. We identify the site on DsrA where Hfq binds, which is a structural element in the middle of DsrA. In addition, we show that although long poly(U) RNAs compete with DsrA for binding to Hfq, a short poly(U) stretch present in DsrA is not necessary for Hfq binding. Finally, unlike other RNAs, DsrA binding to Hfq is not competed with by poly(A) RNA. In fact, DsrA:poly(A):Hfq may form a stable ternary complex, raising the possibility that Hfq has multiple RNA-binding sites.

摘要

DsrA RNA调控大肠杆菌中两种全局调节蛋白的翻译。DsrA激活RpoS的翻译,同时抑制H-NS的翻译。RNA结合蛋白Hfq是DsrA在体内发挥功能所必需的。尽管Hfq在体外与DsrA结合,但Hfq在DsrA介导的调控中的作用尚不清楚。一种假设是,Hfq通过使DsrA解折叠而充当RNA伴侣,从而促进与靶RNA的相互作用。为了验证这一假设,我们在体外研究了与Hfq结合的DsrA的结构。通过核糖核酸酶足迹法、圆二色性和热熔曲线对游离DsrA与结合Hfq的DsrA进行比较,结果表明Hfq不会改变DsrA的二级结构,但可能会影响其三级构象。我们确定了DsrA上Hfq结合的位点,该位点是DsrA中间的一个结构元件。此外,我们表明,尽管长链聚(U)RNA与DsrA竞争与Hfq的结合,但DsrA中存在的短链聚(U)片段对于Hfq结合并非必需。最后,与其他RNA不同,DsrA与Hfq的结合不会被聚(A)RNA竞争。事实上,DsrA:聚(A):Hfq可能形成稳定的三元复合物,这增加了Hfq具有多个RNA结合位点的可能性。

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