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大肠杆菌 RNA 伴侣 Hfq 结合和水解 ATP 的结构和生化研究。

Structural and biochemical studies on ATP binding and hydrolysis by the Escherichia coli RNA chaperone Hfq.

机构信息

Department of Microbiology, Immunobiology and Genetics, Max F. Perutz Laboratories, University of Vienna, Vienna, Austria.

出版信息

PLoS One. 2012;7(11):e50892. doi: 10.1371/journal.pone.0050892. Epub 2012 Nov 30.

Abstract

In Escherichia coli the RNA chaperone Hfq is involved in riboregulation by assisting base-pairing between small regulatory RNAs (sRNAs) and mRNA targets. Several structural and biochemical studies revealed RNA binding sites on either surface of the donut shaped Hfq-hexamer. Whereas sRNAs are believed to contact preferentially the YKH motifs present on the proximal site, poly(A)(15) and ADP were shown to bind to tripartite binding motifs (ARE) circularly positioned on the distal site. Hfq has been reported to bind and to hydrolyze ATP. Here, we present the crystal structure of a C-terminally truncated variant of E. coli Hfq (Hfq(65)) in complex with ATP, showing that it binds to the distal R-sites. In addition, we revisited the reported ATPase activity of full length Hfq purified to homogeneity. At variance with previous reports, no ATPase activity was observed for Hfq. In addition, FRET assays neither indicated an impact of ATP on annealing of two model oligoribonucleotides nor did the presence of ATP induce strand displacement. Moreover, ATP did not lead to destabilization of binary and ternary Hfq-RNA complexes, unless a vast stoichiometric excess of ATP was used. Taken together, these studies strongly suggest that ATP is dispensable for and does not interfere with Hfq-mediated RNA transactions.

摘要

在大肠杆菌中,RNA 伴侣 Hfq 通过协助小调控 RNA(sRNA)与 mRNA 靶标之间的碱基配对,参与核糖调控。几项结构和生化研究揭示了圆环形状的 Hfq 六聚体表面上的 RNA 结合位点。虽然 sRNA 被认为优先与近端位点上存在的 YKH 基序结合,但多聚(A)(15)和 ADP 被证明与远端位点上呈环状排列的三部分结合基序(ARE)结合。已经报道 Hfq 结合并水解 ATP。在这里,我们展示了与 ATP 结合的大肠杆菌 Hfq(Hfq(65))的 C 端截断变体的晶体结构,表明它与远端 R 位结合。此外,我们重新研究了以前报道的纯化为均相的全长 Hfq 的 ATP 酶活性。与以前的报告不同,未观察到 Hfq 的 ATP 酶活性。此外,FRET 测定既没有表明 ATP 对两个模型寡核苷酸退火的影响,也没有表明 ATP 的存在诱导链置换。此外,除非使用大量的化学计量过量的 ATP,否则 ATP 不会导致二元和三元 Hfq-RNA 复合物的不稳定。总之,这些研究强烈表明,ATP 对于 Hfq 介导的 RNA 转导是可有可无的,并且不会干扰其过程。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/6c95/3511402/4513d6d5ce58/pone.0050892.g001.jpg

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