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Hfq在鼠疫耶尔森菌中全局结合并使小RNA和信使核糖核酸不稳定。

Hfq Globally Binds and Destabilizes sRNAs and mRNAs in Yersinia pestis.

作者信息

Han Yanping, Chen Dong, Yan Yanfeng, Gao Xiaofang, Liu Zizhong, Xue Yaqiang, Zhang Yi, Yang Ruifu

机构信息

State Key Laboratory of Pathogen and Biosecurity, Beijing Institute of Microbiology and Epidemiology, Beijing, China.

Center for Genome Analysis, ABLife Inc., Wuhan, Hubei, China.

出版信息

mSystems. 2019 Jul 16;4(4):e00245-19. doi: 10.1128/mSystems.00245-19.

Abstract

Hfq is a ubiquitous Sm-like RNA-binding protein in bacteria involved in physiological fitness and pathogenesis, while its binding nature remains elusive. Here we reported genome-wide Hfq-bound RNAs in , a causative agent of plague, by using cross-linking immunoprecipitation coupled with deep sequencing (CLIP-seq) approach. We show that the Hfq binding density is enriched in more than 80% mRNAs of and that Hfq also globally binds noncoding small RNAs (sRNAs) encoded by the intergenic, antisense, and 3' regions of mRNAs. An Hfq U-rich stretch is highly enriched in sRNAs, while motifs partially complementary to AGAAUAA and GGGGAUUA are enriched in both mRNAs and sRNAs. Hfq-binding motifs are enriched at both terminal sites and in the gene body of mRNAs. Surprisingly, a large fraction of the sRNA and mRNA regions bound by Hfq and those downstream are destabilized, likely via a 5'P-activated RNase E degradation pathway, which is consistent with a model in which Hfq facilitates sRNA-mRNA base pairing and the coupled degradation in These results together have presented a high-quality Hfq-RNA interaction map in , which should be important for further deciphering the regulatory role of Hfq-sRNAs in Discovered in 1968 as an host factor that was essential for replication of the bacteriophage Qβ, the Hfq protein is a ubiquitous and highly abundant RNA-binding protein in many bacteria. With the assistance of Hfq, small RNAs in bacteria play important roles in regulating the stability and translation of mRNAs by base pairing. In this study, we want to elucidate the Hfq-assisted sRNA-mRNA regulation in A global map of Hfq interaction sites in was obtained by sequencing cDNAs converted from the Hfq-bound RNA fragments using UV cross-linking coupled immunoprecipitation technology. We demonstrate that Hfq could bind to hundreds of sRNAs and the majority of mRNAs in The enriched binding motifs in sRNAs and mRNAs are complementary to each other, suggesting a general base-pairing mechanism for sRNA-mRNA interaction. The Hfq-bound sRNA and mRNA regions were both destabilized. The results suggest that Hfq binding facilitates sRNA-mRNA base pairing and coordinates their degradation, which might enable Hfq to surveil the homeostasis of most mRNAs in bacteria.

摘要

Hfq是细菌中一种普遍存在的类Sm RNA结合蛋白,参与生理适应性和致病过程,但其结合性质仍不清楚。在这里,我们通过使用交联免疫沉淀结合深度测序(CLIP-seq)方法,报道了鼠疫病原体耶尔森菌全基因组范围内与Hfq结合的RNA。我们发现,超过80%的耶尔森菌mRNA中Hfq结合密度增加,并且Hfq还全局结合由mRNA的基因间、反义及3'区域编码的非编码小RNA(sRNA)。富含U的Hfq序列在sRNA中高度富集,而与AGAAUAA和GGGGAUUA部分互补的基序在mRNA和sRNA中均有富集。Hfq结合基序在mRNA的末端位点和基因体内均有富集。令人惊讶的是,很大一部分与Hfq结合的sRNA和mRNA区域及其下游区域不稳定,可能是通过5'P激活的核糖核酸酶E降解途径,这与Hfq促进sRNA-mRNA碱基配对及在耶尔森菌中的偶联降解的模型一致。这些结果共同呈现了耶尔森菌中高质量的Hfq-RNA相互作用图谱,这对于进一步解读Hfq-sRNA在耶尔森菌中的调控作用应该是重要的。Hfq蛋白于1968年作为噬菌体Qβ复制所必需的宿主因子被发现,是许多细菌中普遍存在且高度丰富的RNA结合蛋白。在Hfq的协助下,细菌中的小RNA通过碱基配对在调节mRNA的稳定性和翻译中发挥重要作用。在本研究中,我们想阐明耶尔森菌中Hfq辅助的sRNA-mRNA调控。通过使用紫外线交联偶联免疫沉淀技术对与Hfq结合的RNA片段转化的cDNA进行测序,获得了耶尔森菌中Hfq相互作用位点的全局图谱。我们证明Hfq可以结合耶尔森菌中的数百种sRNA和大多数mRNA。sRNA和mRNA中富集的结合基序相互互补,表明sRNA-mRNA相互作用存在普遍的碱基配对机制。与Hfq结合的sRNA和mRNA区域均不稳定。结果表明,Hfq结合促进sRNA-mRNA碱基配对并协调它们的降解,这可能使Hfq能够监测细菌中大多数mRNA的稳态。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/18dc/6635623/f395f18b5289/mSystems.00245-19-f0001.jpg

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