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一种由PhoQ/P调控的小RNA调节大肠杆菌对抗菌肽的敏感性。

A PhoQ/P-regulated small RNA regulates sensitivity of Escherichia coli to antimicrobial peptides.

作者信息

Moon Kyung, Gottesman Susan

机构信息

Laboratory of Molecular Biology, Center for Cancer Research, National Cancer Institute, Bethesda, MD 20892, USA.

出版信息

Mol Microbiol. 2009 Dec;74(6):1314-30. doi: 10.1111/j.1365-2958.2009.06944.x. Epub 2009 Nov 2.

Abstract

Non-coding small RNAs (sRNAs) play a major role in post-transcriptional regulation of gene expression. Of the 80 sRNAs that have been identified in E. coli, one-third bind to the RNA chaperone Hfq. Hfq both stabilizes these sRNAs in vivo and stimulates pairing to targets in vitro. A novel Hfq-dependent RNA, called here MgrR, was identified by its ability to bind Hfq. Expression of MgrR requires the PhoQ/PhoP two-component system; the PhoP response regulator is active under low Mg2+ concentrations and is an important virulence regulator in Salmonella; mgrR is also found in Salmonella species. Negatively regulated targets of MgrR identified using microarrays include eptB, involved in lipopolysaccharide (LPS) modification, and ygdQ, encoding a hypothetical protein. Cell sensitivity to the antimicrobial polymyxin B is affected by LPS modifications, and cells carrying an mgrR deletion were approximately 10 times more resistant than wild-type cells to polymyxin B. Thus, lower Mg2+ concentrations, sensed by PhoQ/PhoP, lead to expression of MgrR, changing LPS. sRNAs have previously been shown to regulate many outer membrane proteins. This work demonstrates that LPS, a major contributor of bacterial interactions with mammalian cells, is also subject to regulation by sRNAs.

摘要

非编码小RNA(sRNA)在基因表达的转录后调控中发挥着重要作用。在大肠杆菌中已鉴定出的80种sRNA中,三分之一与RNA伴侣Hfq结合。Hfq在体内可稳定这些sRNA,并在体外促进其与靶标的配对。一种新的依赖Hfq的RNA,这里称为MgrR,通过其与Hfq结合的能力被鉴定出来。MgrR的表达需要PhoQ/PhoP双组分系统;PhoP反应调节因子在低镁离子浓度下具有活性,是沙门氏菌中一种重要的毒力调节因子;mgrR在沙门氏菌属中也有发现。利用微阵列鉴定出的MgrR的负调控靶标包括参与脂多糖(LPS)修饰的eptB和编码一种假定蛋白的ygdQ。细胞对抗菌多粘菌素B的敏感性受LPS修饰的影响,携带mgrR缺失的细胞对多粘菌素B的抗性比野生型细胞高约10倍。因此,PhoQ/PhoP感知到的较低镁离子浓度会导致MgrR的表达,从而改变LPS。此前已证明sRNA可调控许多外膜蛋白。这项研究表明,LPS作为细菌与哺乳动物细胞相互作用的主要贡献者,也受到sRNA的调控。

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