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Bacterial small-molecule signaling pathways.细菌小分子信号通路。
Science. 2006 Feb 24;311(5764):1113-6. doi: 10.1126/science.1121357.
2
Dendritic BC1 RNA in translational control mechanisms.翻译控制机制中的树突状BC1 RNA
J Cell Biol. 2005 Dec 5;171(5):811-21. doi: 10.1083/jcb.200506006.
3
CsrA and three redundant small RNAs regulate quorum sensing in Vibrio cholerae.CsrA和三种冗余小RNA调节霍乱弧菌中的群体感应。
Mol Microbiol. 2005 Nov;58(4):1186-202. doi: 10.1111/j.1365-2958.2005.04902.x.
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A chemosensory system that regulates biofilm formation through modulation of cyclic diguanylate levels.一种通过调节环二鸟苷水平来调控生物膜形成的化学感应系统。
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Phenotypic convergence mediated by GGDEF-domain-containing proteins.由含GGDEF结构域的蛋白质介导的表型趋同。
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RNase E-based ribonucleoprotein complexes: mechanical basis of mRNA destabilization mediated by bacterial noncoding RNAs.基于核糖核酸酶E的核糖核蛋白复合物:细菌非编码RNA介导的mRNA去稳定化的力学基础
Genes Dev. 2005 Sep 15;19(18):2176-86. doi: 10.1101/gad.1330405.
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RNA sequence and secondary structure participate in high-affinity CsrA-RNA interaction.RNA序列和二级结构参与CsrA-RNA的高亲和力相互作用。
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8
The EAL domain protein VieA is a cyclic diguanylate phosphodiesterase.EAL结构域蛋白VieA是一种环二鸟苷酸磷酸二酯酶。
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C-di-GMP: the dawning of a novel bacterial signalling system.环二鸟苷酸:一种新型细菌信号系统的兴起
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The ubiquitous protein domain EAL is a cyclic diguanylate-specific phosphodiesterase: enzymatically active and inactive EAL domains.普遍存在的蛋白质结构域EAL是一种环二鸟苷酸特异性磷酸二酯酶:具有酶活性和无酶活性的EAL结构域。
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鉴定一种新型调控蛋白(CsrD),该蛋白靶向全局调控RNA CsrB和CsrC,使其被核糖核酸酶E降解。

Identification of a novel regulatory protein (CsrD) that targets the global regulatory RNAs CsrB and CsrC for degradation by RNase E.

作者信息

Suzuki Kazushi, Babitzke Paul, Kushner Sidney R, Romeo Tony

机构信息

Department of Microbiology and Immunology, Emory University School of Medicine, Atlanta, Georgia 30322, USA.

出版信息

Genes Dev. 2006 Sep 15;20(18):2605-17. doi: 10.1101/gad.1461606.

DOI:10.1101/gad.1461606
PMID:16980588
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC1578682/
Abstract

In Escherichia coli, the global regulatory protein CsrA (carbon store regulator A) binds to leader segments of target mRNAs, affecting their translation and stability. CsrA activity is regulated by two noncoding RNAs, CsrB and CsrC, which act by sequestering multiple CsrA dimers. Here, we describe a protein (CsrD) that controls the degradation of CsrB/C RNAs. The dramatic stabilization of CsrB/C RNAs in a csrD mutant altered the expression of CsrA-controlled genes in a manner predicted from the previously described Csr regulatory circuitry. A deficiency in RNase E, the primary endonuclease involved in mRNA decay, also stabilized CsrB/C, although the half-lives of other RNAs that are substrates for RNase E (rpsO, rpsT, and RyhB) were unaffected by csrD. Analysis of the decay of CsrB RNA, both in vitro and in vivo, suggested that CsrD is not a ribonuclease. Interestingly, the CsrD protein contains GGDEF and EAL domains, yet unlike typical proteins in this large superfamily, its activity in the regulation of CsrB/C decay does not involve cyclic di-GMP metabolism. The two predicted membrane-spanning regions are dispensable for CsrD activity, while HAMP-like, GGDEF, and EAL domains are required. Thus, these studies demonstrate a novel process for the selective targeting of RNA molecules for degradation by RNase E and a novel function for a GGDEF-EAL protein.

摘要

在大肠杆菌中,全局调节蛋白CsrA(碳储存调节因子A)与靶标mRNA的前导序列结合,影响其翻译和稳定性。CsrA的活性受两种非编码RNA即CsrB和CsrC的调节,它们通过螯合多个CsrA二聚体发挥作用。在此,我们描述了一种控制CsrB/C RNA降解的蛋白质(CsrD)。在csrD突变体中CsrB/C RNA的显著稳定以先前描述的Csr调节电路所预测的方式改变了CsrA控制基因的表达。参与mRNA降解的主要内切核酸酶RNase E的缺陷也使CsrB/C稳定,尽管作为RNase E底物的其他RNA(rpsO、rpsT和RyhB)的半衰期不受csrD影响。对CsrB RNA在体外和体内降解的分析表明CsrD不是一种核糖核酸酶。有趣的是,CsrD蛋白含有GGDEF和EAL结构域,但与这个大型超家族中的典型蛋白不同,其在调节CsrB/C降解中的活性不涉及环二鸟苷酸代谢。两个预测的跨膜区域对于CsrD活性是可有可无的,而类似HAMP的、GGDEF和EAL结构域是必需的。因此,这些研究证明了一种将RNA分子选择性靶向由RNase E降解的新过程以及一种GGDEF-EAL蛋白的新功能。