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首页> 外文期刊>Molecular Microbiology >Regulation of CsrB/C sRNA decay by EIIA(Glc) of the phosphoenolpyruvate: carbohydrate phosphotransferase system
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Regulation of CsrB/C sRNA decay by EIIA(Glc) of the phosphoenolpyruvate: carbohydrate phosphotransferase system

机译:磷酸烯醇丙酮酸的EIIA(Glc)对CsrB / C sRNA衰变的调控:碳水化合物磷酸转移酶系统

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摘要

Csr is a conserved global regulatory system, which uses the sequence-specific RNA-binding protein CsrA to activate or repress gene expression by binding to mRNA and altering translation, stability and/or transcript elongation. In Escherichia coli, CsrA activity is regulated by two sRNAs, CsrB and CsrC, which bind to multiple CsrA dimers, thereby sequestering this protein away from its mRNA targets. Turnover of CsrB/C sRNAs is tightly regulated by a GGDEF-EAL domain protein, CsrD, which targets them for cleavage by RNase E. Here, we show that EIIA(Glc) of the glucose-specific PTS system is also required for the normal decay of these sRNAs and that it acts by binding to the EAL domain of CsrD. Only the unphosphorylated form of EIIA(Glc) bound to CsrDin vitro and was capable of activating CsrB/C turnover in vivo. Genetic studies confirmed that this mechanism couples CsrB/C sRNA decay to the availability of a preferred carbon source. These findings reveal a new physiological influence on the workings of the Csr system, a novel function for the EAL domain, and an important new way in which EIIA(Glc) shapes global regulatory circuitry in response to nutritional status.
机译:Csr是一种保守的全球调节系统,它使用序列特异性RNA结合蛋白CsrA通过与mRNA结合并改变翻译,稳定性和/或转录本延伸来激活或抑制基因表达。在大肠杆菌中,CsrA的活性受两个sRNA(CsrB和CsrC)的调节,这两个sRNA与多个CsrA二聚体结合,从而使该蛋白质与mRNA靶位隔离。 CsrB / C sRNA的成交量受到GGDEF-EAL域蛋白CsrD的​​严格调控,该蛋白将它们靶向RNase E进行切割。在这里,我们证明了正常葡萄糖还需要葡萄糖特异性PTS系统的EIIA(Glc)这些sRNA的衰变及其通过与CsrD的​​EAL域结合而起作用。 EIIA(Glc)的只有非磷酸化形式在体外与CsrD结合,并能够在体内激活CsrB / C转换。遗传研究证实,这种机制将CsrB / C sRNA衰变与首选碳源的可用性联系在一起。这些发现揭示了对Csr系统运作的新生理影响,EAL域的新功能以及EIIA(Glc)响应营养状况影响全球调节回路的重要新方法。

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