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大肠杆菌中小调控RNA及其mRNA靶标的偶联降解

Coupled degradation of a small regulatory RNA and its mRNA targets in Escherichia coli.

作者信息

Massé Eric, Escorcia Freddy E, Gottesman Susan

机构信息

Laboratory of Molecular Biology, National Cancer Institute, National Institutes of Health, Bethesda, Maryland 20892, USA.

出版信息

Genes Dev. 2003 Oct 1;17(19):2374-83. doi: 10.1101/gad.1127103. Epub 2003 Sep 15.

Abstract

RyhB is a small antisense regulatory RNA that is repressed by the Fur repressor and negatively regulates at least six mRNAs encoding Fe-binding or Fe-storage proteins in Escherichia coli. When Fe is limiting, RyhB levels rise, and target mRNAs are rapidly degraded. RyhB is very stable when measured after treatment of cells with the transcription inhibitor rifampicin, but is unstable when overall mRNA transcription continues. We propose that RyhB turnover is coupled to and dependent on pairing with the target mRNAs. Degradation of both mRNA targets and RyhB is dependent on RNase E and is slowed in degradosome mutants. RyhB requires the RNA chaperone Hfq. In the absence of Hfq, RyhB is unstable, even when general transcription is inhibited; degradation is dependent upon RNase E. Hfq and RNase E bind similar sites on the RNA; pairing may allow loss of Hfq and access by RNase E. Two other Hfq-dependent small RNAs, DsrA and OxyS, are also stable when overall transcription is off, and unstable when it is not, suggesting that they, too, are degraded when their target mRNAs are available for pairing. Thus, this large class of regulatory RNAs share an unexpected intrinsic mechanism for shutting off their action.

摘要

RyhB是一种小的反义调控RNA,受铁摄取调节蛋白(Fur)阻遏物的抑制,并在大肠杆菌中负调控至少六种编码铁结合或铁储存蛋白的mRNA。当铁含量有限时,RyhB水平升高,其靶mRNA会迅速降解。在用转录抑制剂利福平处理细胞后检测时,RyhB非常稳定,但在整体mRNA转录继续进行时则不稳定。我们提出,RyhB的周转与靶mRNA的配对相关并依赖于此。mRNA靶标和RyhB的降解均依赖于核糖核酸酶E(RNase E),并且在降解体突变体中会减缓。RyhB需要RNA伴侣蛋白Hfq。在没有Hfq的情况下,即使一般转录受到抑制,RyhB也不稳定;其降解依赖于RNase E。Hfq和RNase E结合在RNA上的相似位点;配对可能会使Hfq脱离,并使RNase E得以作用。另外两个依赖Hfq的小RNA,DsrA和OxyS,在整体转录关闭时也很稳定,而在转录未关闭时则不稳定,这表明当它们的靶mRNA可用于配对时,它们也会被降解。因此,这类大量的调控RNA具有一种意想不到的内在机制来终止其作用。

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