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大肠杆菌hchA的调控,hchA是一个编码分子伴侣Hsp31的应激诱导基因。

Regulation of Escherichia coli hchA, a stress-inducible gene encoding molecular chaperone Hsp31.

作者信息

Mujacic Mirna, Baneyx François

机构信息

Department of Bioengineering, University of Washington, Seattle, WA, USA.

出版信息

Mol Microbiol. 2006 Jun;60(6):1576-89. doi: 10.1111/j.1365-2958.2006.05207.x.

DOI:10.1111/j.1365-2958.2006.05207.x
PMID:16796689
Abstract

Escherichia coli Hsp31 is a homodimeric member of the ThiI/DJ-1/PfpI superfamily that combines molecular chaperone and aminopeptidase activities. Although it was originally identified on the basis of its induction by heat shock, little is known about the regulation of hchA, the structural gene encoding Hsp31. Here, we show that hchA is transcribed from dual promoters recognized by the sigmaD (sigma70) and sigmaS (sigma38) subunits of RNA polymerase (E). In exponentially growing cells, the nucleoid-binding protein H-NS downregulates Hsp31 synthesis, and hchA thermal induction primarily relies on the relief of H-NS-mediated silencing of EsigmaD-dependent transcription. This uncommon alternative to the use of a heat-shock sigma factor guarantees that Hsp31 concentration remains high throughout the length of the high temperature exposure phase. Entry into stationary phase leads to enhanced hchA transcription from its EsigmaS-dependent promoter. Consistent with a role of Hsp31 in the management of starvation, hchA null mutants exhibit a decrease ability to survive in deep stationary phase relative to hchA+ cells. Based on hchA heat-inducibility and membership in the sigmaS general stress regulon, we propose that Hsp31 performs a protective function under a wide range of stress conditions.

摘要

大肠杆菌Hsp31是ThiI/DJ-1/PfpI超家族的同源二聚体成员,兼具分子伴侣和氨肽酶活性。尽管它最初是根据热休克诱导作用而被鉴定出来的,但对于编码Hsp31的结构基因hchA的调控机制却知之甚少。在此,我们表明hchA由RNA聚合酶(E)的σD(σ70)和σS(σ38)亚基识别的双重启动子转录。在指数生长的细胞中,类核结合蛋白H-NS下调Hsp31的合成,而hchA的热诱导主要依赖于H-NS介导的对σD依赖性转录沉默的解除。这种不寻常的使用热休克σ因子的替代方式确保了在整个高温暴露阶段Hsp31的浓度都保持较高水平。进入稳定期会导致hchA从其σS依赖性启动子转录增强。与Hsp31在饥饿管理中的作用一致,相对于hchA+细胞,hchA缺失突变体在深度稳定期的存活能力下降。基于hchA的热诱导性及其在σS一般应激调节子中的成员身份,我们提出Hsp31在广泛的应激条件下发挥保护作用。

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