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cspA mRNA 作为热传感器调节冷休克蛋白 CspA 的翻译。

The cspA mRNA is a thermosensor that modulates translation of the cold-shock protein CspA.

机构信息

Laboratory of Genetics, Department of Biology MCA, University of Camerino, 62032 Camerino (MC), Italy.

出版信息

Mol Cell. 2010 Jan 15;37(1):21-33. doi: 10.1016/j.molcel.2009.11.033.

Abstract

Cold induction of cspA, the paradigm Escherichia coli cold-shock gene, is mainly subject to posttranscriptional control, partly promoted by cis-acting elements of its transcript, whose secondary structure at 37 degrees C and at cold-shock temperature has been elucidated here by enzymatic and chemical probing. The structures, which were also validated by mutagenesis, demonstrate that cspA mRNA undergoes a temperature-dependent structural rearrangement, likely resulting from stabilization in the cold of an otherwise thermodynamically unstable folding intermediate. At low temperature, the "cold-shock" structure is more efficiently translated and somewhat less susceptible to degradation than the 37 degrees C structure. Overall, our data shed light on a molecular mechanism at the basis of the cold-shock response, indicating that cspA mRNA is able to sense temperature downshifts, adopting functionally distinct structures at different temperatures, even without the aid of trans-acting factors. Unlike with other previously studied RNA thermometers, these structural rearrangements do not result from melting of hairpin structures.

摘要

冷诱导 cspA,模式大肠杆菌冷休克基因,主要受转录后控制,部分受其转录本顺式作用元件的促进,其在 37°C 和冷休克温度下的二级结构已通过酶和化学探测在这里阐明。这些结构也通过突变得到了验证,表明 cspA mRNA 经历了温度依赖性的结构重排,可能是由于在冷条件下,热力学不稳定的折叠中间体稳定。在低温下,“冷休克”结构比 37°C 结构的翻译效率更高,降解的敏感性也稍低。总的来说,我们的数据揭示了冷休克反应的基础上的分子机制,表明 cspA mRNA 能够感知温度下降,在不同的温度下采用功能不同的结构,即使没有辅助的反式作用因子。与其他先前研究的 RNA 温度计不同,这些结构重排不是由发夹结构的融解引起的。

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