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硫胺素衍生物直接结合信使核糖核酸以调控细菌基因表达。

Thiamine derivatives bind messenger RNAs directly to regulate bacterial gene expression.

作者信息

Winkler Wade, Nahvi Ali, Breaker Ronald R

机构信息

Department of Molecular, Cellular and Developmental Biology, Yale University, PO Box 208103, New Haven, Connecticut 06520-8103, USA.

出版信息

Nature. 2002 Oct 31;419(6910):952-6. doi: 10.1038/nature01145. Epub 2002 Oct 16.

Abstract

Although proteins fulfil most of the requirements that biology has for structural and functional components such as enzymes and receptors, RNA can also serve in these capacities. For example, RNA has sufficient structural plasticity to form ribozyme and receptor elements that exhibit considerable enzymatic power and binding specificity. Moreover, these activities can be combined to create allosteric ribozymes that are modulated by effector molecules. It has also been proposed that certain messenger RNAs might use allosteric mechanisms to mediate regulatory responses depending on specific metabolites. We report here that mRNAs encoding enzymes involved in thiamine (vitamin B(1)) biosynthesis in Escherichia coli can bind thiamine or its pyrophosphate derivative without the need for protein cofactors. The mRNA-effector complex adopts a distinct structure that sequesters the ribosome-binding site and leads to a reduction in gene expression. This metabolite-sensing regulatory system provides an example of a 'riboswitch' whose evolutionary origin might pre-date the emergence of proteins.

摘要

尽管蛋白质满足了生物学对诸如酶和受体等结构与功能组件的大部分需求,但RNA也能发挥这些作用。例如,RNA具有足够的结构可塑性,能够形成展现出相当酶活性和结合特异性的核酶及受体元件。此外,这些活性可以组合起来形成受效应分子调控的变构核酶。也有人提出,某些信使RNA可能利用变构机制根据特定代谢物介导调节反应。我们在此报告,编码大肠杆菌中参与硫胺素(维生素B1)生物合成的酶的信使RNA能够在无需蛋白质辅因子的情况下结合硫胺素或其焦磷酸衍生物。信使RNA-效应物复合物采用一种独特的结构,该结构会隔离核糖体结合位点并导致基因表达降低。这种代谢物感应调节系统提供了一个“核糖开关”的例子,其进化起源可能早于蛋白质的出现。

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