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三态机制将配体和温度感应偶联在核糖开关中。

Three-state mechanism couples ligand and temperature sensing in riboswitches.

机构信息

Center for Biomolecular Magnetic Resonance, Institute of Organic Chemistry and Chemical Biology, Johann Wolfgang Goethe-Universität Frankfurt am Main, Max-von-Laue-Strasse 7, 60438 Frankfurt am Main, Germany.

出版信息

Nature. 2013 Jul 18;499(7458):355-9. doi: 10.1038/nature12378. Epub 2013 Jul 10.

Abstract

Riboswitches are cis-acting gene-regulatory RNA elements that can function at the level of transcription, translation and RNA cleavage. The commonly accepted molecular mechanism for riboswitch function proposes a ligand-dependent conformational switch between two mutually exclusive states. According to this mechanism, ligand binding to an aptamer domain induces an allosteric conformational switch of an expression platform, leading to activation or repression of ligand-related gene expression. However, many riboswitch properties cannot be explained by a pure two-state mechanism. Here we show that the regulation mechanism of the adenine-sensing riboswitch, encoded by the add gene on chromosome II of the human Gram-negative pathogenic bacterium Vibrio vulnificus, is notably different from a two-state switch mechanism in that it involves three distinct stable conformations. We characterized the temperature and Mg(2+) dependence of the population ratios of the three conformations and the kinetics of their interconversion at nucleotide resolution. The observed temperature dependence of a pre-equilibrium involving two structurally distinct ligand-free conformations of the add riboswitch conferred efficient regulation over a physiologically relevant temperature range. Such robust switching is a key requirement for gene regulation in bacteria that have to adapt to environments with varying temperatures. The translational adenine-sensing riboswitch represents the first example, to our knowledge, of a temperature-compensated regulatory RNA element.

摘要

核糖开关是顺式作用的基因调控 RNA 元件,可在转录、翻译和 RNA 切割水平发挥作用。普遍接受的核糖开关功能分子机制提出了两种相互排斥状态之间配体依赖性构象转换。根据该机制,配体与适体结构域的结合诱导表达平台的变构构象转换,导致与配体相关的基因表达的激活或抑制。然而,许多核糖开关的特性不能用纯二态机制来解释。在这里,我们表明,人革兰氏阴性致病性细菌创伤弧菌染色体 II 上的 add 基因编码的腺嘌呤感应核糖开关的调控机制明显不同于二态开关机制,因为它涉及三种不同的稳定构象。我们表征了三种构象的群体比例的温度和 Mg2+依赖性以及它们在核苷酸分辨率下的相互转换动力学。观察到的涉及 add 核糖开关两种结构上不同的无配体自由构象的预平衡的温度依赖性赋予了在生理相关温度范围内的有效调控。这种稳健的开关是细菌中基因调控的关键要求,细菌必须适应具有不同温度的环境。翻译腺嘌呤感应核糖开关是我们所知的第一个温度补偿调节 RNA 元件的例子。

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