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线性过渡态折叠使翻译起始因子核糖开关能够快速适应温度变化。

Refolding through a Linear Transition State Enables Fast Temperature Adaptation of a Translational Riboswitch.

机构信息

Johann Wolfgang Goethe University, Institute of Organic Chemistry and Chemical Biology, Center for Biomolecular Magnetic Resonance (BMRZ), Max von Laue Strasse 7, 60438 Frankfurt/Main, Germany.

Institute of Organic Chemistry and Chemical Biology, Max von Laue Strasse 7, 60438 Frankfurt/Main, Germany.

出版信息

Biochemistry. 2020 Mar 17;59(10):1081-1086. doi: 10.1021/acs.biochem.9b01044. Epub 2020 Mar 9.

Abstract

The adenine-sensing riboswitch from the Gram-negative bacterium is an RNA-based gene regulatory element that acts in response to both its cognate low-molecular weight ligand and temperature. The combined sensitivity to environmental temperature and ligand concentration is maintained by an equilibrium of three distinct conformations involving two ligand-free states and one ligand-bound state. The key structural element that undergoes refolding in the ligand-free states comprises a 35-nucleotide temperature response module. Here, we present the structural characterization of this temperature response module. We employ high-resolution NMR spectroscopy and photocaged RNAs as molecular probes to decipher the kinetic and thermodynamic framework of the secondary structure transition in the apo state of the riboswitch. We propose a model for the transition state adopted during the thermal refolding of the temperature response module that connects two mutually exclusive long-lived and stable conformational states. This transition state is characterized by a comparatively low free activation enthalpy. A pseudoknot conformation in the transition state, as commonly seen in RNA refolding, is therefore unlikely. More likely, the transition state of the adenine-sensing riboswitch temperature response module features a linear conformation.

摘要

来自革兰氏阴性菌的腺嘌呤感应核糖开关是一种基于 RNA 的基因调控元件,可响应其同源的低分子量配体和温度。对环境温度和配体浓度的综合敏感性是通过涉及两种无配体状态和一种配体结合状态的三种不同构象的平衡来维持的。在无配体状态下经历重折叠的关键结构元件包括 35 个核苷酸的温度响应模块。在这里,我们介绍了这种温度响应模块的结构特征。我们采用高分辨率 NMR 光谱和光笼 RNA 作为分子探针,以破译核糖开关无配体状态下二级结构转变的动力学和热力学框架。我们提出了一个模型,用于连接两个相互排斥的长寿命和稳定构象状态的温度响应模块在热折叠过程中采用的过渡状态。这个过渡状态的自由焓变较低。因此,在 RNA 重折叠中常见的假结构象不太可能存在。更有可能的是,腺嘌呤感应核糖开关温度响应模块的过渡状态具有线性构象。

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