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溶液中核糖核酸酶P RNA的构象空间。

The conformational space of RNase P RNA in solution.

作者信息

Lee Yun-Tzai, Degenhardt Maximilia F S, Skeparnias Ilias, Degenhardt Hermann F, Bhandari Yuba R, Yu Ping, Stagno Jason R, Fan Lixin, Zhang Jinwei, Wang Yun-Xing

机构信息

Protein-Nucleic Acid Interaction Section, Center for Structural Biology, National Cancer Institute, Frederick, MD, USA.

Laboratory of Molecular Biology, National Institute of Diabetes and Digestive and Kidney Diseases, Bethesda, MD, USA.

出版信息

Nature. 2025 Jan;637(8048):1244-1251. doi: 10.1038/s41586-024-08336-6. Epub 2024 Dec 18.

Abstract

RNA conformational diversity has fundamental biological roles, but direct visualization of its full conformational space in solution has not been possible using traditional biophysical techniques. Using solution atomic force microscopy, a deep neural network and statistical analyses, we show that the ribonuclease P (RNase P) RNA adopts heterogeneous conformations consisting of a conformationally invariant core and highly flexible peripheral structural elements that sample a broad conformational space, with amplitudes as large as 20-60 Å in a multitude of directions, with very low net energy cost. Increasing Mg drives compaction and enhances enzymatic activity, probably by narrowing the conformational space. Moreover, analyses of the correlations and anticorrelations between spatial flexibility and sequence conservation suggest that the functional roles of both the structure and dynamics of key regions are embedded in the primary sequence. These findings reveal the structure-dynamics basis for the embodiment of both enzymatic precision and substrate promiscuity in the RNA component of the RNase P. Mapping the conformational space of the RNase P RNA demonstrates a new general approach to studying RNA structure and dynamics.

摘要

RNA构象多样性具有重要的生物学作用,但利用传统生物物理技术无法直接观察其在溶液中的完整构象空间。我们使用溶液原子力显微镜、深度神经网络和统计分析表明,核糖核酸酶P(RNase P)RNA呈现出异质构象,由构象不变的核心和高度灵活的外围结构元件组成,这些元件可在广阔的构象空间中进行采样,在多个方向上振幅高达20 - 60埃,净能量成本非常低。增加镁离子会促使其压缩并增强酶活性,可能是通过缩小构象空间来实现的。此外,对空间灵活性和序列保守性之间的相关性和反相关性分析表明,关键区域的结构和动力学的功能作用都嵌入在一级序列中。这些发现揭示了RNase P的RNA组分中酶促精确性和底物通用性体现的结构 - 动力学基础。绘制RNase P RNA的构象空间图展示了一种研究RNA结构和动力学的新通用方法。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/424e/11779636/fb18a563a27a/41586_2024_8336_Fig1_HTML.jpg

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