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首页> 外文期刊>Methods: A Companion to Methods in Enzymology >Structural dynamics of protein S1 on the 70S ribosome visualized by ensemble cryo-EM
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Structural dynamics of protein S1 on the 70S ribosome visualized by ensemble cryo-EM

机译:通过集合Cryo-em可视化70s核糖体蛋白质S1的结构动力学

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Bacterial ribosomal protein S1 is the largest and highly flexible protein of the 30S subunit, and one of a few core ribosomal proteins for which a complete structure is lacking. S1 is thought to participate in transcription and translation. Best understood is the role of S1 in facilitating translation of mRNAs with structured 5' UTRs. Here, we present cryo-EM analyses of the 70S ribosome that reveal multiple conformations of S1. Based on comparison of several 3D maximum likelihood classification approaches in Frealign, we propose a streamlined strategy for visualizing a highly dynamic component of a large macromolecular assembly that itself exhibits high compositional and conformational heterogeneity. The resulting maps show how SI docks at the ribosomal protein S2 near the mRNA exit channel. The globular OB-fold domains sample a wide area around the mRNA exit channel and interact with mobile tails of proteins S6 and S18. S1 also interacts with the mRNA entrance channel, where an OB-fold domain can be localized near S3 and 55. Our analyses suggest that S1 cooperates with other ribosomal proteins to form a dynamic mesh near the mRNA exit and entrance channels to modulate the binding, folding and movement of mRNA. (C) 2017 Elsevier Inc. All rights reserved.
机译:细菌核糖体蛋白S1是30s亚基的最大且高度柔韧的蛋白质,并且缺乏完整结构的少数核心核糖体蛋白之一。 S1被认为参与转录和翻译。最好理解的是S1在用结构化5'UTR的推动中促进MRNA的翻译。这里,我们呈现了70s核糖体的低温分析,其揭示了S1的多个构象。基于Frealign中的几个3D最大似然分类方法的比较,我们提出了一种简化的策略,用于可视化大型大分子组件的高度动态分量,本身表现出高的组成和构象异质性。得到的图显示了MRNA出口通道附近的核糖体蛋白S2的SI码头。球状ob折叠域在mRNA出口通道周围围绕宽面积并与蛋白质S6和S18的移动尾部相互作用。 S1还与mRNA入口通道相互作用,其中ob折域可以局部化在S3和55附近。我们的分析表明S1与其他核糖体蛋白配合,以在mRNA出口和入口通道附近形成动态网格以调节绑定, mRNA的折叠和运动。 (c)2017年Elsevier Inc.保留所有权利。

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