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病毒 mRNA 5'UTR 上的一个复杂 IRES 通过 uAUG 中间产物组装功能性 48S 复合物。

A complex IRES at the 5'-UTR of a viral mRNA assembles a functional 48S complex via an uAUG intermediate.

机构信息

Department of Biological Sciences, Columbia University, New York, United States.

Department of Biochemistry and Molecular Biophysics, Columbia University, New York, United States.

出版信息

Elife. 2020 Apr 14;9:e54575. doi: 10.7554/eLife.54575.

Abstract

Taking control of the cellular apparatus for protein production is a requirement for virus progression. To ensure this control, diverse strategies of cellular mimicry and/or ribosome hijacking have evolved. The initiation stage of translation is especially targeted as it involves multiple steps and the engagement of numerous initiation factors. The use of structured RNA sequences, called nternal ibosomal ntry ites (IRES), in viral RNAs is a widespread strategy for the exploitation of eukaryotic initiation. Using a combination of electron cryo-microscopy (cryo-EM) and reconstituted translation initiation assays with native components, we characterized how a novel IRES at the 5'-UTR of a viral RNA assembles a functional initiation complex via an uAUG intermediate. The IRES features a novel extended, multi-domain architecture, that circles the 40S head. The structures and accompanying functional data illustrate the importance of 5'-UTR regions in translation regulation and underline the relevance of the untapped diversity of viral IRESs.

摘要

控制细胞的蛋白质生产机制是病毒进展的必要条件。为了确保这种控制,细胞模拟和/或核糖体劫持的各种策略已经进化。翻译的起始阶段是特别针对的,因为它涉及多个步骤和许多起始因子的参与。在病毒 RNA 中使用称为内部核糖体进入位点(IRES)的结构化 RNA 序列是利用真核起始的广泛策略。我们使用电子低温显微镜(cryo-EM)和用天然成分重建的翻译起始测定的组合,通过 uAUG 中间体表征了病毒 RNA 5'UTR 上的新型 IRES 如何组装功能性起始复合物。IRES 具有新颖的扩展多结构域架构,环绕 40S 头部。结构和伴随的功能数据说明了 5'UTR 区域在翻译调节中的重要性,并强调了病毒 IRES 未开发多样性的相关性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/a39c/7190351/66709d16e4a9/elife-54575-fig1.jpg

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