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无帽依赖翻译增强 RNA 的晶体结构

Crystal structure of a cap-independent translation enhancer RNA.

机构信息

Department of Biochemistry and Molecular Biology, The University of Chicago, Chicago, IL 60637, USA.

Department of Chemistry, The University of Chicago, Chicago, IL 60637, USA.

出版信息

Nucleic Acids Res. 2023 Sep 8;51(16):8891-8907. doi: 10.1093/nar/gkad649.

Abstract

In eukaryotic messenger RNAs, the 5' cap structure binds to the translation initiation factor 4E to facilitate early stages of translation. Although many plant viruses lack the 5' cap structure, some contain cap-independent translation elements (CITEs) in their 3' untranslated region. The PTE (Panicum mosaic virus translation element) class of CITEs contains a G-rich asymmetric bulge and a C-rich helical junction that were proposed to interact via formation of a pseudoknot. SHAPE analysis of PTE homologs reveals a highly reactive guanosine residue within the G-rich region proposed to mediate eukaryotic initiation factor 4E (eIF4E) recognition. Here we have obtained the crystal structure of the PTE from Pea enation mosaic virus 2 (PEMV2) RNA in complex with our structural chaperone, Fab BL3-6. The structure reveals that the G-rich and C-rich regions interact through a complex network of interactions distinct from those expected for a pseudoknot. The motif, which contains a short parallel duplex, provides a structural mechanism for how the guanosine is extruded from the core stack to enable eIF4E recognition. Homologous PTE elements harbor a G-rich bulge and a three-way junction and exhibit covariation at crucial positions, suggesting that the PEMV2 tertiary architecture is conserved among these homologs.

摘要

在真核信使 RNA 中,5'帽结构与翻译起始因子 4E 结合,以促进翻译的早期阶段。尽管许多植物病毒缺乏 5'帽结构,但它们的 3'非翻译区中含有非依赖帽结构的翻译元件 (CITEs)。PTE(Panicum mosaic virus translation element)类 CITE 包含富含 G 的不对称凸起和富含 C 的螺旋连接,据推测它们通过形成假结相互作用。PTE 同源物的 SHAPE 分析揭示了 G 富含区中一个高度反应性的鸟嘌呤残基,据推测该残基介导真核起始因子 4E (eIF4E) 的识别。在这里,我们获得了豌豆花叶病毒 2 (PEMV2) RNA 中 PTE 的晶体结构,与我们的结构伴侣 Fab BL3-6 复合。该结构揭示了富含 G 和富含 C 的区域通过与假结预期的不同的复杂相互作用网络相互作用。该基序包含一个短的平行双链,为鸟嘌呤如何从核心堆叠中挤出以实现 eIF4E 识别提供了结构机制。同源的 PTE 元件含有富含 G 的凸起和三链连接,并在关键位置表现出变异性,表明这些同源物中 PEMV2 的三级结构是保守的。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/632f/10484670/1cd180f480ca/gkad649figgra1.jpg

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