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玉米坏死条纹病毒 3' mRNA I 型结构结合真核翻译因子,通过 eIF4F 介导翻译起始。

The 3' mRNA I-shaped structure of maize necrotic streak virus binds to eukaryotic translation factors for eIF4F-mediated translation initiation.

机构信息

From the Biochemistry and Chemistry Graduate Programs, Graduate Center the City University of New York and.

Department of Chemistry and Biochemistry, Hunter College, City University of New York, New York, New York 10065.

出版信息

J Biol Chem. 2018 Jun 15;293(24):9486-9495. doi: 10.1074/jbc.RA118.003377. Epub 2018 Apr 26.

Abstract

Unlike the mRNAs of their eukaryotic hosts, many RNAs of viruses lack a 5' mGpppN cap and the 3' polyadenosine tail, and yet they are translated efficiently. Plant RNA viruses, in particular, have complex structures within their mRNA UTRs that allow them to bypass some cellular translation control steps. In the 3' UTR of maize necrotic streak virus (MNeSV), an I-shaped RNA structure (ISS) has been shown to bind eukaryotic initiation factor (eIF)4F and to mediate viral translation initiation. A 5'-3' RNA "kissing-loop" interaction is required for optimal translation. However, the details of how the 3' ISS mediates translation initiation are not well understood. Here, we studied the binding of the 3' ISS with eIFs. The eIF4A-eIF4B complex was found to increase binding affinity of eIF4F with the 3' ISS by 4-fold (from = 173 ± 34 nm to = 48 ± 11 nm). Pre-steady-state analysis indicated that the eIF4A-eIF4B complex increased the RNA association rate and decreased the dissociation rate in an ATP-independent manner. Furthermore, our findings suggest that eIF4F could promote binding of the 3' ISS with the MNeSV 5'UTR, enhancing the long-distance kissing-loop interaction. However, the association of the 5'UTR with the 3' ISS-eIF4F complex did not increase 40S ribosomal subunit binding affinity. These quantitative results suggest a stepwise model in which the first committed step is eIF4F binding to the 3' ISS, followed by an interaction with the 5'UTR and subsequent 40S ribosomal subunit binding.

摘要

与真核宿主的 mRNAs 不同,许多病毒的 RNA 缺乏 5' mGpppN 帽和 3' 聚腺苷酸尾巴,但它们的翻译效率很高。特别是植物 RNA 病毒,其 mRNA UTR 内具有复杂的结构,使其能够绕过一些细胞翻译控制步骤。在玉米坏死条纹病毒(MNeSV)的 3'UTR 中,已经证明一种 I 形 RNA 结构(ISS)可以结合真核起始因子(eIF)4F,并介导病毒翻译起始。5'-3'RNA“亲吻环”相互作用是翻译的最佳条件。然而,3'ISS 介导翻译起始的细节尚不清楚。在这里,我们研究了 3'ISS 与 eIFs 的结合。发现 eIF4A-eIF4B 复合物使 eIF4F 与 3'ISS 的结合亲和力增加了 4 倍(从 = 173 ± 34nm 变为 = 48 ± 11nm)。预稳态分析表明,eIF4A-eIF4B 复合物以非依赖 ATP 的方式增加了 RNA 的结合速率并降低了解离速率。此外,我们的研究结果表明,eIF4F 可以促进 MNeSV 5'UTR 与 3'ISS 的结合,增强远距离亲吻环相互作用。然而,5'UTR 与 3'ISS-eIF4F 复合物的结合并没有增加 40S 核糖体亚基的结合亲和力。这些定量结果表明了一个逐步的模型,其中第一步是 eIF4F 与 3'ISS 的结合,然后是与 5'UTR 的相互作用以及随后的 40S 核糖体亚基的结合。

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