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非灵长类肝炎病毒5'非翻译区在翻译起始和病毒复制中的作用

Roles of the 5' Untranslated Region of Nonprimate Hepacivirus in Translation Initiation and Viral Replication.

作者信息

Tanaka Tomohisa, Otoguro Teruhime, Yamashita Atsuya, Kasai Hirotake, Fukuhara Takasuke, Matsuura Yoshiharu, Moriishi Kohji

机构信息

Department of Microbiology, Graduate School of Medical Science, University of Yamanashi, Yamanashi, Japan.

Department of Molecular Virology, Research Institute for Microbial Diseases, Osaka University, Osaka, Japan.

出版信息

J Virol. 2018 Mar 14;92(7). doi: 10.1128/JVI.01997-17. Print 2018 Apr 1.

Abstract

The 5' untranslated region (UTR) of hepatitis C virus (HCV), which is composed of four domains (I, II, III, and IV) and a pseudoknot, is essential for translation and viral replication. Equine nonprimate hepacivirus (EHcV) harbors a 5' UTR consisting of a large 5'-terminal domain (I); three additional domains (I', II, and III), which are homologous to domains I, II, and III, respectively, of HCV; and a pseudoknot, in the order listed. In this study, we investigated the roles of the EHcV 5' UTR in translation and viral replication. The internal ribosome entry site (IRES) activity of the EHcV 5' UTR was lower than that of the HCV 5' UTR in several cell lines due to structural differences in domain III. Domains I and III of EHcV were functional in the HCV 5' UTR in terms of IRES activity and the replication of the subgenomic replicon (SGR), although domain II was not exchangeable between EHcV and HCV for SGR replication. Furthermore, the region spanning domains I and I' of EHcV (the 5'-proximal EHcV-specific region) improved RNA stability and provided the HCV SGR with microRNA 122 (miR-122)-independent replication capability, while EHcV domain I alone improved SGR replication and RNA stability irrespective of miR-122. These data suggest that the region spanning EHcV domains I and I' improves RNA stability and viral replication regardless of miR-122 expression. The 5'-proximal EHcV-specific region may represent an inherent mechanism to facilitate viral replication in nonhepatic tissues. EHcV is the closest viral homolog to HCV among other hepaciviruses. HCV exhibits a narrow host range and liver-specific tropism, while epidemiological reports suggest that EHcV infects the liver and respiratory organs in horses, donkeys, and dogs. However, the mechanism explaining the differences in host or organ tropism between HCV and EHcV is unknown. In this study, our data suggest that the 5' untranslated region (UTR) of EHcV is composed of an internal ribosome entry site (IRES) element that is functionally exchangeable with HCV IRES elements. Furthermore, the 5'-proximal EHcV-specific region enhances viral replication and RNA stability in a miR-122-independent manner. Our data suggest that the region upstream of domain II in the EHcV 5' UTR contributes to the differences in tissue tropism observed between these hepaciviruses.

摘要

丙型肝炎病毒(HCV)的5'非翻译区(UTR)由四个结构域(I、II、III和IV)和一个假结组成,对翻译和病毒复制至关重要。马非灵长类肝炎病毒(EHcV)的5'UTR由一个大的5'末端结构域(I);另外三个结构域(I'、II和III)组成,它们分别与HCV的结构域I、II和III同源;以及一个假结,按所列顺序排列。在本研究中,我们研究了EHcV 5'UTR在翻译和病毒复制中的作用。由于结构域III的结构差异,EHcV 5'UTR的内部核糖体进入位点(IRES)活性在几种细胞系中低于HCV 5'UTR。就IRES活性和亚基因组复制子(SGR)的复制而言,EHcV的结构域I和III在HCV 5'UTR中发挥功能,尽管在SGR复制方面,EHcV和HCV之间的结构域II不可互换。此外,跨越EHcV结构域I和I'的区域(5'近端EHcV特异性区域)提高了RNA稳定性,并为HCV SGR提供了独立于微小RNA 122(miR-122)的复制能力,而单独的EHcV结构域I无论miR-122如何都能提高SGR复制和RNA稳定性。这些数据表明,跨越EHcV结构域I和I'的区域无论miR-122表达如何都能提高RNA稳定性和病毒复制。5'近端EHcV特异性区域可能代表了一种促进病毒在非肝组织中复制的内在机制。EHcV是其他肝炎病毒中与HCV最接近的病毒同源物。HCV表现出狭窄 的宿主范围和肝脏特异性嗜性,而流行病学报告表明EHcV感染马、驴和狗的肝脏和呼吸器官。然而,解释HCV和EHcV之间宿主或器官嗜性差异的机制尚不清楚。在本研究中,我们的数据表明,EHcV的5'非翻译区(UTR)由一个内部核糖体进入位点(IRES)元件组成,该元件在功能上可与HCV IRES元件互换。此外,5'近端EHcV特异性区域以独立于miR-122的方式增强病毒复制和RNA稳定性。我们的数据表明,EHcV 5'UTR中结构域II上游的区域导致了这些肝炎病毒之间观察到的组织嗜性差异。

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