首页> 美国卫生研究院文献>Journal of Virology >Translation of human hepatitis C virus RNA in cultured cells is mediated by an internal ribosome-binding mechanism.
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Translation of human hepatitis C virus RNA in cultured cells is mediated by an internal ribosome-binding mechanism.

机译:人类丙型肝炎病毒RNA在培养细胞中的翻译是由内部核糖体结合机制介导的。

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摘要

The human hepatitis C virus (HCV) contains a long 5' noncoding region (5' NCR). Computer-assisted and biochemical analyses suggest that there is a complex secondary structure in this region that is comparable to the secondary structures that are found in picornaviruses (E.A. Brown, H. Zhang, L.-H. Ping, and S.M. Lemon, Nucleic Acids Res. 20:5041-5045, 1992). Previous in vitro studies suggest that the HCV 5' NCR plays an important role during translation (K. Tsukiyama-Kohara, N. Iizuka, M. Kohara, and A. Nomoto, J. Virol. 66:1476-1483, 1992). Dicistronic and monocistronic expression vectors, in vitro translation, RNA transfections, and deletion mutagenesis studies were utilized to demonstrate unambiguously that the HCV 5' NCR is involved in translational control. Our data strongly support the conclusion that an internal ribosome entry site exists within the 5' noncoding sequences proximal to the initiator AUG. Furthermore, our results suggest that the HCV genome is translated in a cap-independent manner and that the sequences immediately upstream of the initiator AUG are essential for internal ribosome entry site function during translation.
机译:人类丙型肝炎病毒(HCV)包含一个较长的5'非编码区(5'NCR)。计算机辅助和生化分析表明,该区域中存在复杂的二级结构,可与微小RNA病毒中发现的二级结构相比(EA Brown,H。Zhang,L.-H。Ping和SM Lemon,Nucleic Acids Res.20:5041-5045,1992)。先前的体外研究表明,HCV 5'NCR在翻译过程中起重要作用(K.Tsukiyama-Kohara,N.Iizuka,M.Kohara,和A.Nomoto,J.Virol.66:1476-1483,1992)。利用双顺反子和单顺反子表达载体,体外翻译,RNA转染和缺失诱变研究来明确证明HCV 5'NCR参与翻译控制。我们的数据强烈支持以下结论:内部核糖体进入位点存在于启动子AUG附近的5'非编码序列中。此外,我们的结果表明,HCV基因组以不依赖于帽的方式进行翻译,并且在翻译过程中,紧邻起始子AUG上游的序列对于内部核糖体进入位点功能至关重要。

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