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双顺反子病毒mRNA在转染细胞中的翻译:延伸水平的调控

Translation of bicistronic viral mRNA in transfected cells: regulation at the level of elongation.

作者信息

Fajardo J E, Shatkin A J

机构信息

Center for Advanced Biotechnology and Medicine, Piscataway, NJ 08854-5638.

出版信息

Proc Natl Acad Sci U S A. 1990 Jan;87(1):328-32. doi: 10.1073/pnas.87.1.328.

Abstract

The S1 species of mammalian reovirus mRNA, like a number of other viral but not cellular mRNAs, codes for two dissimilar polypeptides by initiation of translation at two 5'-proximal, out-of-frame AUG codons. To determine if uninfected cells can utilize bicistronic genes, a bovine papilloma virus-based vector system was used to select mouse C127 cell lines containing multiple integrated copies of the reovirus S1 gene. These cell lines produced both reovirus polypeptides from a single mRNA. In addition, studies of COS cells transfected with the S1 gene containing small changes around the first AUG suggest that bicistronic mRNA translation is regulated at the level of elongation. A model is proposed in which ribosomes engaged in translation of one reading frame interfere with movement of ribosomes in the other frame because of differences in codon usage. Expression of bicistronic genes may be similarly regulated in virus-infected cells.

摘要

哺乳动物呼肠孤病毒mRNA的S1种类,与许多其他病毒而非细胞mRNA一样,通过在两个5'近端、移码的AUG密码子处起始翻译来编码两种不同的多肽。为了确定未感染的细胞是否能利用双顺反子基因,基于牛乳头瘤病毒的载体系统被用于筛选含有呼肠孤病毒S1基因多个整合拷贝的小鼠C127细胞系。这些细胞系从单个mRNA产生两种呼肠孤病毒多肽。此外,对用在第一个AUG周围含有小变化的S1基因转染的COS细胞的研究表明,双顺反子mRNA的翻译在延伸水平受到调控。提出了一个模型,其中由于密码子使用的差异,参与一个阅读框翻译的核糖体干扰另一个阅读框中核糖体的移动。双顺反子基因的表达在病毒感染的细胞中可能受到类似的调控。

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