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Picornavirus internal ribosome entry segments: comparison of translation efficiency and the requirements for optimal internal initiation of translation in vitro.

机译:小核糖核酸病毒内部核糖体进入片段:翻译效率与体外最佳内部翻译起始条件的比较。

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摘要

On the basis of primary sequence comparisons and secondary structure predictions, picornavirus internal ribosome entry segments (IRESes) have been divided into three groups (entero- and rhinoviruses; cardio- and and aphthoviruses; and hepatitis A virus). Here, we describe a detailed comparison of the ability of IRESes from each group to direct internal initiation of translation in vitro using a single dicistronic mRNA (the only variable being the IRES inserted into the dicistronic region). We studied the influence of various parameters on the capacity of six different picornaviral IRESes, and the non-picornaviral hepatitis C virus IRES, to direct internal initiation of translation: salt concentration, the addition of HeLa cell proteins to rabbit reticulocyte lysate translation reactions, the presence of foot-and-mouth disease virus Lb or human rhinovirus 2A proteinase. On the basis of the characteristics of IRES-driven translation in vitro, the picornaviral IRESes can be classified in a similar manner to when sequence homologies are considered. IRESes from each of the three groups responded differently to all of the parameters tested, indicating that while all of these elements can direct internal ribosome entry, the functional requirements for efficient IRES activity vary dramatically. In the individual optimal conditions for translation initiation, the best IRESes were those from the cardio- and aphthoviruses, followed by those from the enteroviruses, which exhibited up to 70% of the efficiency of the EMCV element in directing internal initiation of translation.
机译:根据一级序列比较和二级结构预测,小核糖核酸病毒内部核糖体进入片段(IRESes)已分为三类(肠病毒和鼻病毒;心脏和肺病毒;以及甲型肝炎病毒)。在这里,我们描述了使用单个双顺反子mRNA(唯一的变量是插入双顺反子区域的IRES)从每组IRESes指导体外翻译内部直接启动的能力的详细比较。我们研究了各种参数对六个不同的小核糖核酸病毒IRES和非丙型肝炎丙型肝炎病毒IRES的能力的影响,以指导翻译的内部启动:盐浓度,向兔网织红细胞裂解物翻译反应中添加HeLa细胞蛋白,口蹄疫病毒Lb或人鼻病毒2A蛋白酶的存在。基于IRES驱动的体外翻译的特征,可以与考虑序列同源性时相似的方式对微核糖核酸IRES进行分类。三组中的每组的IRES对测试的所有参数的反应都不同,表明尽管所有这些元素都可以指导内部核糖体进入,但有效IRES活性的功能要求却有很大差异。在翻译起始的各个最佳条件中,最佳的IRES是来自心房和水痘病毒的,然后是来自肠病毒的,其在指导内部翻译起始中表现出高达EMVC元件效率的70%。

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