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Functional and Structural Similarities between the Internal Ribosome Entry Sites of Hepatitis C Virus and Porcine Teschovirus a Picornavirus

机译:丙型肝炎病毒的内部核糖体进入位点和猪细支病毒(猪细小病毒)的功能和结构相似性

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摘要

Initiation of protein synthesis on picornavirus RNA requires an internal ribosome entry site (IRES). Typically, picornavirus IRES elements contain about 450 nucleotides (nt) and use most of the cellular translation initiation factors. However, it is now shown that just 280 nt of the porcine teschovirus type 1 Talfan (PTV-1) 5′ untranslated region direct the efficient internal initiation of translation in vitro and within cells. In toeprinting assays, assembly of 48S preinitiation complexes from purified components on the PTV-1 IRES was achieved with just 40S ribosomal subunits plus eIF2 and Met-tRNAiMet. Indeed, a binary complex between 40S subunits and the PTV-1 IRES is formed. Thus, the PTV-1 IRES has properties that are entirely different from other picornavirus IRES elements but highly reminiscent of the hepatitis C virus (HCV) IRES. Comparison between the PTV-1 IRES and HCV IRES elements revealed islands of high sequence identity that occur in regions critical for the interactions of the HCV IRES with the 40S ribosomal subunit and eIF3. Thus, there is significant functional and structural similarity between the IRES elements from the picornavirus PTV-1 and HCV, a flavivirus.
机译:在小核糖核酸RNA上蛋白质合成的启动需要一个内部核糖体进入位点(IRES)。通常,微小RNA病毒IRES元件包含约450个核苷酸(nt),并使用大多数细胞翻译起始因子。但是,现在表明,仅280 nt的猪1型猪瘟病毒Talfan(PTV-1)5'非翻译区指导着体外和细胞内翻译的有效内部启动。在印迹分析中,仅用40S核糖体亚基加上eIF2和Met-tRNAi Met 即可在PTV-1 IRES上从纯化的组分组装48S预起始复合物。实际上,在40S亚基和PTV-1 IRES之间形成了二元复合物。因此,PTV-1 IRES具有与其他小核糖核酸IRES元素完全不同的特性,但高度让人联想到丙型肝炎病毒(HCV)IRES。 PTV-1 IRES和HCV IRES元件之间的比较显示,在HCV IRES与40S核糖体亚基和eIF3相互作用至关重要的区域中出现了具有高序列同一性的岛。因此,来自小核糖核酸病毒PTV-1的IRES元件和黄病毒HCV之间存在明显的功能和结构相似性。

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