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Secondary structure of the 5′ nontranslated regions of hepatitis C virus and pestivirus genomic RNAs

机译:丙型肝炎病毒和瘟病毒基因组RNA的5'非翻译区的二级结构

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摘要

The RNA genomes of human hepatitis C virus (HCV) and the animal pestiviruses responsible for bovine viral diarrhea (BVDV) and hog cholera (HChV) have relatively lengthy 5′ nontranslated regions (5′NTRs) sharing short segments of conserved primary nucleotlde sequence. The functions of these 5′NTRs are poorly understood. By comparative sequence analysis and thermodynamic modeling of the 5′NTRs of multiple BVDV and HChV strains, we developed models of the secondary structures of these RNAs. These pestiviral 5′NTRs are highly conserved structurally, despite substantial differences in their primary nucleotlde sequences. The assignment of similar structures to conserved segments of primary nucleotide sequence present in the 5′NTR of HCV resulted in a model of the secondary structure of the HCV 5′NTR which was refined by determining sites at which synthetic HCV RNA was cleaved by double- and single-strand specific RNases. These studies indicate the existence of a large conserved stem-loop structure within the 3′ 200 bases of the 5′NTRs of both HCV and pestiviruses which corresponds to the ribosomal landing pad (Internal ribosomal entry site) of HCV. This structure shows little relatedness to the ribosomal landing pad of hepatitis A virus, suggesting that these functionally similar structures may have evolved independently.
机译:人类丙型肝炎病毒(HCV)和负责牛病毒性腹泻(BVDV)和猪霍乱(HChV)的动物瘟病毒的RNA基因组具有相对较长的5'非翻译区(5'NTR),它们具有保守的初级核苷酸序列的短片段。这些5'NTR的功能了解甚少。通过比较序列分析和多个BVDV和HChV株的5'NTRs的热力学建模,我们开发了这些RNA二级结构的模型。尽管其初级核苷酸序列存在实质性差异,但这些瘟病毒5'NTR在结构上高度保守。将相似的结构分配给HCV 5'NTR中保守的一级核苷酸序列的保守片段,从而形成了HCV 5'NTR二级结构的模型,该模型可通过确定合成HCV RNA被双链断裂的位点进行精制和单链特异性RNase。这些研究表明,在HCV和瘟病毒的5'NTR的3'200碱基内存在一个大的保守茎环结构,这与HCV的核糖体着陆垫(内部核糖体进入位点)相对应。该结构与甲型肝炎病毒的核糖体着陆垫几乎没有相关性,表明这些功能相似的结构可能已经独立进化。

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