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Bacteriophage MS2 genomic RNA encodes an assembly instruction manual for its capsid

机译:噬菌体ms2基因组RNa编码其衣壳的组装说明书

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摘要

Using RNA-coat protein crosslinking we have shown that the principal RNA recognition surface on the interior of infectious MS2 virions overlaps with the known peptides that bind the high affinity translational operator, TR, within the phage genome. The data also reveal the sequences of genomic fragments in contact with the coat protein shell. These show remarkable overlap with previous predictions based on the hypothesis that virion assembly is mediated by multiple sequences-specific contacts at RNA sites termed Packaging Signals (PSs). These PSs are variations on the TR stem-loop sequence and secondary structure. They act co-operatively to regulate the dominant assembly pathway and ensure cognate RNA encapsidation. In MS2, they also trigger conformational change in the dimeric capsomere creating the A/B quasi-conformer, 60 of which are needed to complete the T=3 capsid. This is the most compelling demonstration to date that this ssRNA virus, and by implications potentially very many of them, assemble via a PS-mediated assembly mechanism.
机译:使用RNA外壳蛋白交联,我们已经表明,感染性MS2病毒体内部的主要RNA识别表面与噬菌体基因组内结合高亲和力翻译操纵子TR的已知肽重叠。数据还揭示了与外壳蛋白外壳接触的基因组片段的序列。这些显示与基于病毒体装配是由称为包装信号(PS)的RNA位点的多个序列特异性接触介导的假设的先前预测有显着重叠。这些PS是TR茎环序列和二级结构的变异。它们协同作用来调节显性装配途径,并确保相关的RNA衣壳化。在MS2中,它们还会触发二聚体体中的构象变化,从而形成A / B准构象异构体,其中60个是完整的T = 3衣壳。这是迄今为止最引人注目的证明,这种ssRNA病毒通过PS介导的组装机制进行组装,并暗示其中很多。

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