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对一种可变病毒在功能性衣壳区域引入有害突变后的遗传反应进行系统研究。

Systematic study of the genetic response of a variable virus to the introduction of deleterious mutations in a functional capsid region.

作者信息

Luna Eva, Rodríguez-Huete Alicia, Rincón Verónica, Mateo Roberto, Mateu Mauricio G

机构信息

Centro de Biología Molecular Severo Ochoa, Universidad Autónoma de Madrid, Cantoblanco, 28049 Madrid, Spain.

出版信息

J Virol. 2009 Oct;83(19):10140-51. doi: 10.1128/JVI.00903-09. Epub 2009 Jul 22.

Abstract

We have targeted the intersubunit interfaces in the capsid of foot-and-mouth disease virus to investigate the genetic response of a variable virus when individual deleterious mutations are systematically introduced along a functionally defined region of its genome. We had previously found that the individual truncation (by mutation to alanine) of 28 of the 42 amino acid side chains per protomer involved in interactions between capsid pentameric subunits severely impaired infectivity. We have now used viral RNAs individually containing each of those 28 deleterious mutations (or a few others) to carry out a total of 96 transfections of susceptible cells, generally followed by passage(s) of the viral progeny in cell culture. The results revealed a very high frequency of fixation in the capsid of second-site, stereochemically diverse substitutions that compensated for the detrimental effect of primary substitutions at many different positions. Most second-site substitutions occurred at or near the capsid interpentamer interfaces and involved residues that are spatially very close to the originally substituted residue. However, others occurred far from the primary substitution, and even from the interpentamer interfaces. Remarkably, most second-site substitutions involved only a few capsid residues, which acted as "second-site hot spots." Substitutions at these hot spots compensated for the deleterious effects of many different replacements at diverse positions. The remarkable capacity of the virus to respond to the introduction of deleterious mutations in the capsid with the frequent fixation of diverse second-site mutations, and the existence of second-site hot spots, may have important implications for virus evolution.

摘要

我们将口蹄疫病毒衣壳中的亚基间界面作为研究目标,以探究当沿着其基因组功能定义区域系统引入个体有害突变时,可变病毒的遗传反应。我们之前发现,每个原体中参与衣壳五聚体亚基间相互作用的42个氨基酸侧链中的28个被逐个截短(通过突变为丙氨酸)会严重损害感染性。我们现在使用分别含有这28个有害突变(或其他一些突变)的病毒RNA对易感细胞进行了总共96次转染,通常随后在细胞培养中传代病毒后代。结果显示,在衣壳中第二位点立体化学上不同的替代物的固定频率非常高,这些替代物补偿了许多不同位置上初级替代物的有害影响。大多数第二位点替代发生在衣壳五聚体间界面处或其附近,涉及在空间上与最初被替代残基非常接近的残基。然而,其他替代发生在远离初级替代物的位置,甚至远离五聚体间界面。值得注意的是,大多数第二位点替代仅涉及少数衣壳残基,这些残基充当“第二位点热点”。这些热点处的替代补偿了不同位置上许多不同替代物的有害影响。病毒对衣壳中有害突变的引入以不同第二位点突变的频繁固定做出反应的显著能力以及第二位点热点的存在,可能对病毒进化具有重要意义。

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