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莫洛尼鼠白血病病毒Gag-Pol和基因组RNA比例的决定因素。

Determinants of Moloney murine leukemia virus Gag-Pol and genomic RNA proportions.

作者信息

Johnson Silas F, Collins John T, D'Souza Victoria M, Telesnitsky Alice

机构信息

Department of Microbiology and Immunology, University of Michigan, Ann Arbor, Michigan, USA.

Department of Molecular and Cellular Biology, Harvard University, Cambridge, Massachusetts, USA.

出版信息

J Virol. 2014 Jul;88(13):7267-75. doi: 10.1128/JVI.03513-13. Epub 2014 Apr 16.

Abstract

UNLABELLED

The Moloney murine leukemia virus (MoMLV) ribonucleoprotein complex is composed of an approximately 20:1 mixture of Gag and Gag-Pol polyproteins plus a single genomic RNA (gRNA) dimer. The mechanisms that regulate these proportions are unknown. Here, we examined whether virion proportions of Gag, Gag-Pol, and gRNA were determined by sampling (that is, if they reflected expression ratios or intracellular concentrations) or more specific recruitment. To this end, MoMLV Gag, Gag-Pol, and gRNA were expressed separately or together in various ratios. Varying the expression ratios of Gag and Gag-Pol revealed that Gag-Pol incorporation was stochastic and that the conserved 20:1 Gag/Gag-Pol ratio coincided with maximal particle production. When skewed expression ratios resulted in excess Gag-Pol, the released virions maintained the intracellular Gag/Gag-Pol ratios and the infectivity per virion was largely maintained, but virion production decreased sharply with high levels of Gag-Pol. The determinants of gRNA proportions were addressed by manipulating the amounts and contexts of functional nucleocapsid (NC) and the ratios of Gag to gRNA. The results showed that the NC domain of either Gag or Gag-Pol could provide gRNA packaging functions equally well. Unlike Gag-Pol, gRNA incorporation was saturable. An upper limit of gRNA incorporation was observed, and particle production was not disrupted by excess gRNA expression. These results indicate that the determinants of Gag/Gag-Pol proportions differ from those for Gag/gRNA. On the basis of the assumption that MoMLV evolved to produce virion components in optimal proportions, these data provide a means of estimating the proportion of unspliced MoMLV RNA that serves as genomic RNA.

IMPORTANCE

Viruses assemble their progeny from within the cells that they parasitize, where they must sort through a rich milieu of host proteins and nucleic acids to gather together their own building blocks, which are also proteins and nucleic acids. The research described here addresses whether or not the proportions of viral proteins and nucleic acids that are brought together to form a retroviral particle are determined by random sampling from the cell-and thus dictated by the components' availabilities within the cell-or if the amounts of each molecule are specified by the virus replication process. The results indicated that protein components of the murine retrovirus studied here are recruited by chance but that a specific counting mechanism defines the amount of nucleic acid incorporated into each progeny virion.

摘要

未标记

莫洛尼鼠白血病病毒(MoMLV)核糖核蛋白复合体由Gag和Gag-Pol多蛋白按约20:1的比例混合以及单个基因组RNA(gRNA)二聚体组成。调节这些比例的机制尚不清楚。在这里,我们研究了Gag、Gag-Pol和gRNA的病毒体比例是由抽样决定的(即它们是否反映了表达比例或细胞内浓度)还是由更特定的募集决定的。为此,MoMLV的Gag、Gag-Pol和gRNA以不同比例单独或共同表达。改变Gag和Gag-Pol的表达比例表明,Gag-Pol的掺入是随机的,保守的20:1的Gag/Gag-Pol比例与最大颗粒产生相吻合。当表达比例倾斜导致Gag-Pol过量时,释放的病毒体维持细胞内的Gag/Gag-Pol比例,并且每个病毒体的感染性在很大程度上得以维持,但随着Gag-Pol水平升高,病毒体产生急剧下降。通过操纵功能性核衣壳(NC)的数量和背景以及Gag与gRNA的比例来研究gRNA比例的决定因素。结果表明,Gag或Gag-Pol的NC结构域均可同样良好地提供gRNA包装功能。与Gag-Pol不同,gRNA的掺入是可饱和的。观察到gRNA掺入的上限,并且过量的gRNA表达不会破坏颗粒产生。这些结果表明,Gag/Gag-Pol比例的决定因素与Gag/gRNA的决定因素不同。基于MoMLV进化为以最佳比例产生病毒体成分这一假设,这些数据提供了一种估算用作基因组RNA的未剪接MoMLV RNA比例的方法。

重要性

病毒在其寄生的细胞内组装后代,在那里它们必须从丰富的宿主蛋白质和核酸环境中筛选,以聚集它们自己的构建块,这些构建块也是蛋白质和核酸。这里描述的研究探讨了组装成逆转录病毒颗粒的病毒蛋白质和核酸的比例是由从细胞中的随机抽样决定的——因此由细胞内各成分的可用性决定——还是每个分子的数量由病毒复制过程指定。结果表明,此处研究的鼠逆转录病毒的蛋白质成分是随机募集的,但一种特定的计数机制决定了掺入每个后代病毒体的核酸量。

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Diverse interactions of retroviral Gag proteins with RNAs.逆转录病毒 Gag 蛋白与 RNA 的多种相互作用。
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