Banerjee Shefali, Smith Cathy, Geballe Adam P, Rothenburg Stefan, Kitzman Jacob O, Brennan Greg
Department of Medical Microbiology and Immunology, School of Medicine, University of California, Davis, CA 95616, USA.
Departments of Microbiology and Medicine, University of Washington, Seattle, WA 98195, USA.
Virus Evol. 2022 Nov 14;8(2):veac105. doi: 10.1093/ve/veac105. eCollection 2022.
Cross-species spillover events are responsible for many of the pandemics in human history including COVID-19; however, the evolutionary mechanisms that enable these events are poorly understood. We have previously modeled this process using a chimeric vaccinia virus expressing the rhesus cytomegalovirus-derived protein kinase R (PKR) antagonist RhTRS1 in place of its native PKR antagonists: E3L and K3L (VACVΔEΔK + RhTRS1). Using this virus, we demonstrated that gene amplification of occurred early during experimental evolution and was sufficient to fully rescue virus replication in partially resistant African green monkey (AGM) fibroblasts. Notably, this rapid gene amplification also allowed limited virus replication in otherwise completely non-permissive human fibroblasts, suggesting that gene amplification may act as a 'molecular foothold' to facilitate viral adaptation to multiple species. In this study, we demonstrate that there are multiple barriers to VACVΔEΔK + RhTRS1 replication in human cells, mediated by both PKR and ribonuclease L (RNase L). We experimentally evolved three AGM-adapted virus populations in human fibroblasts. Each population adapted to human cells bimodally, via an initial 10-fold increase in replication after only two passages followed by a second 10-fold increase in replication by passage 9. Using our Illumina-based pipeline, we found that some single nucleotide polymorphisms (SNPs) which had evolved during the prior AGM adaptation were rapidly lost, while thirteen single-base substitutions and short indels increased over time, including two SNPs unique to human foreskin fibroblast (HFF)-adapted populations. Many of these changes were associated with components of the viral RNA polymerase, although no variant was shared between all three populations. Taken together, our results demonstrate that amplification was sufficient to increase viral tropism after passage in an 'intermediate species' and subsequently enabled the virus to adopt different, species-specific adaptive mechanisms to overcome distinct barriers to viral replication in AGM and human cells.
跨物种传播事件导致了人类历史上的许多大流行,包括新冠疫情;然而,促成这些事件的进化机制却鲜为人知。我们之前曾使用一种嵌合痘苗病毒对这一过程进行建模,该病毒表达恒河猴巨细胞病毒衍生的蛋白激酶R(PKR)拮抗剂RhTRS1,以取代其天然的PKR拮抗剂:E3L和K3L(VACVΔEΔK + RhTRS1)。利用这种病毒,我们证明基因扩增在实验进化早期就已发生,并且足以在部分抗性的非洲绿猴(AGM)成纤维细胞中完全挽救病毒复制。值得注意的是,这种快速的基因扩增还使得病毒能够在原本完全不允许其复制的人成纤维细胞中进行有限的复制,这表明基因扩增可能作为一个“分子立足点”,以促进病毒适应多种物种。在本研究中,我们证明在人细胞中,VACVΔEΔK + RhTRS1的复制存在多个障碍,这些障碍由PKR和核糖核酸酶L(RNase L)介导。我们在人成纤维细胞中对三个适应AGM的病毒群体进行了实验进化。每个群体对人细胞的适应呈双峰模式,先是在仅传代两次后复制能力最初提高10倍,然后到传代9时复制能力再次提高10倍。使用我们基于Illumina的流程,我们发现一些在之前适应AGM过程中进化出的单核苷酸多态性(SNP)迅速消失,而随着时间的推移,有13个单碱基替换和短插入缺失增加,包括在适应人包皮成纤维细胞(HFF)的群体中特有的两个SNP。这些变化中的许多与病毒RNA聚合酶的组分有关,尽管所有三个群体之间没有共同的变体。综上所述,我们的结果表明基因扩增足以在经过“中间物种”传代后增加病毒嗜性,随后使病毒能够采用不同的、物种特异性的适应性机制来克服AGM和人细胞中病毒复制的不同障碍。
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