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卢日病毒的反向遗传学恢复及其在病毒高效生长中的 RNA 二级结构的作用。

Reverse genetics recovery of Lujo virus and role of virus RNA secondary structures in efficient virus growth.

机构信息

Viral Special Pathogens Branch, Division of High-Consequence Pathogens and Pathology, Centers for Disease Control and Prevention, Atlanta, Georgia, USA.

出版信息

J Virol. 2012 Oct;86(19):10759-65. doi: 10.1128/JVI.01144-12. Epub 2012 Jul 25.

Abstract

Arenaviruses are rodent-borne viruses with a bisegmented RNA genome. A genetically unique arenavirus, Lujo virus, was recently discovered as the causal agent of a nosocomial outbreak of acute febrile illness with hemorrhagic manifestations in Zambia and South Africa. The outbreak had a case fatality rate of 80%. A reverse genetics system to rescue infectious Lujo virus from cDNA was established to investigate the biological properties of this virus. Sequencing the genomic termini showed unique nucleotides at the 3' terminus of the S segment promoter element. While developing this system, we discovered that reconstructing infectious Lujo virus using the previously reported L segment intergenic region (IGR), comprising the arenaviral transcription termination signal, yielded an attenuated Lujo virus. Resequencing revealed that the correct L segment IGR was 36 nucleotides longer, and incorporating it into the reconstructed Lujo virus restored the growth rate to that of the authentic clinical virus isolate. These additional nucleotides were predicted to more than double the free energy of the IGR main stem-loop structure. In addition, incorporating the newly determined L-IGR into a replicon reporter system enhanced the expression of a luciferase reporter L segment. Overall, these results imply that an extremely stable secondary structure within the L-IGR is critical for Lujo virus propagation and viral protein production. The technology for producing recombinant Lujo virus now provides a method to precisely investigate the molecular determinants of virulence of this newly identified pathogen.

摘要

沙粒病毒是一种具有双节段 RNA 基因组的啮齿动物传播病毒。最近发现一种遗传上独特的沙粒病毒——卢约病毒,是赞比亚和南非发生的一起医院感染性急性发热伴出血表现疾病暴发的病原体。该暴发的病死率为 80%。建立了一种从 cDNA 拯救传染性卢约病毒的反向遗传学系统,以研究该病毒的生物学特性。测序基因组末端显示 S 片段启动子元件 3' 末端具有独特的核苷酸。在开发该系统的过程中,我们发现使用先前报道的 L 片段基因间区(IGR)重建传染性卢约病毒,该 IGR 包含沙粒病毒转录终止信号,会产生减毒的卢约病毒。重新测序显示正确的 L 片段 IGR 长 36 个核苷酸,将其纳入重建的卢约病毒中可恢复其与真实临床病毒分离株相当的生长速率。这些额外的核苷酸预计会使 IGR 主要茎环结构的自由能增加一倍以上。此外,将新确定的 L-IGR 纳入复制子报告系统会增强荧光素酶报告 L 片段的表达。总的来说,这些结果表明,L-IGR 内极其稳定的二级结构对于卢约病毒的增殖和病毒蛋白的产生至关重要。现在生产重组卢约病毒的技术为精确研究这种新发现病原体的毒力分子决定因素提供了一种方法。

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