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安第斯病毒在叙利亚仓鼠中连续传代后的高基因组稳定性。

High genomic stability of Andes virus following successive passage in Syrian hamsters.

作者信息

Warner Bryce M, Prévost Jérémie, Tailor Nikesh, Deschambault Yvon, Sloan Angela, Allarie Julina, Klassen Levi, Frost Kathy, Booth Stephanie, Audet Jonathan, Soule Geoff, Safronetz David

机构信息

Vaccine and Infectious Disease Organization, University of Saskatchewan, Saskatoon, Canada.

Department of Biochemistry, Microbiology, and Immunology, University of Saskatchewan, , Saskatoon, Canada.

出版信息

J Virol. 2025 Jul 24:e0051225. doi: 10.1128/jvi.00512-25.

Abstract

Andes virus (ANDV) is a South American hantavirus that causes hantavirus cardiopulmonary syndrome (HCPS), a severe respiratory infection with a case fatality rate as high as 40%. A critical model for studying HCPS is the Syrian hamster model, which faithfully recapitulates key aspects of the disease. Recent studies have shown that strains of ANDV from different origins, i.e., from rodent or human hosts, can produce widely different outcomes in the hamster model. CHI-7913, a human isolate, does not cause lethal disease and replicates poorly in hamster tissues compared with the classical rodent isolate Chile-9717869. Here, we passaged CHI-7913 in Syrian hamsters 25 times and infected groups of hamsters with virus from passages 2, 12, and 24 to assess whether viral adaptation occurs that might ultimately drive the phenotype of the virus during infection in this model. Very few mutations occurred during passage in hamsters, with only a single coding mutation discovered after 25 passages. Nearly all mutations occurring in hamsters occurred early, within two passages, and none of the passaged virus caused overt disease or pathology in infected hamsters, consistent with minimal changes in the viral genome. Early in infection, CHI-7913 viral RNA levels were still well below those seen in lethal Chile-9717869 infection. Overall, our data offer insights into the lack of selective pressure on hantaviruses in certain hosts and further evidence of distinct outcomes between rodent and human-derived viral isolates that should be studied further in additional viral species.IMPORTANCEInfection of Syrian hamsters with Andes virus (ANDV) can result in disparate outcomes, depending on the source of the virus used for the infection. The ANDV strain CHI-7913 does not cause lethal disease in hamsters but is able to replicate in hamster tissues. We successively passaged CHI-7913 to study how continued infection influences adaptation in hamsters and whether passaging would lead to the development of a lethal model, as sometimes occurs with other viruses. Surprisingly, even after 25 passages, minimal mutations occurred in ANDV CHI-7913 genomes, with only one coding mutation present above consensus by passage 25, in the viral glycoprotein. Our data suggest that depending on both viral origin and the host, hantaviruses may face minimal selective pressure to mutate toward a disease phenotype. Studies with additional ANDV strains and other hantavirus species are warranted to further study this phenomenon.

摘要

安第斯病毒(ANDV)是一种南美汉坦病毒,可引起汉坦病毒心肺综合征(HCPS),这是一种严重的呼吸道感染,病死率高达40%。研究HCPS的一个关键模型是叙利亚仓鼠模型,该模型能如实地再现该疾病的关键特征。最近的研究表明,来自不同来源(即啮齿动物或人类宿主)的ANDV毒株在仓鼠模型中可产生截然不同的结果。与经典的啮齿动物分离株智利-9717869相比,人类分离株CHI-7913不会引发致命疾病,且在仓鼠组织中的复制能力较差。在此,我们将CHI-7913在叙利亚仓鼠体内传代25次,并将第2、12和24代的病毒感染仓鼠组,以评估是否会发生病毒适应性变化,这种变化最终可能会在该模型的感染过程中驱动病毒的表型。在仓鼠传代过程中发生的突变极少,25代后仅发现一个编码突变。仓鼠体内发生的几乎所有突变都发生在早期,即在两代内,并且传代后的病毒在感染的仓鼠中均未引起明显疾病或病理变化,这与病毒基因组的微小变化一致。在感染早期,CHI-7913的病毒RNA水平仍远低于致命性智利-9717869感染时的水平。总体而言,我们的数据为某些宿主中汉坦病毒缺乏选择压力提供了见解,并进一步证明了啮齿动物源和人类源病毒分离株之间存在不同结果,这一现象应在其他病毒种类中进一步研究。

重要性

用安第斯病毒(ANDV)感染叙利亚仓鼠会导致不同的结果,这取决于用于感染的病毒来源。ANDV毒株CHI-7913在仓鼠中不会引起致命疾病,但能够在仓鼠组织中复制。我们连续传代CHI-7913,以研究持续感染如何影响其在仓鼠中的适应性,以及传代是否会导致致死模型的出现,就像其他病毒有时会发生的那样。令人惊讶的是,即使传代25次后,ANDV CHI-7913基因组中发生的突变也极少,到第25代时,仅在病毒糖蛋白中发现一个高于共识序列的编码突变。我们的数据表明,取决于病毒来源和宿主,汉坦病毒可能面临极小的向疾病表型突变的选择压力。有必要对其他ANDV毒株和其他汉坦病毒种类进行研究,以进一步探究这一现象。

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