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Deletion of the Monkeypox Virus Inhibitor of Complement Enzymes Locus Impacts the Adaptive Immune Response to Monkeypox Virus in a Nonhuman Primate Model of Infection ▿ §

机译:互补酶基因座的猴痘病毒抑制剂的删除影响非人类灵长类动物感染模型中对猴痘病毒的适应性免疫反应

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摘要

Monkeypox virus (MPXV) is an orthopoxvirus closely related to variola virus, the causative agent of smallpox. Human MPXV infection results in a disease that is similar to smallpox and can also be fatal. Two clades of MPXV have been identified, with viruses of the central African clade displaying more pathogenic properties than those within the west African clade. The monkeypox inhibitor of complement enzymes (MOPICE), which is not expressed by viruses of the west African clade, has been hypothesized to be a main virulence factor responsible for increased pathogenic properties of central African strains of MPXV. To gain a better understanding of the role of MOPICE during MPXV-mediated disease, we compared the host adaptive immune response and disease severity following intrabronchial infection with MPXV-Zaire (n = 4), or a recombinant MPXV-Zaire (n = 4) lacking expression of MOPICE in rhesus macaques (RM). Data presented here demonstrate that infection of RM with MPXV leads to significant viral replication in the peripheral blood and lungs and results in the induction of a robust and sustained adaptive immune response against the virus. More importantly, we show that the loss of MOPICE expression results in enhanced viral replication in vivo, as well as a dampened adaptive immune response against MPXV. Taken together, these findings suggest that MOPICE modulates the anti-MPXV immune response and that this protein is not the sole virulence factor of the central African clade of MPXV.
机译:猴痘病毒(MPXV)是一种正痘病毒,与天花的病原体天花病毒密切相关。人类MPXV感染导致的疾病类似于天花,也可能是致命的。已鉴定出两个MPXV进化枝,中非进化枝的病毒显示出比西非进化枝更强的致病特性。西非进化枝病毒未表达的补体酶猴痘抑制剂(MOPICE)被认为是导致非洲中部MPXV菌株致病性增加的主要毒力因子。为了更好地了解MOPICE在MPXV介导的疾病中的作用,我们比较了MPXV-Zaire(n = 4)或重组MPXV-Zaire(n = 4)支气管内感染后宿主的适应性免疫反应和疾病严重程度在恒河猴(RM)中缺乏MOPICE表达。此处提供的数据表明,用MPXV感染RM会导致外周血和肺中大量病毒复制,并导致诱导出针对该病毒的强大而持续的适应性免疫应答。更重要的是,我们显示MOPICE表达的丧失导致体内病毒复制增强,以及针对MPXV的适应性免疫反应减弱。综上所述,这些发现表明,MOPICE调节了抗MPXV的免疫反应,并且该蛋白质不是非洲MPXV进化枝的唯一毒力因子。

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