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结构导向鉴定具有人畜共患病潜力的非人类麻疹病毒。

Structure-Guided Identification of a Nonhuman Morbillivirus with Zoonotic Potential.

机构信息

The Pirbright Institute, Surrey, United Kingdom.

The University of Birmingham, Birmingham, United Kingdom.

出版信息

J Virol. 2018 Nov 12;92(23). doi: 10.1128/JVI.01248-18. Print 2018 Dec 1.

Abstract

Morbilliviruses infect a broad range of mammalian hosts, including ruminants, carnivores, and humans. The recent eradication of rinderpest virus (RPV) and the active campaigns for eradication of the human-specific measles virus (MeV) have raised significant concerns that the remaining morbilliviruses may emerge in so-called vacated ecological niches. Seeking to assess the zoonotic potential of nonhuman morbilliviruses within human populations, we found that peste des petits ruminants virus (PPRV)-the small-ruminant morbillivirus-is restricted at the point of entry into human cells due to deficient interactions with human SLAMF1-the immune cell receptor for morbilliviruses. Using a structure-guided approach, we characterized a single amino acid change, mapping to the receptor-binding domain in the PPRV hemagglutinin (H) protein, which overcomes this restriction. The same mutation allowed escape from some cross-protective, human patient, anti-MeV antibodies, raising concerns that PPRV is a pathogen with zoonotic potential. Analysis of natural variation within human and ovine SLAMF1 also identified polymorphisms that could correlate with disease resistance. Finally, the mechanistic nature of the PPRV restriction was also investigated, identifying charge incompatibility and steric hindrance between PPRV H and human SLAMF1 proteins. Importantly, this research was performed entirely using surrogate virus entry assays, negating the requirement for derivation of a human-tropic PPRV and illustrating alternative strategies for identifying gain-of-function mutations in viral pathogens. A significant proportion of viral pandemics occur following zoonotic transmission events, where animal-associated viruses jump species into human populations. In order to provide forewarnings of the emergence of these viruses, it is necessary to develop a better understanding of what determines virus host range, often at the genetic and structural levels. In this study, we demonstrated that the small-ruminant morbillivirus, a close relative of measles, is unable to use human receptors to enter cells; however, a change of a single amino acid in the virus is sufficient to overcome this restriction. This information will be important for monitoring this virus's evolution in the field. Of note, this study was undertaken , without generation of a fully infectious virus with this phenotype.

摘要

麻疹病毒属可感染多种哺乳动物宿主,包括反刍动物、食肉动物和人类。牛瘟病毒(RPV)的近期根除以及人类麻疹病毒(MeV)的积极根除活动引发了重大关注,即剩余的麻疹病毒可能会出现在所谓的空缺生态位中。为了评估人类群体中非人类麻疹病毒的人畜共患病潜力,我们发现小反刍动物瘟病毒(PPRV)-小反刍动物麻疹病毒-由于与人类 SLAMF1 的相互作用不足而受到限制,后者是麻疹病毒的免疫细胞受体。通过结构导向方法,我们鉴定了一个单点氨基酸变化,该变化映射到 PPRV 血凝素(H)蛋白的受体结合域,该变化克服了这种限制。相同的突变使病毒能够逃避一些交叉保护的、来自人类患者的抗-MeV 抗体,这引发了对 PPRV 具有人畜共患病潜力的担忧。对人类和绵羊 SLAMF1 中的自然变异进行分析还鉴定了可能与疾病抗性相关的多态性。最后,还研究了 PPRV 限制的机制性质,确定了 PPRV H 和人类 SLAMF1 蛋白之间的电荷不兼容性和空间位阻。重要的是,这项研究完全使用替代病毒进入测定法进行,从而消除了对衍生出人类亲和性 PPRV 的需求,并说明了鉴定病毒病原体获得功能突变的替代策略。重大的病毒性大流行中的很大一部分是在人畜共患病传播事件之后发生的,在这些事件中,与动物相关的病毒会跨越物种进入人类群体。为了对这些病毒的出现提供预警,有必要在遗传和结构水平上更好地了解决定病毒宿主范围的因素。在这项研究中,我们证明了小反刍动物麻疹病毒,一种与麻疹密切相关的病毒,无法使用人类受体进入细胞;但是,病毒中的单个氨基酸变化足以克服这种限制。该信息对于监测该病毒在野外的进化将非常重要。值得注意的是,这项研究是在没有生成具有这种表型的完全感染性病毒的情况下进行的。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/4e48/6232486/475ceb35ec9d/zjv0231840350001.jpg

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