使用唾液酸作为附着因子是肠病毒d种的共同特征。

IF 4 2区 医学 Q2 VIROLOGY
Typhaine Filhol, Alice Mac Kain, Marie-Line Joffret, Nolwenn Jouvenet, Vincent Caval, Maël Bessaud
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引用次数: 0

摘要

在数百种感染人类的肠病毒(ev)中,EV-D(肠病毒解结)种的成员表现出原始的特征。首先,在该物种中只有五种已知的血清型,而其他EV物种每种都有数十种血清型。其次,ev - d表现出广泛的趋向性:ev - d68是呼吸道病毒,ev - d70是眼部病毒,而ev - d94、ev - d111和ev - d120似乎是肠道病毒。此外,虽然在人类中检测到ev - d68、ev - d70和ev - d94,但ev - d120仅在非人灵长类动物中发现,最后一种病毒类型EV-D111在这两种病毒中均被发现。这和其他观察结果导致了ev - d可能具有人畜共患起源的假设。先前的研究表明,EV-D68、EV-D70和EV-D94使用唾液酸(Sias)作为细胞附着因子。我们通过唾液酸酶治疗和人类和猿类细胞的功能丧失实验,研究了Sias在EV-D111感染中的作用。通过RT-qPCR分析评估病毒RNA产量和通过滴定试验评估感染性病毒颗粒产量表明,细胞表面Sias的缺失显著减缓了EV-D111的感染动力学,但没有消除它。这表明Sia是一种依恋因素。虽然ev通常不使用Sias,但ev - d似乎依赖它们在培养细胞中进行最佳复制。因此,Sia的使用可能是这个物种的一个祖先特征。我们还研究了一种猿类肠道病毒EV-B114,发现它不使用Sias。我们的工作提供了新的见解关于肠道病毒,在人类中循环,并表现出不同寻常的生态特征。除1970年代和1980年代的几次流行外,ev - d对人类健康的影响一直不大,直到2010年代。2014年,EV-D68偶尔会导致严重呼吸窘迫和致命的肌肉麻痹病例。因此,ev - d具有对人类致病的能力,因此研究它们很重要。最近发现的EV-D111在人类和猿类样本中均已检测到,其中仅有少数分离株,表明可能存在人畜共患来源。我们描述了EV-D111复制的早期步骤,重点关注了它使用Sias作为附着因子的能力。我们发现EV-D111与EV-D物种的其他成员一样,但与大多数ev不同,它依赖于Sia进行最佳复制。我们的工作提供了对EV-D111生物学的更好理解,这对于确定其趋向性和在人类中出现的潜力至关重要。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
The use of sialic acids as attachment factors is a common feature of Enterovirus-D species.

Among the hundreds of enteroviruses (EVs) infecting humans, the members of the species EV-D (Enterovirus deconjuncti) display original traits. First, only five serotypes are known within this species, while other EV species have tens of serotypes each. Second, EV-Ds display a wide variety of tropisms: EV-D68s are respiratory viruses, EV-D70s have an ocular tropism, while EV-D94s, EV-D111s, and EV-D120s seem to be enteric viruses. Besides, while EV-D68s, EV-D70s, and EV-D94s have been detected in humans, EV-D120s were found exclusively in non-human primates, and the last virus type, EV-D111, was found in both. This and other observations have led to the hypothesis that EV-Ds could have a zoonotic origin. Previous studies have shown that EV-D68, EV-D70, and EV-D94 use sialic acids (Sias) as cellular attachment factors. We investigated the role of Sias in EV-D111 infection using sialidase treatments and loss-of-function experiments in human and simian cells. Assessing viral RNA yield by RT-qPCR analyses and infectious viral particle production by titration assays showed that the absence of Sias at the cell surface significantly slowed down EV-D111 infection kinetics without abolishing it. This suggests that Sia acts as an attachment factor. While EVs generally do not use Sias, EV-Ds seem to rely on them for optimal replication in cultured cells. Sia usage may therefore be an ancestral trait of this species. We also studied EV-B114, a simian enterovirus, and found that it does not use Sias. Our work provides new insight regarding an enterovirus that circulates in humans and exhibits unusual ecological traits.IMPORTANCEExcept for a few epidemics in the 1970s and 1980s, the impact of EV-Ds on human health remained modest until the 2010s. In 2014, EV-D68 was occasionally responsible for severe respiratory distress and fatal cases of muscular paralysis. EV-Ds have thus the ability to become pathogenic in humans, hence the importance of studying them. The recently discovered EV-D111, of which only a few isolates are available, has been detected in both human and simian samples, suggesting a potential zoonotic origin. We characterized the early steps of EV-D111 replication, with a focus on its ability to use Sias as attachment factors. We found that EV-D111, like other members of the EV-D species, but unlike most EVs, relies on Sia for optimal replication. Our work provides a better understanding of EV-D111 biology, which is essential to determine its tropism and its potential to emerge in humans.

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来源期刊
Journal of Virology
Journal of Virology 医学-病毒学
CiteScore
10.10
自引率
7.40%
发文量
906
审稿时长
1 months
期刊介绍: Journal of Virology (JVI) explores the nature of the viruses of animals, archaea, bacteria, fungi, plants, and protozoa. We welcome papers on virion structure and assembly, viral genome replication and regulation of gene expression, genetic diversity and evolution, virus-cell interactions, cellular responses to infection, transformation and oncogenesis, gene delivery, viral pathogenesis and immunity, and vaccines and antiviral agents.
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