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Early Steps in Rotavirus Cell Entry

机译:轮状病毒细胞进入的早期步骤

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Rota-viruses, the leading cause of severe dehydrating diarrhea in infants and young children worldwide, are non-enveloped viruses formed by three concentric layers of protein that enclose a genome of double-stranded RNA. These viruses have a specific cell tropism in vivo, infecting primarily the mature enterocytes of the villi of the small intestine. It has been found that rotavirus cell entry is a complex mul-tistep process, in which different domains of the rotavirus surface proteins interact sequentially with different cell surface molecules, which act as attachment and entry receptors. These recently described molecules include integrins (alpha2betal, alphavbeta3, and alphaxbeta2) and a heat shock protein (hsc70), and have been found to be associated with cell membrane lipid micro domains. The requirement for several cell molecules, which might need to be present and organized in a precise fashion, could explain the cell and tissue tropism of these viruses. This review focuses on recent data describing the interactions between the virus and its receptors, the role of lipid microdomains in rotavirus infection, and the possible mechanism of rotavirus cell entry.
机译:轮状病毒是全世界婴幼儿严重脱水腹泻的主要原因,它是由三层同心蛋白质层构成的非包膜病毒,其中三层同心蛋白质包围着双链RNA基因组。这些病毒在体内具有特定的细胞嗜性,主要感染小肠绒毛的成熟肠上皮细胞。已经发现轮状病毒细胞进入是一个复杂的多步过程,其中轮状病毒表面蛋白的不同结构域与充当附着和进入受体的不同细胞表面分子顺序地相互作用。这些最近描述的分子包括整联蛋白(alpha2betal,alphavbeta3和alphaxbeta2)和热激蛋白(hsc70),并且已发现与细胞膜脂质微结构域相关。对几种细胞分子的需求(可能需要以精确的方式呈现和组织)可以解释这些病毒在细胞和组织上的嗜性。这篇综述集中在描述病毒与其受体之间的相互作用,脂质微结构域在轮状病毒感染中的作用以及轮状病毒细胞进入的可能机制的最新数据。

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