VLDLR和ApoER2是多种阿尔法病毒的受体-小柯机器人-科学网

VLDLR和ApoER2是多种阿尔法病毒的受体

2021-12-24 23:33

美国哈佛医学院Jonathan Abraham研究小组发现，VLDLR和ApoER2是多种阿尔法病毒的受体。相关论文于2021年12月20日在线发表在《自然》杂志上。

研究人员发现，极低密度脂蛋白受体（VLDLR）是原型阿尔法病毒Semliki Forest病毒（SFV）的受体。结果表明，SFV、东部马脑炎（EEEV）和Sindbis（SINV）病毒的E2/E1糖蛋白与VLDLR和脂蛋白E受体2（ApoER2）的配体结合域（LBD）相互作用。这两种蛋白的异位表达有利于细胞的附着和病毒样颗粒（VLP）的内化，VLDLR LBD-Fc融合蛋白或配体结合拮抗剂在培养中阻断SFV E2/E1介导的人和小鼠神经元感染，并且给予VLDLR LBD-Fc融合蛋白对小鼠胎儿的快速致命SFV感染有保护作用。研究人员进一步表明，在进化过程中与脊椎动物相距甚远的无脊椎动物受体直系亲属如蚊子和蠕虫可以作为功能性的阿尔法病毒受体。研究人员提出，一些阿尔法病毒感染广泛宿主的能力是它们与进化上保守的脂蛋白受体接触的结果，并有助于其致病机制。

据了解，阿尔法病毒，像许多其他节肢动物传播的病毒一样，感染脊椎动物和昆虫载体，它们之间有数亿年的进化历史。进入进化不同的宿主细胞可能是通过识别不同物种的不同细胞受体，或与不同物种间高度保守的受体结合而完成的。尽管多种阿尔法病毒受体已被描述，但大多数在脊椎动物和无脊椎动物宿主之间并不共享。

附：英文原文

Title: VLDLR and ApoER2 are receptors for multiple alphaviruses

Author: Clark, Lars E., Clark, Sarah A., Lin, ChieYu, Liu, Jianying, Coscia, Adrian, Nabel, Katherine G., Yang, Pan, Neel, Dylan V., Lee, Hyo, Brusic, Vesna, Stryapunina, Iryna, Plante, Kenneth S., Ahmed, Asim A., Catteruccia, Flaminia, Young-Pearse, Tracy L., Chiu, Isaac M., Llopis, Paula Montero, Weaver, Scott C., Abraham, Jonathan

Issue&Volume: 2021-12-20

Abstract: Alphaviruses, like many other arthropod-borne viruses, infect vertebrate species and insect vectors separated by hundreds of millions of years of evolutionary history. Entry in evolutionarily divergent host cells could be accomplished by recognition of different cellular receptors in different species, or by binding to receptors that are highly conserved across species. Although multiple alphavirus receptors have been described1–3, most are not shared among vertebrate and invertebrate hosts. Here, we identify the very low-density lipoprotein receptor (VLDLR) as a receptor for the prototypic alphavirus Semliki Forest virus (SFV). We show that the E2/E1 glycoproteins of SFV, eastern equine encephalitis (EEEV), and Sindbis (SINV) viruses interact with the ligand binding domains (LBDs) of VLDLR and apolipoprotein E receptor 2 (ApoER2), a closely related receptor. Ectopic expression of either protein facilitates cellular attachment and internalization of virus-like particles (VLPs), a VLDLR LBD-Fc fusion protein or a ligand binding antagonist block SFV E2/E1-mediated infection of human and mouse neurons in culture, and administration of a VLDLR LBD-Fc fusion protein has protective activity against rapidly fatal SFV infection in mouse neonates. We further show that invertebrate receptor orthologues as evolutionary distant from vertebrates as mosquitoes and worms can serve as functional alphavirus receptors. We propose that the ability of some alphaviruses to infect a wide range of hosts is a result of their engagement of evolutionarily conserved lipoprotein receptors and contributes to their pathogenesis.

DOI: 10.1038/s41586-021-04326-0

Source: https://www.nature.com/articles/s41586-021-04326-0

Nature：《自然》，创刊于1869年。隶属于施普林格·自然出版集团，最新IF：69.504
官方网址：http://www.nature.com/
投稿链接：http://www.nature.com/authors/submit_manuscript.html

本期文章：《自然》：Online/在线发表

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