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糖基结合病毒:受体转换和特异性。

Glycan Engagement by Viruses: Receptor Switches and Specificity.

机构信息

Interfaculty Institute of Biochemistry, University of Tübingen, D-72076 Tübingen, Germany; email:

Department of Pediatrics, Vanderbilt University School of Medicine, Nashville, Tennessee 37232.

出版信息

Annu Rev Virol. 2014 Nov;1(1):285-306. doi: 10.1146/annurev-virology-031413-085417. Epub 2014 Jun 27.

Abstract

A large number of viruses, including many human pathogens, bind cell-surface glycans during the initial steps of infection. Viral glycan receptors such as glycosaminoglycans and sialic acid-containing carbohydrates are often negatively charged, but neutral glycans such as histo-blood group antigens can also function as receptors. The engagement of glycans facilitates attachment and entry and, consequently, is often a key determinant of the host range, tissue tropism, pathogenicity, and transmissibility of viruses. Here, we review current knowledge about virus-glycan interactions using representative crystal structures of viral attachment proteins in complex with glycans. We illuminate the determinants of specificity utilized by different glycan-binding viruses and explore the potential of these interactions for switching receptor specificities within or even between glycan classes. A detailed understanding of these parameters is important for the prediction of binding sites where structural information is not available, and is invaluable for the development of antiviral therapeutics.

摘要

大量病毒,包括许多人类病原体,在感染的初始步骤中与细胞表面糖结合。病毒糖受体,如糖胺聚糖和含有唾液酸的碳水化合物,通常带负电荷,但中性糖,如组织血型抗原,也可以作为受体。糖的结合促进了附着和进入,因此通常是病毒宿主范围、组织嗜性、致病性和传染性的关键决定因素。在这里,我们使用糖结合病毒的代表性晶体结构,综述了有关病毒-糖相互作用的最新知识。我们阐明了不同糖结合病毒所利用的特异性决定因素,并探讨了这些相互作用在糖类内部甚至之间切换受体特异性的潜力。详细了解这些参数对于预测结合部位(在这些部位结构信息不可用)非常重要,对于开发抗病毒治疗药物也非常重要。

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