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Structural and functional studies of the measles virus hemagglutinin: identification of a novel site required for CD46 interaction.麻疹病毒血凝素的结构与功能研究:鉴定CD46相互作用所需的新位点
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A single amino acid change in the hemagglutinin protein of measles virus determines its ability to bind CD46 and reveals another receptor on marmoset B cells.麻疹病毒血凝素蛋白中的单个氨基酸变化决定了其结合CD46的能力,并揭示了狨猴B细胞上的另一种受体。
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两个CD46结构域的晶体结构揭示了一个扩展的麻疹病毒结合表面。

Crystal structure of two CD46 domains reveals an extended measles virus-binding surface.

作者信息

Casasnovas J M, Larvie M, Stehle T

机构信息

Department of Biosciences at NOVUM, Karolinska Institute, 14157 Huddinge, Sweden.

出版信息

EMBO J. 1999 Jun 1;18(11):2911-22. doi: 10.1093/emboj/18.11.2911.

DOI:10.1093/emboj/18.11.2911
PMID:10357804
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC1171373/
Abstract

Measles virus is a paramyxovirus which, like other members of the family such as respiratory syncytial virus, is a major cause of morbidity and mortality worldwide. The cell surface receptor for measles virus in humans is CD46, a complement cofactor. We report here the crystal structure at 3.1 A resolution of the measles virus-binding fragment of CD46. The structure reveals the architecture and spatial arrangement of two glycosylated short consensus repeats with a pronounced interdomain bend and some flexibility at the domain interface. Amino acids involved in measles virus binding define a large, glycan-free surface that extends from the top of the first to the bottom of the second repeat. The extended virus-binding surface of CD46 differs strikingly from those reported for the human virus receptor proteins CD4 and intercellular cell adhesion molecule-1 (ICAM-1), suggesting that the CD46 structure utilizes a novel mode of virus recognition. A highly hydrophobic and protruding loop at the base of the first repeat bears a critical virus-binding residue, thereby defining an important recognition epitope. Molecules that mimic the conformation of this loop potentially could be effective anti-viral agents by preventing binding of measles virus to CD46.

摘要

麻疹病毒是一种副粘病毒,与该病毒家族的其他成员(如呼吸道合胞病毒)一样,是全球发病和死亡的主要原因。人类麻疹病毒的细胞表面受体是CD46,一种补体辅助因子。我们在此报告了CD46的麻疹病毒结合片段在3.1埃分辨率下的晶体结构。该结构揭示了两个糖基化的短共有重复序列的结构和空间排列,其结构域间有明显的弯曲,且在结构域界面处具有一定的灵活性。参与麻疹病毒结合的氨基酸定义了一个从第一个重复序列顶部延伸到第二个重复序列底部的大的无糖基表面。CD46的扩展病毒结合表面与报道的人类病毒受体蛋白CD4和细胞间细胞粘附分子1(ICAM-1)的表面显著不同,这表明CD46结构利用了一种新的病毒识别模式。第一个重复序列底部的一个高度疏水且突出的环带有一个关键的病毒结合残基,从而定义了一个重要的识别表位。模拟该环构象的分子可能通过阻止麻疹病毒与CD46结合而成为有效的抗病毒药物。