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SCR 2区域的N-聚糖对于膜辅因子蛋白(CD46)作为麻疹病毒受体发挥功能至关重要。

The N-glycan of the SCR 2 region is essential for membrane cofactor protein (CD46) to function as a measles virus receptor.

作者信息

Maisner A, Alvarez J, Liszewski M K, Atkinson D J, Atkinson J P, Herrler G

机构信息

Institut für Virologie, Philipps-Universität Marburg, Germany.

出版信息

J Virol. 1996 Aug;70(8):4973-7. doi: 10.1128/JVI.70.8.4973-4977.1996.

Abstract

Membrane cofactor protein (MCP) (CD46), a complement-regulatory protein, serves as a cellular receptor for measles virus. Its amino-terminal portion is composed of four short consensus repeats (SCR), three of which (SCR1, SCR2, and SCR4) carry an N-linked oligosaccharide. In order to determine the importance of the three N-glycans for the function of MCP as a measles virus receptor, we established Chinese hamster ovary (CHO) cell lines that stably express mutant MCPs lacking one of the three motifs for N glycosylation (NQ1, NQ2, and NQ4). In an additional mutant (NQ1-2), two glycosylation motifs were altered, allowing the addition of an N-linked oligosaccharide only in SCR4. The abilities of the mutant MCPs to function as measles virus receptors were analyzed with three different assays: (i) binding of measles virus hemagglutinin to MCP immobilized on nitrocellulose; (ii) binding of measles virus to CHO cells expressing wild-type or mutant MCP; and (iii) infection of the transfected CHO cells by measles virus. In all three assays, the abilities of the NQ2 and NQ1-2 mutants to serve as measles virus receptors were drastically impaired. The NQ1 and NQ4 mutants were recognized by measles virus almost as efficiently as the wild-type protein. These results indicate that the N-glycan attached to SCR2 is essential for MCP to serve as a measles virus receptor, while the oligosaccharides attached to SCR1 and SCR4 are of only minor importance.

摘要

膜辅因子蛋白(MCP)(CD46)是一种补体调节蛋白,作为麻疹病毒的细胞受体。其氨基末端部分由四个短共识重复序列(SCR)组成,其中三个(SCR1、SCR2和SCR4)带有N-连接寡糖。为了确定这三种N-聚糖对MCP作为麻疹病毒受体功能的重要性,我们建立了稳定表达缺少三种N-糖基化基序之一(NQ1、NQ2和NQ4)的突变型MCP的中国仓鼠卵巢(CHO)细胞系。在另一个突变体(NQ1-2)中,两个糖基化基序发生了改变,仅在SCR4中允许添加N-连接寡糖。用三种不同的试验分析了突变型MCP作为麻疹病毒受体的功能能力:(i)麻疹病毒血凝素与固定在硝酸纤维素上的MCP的结合;(ii)麻疹病毒与表达野生型或突变型MCP的CHO细胞的结合;(iii)麻疹病毒对转染的CHO细胞的感染。在所有这三种试验中,NQ2和NQ1-2突变体作为麻疹病毒受体的能力都受到了极大的损害。NQ1和NQ4突变体被麻疹病毒识别的效率几乎与野生型蛋白相同。这些结果表明,连接到SCR2上的N-聚糖对于MCP作为麻疹病毒受体至关重要,而连接到SCR1和SCR4上的寡糖则只有次要重要性。

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