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人副流感病毒3型血凝素神经氨酸酶上的第二个受体结合位点有助于融合机制的激活。

A second receptor binding site on human parainfluenza virus type 3 hemagglutinin-neuraminidase contributes to activation of the fusion mechanism.

作者信息

Porotto Matteo, Fornabaio Micaela, Kellogg Glen E, Moscona Anne

机构信息

Department of Pediatrics, Weill Medical College of Cornell University, 515 East 71st Street, New York, NY 10021, USA.

出版信息

J Virol. 2007 Apr;81(7):3216-28. doi: 10.1128/JVI.02617-06. Epub 2007 Jan 17.

Abstract

The hemagglutinin-neuraminidase (HN) protein of paramyxoviruses carries out three discrete activities that each affect the ability of HN to promote viral fusion and entry: receptor binding, receptor cleaving (neuraminidase), and triggering of the fusion protein. The interrelationship between the receptor binding and fusion-triggering functions of HN has not been clear. For human parainfluenza type 3 (HPIV3), one bifunctional site on HN can carry out both receptor binding and neuraminidase activities, and this site's receptor binding can be inhibited by the small receptor analog zanamivir. We now report experimental evidence, complemented by computational data, for a second receptor binding site near the HPIV3 HN dimer interface. This second binding site can mediate receptor binding even in the presence of zanamivir, and it differs from the second receptor binding site of the paramyxovirus Newcastle disease virus in its function and its relationship to the primary binding site. This second binding site of HPIV3 HN is involved in triggering F. We suggest that the two receptor binding sites on HPIV3 HN each contribute in distinct ways to virus-cell interaction; one is the multifunctional site that contains both binding and neuraminidase activities, and the other contains binding activity and also is involved in fusion promotion.

摘要

副粘病毒的血凝素神经氨酸酶(HN)蛋白具有三种不同的活性,每种活性都会影响HN促进病毒融合和进入的能力:受体结合、受体切割(神经氨酸酶)以及触发融合蛋白。HN的受体结合功能与融合触发功能之间的相互关系尚不清楚。对于3型人副流感病毒(HPIV3),HN上的一个双功能位点可同时进行受体结合和神经氨酸酶活性,并且该位点的受体结合可被小受体类似物扎那米韦抑制。我们现在报告实验证据,并辅以计算数据,证明在HPIV3 HN二聚体界面附近存在第二个受体结合位点。即使在存在扎那米韦的情况下,这个第二个结合位点也能介导受体结合,并且其在功能以及与主要结合位点的关系方面与副粘病毒新城疫病毒的第二个受体结合位点不同。HPIV3 HN的这个第二个结合位点参与触发F。我们认为,HPIV3 HN上的两个受体结合位点以不同的方式对病毒与细胞的相互作用做出贡献;一个是包含结合和神经氨酸酶活性的多功能位点,另一个具有结合活性并且也参与融合促进。

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