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口蹄疫病毒外衣壳蛋白VP1上参与中和作用及细胞附着的表位。

Epitopes on foot-and-mouth disease virus outer capsid protein VP1 involved in neutralization and cell attachment.

作者信息

Baxt B, Morgan D O, Robertson B H, Timpone C A

出版信息

J Virol. 1984 Aug;51(2):298-305. doi: 10.1128/JVI.51.2.298-305.1984.

Abstract

Foot-and-mouth disease virus structural protein VP1 elicits neutralizing and protective antibody and is probably the viral attachment protein which interacts with cellular receptor sites on cultured cells. To study the relationships between epitopes on the molecule related to neutralization and cell attachment, we tested monoclonal antibodies prepared against type A12 virus, isolated A12 VP1, and a CNBr-generated A12 VP1 fragment for neutralization and effect on viral absorption. The antibodies selected for analysis neutralized viral infectivity with varying efficiencies. One group of antibodies caused a high degree of viral aggregation and inhibited the adsorption of virus to cells by 50 to 70%. A second group of antibodies caused little or no viral aggregation but inhibited the adsorption of virus to cells by 80 to 90%. One antibody, which is specific for the intact virion, caused little viral aggregation and had no effect on the binding of virus to specific cellular receptor sites. Thus, at least three antigenic areas on the surface of foot-and-mouth disease virus which were involved in neutralization were demonstrated. One of the antigenic sites appears to have been responsible for interaction with the cellular receptor sites on the surface of susceptible cells.

摘要

口蹄疫病毒结构蛋白VP1可诱导产生中和性及保护性抗体,它可能是与培养细胞上的细胞受体位点相互作用的病毒附着蛋白。为了研究该分子上与中和作用及细胞附着相关的表位之间的关系,我们检测了针对A12型病毒、分离得到的A12 VP1以及一种经溴化氰处理产生的A12 VP1片段制备的单克隆抗体的中和作用及其对病毒吸附的影响。挑选用于分析的抗体以不同效率中和病毒感染性。一组抗体导致高度的病毒聚集,并使病毒对细胞的吸附抑制50%至70%。第二组抗体几乎不引起或不引起病毒聚集,但使病毒对细胞的吸附抑制80%至90%。一种对完整病毒粒子具有特异性的抗体几乎不引起病毒聚集,且对病毒与特定细胞受体位点的结合没有影响。因此,证实了口蹄疫病毒表面至少有三个参与中和作用的抗原区域。其中一个抗原位点似乎负责与易感细胞表面的细胞受体位点相互作用。

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