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犬细小病毒病毒粒子和重组VP2衣壳的拓扑分析。

Topographical analysis of canine parvovirus virions and recombinant VP2 capsids.

作者信息

Cortes E, San Martin C, Langeveld J, Meloen R, Dalsgaard K, Vela C, Casal I

机构信息

Centro de Biologia Molecular, CSIC-UAM, Cantoblanco, Madrid, Spain.

出版信息

J Gen Virol. 1993 Sep;74 ( Pt 9):2005-10. doi: 10.1099/0022-1317-74-9-2005.

Abstract

The distribution of epitopes defined by monoclonal antibodies (MAbs) on the surface of canine parvovirus (CPV) virions and recombinant VP2-capsids was established using immunoelectron microscopy. A correlation appeared to exist between the linear position, neutralizing activity and immunogold staining. Both viral capsids and recombinant capsids gave similar patterns of immunostaining. The neutralizing MAbs that recognized epitopes not previously identified by Pepscan or immunoblotting gave a clear staining. However, MAbs 3C9 and 3C10, identified by Pepscan and immunoblotting as recognizing linear epitopes, did not show any labelling (3C9) or only scattered labelling (3C10). MAb 3C9 recognizes an N-terminal domain of VP2. MAb 4AG6, which recognizes the same linear epitope as 3C10, did not bind to the capsids, indicating a different orientation. An immunofluorescence assay was performed to supplement the B cell epitope characterization. In contrast to other MAbs that gave nuclear and cytoplasmic staining, MAb 3C9 gave a preferential nuclear staining. Based on these results, it is hypothesized that the N terminus of VP2 is barely, or not at all, exposed on the surface of the native virions, but becomes accessible after some virion steric change (e.g. after attachment to the cell receptor).

摘要

利用免疫电子显微镜确定了单克隆抗体(MAb)所定义的表位在犬细小病毒(CPV)病毒粒子和重组VP2衣壳表面的分布。线性位置、中和活性与免疫金染色之间似乎存在相关性。病毒衣壳和重组衣壳给出了相似的免疫染色模式。识别先前未通过肽扫描或免疫印迹鉴定的表位的中和单克隆抗体给出了清晰的染色。然而,通过肽扫描和免疫印迹鉴定为识别线性表位的单克隆抗体3C9和3C10未显示任何标记(3C9)或仅显示散在标记(3C10)。单克隆抗体3C9识别VP2的N端结构域。识别与3C10相同线性表位的单克隆抗体4AG6不与衣壳结合,表明其方向不同。进行了免疫荧光试验以补充B细胞表位特征分析。与其他给出核和细胞质染色的单克隆抗体不同,单克隆抗体3C9给出优先的核染色。基于这些结果,推测VP2的N端在天然病毒粒子表面几乎不暴露或根本不暴露,但在病毒粒子发生一些空间变化后(例如在附着于细胞受体后)变得可及。

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