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针对人嗜T细胞病毒1型和2型gp46构象表位的人源中和性单克隆抗体。

Neutralizing human monoclonal antibodies to conformational epitopes of human T-cell lymphotropic virus type 1 and 2 gp46.

作者信息

Hadlock K G, Rowe J, Perkins S, Bradshaw P, Song G Y, Cheng C, Yang J, Gascon R, Halmos J, Rehman S M, McGrath M S, Foung S K

机构信息

Department of Pathology, Stanford University School of Medicine, California 94305, USA.

出版信息

J Virol. 1997 Aug;71(8):5828-40. doi: 10.1128/JVI.71.8.5828-5840.1997.

DOI:10.1128/JVI.71.8.5828-5840.1997
PMID:9223472
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC191838/
Abstract

Ten human monoclonal antibodies derived from peripheral B cells of a patient with human T-cell lymphotropic virus (HTLV)-associated myelopathy are described. One monoclonal antibody recognized a linear epitope within the carboxy-terminal 43 amino acids of HTLV gp21, and two monoclonal antibodies recognized linear epitopes within HTLV type 1 (HTLV-1) gp46. The remaining seven monoclonal antibodies recognized denaturation-sensitive epitopes within HTLV-1 gp46 that were expressed on the surfaces of infected cells. Two of these antibodies also bound to viable HTLV-2 infected cells and immunoprecipitated HTLV-2 gp46. Virus neutralization was determined by syncytium inhibition assays. Eight monoclonal antibodies, including all seven that recognized denaturation-sensitive epitopes within HTLV-1 gp46, possessed significant virus neutralization activity. By competitive inhibition analysis it was determined that these antibodies recognized at least four distinct conformational epitopes within HTLV-1 gp46. These findings indicate the importance of conformational epitopes within HTLV-1 gp46 in mediating a neutralizing antibody response to HTLV infection.

摘要

本文描述了从一名患有人嗜T淋巴细胞病毒(HTLV)相关脊髓病患者的外周B细胞中获得的十种人单克隆抗体。一种单克隆抗体识别HTLV gp21羧基末端43个氨基酸内的线性表位,两种单克隆抗体识别1型HTLV(HTLV-1)gp46内的线性表位。其余七种单克隆抗体识别HTLV-1 gp46内的变性敏感表位,这些表位在受感染细胞表面表达。其中两种抗体也与活的HTLV-2感染细胞结合,并免疫沉淀HTLV-2 gp46。通过合胞体抑制试验测定病毒中和作用。包括所有七种识别HTLV-1 gp46内变性敏感表位的单克隆抗体在内的八种单克隆抗体具有显著的病毒中和活性。通过竞争抑制分析确定,这些抗体识别HTLV-1 gp46内至少四个不同的构象表位。这些发现表明HTLV-1 gp46内的构象表位在介导对HTLV感染的中和抗体反应中的重要性。

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