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逆转录病毒诱导的小鼠抗TCR单克隆抗体可增强体外T细胞对细菌超抗原的增殖反应。

Retrovirally induced mouse anti-TCR monoclonals can synergize the in vitro proliferative T cell response to bacterial superantigens.

作者信息

Dehghanpisheh K, Marchalonis J J

机构信息

Department of Microbiology and Immunology, College of Medicine, University of Arizona, Tucson, USA.

出版信息

Scand J Immunol. 1997 Jun;45(6):645-54. doi: 10.1046/j.1365-3083.1997.d01-439.x.

Abstract

Antibodies directed against the beta chain of the T-cell receptor (TCR) have been detected in animals and in humans in a number of distinct immune states that do not involve direct immunization with either T cells or TCR epitopes. When C57B1/6 mice are infected experimentally with the LP-BM5 retrovirus mixture they produce increased titres of autoantibodies directed against TCR V beta complementarity determining region 1 (CDR1) epitopes. Here, the authors utilized hybridoma technology to isolate monoclonal immunoglobulin (Ig)M antibodies (MoAbs) that arose at the peak of infection. The authors characterized the binding specificity tested using synthetic peptides modelling the CDR1 segments of 24 distinct V beta gene products and determined the VH gene usage by two such monoclonals. One binds to a restricted set of TCR V beta CDR1 peptides, and the second reacts with approximately half of the CDR1 peptide homologues. These MoAbs are specific for T-cell receptor beta chains and do not bind to immunoglobulin light chains or to unrelated protein molecules. Both MoAbs bind to intact T cells expressing the V beta domain (human V beta 8 and mouse V beta 11) from which selection peptides were derived, and costimulate a V beta specific in vitro T cell proliferative response induced by the staphylcoccal enterotoxin E (SEE) superantigen.

摘要

在许多不涉及用T细胞或T细胞受体(TCR)表位直接免疫的不同免疫状态下,已经在动物和人类中检测到针对T细胞受体β链的抗体。当C57B1/6小鼠通过实验感染LP - BM5逆转录病毒混合物时,它们会产生针对TCR Vβ互补决定区1(CDR1)表位的自身抗体滴度增加。在此,作者利用杂交瘤技术分离出在感染高峰期出现的单克隆免疫球蛋白(Ig)M抗体(单克隆抗体)。作者使用模拟24种不同Vβ基因产物CDR1区段的合成肽来表征所测试的结合特异性,并通过两种这样的单克隆抗体确定VH基因的使用情况。一种与一组受限的TCR Vβ CDR1肽结合,另一种与大约一半的CDR1肽同源物反应。这些单克隆抗体对T细胞受体β链具有特异性,不与免疫球蛋白轻链或无关的蛋白质分子结合。两种单克隆抗体都与表达从中衍生出选择肽的Vβ结构域(人Vβ8和小鼠Vβ11)的完整T细胞结合,并共刺激由葡萄球菌肠毒素E(SEE)超抗原诱导的Vβ特异性体外T细胞增殖反应。

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