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带有独特分化抗原的两种人类T细胞亚类的检测、分离及功能特性分析

Detection, isolation, and functional characterization of two human T-cell subclasses bearing unique differentiation antigens.

作者信息

Evans R L, Breard J M, Lazarus H, Schlossman S F, Chess L

出版信息

J Exp Med. 1977 Jan 1;145(1):221-33. doi: 10.1084/jem.145.1.221.

Abstract

A heterologous antihuman T-cell serum (anti-TH1), raised against purified peripheral T cells, and absorbed with an autologous Ig+ line, was shown to bind specifically to T- but not to B-lymphoid cells by both a complement-dependent cytotoxic assay and indirect immunofluorescence. Whereas 90% fetal thymocytes and thymocytes were killed by anti-TH1 and complement, a consistently restricted population (50-60%) of peripheral T cells from several normal donors were lysed, indicating that anti-TH1 is directed against one or more thymus-specific antigens which are lost or reduced on a subpopulation of human T cells in the periphery. Functional analysis of the unreactive (TH1-) and reactive (TH1+) T-cell subclasses demonstrated that TH1- cells mounted a good proliferative response to a battery of specific soluble antigens (mumps, PPD, tetanus toxoid) but neither responded in MLC, nor elaborated LMF in response to tetanus toxoid. In contrast TH1+ cells proliferated in MLC and elaborated LMF but did not respond by 3H-incorporation to soluble antigens. The relevance of these findings to human T-cell functions in vivo and to previously described functional subclasses of murine T cells is discussed.

摘要

一种针对纯化外周血T细胞制备的、并用自体Ig + 细胞系吸收的异种抗人T细胞血清(抗TH1),通过补体依赖性细胞毒性试验和间接免疫荧光法显示,它能特异性结合T淋巴细胞而非B淋巴细胞。抗TH1和补体可杀死90%的胎儿胸腺细胞和胸腺细胞,而来自几个正常供体的外周血T细胞中,始终有一个受限群体(50 - 60%)被裂解,这表明抗TH1针对的是一种或多种胸腺特异性抗原,这些抗原在外周血人类T细胞的一个亚群中丢失或减少。对无反应性(TH1 -)和反应性(TH1 +)T细胞亚类的功能分析表明,TH1 - 细胞对一系列特异性可溶性抗原(腮腺炎、结核菌素纯蛋白衍生物、破伤风类毒素)有良好的增殖反应,但在混合淋巴细胞培养中无反应,对破伤风类毒素也不产生淋巴毒素。相比之下,TH1 + 细胞在混合淋巴细胞培养中增殖并产生淋巴毒素,但对可溶性抗原不通过3H掺入法产生反应。本文讨论了这些发现与人类体内T细胞功能以及先前描述的小鼠T细胞功能亚类的相关性。

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