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对一种与52 kDa胰岛蛋白反应的人T细胞系的表征。

Characterization of a human T cell line reactive to a 52 kDa islet protein.

作者信息

Sobel D O, Fleisher T, Karounos D G

机构信息

Department of Pediatrics and Lombardi Cancer Center, Georgetown University School of Medicine, Washington, DC 20007-2197, USA.

出版信息

J Autoimmun. 1997 Aug;10(4):387-94. doi: 10.1006/jaut.1997.0151.

Abstract

A 52 kDa islet protein has recently been identified as the target of autoantibodies in the NOD mouse model of IDDM and humans with IDDM. However, the presence of T cell immunity against the 52 kDa islet protein in IDDM has not been reported. We report the establishment and characterization of a T cell line (19KW) that reacts to purified 52 kDa islet protein (purified p52) from a subject with IDDM. The purified p52 induced a proliferative response as measured by thymidine incorporation in the 19KW T cell line with a stimulating index of up to 48. The proliferative responses were greater with increasing doses of purified p52 (0.1, 0.5, 2.0, and 6.0 microg/well). No reactivity was found to a liver fraction purified in the same manner as 52 kDa protein, BSA, ovalbumin, extracts of rat muscle, fibroblast, adrenal, or pituitary tissue and to a rat exocrine cell tumor. Irradiated PBMC were required as antigen presenting cells (APC) for 19KW reactivity to the purified p52. The addition of anti-HLA DR or anti-HLA DQ antibodies significantly decreased the islet antigen-induced proliferative response. The addition of antibodies to HLA DP and class I MHC had no effect. Flow cytometric analysis revealed that the majority of T cells expressed CD4 and CD45RO molecules. T cell receptors Vbeta6 and Vbeta5.1 were found on 30 and 14% of the CD3+ (T cells) 19KW cells, respectively. In conclusion, a purified p52-reactive human T cell line predominantly consisting of TCR Vbeta6+ and Vbeta5.1+ cells has been established from a subject with IDDM. Reactivity to the purified p52 is antigen dose-dependent, tissue specific, requires irradiated PBMC as antigen presenting cells, and is HLA DR- and HLA DQ-restricted. T cell lines specifically reactive to p52 may be useful for investigating further the role of this antigen in the pathogenesis of IDDM.

摘要

一种52 kDa的胰岛蛋白最近在IDDM的NOD小鼠模型和患IDDM的人类中被确定为自身抗体的靶标。然而,尚未有关于IDDM中针对52 kDa胰岛蛋白的T细胞免疫反应的报道。我们报告了一种T细胞系(19KW)的建立及其特性,该细胞系对一名IDDM患者的纯化52 kDa胰岛蛋白(纯化的p52)有反应。通过在19KW T细胞系中检测胸苷掺入量来测定,纯化的p52诱导了增殖反应,刺激指数高达48。随着纯化p52剂量(0.1、0.5、2.0和6.0微克/孔)增加,增殖反应增强。未发现对以与52 kDa蛋白相同方式纯化的肝脏组分、牛血清白蛋白、卵清蛋白、大鼠肌肉、成纤维细胞、肾上腺或垂体组织提取物以及大鼠外分泌细胞瘤有反应。需要经辐照的外周血单核细胞(PBMC)作为抗原呈递细胞(APC)才能使19KW对纯化的p52产生反应。添加抗HLA DR或抗HLA DQ抗体可显著降低胰岛抗原诱导的增殖反应。添加针对HLA DP和I类MHC的抗体则无作用。流式细胞术分析显示,大多数T细胞表达CD4和CD45RO分子。在19KW细胞的CD3 +(T细胞)中,分别有30%和14%的细胞发现有T细胞受体Vbeta6和Vbeta5.1。总之,已从一名IDDM患者中建立了一种主要由TCR Vbeta6 +和Vbeta5.1 +细胞组成的纯化p52反应性人T细胞系。对纯化p52的反应具有抗原剂量依赖性、组织特异性,需要经辐照的PBMC作为抗原呈递细胞,并且受HLA DR和HLA DQ限制。对p52具有特异性反应的T细胞系可能有助于进一步研究该抗原在IDDM发病机制中的作用。

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