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系统性红斑狼疮患者体外T细胞与B细胞活性及血清白细胞介素-2水平的相关性

Correlation of T and B cell activities in vitro and serum IL-2 levels in systemic lupus erythematosus.

作者信息

Huang Y P, Perrin L H, Miescher P A, Zubler R H

机构信息

Department of Medicine, Geneva University Hospital, Switzerland.

出版信息

J Immunol. 1988 Aug 1;141(3):827-33.

PMID:3135313
Abstract

There have been only a few studies indicating that B cell hyperactivity in SLE could depend on Th cell activation. In particular, circulating CD4+ cells were found to express Ia. Our own previous investigations have shown that the decreased IL-2 secretion capacity in vitro of CD4+ cells in SLE is restored to normal when the cells are rested for a few days in culture. This suggested the presence of activated, exhausted T cells in the circulation. In this study, we report several observations concerning T cell function in SLE. 1) Decreased IL-2 secretion in vitro of PBL was found to correlate significantly with increased spontaneous IgG secretion of such cells; immunosuppressive treatment of 22 patients with steroids plus cyclosporin A led, to a large extent, to a correction of both abnormalities. 2) 9 of 18 patients with active disease (and low IL-2 secretion in vitro) had increased IL-2 levels in serum by ELISA; two sera contained IL-2 biologic activity, and chromatography of one serum showed IL-2 in a high molecular size complex (Mr approximately 50,000) dissociable with 6 M urea. The serum levels of IL-2R were also frequently increased, even in less active SLE. 3) In cell culture experiments, the IgG secretion by purified B cells from 6 of 9 patients with active SLE was increased by autologous T cells acting either alone (3 patients) or synergistically with rIL-2 (3 patients); the B cells from all 9 patients showed increased IL-2 responsiveness compared with blood donor B cells. Taken together, these results provide new evidence that increased T cell activation occurs and plays a role in SLE.

摘要

仅有少数研究表明,系统性红斑狼疮(SLE)中B细胞的过度活跃可能依赖于Th细胞的激活。特别是,发现循环中的CD4+细胞表达Ia。我们自己之前的研究表明,当SLE患者的CD4+细胞在培养中静置几天时,其体外IL-2分泌能力的下降可恢复正常。这表明循环中存在活化的、耗竭的T细胞。在本研究中,我们报告了一些关于SLE中T细胞功能的观察结果。1)发现外周血淋巴细胞(PBL)体外IL-2分泌减少与这些细胞自发IgG分泌增加显著相关;对22例患者用类固醇加环孢素A进行免疫抑制治疗,在很大程度上纠正了这两种异常情况。2)18例活动期疾病患者(体外IL-2分泌低)中有9例通过酶联免疫吸附测定(ELISA)血清中IL-2水平升高;两份血清含有IL-2生物活性,一份血清的色谱分析显示IL-2存在于一种可被6M尿素解离的高分子量复合物(分子量约50,000)中。即使在病情不太活跃的SLE患者中,IL-2受体的血清水平也经常升高。3)在细胞培养实验中,9例活动期SLE患者中有6例的纯化B细胞单独受到自体T细胞作用(3例患者)或与重组白细胞介素-2(rIL-2)协同作用(3例患者)时,IgG分泌增加;与献血者B细胞相比,所有9例患者的B细胞对IL-2的反应性均增强。综上所述,这些结果提供了新的证据,表明T细胞活化增加在SLE中发生并起作用。

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