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CD58(淋巴细胞功能相关抗原-3)刺激可提供一种不同于CD40的信号,用于人类抗体亚型转换和IgE产生。

CD58 (LFA-3) stimulation provides a signal for human isotype switching and IgE production distinct from CD40.

作者信息

Diaz-Sanchez D, Chegini S, Zhang K, Saxon A

机构信息

Hart and Louise Lyon Laboratory, Department of Medicine, UCLA School of Medicine 90024-1680.

出版信息

J Immunol. 1994 Jul 1;153(1):10-20.

PMID:7515920
Abstract

Induction of an IgE response involves several discrete steps: 1) induction of epsilon germ line transcription, 2) DNA recombination, and 3) mature RNA transcription/translation. Here we show that ligation of B cell CD58 by CD2, its natural ligand on T cells, or by mAb, provides a novel IL-4-dependent signal for the latter two steps. Highly purified human B cells were induced to produce IgE by costimulation with IL-4 and CD58 mAb. Although CD58 ligation alone was unable to induce epsilon germ-line transcription, in concert with IL-4-stimulated epsilon germ-line transcription it induced the appearance of productive epsilon transcripts and IgE production. The direct involvement of CD2 was demonstrated: B cells cultured with IL-4 plus murine T hybridoma cells transfected with human CD2 produced IgE. A CD40 Fc fusion protein had no effect on CD58-driven IgE production while inhibiting CD40-dependent responses. Furthermore, cells from patients with common variable immunodeficiency produced IgE in response to IL-4 plus CD40 mAb but not to IL-4 plus CD58 mAb. CD58-driven IgE synthesis was IFN-gamma independent and was not enhanced by exogenous IL-6. Functional differences between CD40 and CD58 IgE stimulation were demonstrated. Thus, the CD2:CD58 ligand/counterligand system provides an alternative pathway by which cell contact signaling may regulate IgE. Given the relative importance of CD2 triggering on mucosal T cells and the mucosal location of IgE production, this may be especially true on mucosal surfaces.

摘要

IgE反应的诱导涉及几个离散步骤:1)ε种系转录的诱导,2)DNA重组,以及3)成熟RNA转录/翻译。在这里,我们表明,T细胞上的天然配体CD2或单克隆抗体与B细胞CD58的结合为后两个步骤提供了一种新的IL-4依赖性信号。高度纯化的人B细胞通过IL-4和CD58单克隆抗体的共刺激被诱导产生IgE。尽管单独的CD58连接不能诱导ε种系转录,但与IL-4刺激的ε种系转录协同作用时,它诱导了有活性的ε转录本的出现和IgE的产生。CD2的直接参与得到了证实:用IL-4加上转染了人CD2的鼠T杂交瘤细胞培养的B细胞产生了IgE。一种CD40 Fc融合蛋白对CD58驱动的IgE产生没有影响,同时抑制了CD40依赖性反应。此外,常见可变免疫缺陷患者的细胞对IL-4加CD40单克隆抗体有反应而产生IgE,但对IL-4加CD58单克隆抗体没有反应。CD58驱动的IgE合成不依赖于IFN-γ,并且不会因外源性IL-6而增强。证明了CD40和CD58 IgE刺激之间的功能差异。因此,CD2:CD58配体/反配体系统提供了一种细胞接触信号可能调节IgE的替代途径。鉴于CD2触发对黏膜T细胞的相对重要性以及IgE产生的黏膜位置,这在黏膜表面可能尤其如此。

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CD58 (LFA-3) stimulation provides a signal for human isotype switching and IgE production distinct from CD40.CD58(淋巴细胞功能相关抗原-3)刺激可提供一种不同于CD40的信号,用于人类抗体亚型转换和IgE产生。
J Immunol. 1994 Jul 1;153(1):10-20.
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