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通过CD40发出的信号可挽救X连锁高IgM免疫缺陷中IgE的分泌,但不能挽救IgG或IgA的分泌。

Signaling through CD40 rescues IgE but not IgG or IgA secretion in X-linked immunodeficiency with hyper-IgM.

作者信息

Saiki O, Tanaka T, Wada Y, Uda H, Inoue A, Katada Y, Izeki M, Iwata M, Nunoi H, Matsuda I

机构信息

Department of Clinical Investigation, Osaka Minami National Hospital, Japan.

出版信息

J Clin Invest. 1995 Feb;95(2):510-4. doi: 10.1172/JCI117692.

Abstract

The ligand for CD40 (CD40L) is a membrane protein on activated T cells that induces B cell proliferation and differentiation. Several mutations of the CD40L gene were reported responsible for defective class switching of B cells in an X-linked immunodeficiency with hyper IgM (X-HIM). We studied four affected males from three families and found three independent mutations including new mutations of CD40L gene. In every X-HIM patient tested, however, anti-CD40 plus IL-10 did not induce class switching from IgM to IgG or IgA, even in the presence of Staphylococcus aureus Cowan I strain (SAC). CD4+ T cell clones, expressing CD40L on their surface, also did not rescue IgG or IgA induction by X-HIM peripheral blood B cells in vitro. But signaling through CD40 induced both B cell proliferation and IgE secretion when IL-4 was added to the culture. Taken together, these results show that in vitro signaling through CD40 rescues IgE but not IgG or IgA secretion by peripheral blood X-HIM B cells and suggest that in vivo CD40 and CD40L interaction might be necessary for IgG and IgA differentiation in X-HIM.

摘要

CD40的配体(CD40L)是活化T细胞上的一种膜蛋白,可诱导B细胞增殖和分化。据报道,CD40L基因的几种突变与X连锁高IgM免疫缺陷病(X-HIM)中B细胞的类别转换缺陷有关。我们研究了来自三个家族的四名患病男性,发现了三个独立的突变,包括CD40L基因的新突变。然而,在每个接受检测的X-HIM患者中,即使存在金黄色葡萄球菌考恩I株(SAC),抗CD40加IL-10也不能诱导从IgM到IgG或IgA的类别转换。表面表达CD40L的CD4+T细胞克隆在体外也不能挽救X-HIM外周血B细胞诱导的IgG或IgA产生。但是,当向培养物中添加IL-4时,通过CD40的信号传导可诱导B细胞增殖和IgE分泌。综上所述,这些结果表明,体外通过CD40的信号传导可挽救外周血X-HIM B细胞分泌IgE,但不能挽救IgG或IgA分泌,这表明在X-HIM中,体内CD40与CD40L的相互作用可能是IgG和IgA分化所必需的。

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