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CD21上的爱泼斯坦-巴尔病毒结合位点参与CD23结合以及人B细胞中白细胞介素-4诱导的IgE和IgG4产生。

The Epstein-Barr virus-binding site on CD21 is involved in CD23 binding and interleukin-4-induced IgE and IgG4 production by human B cells.

作者信息

Henchoz-Lecoanet S, Jeannin P, Aubry J P, Graber P, Bradshaw C G, Pochon S, Bonnefoy J Y

机构信息

Glaxo Institute for Molecular Biology, Geneva, Switzerland.

出版信息

Immunology. 1996 May;88(1):35-9. doi: 10.1046/j.1365-2567.1996.d01-651.x.

Abstract

Human CD21 has previously been described as a receptor for the C3d,g and iC3b proteins of complement, as a receptor for the gp350/220 envelope glycoprotein of the Epstein-Barr virus (EBV) and also as a receptor for inerferon-alpha (IFN-alpha). Structurally, CD21 consists of 15 to 16 short consensus repeats (SCR) of 60 to 75 amino acids followed by a transmembrane domain and an intracytoplasmic region. We reported that CD23, a low-affinity receptor for IgE (Fc epsilon R2), is a new functional ligand for CD21. We recently found that the sites of interaction of CD23 on CD21 are on SCR 5 to 8 and 1-2. The first site is a lectin-sugar type of interaction and the second site is a protein-protein interaction. We report here that amongst the other ligands for CD21 (EBV, C3d,g and IFN-alpha), only EBV is able to inhibit the binding of CD23 to CD21. Furthermore, even a peptide from gp350/220 of EBV known to bind to CD21 is able to decrease CD23 binding to CD21. Since CD23/CD21 pairing is important in the control of IgE production, we tested the effect of the EBV-derived peptide on immunoglobulin production from peripheral blood mononuclear cells and purified tonsillar B cells. Interestingly, the EBV-peptide inhibited IgE and IgG4 production induced by interleukin-4, in a dose-dependent manner. The same results were obtained using either peripheral blood mononuclear cells or purified tonsillar B cells. Another CD21 ligand, C3, did not affect binding of CD23 to CD21 nor the production of IgE and IgG4. This study indicates that blocking CD23 binding to CD21 SCR 2 on human B cells selectively modulates immunoglobulin production.

摘要

人CD21此前被描述为补体C3d,g和iC3b蛋白的受体、爱泼斯坦-巴尔病毒(EBV)的gp350/220包膜糖蛋白的受体以及干扰素-α(IFN-α)的受体。从结构上看,CD21由15至16个60至75个氨基酸的短共有重复序列(SCR)组成,后面接着一个跨膜结构域和一个胞质内区域。我们报道过,CD23,即IgE的低亲和力受体(FcεR2),是CD21的一种新的功能性配体。我们最近发现,CD23在CD21上的相互作用位点位于SCR 5至8和1 - 2。第一个位点是凝集素-糖类型的相互作用,第二个位点是蛋白质-蛋白质相互作用。我们在此报告,在CD21的其他配体(EBV、C3d,g和IFN-α)中,只有EBV能够抑制CD23与CD21的结合。此外,即使是已知与CD21结合的EBV的gp350/220的一个肽段也能够减少CD23与CD21的结合。由于CD23/CD21配对在控制IgE产生中很重要,我们测试了EBV衍生肽对外周血单个核细胞和纯化的扁桃体B细胞产生免疫球蛋白的影响。有趣的是,EBV肽以剂量依赖的方式抑制白细胞介素-4诱导的IgE和IgG4产生。使用外周血单个核细胞或纯化的扁桃体B细胞均得到相同结果。另一种CD21配体C3不影响CD23与CD21的结合,也不影响IgE和IgG4的产生。这项研究表明,阻断人B细胞上CD23与CD21 SCR 2的结合可选择性调节免疫球蛋白的产生。

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