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T细胞CD40配体的表达缺陷导致X连锁高IgM免疫缺陷。

Defective expression of T-cell CD40 ligand causes X-linked immunodeficiency with hyper-IgM.

作者信息

Korthäuer U, Graf D, Mages H W, Brière F, Padayachee M, Malcolm S, Ugazio A G, Notarangelo L D, Levinsky R J, Kroczek R A

机构信息

Max-Planck-Gesellschaft, Arbeitsgruppe Immunologie, Universität Erlangen, Germany.

出版信息

Nature. 1993 Feb 11;361(6412):539-41. doi: 10.1038/361539a0.

Abstract

X chromosome-linked immunodeficiency with hyper-IgM (HIGM1, MIM number 308230) is a rare disorder characterized by recurrent bacterial infections, very low or absent IgG, IgA and IgE, and normal to increased IgM and IgD serum levels. HIGM1 has been suggested to result from ineffective T-cell help for B cells. We and others have identified a novel, TNF-related activation protein (TRAP) that is exclusively expressed on the surface of stimulated T cells. TRAP, a type II transmembrane protein of M(r) 33,000, is the physiological ligand for CD40 (refs 5-8). Crosslinking of CD40 on B cells induces, in the presence of lymphokines, immunoglobulin class switching from IgM to IgG, IgA or IgE. Mapping of the TRAP gene to the X-chromosomal location q26.3-q27.1 (ref. 6) suggested a causal relationship to HIGM1, which had previously been assigned to Xq26 (refs 12-14). Here we present evidence that point mutations in the TRAP gene give rise to nonfunctional or defective expression of TRAP on the surface of T cells in patients with HIGM1. The resultant failure of TRAP to interact with CD40 on functionally intact B cells is responsible for the observed immunoglobulin isotype defect in HIGM1.

摘要

X染色体连锁的高IgM免疫缺陷症(HIGM1,MIM编号308230)是一种罕见的疾病,其特征为反复发生细菌感染、IgG、IgA和IgE水平极低或缺失,而IgM和IgD血清水平正常或升高。HIGM1被认为是由于T细胞对B细胞的辅助功能无效所致。我们和其他人已经鉴定出一种新的肿瘤坏死因子相关激活蛋白(TRAP),它仅在受刺激的T细胞表面表达。TRAP是一种分子量为33,000的II型跨膜蛋白,是CD40的生理配体(参考文献5 - 8)。在细胞因子存在的情况下,B细胞上CD40的交联会诱导免疫球蛋白类别转换,从IgM转换为IgG、IgA或IgE。TRAP基因定位于X染色体q26.3 - q27.1位置(参考文献6),提示其与HIGM1存在因果关系,HIGM1此前被定位于Xq26(参考文献12 - 14)。在此我们提供证据表明,TRAP基因中的点突变导致HIGM1患者T细胞表面的TRAP无功能或表达缺陷。TRAP无法与功能完整的B细胞上的CD40相互作用,导致了HIGM1中观察到的免疫球蛋白同种型缺陷。

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