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免疫信号素CD100/SEMA4D的结构与功能

Structure and function of the immune semaphorin CD100/SEMA4D.

作者信息

Elhabazi Abdellah, Marie-Cardine Anne, Chabbert-de Ponnat Isabelle, Bensussan Armand, Boumsell Laurence

机构信息

Department of Biology, Faculty of Sciences, El Jadida Morocco.

出版信息

Crit Rev Immunol. 2003;23(1-2):65-81. doi: 10.1615/critrevimmunol.v23.i12.40.

DOI:10.1615/critrevimmunol.v23.i12.40
PMID:12906260
Abstract

Semaphorins are a large family of membrane-bound and secreted molecules involved in numerous functions, including axon guidance, morphogenesis, carcinogenesis, and immunomodulation. A growing number of semaphorins--namely, human CD100/SEMA4D, CD108/SEMA7A, and SEMA3A; viral semaphorins, SemaVA and SemaVB; and, very recently, mouse Sema4A--were reported to regulate immune cell responses. Among them, the role of CD100 has been well documented in both humans and mice. CD100, in particular, has been shown to influence monocyte migration, T-cell activation, B-cell survival as well as T/B and T/dendritic cell cooperation. In contrast to other semaphorins, CD100 is the only semaphorin for which membrane and soluble forms are endowed with functional properties, and for which bidirectional signaling has been suggested. The human membrane-bound CD100 engagement triggers costimulatory signals to T cells through its interaction with membrane protein tyrosine phosphatase CD45 and an intracellular serine kinase. Its soluble extracellular region acts most likely through its receptors, human PlexinB1 and mouse CD72, to promote T-cell priming, B-cell survival and antibody production in response to T-dependent antigens. Human soluble CD100 also induces monocyte paralysis and the arrest of its spontaneous and chemokine-induced migration by signaling through an as yet unknown receptor that is different from PlexinB1 and CD72. In this review, we discuss recent advances in research studies on human and murine CD100, and we describe the relationship of CD100 function to its expression and structure. The signaling events that support CD100 function are also discussed.

摘要

信号素是一大类膜结合和分泌型分子,参与多种功能,包括轴突导向、形态发生、肿瘤发生和免疫调节。越来越多的信号素——即人类CD100/SEMA4D、CD108/SEMA7A和SEMA3A;病毒信号素SemaVA和SemaVB;以及最近发现的小鼠Sema4A——被报道可调节免疫细胞反应。其中,CD100在人类和小鼠中的作用已有充分记载。特别是,CD100已被证明可影响单核细胞迁移、T细胞活化、B细胞存活以及T/B和T/树突状细胞的合作。与其他信号素不同,CD100是唯一一种膜形式和可溶性形式都具有功能特性且已被提出存在双向信号传导的信号素。人类膜结合型CD100与膜蛋白酪氨酸磷酸酶CD45和一种细胞内丝氨酸激酶相互作用,从而触发对T细胞的共刺激信号。其可溶性细胞外区域很可能通过其受体人类PlexinB1和小鼠CD72发挥作用,以促进T细胞启动、B细胞存活以及对T依赖性抗原产生抗体。人类可溶性CD100还通过一种不同于PlexinB1和CD72的未知受体发出信号,诱导单核细胞麻痹并阻止其自发迁移和趋化因子诱导的迁移。在这篇综述中,我们讨论了关于人类和小鼠CD100的研究最新进展,并描述了CD100功能与其表达和结构的关系。还讨论了支持CD100功能的信号转导事件。

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