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CD19具有一个潜在的与CD77(球三糖神经酰胺)结合的位点,其序列与志贺毒素B亚单位相似:分子模拟对B细胞黏附及肠出血性大肠杆菌发病机制的影响。

CD19 has a potential CD77 (globotriaosyl ceramide)-binding site with sequence similarity to verotoxin B-subunits: implications of molecular mimicry for B cell adhesion and enterohemorrhagic Escherichia coli pathogenesis.

作者信息

Maloney M D, Lingwood C A

机构信息

Department of Microbiology, Hospital for Sick Children, Toronto, Ontario, Canada.

出版信息

J Exp Med. 1994 Jul 1;180(1):191-201. doi: 10.1084/jem.180.1.191.

Abstract

The glycosphingolipid globotriaosyl ceramide (CD77) and other globo-series glycolipids containing terminal galactose (Gal)alpha 1-4Gal residues function as receptors for the verotoxin (Shiga-like toxin) family of Escherichia coli-elaborated toxins. CD77 is also a marker for germinal center B lymphocytes and Burkitt's lymphoma cells. The pan B cell marker CD19 is a 95-kD membrane protein that appears early in B cell differentiation and is only lost upon terminal differentiation to plasma cells. CD19 is involved in signal transduction and has a regulatory role in B cell proliferation and differentiation in response to activation in vitro. However, an endogenous ligand for CD19 has not yet been identified. We report herein that the extracellular domain of CD19 has a potential CD77-binding site with extensive sequence similarity to the verotoxin B-subunits. These B-subunit-like sequences on CD19 are in close proximity following the organization of intervening amino acids into disulfide-linked domains. Cocapping of CD19 and CD77 on Burkitt's lymphoma-derived Daudi cells with anti-CD19 antibodies indicates that CD19 and CD77 are associated on the B cell surface. Cell surface binding of anti-CD19 antibodies is decreased on CD77-deficient mutant Daudi cells, suggesting that CD77 expression influences the surface expression of CD19. Wild-type Daudi cells, but not the CD19/CD77-deficient mutants, bind to matrices expressing the carbohydrate moiety of CD77 or other Gal alpha 1-4Gal containing glycolipids. This binding can be inhibited by anti-CD77 antibodies, the CD77-binding verotoxin B-subunit or anti-CD19 antibodies. Daudi cells exhibit a degree of spontaneous homotypic adhesion in culture while the CD77/CD19-deficient Daudi mutants grow as single cells. The stronger homotypic adhesion that occurs in B cells after antibody ligation of CD19 and that involves, to some extent, the integrin system, is also dramatically lower in the mutant cells relative to the parent cell line. However, reconstitution of mutant cells with CD77 restores the anti-CD19 mAb-induced adhesion to wild-type Daudi cell levels. These studies represent the first time that CD19-mediated signaling has been reconstituted in a low-responder B cell line. These convergent observations provide compelling evidence that CD19/CD77 interactions function in adhesion and signal transduction at a specific stage in B cell development and suggest that such interactions have a role in B lymphocyte homing and germinal center formation in vivo. By targeting CD77+ B cells, verotoxins may suppress the humoral arm of the immune response during infection.(ABSTRACT TRUNCATED AT 400 WORDS)

摘要

糖鞘脂球三糖神经酰胺(CD77)和其他含有末端半乳糖(Gal)α1-4Gal残基的球系列糖脂作为大肠杆菌产生的毒素中维罗毒素(志贺样毒素)家族的受体。CD77也是生发中心B淋巴细胞和伯基特淋巴瘤细胞的标志物。泛B细胞标志物CD19是一种95-kD的膜蛋白,在B细胞分化早期出现,仅在终末分化为浆细胞时才消失。CD19参与信号转导,在体外对激活的反应中对B细胞增殖和分化具有调节作用。然而,尚未鉴定出CD19内源性配体。我们在此报告,CD19的胞外结构域有一个潜在的CD77结合位点,与维罗毒素B亚基有广泛的序列相似性。CD19上这些类似B亚基的序列在中间氨基酸组织成二硫键连接结构域后紧密相邻。用抗CD19抗体对伯基特淋巴瘤来源的Daudi细胞上的CD19和CD77进行共帽实验表明,CD19和CD77在B细胞表面相关联。在CD77缺陷的突变Daudi细胞上,抗CD19抗体的细胞表面结合减少,这表明CD77的表达影响CD19的表面表达。野生型Daudi细胞,而非CD19/CD77缺陷型突变体,能与表达CD77碳水化合物部分或其他含Galα1-4Gal糖脂的基质结合。这种结合可被抗CD77抗体、与CD77结合的维罗毒素B亚基或抗CD19抗体抑制。Daudi细胞在培养中表现出一定程度的自发同型黏附,而CD77/CD19缺陷的Daudi突变体则以单细胞形式生长。在CD19抗体连接后B细胞中发生的更强的同型黏附,在一定程度上涉及整合素系统,在突变细胞中相对于亲本细胞系也显著降低。然而,用CD77重建突变细胞可将抗CD19单克隆抗体诱导的黏附恢复到野生型Daudi细胞水平。这些研究首次在低反应性B细胞系中重建了CD19介导的信号传导。这些一致的观察结果提供了令人信服的证据,表明CD19/CD77相互作用在B细胞发育的特定阶段的黏附和信号转导中起作用,并表明这种相互作用在体内B淋巴细胞归巢和生发中心形成中起作用。通过靶向CD77+B细胞,维罗毒素可能在感染期间抑制免疫反应的体液分支。(摘要截短于400字)

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