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蛋白聚糖凝集素结构域结合硫酸化的细胞表面糖脂并促进细胞黏附。

The proteoglycan lectin domain binds sulfated cell surface glycolipids and promotes cell adhesion.

作者信息

Miura R, Aspberg A, Ethell I M, Hagihara K, Schnaar R L, Ruoslahti E, Yamaguchi Y

机构信息

Burnham Institute, La Jolla, California 92037, USA.

出版信息

J Biol Chem. 1999 Apr 16;274(16):11431-8. doi: 10.1074/jbc.274.16.11431.

Abstract

The lecticans are a group of chondroitin sulfate proteoglycans characterized by the presence of C-type lectin domains. Despite the suggestion that their lectin domains interact with carbohydrate ligands, the identity of such ligands has not been elucidated. We previously showed that brevican, a nervous system-specific lectican, binds the surface of B28 glial cells (Yamada, H., Fredette, B., Shitara, K., Hagihara, K., Miura, R., Ranscht, B., Stallcup, W. B., and Yamaguchi, Y. (1997) J. Neurosci. 17, 7784-7795). In this paper, we demonstrate that two classes of sulfated glycolipids, sulfatides and HNK-1-reactive sulfoglucuronylglycolipids (SGGLs), act as cell surface receptors for brevican. The lectin domain of brevican binds sulfatides and SGGLs in a calcium-dependent manner as expected of a C-type lectin domain. Intact, full-length brevican also binds both sulfatides and SGGLs. The lectin domain immobilized as a substrate supports adhesion of cells expressing SGGLs or sulfatides, which was inhibited by monoclonal antibodies against these glycolipids or by treatment of the substrate with SGGLs or sulfatides. Our findings demonstrate that the interaction between the lectin domains of lecticans and sulfated glycolipids comprises a novel cell substrate recognition system, and suggest that lecticans in extracellular matrices serve as substrate for adhesion and migration of cells expressing these glycolipids in vivo.

摘要

凝集素是一类硫酸软骨素蛋白聚糖,其特征在于存在C型凝集素结构域。尽管有人认为它们的凝集素结构域与碳水化合物配体相互作用,但此类配体的身份尚未阐明。我们之前表明,短蛋白聚糖是一种神经系统特异性凝集素,可结合B28神经胶质细胞的表面(山田,H.,弗雷德特,B.,志田,K.,萩原,K.,三浦,R.,兰施特,B.,斯托尔库普,W.B.,和山口,Y.(1997年)《神经科学杂志》17,7784 - 7795)。在本文中,我们证明了两类硫酸化糖脂,硫苷脂和HNK - 1反应性硫酸葡萄糖醛酸糖脂(SGGLs),作为短蛋白聚糖的细胞表面受体。正如C型凝集素结构域所预期的那样,短蛋白聚糖的凝集素结构域以钙依赖的方式结合硫苷脂和SGGLs。完整的全长短蛋白聚糖也结合硫苷脂和SGGLs。固定为底物的凝集素结构域支持表达SGGLs或硫苷脂的细胞的黏附,这被针对这些糖脂的单克隆抗体或用SGGLs或硫苷脂处理底物所抑制。我们的研究结果表明,凝集素的凝集素结构域与硫酸化糖脂之间的相互作用构成了一种新型的细胞 - 底物识别系统,并表明细胞外基质中的凝集素在体内作为表达这些糖脂的细胞黏附和迁移的底物。

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