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聚集蛋白对免疫突触的生理调节

Physiological regulation of the immunological synapse by agrin.

作者信息

Khan A A, Bose C, Yam L S, Soloski M J, Rupp F

机构信息

Outer Banks Neuroscience, Baltimore, MD 21218, USA.

出版信息

Science. 2001 Jun 1;292(5522):1681-6. doi: 10.1126/science.1056594. Epub 2001 May 10.

Abstract

T cell activation is dependent on both a primary signal delivered through the T cell receptor and a secondary costimulatory signal mediated by coreceptors. Although controversial, costimulation is thought to act through the specific redistribution and clustering of membrane and intracellular kinase-rich lipid raft microdomains at the contact site between T cells and antigen-presenting cells. This site has been termed the immunological synapse. Endogenous mediators of raft clustering in lymphocytes have not been identified, although they are essential for T cell activation. We now demonstrate that agrin, an aggregating protein crucial for formation of the neuromuscular junction, is also expressed in lymphocytes and is important in reorganization of membrane lipid microdomains and setting the threshold for T cell signaling. Our data show that agrin induces the aggregation of signaling proteins and the creation of signaling domains in both immune and nervous systems through a common lipid raft pathway.

摘要

T细胞的激活既依赖于通过T细胞受体传递的初级信号,也依赖于由共受体介导的次级共刺激信号。尽管存在争议,但人们认为共刺激作用是通过膜和富含细胞内激酶的脂筏微结构域在T细胞与抗原呈递细胞接触部位的特异性重新分布和聚集来实现的。这个部位被称为免疫突触。淋巴细胞中脂筏聚集的内源性介质尚未被确定,尽管它们对T细胞激活至关重要。我们现在证明,聚集蛋白聚糖(一种对神经肌肉接头形成至关重要的聚集蛋白)也在淋巴细胞中表达,并且在膜脂微结构域的重组以及设定T细胞信号传导阈值方面发挥重要作用。我们的数据表明,聚集蛋白聚糖通过共同的脂筏途径诱导免疫和神经系统中信号蛋白的聚集以及信号域的形成。

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