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通过糖磷脂锚定的Thy-1交联激活T淋巴细胞,可动员与抗原受体/CD3复合物诱导产生的细胞内第二信使不同的池。

Activation of T lymphocytes by cross-linking of glycophospholipid-anchored Thy-1 mobilizes separate pools of intracellular second messengers to those induced by the antigen-receptor/CD3 complex.

作者信息

Barboni E, Gormley A M, Pliego Rivero F B, Vidal M, Morris R J

机构信息

Norman and Sadie Lee Research Centre, National Institute for Medical Research, Mill Hill, London, U.K.

出版信息

Immunology. 1991 Apr;72(4):457-63.

Abstract

T cells can be activated, not only by the conventional (antigen-receptor/CD3 complex) route, but also by cross-linking any one of their lipid-anchored surface glycoproteins. We have compared early transmembrane signalling events mediated through CD3 with those mediated through Thy-1, a lipid-linked surface glycoprotein, on the human lymphoid cell line Jurkat and transfectants expressing higher levels of Thy-1. Cross-linking of Thy-1 causes immediate phosphatidylinositol (PI) turnover and an influx of extracellular Ca2+, while releasing very little Ca2+ from intracellular stores. CD3 activation, on the other hand, causes PI turnover which releases intracellular Ca2+, and only secondarily induces an influx of extracellular ions. The Thy-1 response is detectable at very low levels of surface Thy-1, and is not mimicked by enzymatic removal of lipid-linked proteins from the cell surface. The Thy-1-induced Ca2+ influx is more sensitive to L channel blockers than the CD3-mediated flux. These results indicate that the initial stages of Thy-1-mediated activation involve the rapid and extensive mobilization of the intracellular second messengers, PI and Ca2+, by mechanisms separate to those activated by the antigen-receptor/CD3 complex.

摘要

T细胞不仅可以通过传统途径(抗原受体/CD3复合物)被激活,还可以通过交联其任何一种脂质锚定的表面糖蛋白来激活。我们已经比较了通过CD3介导的早期跨膜信号事件与通过Thy-1(一种脂质连接的表面糖蛋白)在人淋巴细胞系Jurkat和表达更高水平Thy-1的转染子上介导的早期跨膜信号事件。Thy-1的交联导致立即的磷脂酰肌醇(PI)周转和细胞外Ca2+的流入,同时从细胞内储存库释放很少的Ca2+。另一方面,CD3激活导致PI周转,释放细胞内Ca2+,并且仅其次诱导细胞外离子的流入。在非常低水平的表面Thy-1时就可以检测到Thy-1反应,并且细胞表面脂质连接蛋白的酶促去除不会模拟该反应。Thy-1诱导的Ca2+流入比CD3介导的通量对L通道阻滞剂更敏感。这些结果表明,Thy-1介导的激活的初始阶段涉及通过与抗原受体/CD3复合物激活的机制分开的机制,快速而广泛地动员细胞内第二信使PI和Ca2+。

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