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细胞内介质在CD2介导的T细胞活化过程中调节CD2的侧向扩散和细胞质Ca2+动员。

Intracellular mediators regulate CD2 lateral diffusion and cytoplasmic Ca2+ mobilization upon CD2-mediated T cell activation.

作者信息

Liu S J, Hahn W C, Bierer B E, Golan D E

机构信息

Department of Biological Chemistry, Dana-Farber Cancer Institute, Boston, Massachusetts.

出版信息

Biophys J. 1995 Feb;68(2):459-70. doi: 10.1016/S0006-3495(95)80207-9.

Abstract

CD2 is a T cell surface glycoprotein that participates in T cell adhesion and activation. These processes are dynamically interrelated, in that T cell activation regulates the strength of CD2-mediated T cell adhesion. The lateral redistribution of CD2 and its ligand CD58 (LFA-3) in T cell and target membranes, respectively, has also been shown to affect cellular adhesion strength. We have used the fluorescence photobleaching recovery technique to measure the lateral mobility of CD2 in plasma membranes of resting and activated Jurkat T leukemia cells. CD2-mediated T cell activation caused lateral immobilization of 90% of cell surface CD2 molecules. Depleting cells of cytoplasmic Ca2+, loading cells with dibutyric cAMP, and disrupting cellular microfilaments each partially reversed the effect of CD2-mediated activation on the lateral mobility of CD2. These intracellular mediators apparently influence the same signal transduction pathways, because the effects of the mediators on CD2 lateral mobility were not additive. In separate experiments, activation-associated cytoplasmic Ca2+ mobilization was found to require microfilament integrity and to be negatively regulated by cAMP. By directly or indirectly controlling CD2 lateral diffusion and cell surface distribution, cytoplasmic Ca2+ mobilization may have an important regulatory role in CD2 mediated T cell adhesion.

摘要

CD2是一种T细胞表面糖蛋白,参与T细胞黏附和激活。这些过程是动态相互关联的,因为T细胞激活调节CD2介导的T细胞黏附强度。CD2及其配体CD58(淋巴细胞功能相关抗原3)分别在T细胞和靶细胞膜中的侧向再分布也已被证明会影响细胞黏附强度。我们使用荧光光漂白恢复技术来测量静息和活化的Jurkat T白血病细胞质膜中CD2的侧向流动性。CD2介导的T细胞激活导致90%的细胞表面CD2分子侧向固定。耗尽细胞质中的Ca2+、用二丁酰cAMP加载细胞以及破坏细胞微丝,每一种方法都部分逆转了CD2介导的激活对CD2侧向流动性的影响。这些细胞内介质显然影响相同的信号转导途径,因为这些介质对CD2侧向流动性的影响不是相加的。在单独的实验中,发现激活相关的细胞质Ca2+动员需要微丝完整性,并受到cAMP的负调节。通过直接或间接控制CD2侧向扩散和细胞表面分布,细胞质Ca2+动员可能在CD2介导的T细胞黏附中起重要调节作用。

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