磷脂酶D的激活:一个由T淋巴细胞抗原受体/CD3复合物的扰动而启动的信号系统。

S J Stewart, G R Cunningham, J A Strupp, F S House, L L Kelley, G S Henderson, J H Exton, S B Bocckino
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引用次数: 26

摘要

许多细胞信号系统通过T淋巴细胞抗原受体/CD3复合物与其同源抗原的相互作用而发挥作用。良好描述的信号系统包括磷酸肌肽转换、酪氨酸磷酸化、蛋白激酶C激活和胞质钙增加。我们已经探索了另一种最近描述的信号系统的可能性,磷脂酶D的激活可能起作用。本文提供的数据表明,通过磷脂酰乙醇和磷脂酸的产生,用抗cd3抗体或磷脂酯刺激Jurkat T细胞导致磷脂酶D的激活。抗cd3抗体与磷酸酯的结合导致磷脂酰乙醇的产量大于添加剂,而磷脂酸的添加剂产量(不含乙醇)大于添加剂产量。含抗cd3抗体的酚酯作为第二种刺激导致细胞中二酰基甘油含量的增加,但没有增加肌醇磷酸的产生,这表明这些细胞中的二酰基甘油的产生是由含有脂质的非肌醇和磷脂苷水解产生的。磷脂酸的外源性添加导致胞质钙的增加,这取决于所使用的浓度,是由细胞内钙储存的释放和细胞外钙的流入造成的。在没有肌醇磷酸产生的情况下,胞质钙发生变化。这些研究确定了磷脂酶D活性增加在T淋巴细胞活化中的作用。
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Activation of phospholipase D: a signaling system set in motion by perturbation of the T lymphocyte antigen receptor/CD3 complex.

A number of cellular signaling systems are called into play by interaction of the T lymphocyte antigen receptor/CD3 complex with its cognate antigen. Well-described signaling systems include phosphoinositide turnover, tyrosine phosphorylation, protein kinase C activation, and increased cytosolic calcium. We have explored the possibility that another recently described signaling system, activation of phospholipase D, may be operative. Data presented here demonstrate that stimulation of Jurkat T cells with anti-CD3 antibodies or phorbol esters resulted in activation of phospholipase D, as measured by production of phosphatidylethanol and phosphatidic acid. The combination of anti-CD3 antibody plus phorbol ester led to a greater than additive production of phosphatidylethanol and to the additive production of phosphatidic acid (in the absence of ethanol). Phorbol esters as a second stimulus with anti-CD3 antibody led to a additive increase in cellular diacylglycerol content but provided no increased production of inositol phosphates, suggesting that diacylglycerol production in these cells results from hydrolysis of noninositol containing lipids as well as from phosphinositides. Exogenous addition of phosphatidic acid led to increases in cytosolic calcium that, depending on the concentration used, resulted from release of an intracellular store of calcium and influx of extracellular calcium. Changes in cytosolic calcium occurred in the absence of inositol phosphates production. These studies establish a role for increased phospholipase D activity in T lymphocyte activation.

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