血小板中αIIbβ3信号传导中Syk功能的遗传和药理学分析。

Genetic and pharmacological analyses of Syk function in alphaIIbbeta3 signaling in platelets.

作者信息

Law D A, Nannizzi-Alaimo L, Ministri K, Hughes P E, Forsyth J, Turner M, Shattil S J, Ginsberg M H, Tybulewicz V L, Phillips D R

机构信息

COR Therapeutics, Inc, South San Francisco, CA, USA.

出版信息

Blood. 1999 Apr 15;93(8):2645-52.

PMID:10194444

Abstract

Agonists induce inside-out alphaIIbbeta3 signaling resulting in fibrinogen binding and platelet aggregation. These in turn trigger outside-in signaling resulting in further platelet stimulation. Because the Syk tyrosine kinase is activated during both phases of integrin signaling, we evaluated its role in alphaIIbbeta3 function in murine platelets rendered null for Syk by gene targeting and in human platelets incubated with piceatannol, a tyrosine kinase inhibitor reportedly selective for Syk. Both Syk null murine platelets and piceatannol-treated human platelets exhibited a partial, but statistically significant defect in activation of alphaIIbbeta3 by adenine diphosphate (ADP) +/- epinephrine as assessed by fibrinogen binding. Syk null platelets adhered normally to immobilized fibrinogen, and mice with these platelets exhibited normal tail bleeding times. In contrast, piceatannol treatment of human platelets completely inhibited platelet adhesion to immobilized fibrinogen. The discrepancy in extent of integrin dysfunction between murine and human platelet models may be due to lack of specificity of piceatannol, because this compound inhibited the activity of Src and FAK as well as Syk and also reduced tyrosine phosphorylation of multiple platelet proteins. These results provide genetic evidence that Syk plays a role in alphaIIbbeta3 signaling in platelets and pharmacological evidence that, although piceatannol also inhibits alphaIIbbeta3 signaling, it does so by inhibtion of multiple protein tyrosine kinases.

摘要

激动剂诱导由内向外的αIIbβ3信号传导，导致纤维蛋白原结合和血小板聚集。这些反过来又触发由外向内的信号传导，导致进一步的血小板刺激。由于Syk酪氨酸激酶在整合素信号传导的两个阶段均被激活，我们通过基因靶向使Syk基因缺失的小鼠血小板以及用白藜芦醇（一种据报道对Syk具有选择性的酪氨酸激酶抑制剂）孵育的人血小板，评估了其在αIIbβ3功能中的作用。通过纤维蛋白原结合评估，Syk基因缺失的小鼠血小板和经白藜芦醇处理的人血小板在二磷酸腺苷（ADP）+/-肾上腺素激活αIIbβ3方面均表现出部分但具有统计学意义的缺陷。Syk基因缺失的血小板能正常黏附于固定化纤维蛋白原，具有这些血小板的小鼠尾部出血时间正常。相比之下，用白藜芦醇处理人血小板则完全抑制了血小板对固定化纤维蛋白原的黏附。小鼠和人血小板模型中整合素功能障碍程度的差异可能是由于白藜芦醇缺乏特异性，因为该化合物不仅抑制Syk的活性，还抑制Src和FAK的活性，并且还减少了多种血小板蛋白的酪氨酸磷酸化。这些结果提供了遗传学证据，表明Syk在血小板αIIbβ3信号传导中起作用，以及药理学证据，表明尽管白藜芦醇也抑制αIIbβ3信号传导，但其作用方式是抑制多种蛋白酪氨酸激酶。