生长因子受体结合蛋白 2 有助于 (hem)免疫受体酪氨酸激活基序介导的血小板信号转导。
Growth factor receptor-bound protein 2 contributes to (hem)immunoreceptor tyrosine-based activation motif-mediated signaling in platelets.
机构信息
Department of Experimental Biomedicine, University Hospital Würzburg (S.D., T.V., M.M., S.S., B.N.) and Rudolf Virchow Center for Experimental Biomedicine (S.D., T.V., C.M.S., H.M.H., B.N.), University of Würzburg, Würzburg, Germany; Centre for Cardiovascular Sciences, Institute for Biomedical Research, College of Medical and Dental Sciences, University of Birmingham, Birmingham, United Kingdom (S.K.W., C.E.H., S.P.W.); and Department of Biology, Division of Genetics, University of Erlangen, Erlangen, Germany (J.A.A., D.R., L.N.).
出版信息
Circ Res. 2014 Jan 31;114(3):444-453. doi: 10.1161/CIRCRESAHA.114.302670. Epub 2013 Nov 21.
RATIONALE
Platelets are anuclear cell fragments derived from bone marrow megakaryocytes (MKs) that safeguard vascular integrity but may also cause pathological vessel occlusion. One major pathway of platelet activation is triggered by 2 receptors that signal through an (hem)immunoreceptor tyrosine-based activation motif (ITAM), the activating collagen receptor glycoprotein (GP) VI and the C-type lectin-like receptor 2 (CLEC-2). Growth factor receptor-bound protein 2 (Grb2) is a ubiquitously expressed adapter molecule involved in signaling processes of numerous receptors in different cell types, but its function in platelets and MKs is unknown.
OBJECTIVE
We tested the hypothesis that Grb2 is a crucial adapter protein in (hem)immunoreceptor tyrosine-based activation motif signaling in platelets.
METHODS AND RESULTS
Here, we show that genetic ablation of Grb2 in MKs and platelets did not interfere with MK differentiation or platelet production. However, Grb2-deficiency severely impaired glycoprotein VI-mediated platelet activation because of defective stabilization of the linker of activated T-cell (LAT) signalosome and activation of downstream signaling proteins that resulted in reduced adhesion, aggregation, and coagulant activity on collagen in vitro. Similarly, CLEC-2-mediated signaling was impaired in Grb2-deficient platelets, whereas the cells responded normally to stimulation of G protein-coupled receptors. In vivo, this selective (hem)immunoreceptor tyrosine-based activation motif signaling defect resulted in prolonged bleeding times but affected arterial thrombus formation only after concomitant treatment with acetylsalicylic acid, indicating that defective glycoprotein VI signaling in the absence of Grb2 can be compensated through thromboxane A2-induced G protein-coupled receptor signaling pathways.
CONCLUSIONS
These results reveal an important contribution of Grb2 in (hem)immunoreceptor tyrosine-based activation motif signaling in platelets in hemostasis and thrombosis by stabilizing the LAT signalosome.
背景
血小板是源自骨髓巨核细胞(MKs)的无核细胞碎片,可保护血管完整性,但也可能导致病理性血管阻塞。血小板激活的一个主要途径是由 2 种通过(免疫)受体酪氨酸基激活基序(ITAM)信号的受体触发的,即激活胶原受体糖蛋白(GP)VI 和 C 型凝集素样受体 2(CLEC-2)。生长因子受体结合蛋白 2(Grb2)是一种广泛表达的衔接分子,参与不同细胞类型中许多受体的信号转导过程,但它在血小板和 MKs 中的功能尚不清楚。
目的
我们检验了 Grb2 是血小板中(免疫)受体酪氨酸基激活基序信号中的关键衔接蛋白这一假说。
方法和结果
在这里,我们表明 MK 和血小板中 Grb2 的基因缺失不干扰 MK 分化或血小板生成。然而,Grb2 缺陷严重损害了糖蛋白 VI 介导的血小板激活,因为衔接蛋白激活 T 细胞(LAT)信号体的稳定性受损,以及下游信号蛋白的激活,导致在体外胶原上的粘附、聚集和凝血活性降低。同样,Grb2 缺陷血小板中 CLEC-2 介导的信号也受损,而细胞对 G 蛋白偶联受体的刺激反应正常。在体内,这种选择性(免疫)受体酪氨酸基激活基序信号缺陷导致出血时间延长,但仅在同时给予乙酰水杨酸治疗后才会影响动脉血栓形成,表明 Grb2 缺失时糖蛋白 VI 信号的缺陷可以通过血栓素 A2 诱导的 G 蛋白偶联受体信号通路得到补偿。
结论
这些结果揭示了 Grb2 在血小板止血和血栓形成中(免疫)受体酪氨酸基激活基序信号中的重要作用,通过稳定 LAT 信号体来实现。
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