Arias-Salgado Elena Garcia, Haj Fawaz, Dubois Christophe, Moran Barry, Kasirer-Friede Ana, Furie Barbara C, Furie Bruce, Neel Benjamin G, Shattil Sanford J
Department of Medicine, University of California, San Diego, La Jolla, CA 92093, USA.
J Cell Biol. 2005 Aug 29;170(5):837-45. doi: 10.1083/jcb.200503125. Epub 2005 Aug 22.
Outside-in integrin alphaIIbbeta3 signaling is required for normal platelet thrombus formation and is triggered by c-Src activation through an unknown mechanism. In this study, we demonstrate an essential role for protein-tyrosine phosphatase (PTP)-1B in this process. In resting platelets, c-Src forms a complex with alphaIIbbeta3 and Csk, which phosphorylates c-Src tyrosine 529 to maintain c-Src autoinhibition. Fibrinogen binding to alphaIIbbeta3 triggers PTP-1B recruitment to the alphaIIbbeta3-c-Src-Csk complex in a manner that is dependent on c-Src and specific tyrosine (tyrosine 152 and 153) and proline (proline 309 and 310) residues in PTP-1B. Studies of PTP-1B-deficient mouse platelets indicate that PTP-1B is required for fibrinogen-dependent Csk dissociation from alphaIIbbeta3, dephosphorylation of c-Src tyrosine 529, and c-Src activation. Furthermore, PTP-1B-deficient platelets are defective in outside-in alphaIIbbeta3 signaling in vitro as manifested by poor spreading on fibrinogen and decreased clot retraction, and they exhibit ineffective Ca2+ signaling and thrombus formation in vivo. Thus, PTP-1B is an essential positive regulator of the initiation of outside-in alphaIIbbeta3 signaling in platelets.
外向内整合素αIIbβ3信号传导是正常血小板血栓形成所必需的,并且通过未知机制由c-Src激活触发。在本研究中,我们证明了蛋白酪氨酸磷酸酶(PTP)-1B在此过程中的重要作用。在静息血小板中,c-Src与αIIbβ3和Csk形成复合物,Csk使c-Src酪氨酸529磷酸化以维持c-Src的自抑制。纤维蛋白原与αIIbβ3结合以依赖于c-Src以及PTP-1B中特定酪氨酸(酪氨酸152和153)和脯氨酸(脯氨酸309和310)残基的方式触发PTP-1B募集到αIIbβ3-c-Src-Csk复合物。对PTP-1B缺陷型小鼠血小板的研究表明,PTP-1B是纤维蛋白原依赖性Csk从αIIbβ3解离、c-Src酪氨酸529去磷酸化以及c-Src激活所必需的。此外,PTP-1B缺陷型血小板在体外外向内αIIbβ3信号传导方面存在缺陷,表现为在纤维蛋白原上铺展不良和凝块收缩减少,并且它们在体内表现出无效的Ca2+信号传导和血栓形成。因此,PTP-1B是血小板中外向内αIIbβ3信号传导起始的必需正向调节因子。
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