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Platelet Rho GTPase regulation in physiology and disease

机译:血小板rho GTP酶治疗生理和疾病调控

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Rho GTPases are master orchestrators of cytoskeletal dynamics and serve critical roles in platelet physiology to promote hemostasis or pathology in thrombotic, inflammatory and other disease states. Over the past 25 years, specific platelet cell biological outputs have been linked to the activities of Rho GTPases, including RhoA, Rac1, Cdc42, and RhoG in shape change and secretion as well as cytoskeletal assembly events underlying platelet aggregation and thrombus stability. Rho GTPases have also more recently been noted to serve more specialized roles in platelet function and to cooperate with one another in mediating essential platelet responses. The evolving molecular mechanisms regulating platelet Rho GTPase functions are increasingly complex, involving an interdependent array of signal transduction molecules, including several protein kinases as well as numerous Rho GEFs, GAPs, and GDI proteins such as LARG, ARHGEF6 (Cool-2, alpha-Pix), ARHGEF10, GIT1, ARHGAP17 (Nadrin, Rich1), OPHN1, and Ly-GDI. In this review, we provide an update of recent work and developing hypotheses further establishing more specialized as well as cooperative roles for Rho GTPases in platelet physiology and emerging regulatory and downstream effector mechanisms whereby Rho GTPases participate in platelet activation programs in physiology and an expanding set of platelet-associated disease states.
机译:Rho GTP酶是细胞骨骼动态的母体协调器,并在血小板生理中提供关键作用,以促进血栓形成,炎症和其他疾病状态的止血或病理学。在过去的25年中,特定的血小板细胞生物产出与Rho GTP酶的活性有关,包括RhoA,Rac1,CDC42和形状变化和分泌的rhog以及血小板聚集和血栓稳定性的细胞骨骼组件事件。 Rho GTP酶最近已经预议的是在血小板函数中提供更专业的作用,并在介导的基本血小板反应中彼此合作。调节血小板rOO GTP酶功能的演变分子机制越来越复杂,涉及相互依赖的信号转导分子阵列,包括几种蛋白激酶以及许多rho Gefs,间隙和GDI蛋白,如蝎子,arhgef6(Cool-2,α- PIX),ARHGEF10,GIT1,ARHGAP17(Nadrin,Rich1),OPHN1和LY-GDI。在本次审查中,我们提供最近的工作和发展假设的更新,进一步建立了血小板生理学和新出现的调节和下游效应机制中的Rho GTP酶的更多专业化以及合作作用,其中Rho GTP酶参与生理学中的血小板激活计划和扩展集血小板相关疾病状态。

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