首页> 外文期刊>Thrombosis and Haemostasis: Journal of the International Society on Thrombosis and Haemostasis >The contribution of thrombin-induced platelet activation to thrombus growth is diminished under pathological blood shear conditions
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The contribution of thrombin-induced platelet activation to thrombus growth is diminished under pathological blood shear conditions

机译:在病理性血液剪切条件下,凝血酶诱导的血小板活化对血栓生长的贡献减少。

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摘要

Developing novel anti-platelet therapies is an important clinical strategy for the prevention of arterial thromboses which cause heart attacks and most strokes. Thrombin activates platelets via protease-activated receptors (PARs), and PAR antagonists are currently under investigation as antithrombotics. Yet despite these clinical advances, the importance of PARs to platelet activation during thromboses formed under pathological conditions has not been investigated. To this end, we examined the role of PAR-dependent platelet activation in thrombus formation in the presence of elevated blood shear rates. We used two in vivo thrombosis models and an ex vivo whole blood flow approach in PAR4-/- mice, whose platelets are unresponsive to thrombin, to show that the contribution of PAR-mediated platelet activation to thrombosis is dim- inished at pathological blood shear rates as a direct result of decreased incorporation of thrombin-activated platelets into growing thrombi. Our ex vivo observations were replicated in human whole blood treated with a PAR1 antagonist. These results define a novel, shear-regulated role for thrombin/PAR-dependent platelet activation during thrombosis and provide important insights into the conditions under which PAR antagonists may best be used for the prevention of acute coronary syndromes
机译:开发新的抗血小板疗法是预防引起心脏病和大多数中风的动脉血栓形成的重要临床策略。凝血酶通过蛋白酶激活受体(PARs)激活血小板,目前正在研究PAR拮抗剂作为抗血栓形成剂。尽管有这些临床进展,但尚未研究在病理条件下形成的血栓形成过程中PAR对血小板活化的重要性。为此,我们在血液剪切速率升高的情况下检查了PAR依赖性血小板活化在血栓形成中的作用。我们在血小板对凝血酶无反应的PAR4-/-小鼠中使用了两种体内血栓形成模型和离体全血流方法,以证明在病理性血液剪切作用下,PAR介导的血小板活化对血栓形成的作用减弱了。凝血酶活化的血小板减少并入生长中的血栓的直接结果是其发生率升高。我们的离体观察结果在用PAR1拮抗剂治疗的人全血中得以复制。这些结果为血栓形成过程中凝血酶/ PAR依赖的血小板活化定义了一种新的剪切调节作用,并为重要的洞察条件提供了最佳的PAR拮抗剂预防急性冠状动脉综合征的条件。

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