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首页> 外文期刊>Thrombosis Research: An International Journal on Vascular Obstruction, Hemorrhage and Hemostasis >Tissue factor storage, synthesis and function in normal and activated human platelets.
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Tissue factor storage, synthesis and function in normal and activated human platelets.

机译:在正常和活化的人类血小板中组织因子的储存,合成和功能。

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摘要

The source and significance of blood-borne tissue factor (TF) are controversial. The presence of TF in platelets was initially attributed to transfer of the protein from other cells (e.g., monocytes) and/or TF-bearing microparticles. Recently, TF-mRNA, neo-synthesis of the protein and TF-dependent procoagulant activity (PCA) have been reported in human platelets. The storage of "encrypted", potentially active TF in circulating, non-stimulated platelets remains debatable. One report strongly suggests that the starting of platelet PCA depends on de novo TF synthesis induced by platelet activation, whereas others provide persuasive evidence that platelets circulate with preformed TF, readily functional upon demand. These findings may have an impact on our current ideas of physiological hemostasis and thrombus formation. In fact, platelets would lead not only the formation of the primary plug, but in this microenvironment they would also contribute to the triggering of thrombin generation, fibrin deposition, clot consolidation and initial protection from fibrinolysis. Much research is needed to validate this platelet-based hemostasis model.
机译:血源性组织因子(TF)的来源和意义存在争议。血小板中TF的存在最初归因于蛋白质从其他细胞(例如单核细胞)和/或带有TF的微粒的转移。最近,有人血小板中报道了TF-mRNA,该蛋白的新合成和TF依赖性促凝活性(PCA)。在循环的,未刺激的血小板中“加密的”,可能具有活性的TF的存储仍然值得商bat。一份报告强烈表明,血小板PCA的启动取决于血小板活化引起的从头开始的TF合成,而其他报告则提供了有说服力的证据,表明血小板可以随需要随即起作用的预制TF循环。这些发现可能会对我们目前的生理止血和血栓形成观念产生影响。实际上,血小板不仅会导致初次栓塞的形成,而且在这种微环境中,它们还将有助于触发凝血酶的产生,血纤蛋白的沉积,血凝块固结和对纤维蛋白溶解的初步保护。需要大量研究来验证这种基于血小板的止血模型。

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