The haemostatic balance -- Astrup revisited.

Haemostasis Pub Date : 1999-09-01 DOI:10.1159/000022461
P J Gaffney, T A Edgell, C M Whitton
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引用次数: 35

Abstract

Prof. Tage Astrup first elaborated the notion that blood fluidity involved a balance between the tendency of blood to clot and for such clots to lyse. It would seem that, at that time, this haemostatic balance involved the notion that forming fibrin orchestrated its own destruction by stimulating fibrinolytic activity. In this review, we have clarified the detail of this balance and developed the thesis that Astrup’s far-sighted balance notions involve a variety of control mechanisms. These involve the notion that thrombin, being at first sight a procoagulant, can also, in conjunction with thrombomodulin, act as a stimulus of anticoagulant activity by the generation of activated protein C. The thrombin-activatable fibrinolytic inhibitor (TAFI) is also involved in this balance since the generation of thrombin provokes the neutralisation of fibrinolysis by the TAFI pathway. The kallikrein/factor XII/urokinase pathway is discussed indicating yet another aspect of balance between the generation of coagulation and fibrinolysis. The overall theme of this review, apart from an insight into various aspects of the haemostatic balance, is that blood has a strong tendency to clot when tissue is damaged, and the intact vasculature requires major anticoagulant systems to prevent clots adhering to and stabilising in the vasculature.
止血平衡——Astrup重新审视。
Tage Astrup教授首先阐述了血液流动性涉及血液凝块倾向和凝块溶解之间的平衡这一概念。似乎,在那个时候,这种止血平衡涉及到形成纤维蛋白通过刺激纤维蛋白溶解活性来协调自身破坏的概念。在这篇综述中,我们澄清了这种平衡的细节,并提出了Astrup的远视平衡概念涉及多种控制机制的论点。其中包括凝血酶,乍一看是一种促凝剂,也可以与血栓调节蛋白一起,通过产生活化蛋白c来刺激抗凝活性。凝血酶活化的纤维蛋白溶解抑制剂(TAFI)也参与这种平衡,因为凝血酶的产生通过TAFI途径刺激纤维蛋白溶解的中和。讨论了激肽激酶/因子XII/尿激酶途径,表明凝血和纤溶产生之间的平衡的另一个方面。本综述的总体主题,除了对止血平衡的各个方面的深入了解外,是当组织受损时,血液有很强的凝块倾向,而完整的血管系统需要主要的抗凝系统来防止凝块粘附和稳定血管系统。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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