Biochemical aspects of the pathogenesis of venous thrombosis.

J Felez
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Abstract

In this review, an attempt has been made to present new data on the mechanisms that can be involved in DVT and to emphasize the role of the cell in these processes. It has been demonstrated that cells can mediate the relevant expression of tissue factor without cell disruption and that the fibrinolytic responses can also be modulated by the cells. It has also been demonstrated that the fibrinolytic system seems to be designed to work on the cell surface based upon (1) the existence of specific receptors, (2) the modulation of the expression of these receptors and (3) the comprehensive increase in plasmin generation by up-regulating, for example, the plasminogen receptors. It could also be worthwhile to attempt to explain some beneficial effects of drugs such as heparins by studying their action on these compartments. It is important to note that recently Rosenfeld et al. have described an increase in t-PA and u-PA binding to endothelium by pre-incubation of endothelial cells with unfractionated heparin. This work would be a first step in a very exciting and interesting new era in the prevention of venous thromboembolism.

静脉血栓形成的生化机制。
在这篇综述中,我们试图提供有关深静脉血栓形成机制的新数据,并强调细胞在这些过程中的作用。研究表明,细胞可以在不破坏细胞的情况下介导组织因子的相关表达,并且纤维蛋白溶解反应也可以由细胞调节。也有研究表明,纤溶系统似乎是基于(1)特定受体的存在,(2)这些受体表达的调节,以及(3)通过上调(例如,纤溶酶原受体)来全面增加纤溶酶的产生,从而在细胞表面起作用。通过研究肝素等药物对这些隔室的作用,试图解释它们的一些有益作用也是值得的。值得注意的是,最近Rosenfeld等人描述了通过未分离肝素对内皮细胞进行预孵育,t-PA和u-PA与内皮结合的增加。这项工作将是一个非常令人兴奋和有趣的预防静脉血栓栓塞新时代的第一步。
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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