The Von Willebrand factor-ADAMTS-13 axis: a two-faced Janus in bleeding and thrombosis

S. Lancellotti, M. Sacco, M. Tardugno, A. Ferretti, R. De Cristofaro
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引用次数: 1

Abstract

Von Willebrand factor (VWF), a blood multimeric protein with a very high molecular weight, plays a crucial role in the primary hemostasis, the physiological process characterized by the adhesion of blood platelets to the injured vessel wall. Hydrodynamic forces are responsible for the VWF multimers conformational transitions from a globular to a stretched linear conformation. These characteristics render this protein a valuable object to be investigated by mechanochemistry, the biophysical chemistry branch that studies the effects of shear forces on protein conformation. This review will focus on the structural elements of the VWF molecule involved in the biochemical response to shear forces. The stretched VWF conformation favors the interaction with the platelet GpIb and at the same time with ADAMTS-13, the zinc-protease that cleaves VWF in the A2 domain, limiting its prothrombotic capacity. It is important to consider the level or the function of VWF or ADAMTS-13 always in relation each other, keeping in mind that in many thrombotic forms of microangiopathies the reduction of the ratio between the ADAMTS-13 activity and the VWF level (lower than 0.5) can be a valuable parameter to predict a real thrombotic risk. Hence, a significant increase in VWF level alone, even without any reduction of ADAMTS-13 concentration, would still be responsible for a significant reduction of the ADAMTS-13/VWF ratio, which ultimately could reflect or predict a prothrombotic risk. Future studies will have to validate the concept whether ADAMTS-13/VWF ratio could a valuable and reliable biomarker to predict or confirm the presence of thrombotic risk in several morbid conditions.
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血管性血友病因子- adamts -13轴:出血和血栓形成的双面两面
血管性血友病因子(VWF)是一种具有极高分子量的血液多聚体蛋白,在原发性止血中起着至关重要的作用,原发性止血是一种以血小板粘附在受伤血管壁上为特征的生理过程。水动力作用是VWF多聚体从球形构象到拉伸线性构象转变的主要原因。这些特性使这种蛋白质成为机械化学(研究剪切力对蛋白质构象影响的生物物理化学分支)研究的一个有价值的对象。本文将重点介绍参与剪切力生化反应的VWF分子的结构成分。拉伸的VWF构象有利于与血小板GpIb相互作用,同时也有利于与ADAMTS-13相互作用,后者是一种锌蛋白酶,可在A2结构域切割VWF,限制其血栓形成前的能力。重要的是要考虑VWF或ADAMTS-13的水平或功能总是相互关联的,记住,在许多血栓形成的微血管病变中,ADAMTS-13活性与VWF水平之比的降低(低于0.5)可以是预测真正血栓形成风险的一个有价值的参数。因此,即使没有ADAMTS-13浓度的降低,仅VWF水平的显著增加仍然会导致ADAMTS-13/VWF比值的显著降低,而ADAMTS-13/VWF比值最终可以反映或预测血栓形成前的风险。未来的研究必须验证ADAMTS-13/VWF比值是否可以作为一种有价值和可靠的生物标志物来预测或确认几种病态条件下血栓形成风险的存在。
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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