Chung Dominic W, Chen Junmei, Ling Minhua, Fu Xiaoyun, Blevins Teri, Parsons Scott, Le Jennie, Harris Jeff, Martin Thomas R, Konkle Barbara A, Zheng Ying, López José A
Bloodworks Research Institute, Seattle, WA; Department of Biochemistry.
Bloodworks Research Institute, Seattle, WA;
Blood. 2016 Feb 4;127(5):637-45. doi: 10.1182/blood-2014-09-599530. Epub 2015 Nov 9.
The ability of von Willebrand factor (VWF) to initiate platelet adhesion depends on the number of monomers in individual VWF multimers and on the self-association of individual VWF multimers into larger structures. VWF self-association is accelerated by shear stress. We observed that VWF self-association occurs during adsorption of VWF onto surfaces, assembly of secreted VWF into hyperadhesive VWF strings on the endothelial surface, and incorporation of fluid-phase VWF into VWF fibers. VWF adsorption under static conditions increased with increased VWF purity and was prevented by a component of plasma. We identified that component as high-density lipoprotein (HDL) and its major apolipoprotein ApoA-I. HDL and ApoA-I also prevented VWF on the endothelium from self-associating into longer strands and inhibited the attachment of fluid-phase VWF onto vessel wall strands. Platelet adhesion to VWF fibers was reduced in proportion to the reduction in self-associated VWF. In a mouse model of thrombotic microangiopathy, HDL also largely prevented the thrombocytopenia induced by injection of high doses of human VWF. Finally, a potential role for ApoA-I in microvascular occlusion associated with thrombotic thrombocytopenic purpura and sepsis was revealed by the inverse relationship between the concentration of ApoA-I and that of hyperadhesive VWF. These results suggest that interference with VWF self-association would be a new approach to treating thrombotic disorders.
血管性血友病因子(VWF)启动血小板黏附的能力取决于单个VWF多聚体中的单体数量以及单个VWF多聚体自组装成更大结构的情况。VWF的自组装会因剪切应力而加速。我们观察到,VWF的自组装发生在VWF吸附到表面的过程中、分泌的VWF在内皮表面组装成高黏附性VWF链的过程中以及液相VWF掺入VWF纤维的过程中。在静态条件下,VWF的吸附随着VWF纯度的增加而增加,并受到血浆中一种成分的抑制。我们确定该成分是高密度脂蛋白(HDL)及其主要载脂蛋白ApoA-I。HDL和ApoA-I还可防止内皮上的VWF自组装成长链,并抑制液相VWF附着到血管壁链上。血小板对VWF纤维的黏附随着自组装VWF的减少而相应降低。在血栓性微血管病的小鼠模型中,HDL还在很大程度上预防了高剂量人VWF注射诱导的血小板减少症。最后,ApoA-I浓度与高黏附性VWF浓度之间的负相关关系揭示了ApoA-I在与血栓性血小板减少性紫癜和脓毒症相关的微血管闭塞中的潜在作用。这些结果表明,干扰VWF的自组装将是治疗血栓性疾病的一种新方法。