Increased Platelet Adhesiveness in Patients with Venous Thromboembolic Disease.

Julia Martinez-Sanchez, Sergi Torramade-Moix, Ana Belén Moreno-Castaño, Dolors Llobet, Didac Jerez-Dolz, Pablo Sanchez, Marina Carrasco, Sergi Mojal, Carla Moret, Mercedes Camacho, José Manuel Soria, Marta Palomo, Laura Martin-Fernandez, Francisco Vidal, Gines Escolar, Maribel Diaz-Ricart, Juan Carlos Souto
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Abstract

Background  Association between global platelet function and the risk of venous thromboembolic disease (VTE) has been proposed, though the mechanisms do not involve increased platelet aggregation. However, platelet adhesiveness has not been systematically explored in VTE patients. Objectives  To evaluate platelet adhesive functions in VTE patients. Methods  Platelet adhesion was evaluated by using whole blood samples from VTE patients, selected based on short closure times on the PFA-100 ( n  = 54), and matched healthy individuals ( n  = 57) in: (i) the PFA-100, (ii) a cone plate analyzer (CPA), on a plastic surface, (iii) microfluidic devices, with two- and three-dimensional evaluation, and (iv) membrane glycoprotein analysis. Intraplatelet signaling was evaluated in isolated collagen type I (Col-I) activated platelets and platelets adhered on Col-I or von Willebrand factor (VWF) coated coverslips under flow. VWF antigen and ADAMTS-13 activity were measured in plasma samples. Results  PFA-100 closure times remained significantly shorter in patients. The CPA test showed a significant increase in the platelet aggregates size when using blood from VTE patients. Platelet adhesion on Col-I revealed a higher area covered by platelets and increased aggregate volume when exposed to samples from VTE patients. Protein P-ZAP70/SYK72 showed a phosphorylation level significantly increased in patients' platelets. Plasma VWF was significantly elevated in VTE patients. Conclusions  Platelets from VTE patients exhibit a proadhesive phenotype under flow conditions potentially related to the shortened occlusion times with the PFA-100. This enhanced adhesiveness may be explained by higher intraplatelet ZAP70/SYK72 phosphorylation and increased plasma VWF in patients. Therefore, primary hemostasis plays a significant role in the pathophysiology of VTE.

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静脉血栓栓塞性疾病患者血小板黏附性增高
背景血小板功能与静脉血栓栓塞性疾病(VTE)风险之间的关联已经被提出,尽管其机制不涉及血小板聚集增加。然而,血小板粘附性在静脉血栓栓塞患者中尚未得到系统的探讨。目的探讨静脉血栓栓塞患者血小板粘附功能。方法采用静脉血栓栓塞(VTE)患者全血样本,根据PFA-100闭合时间短(n = 54)和匹配健康个体(n = 57)进行血小板粘附评估:(i) PFA-100, (ii)锥形板分析仪(CPA),塑料表面,(iii)微流控装置,二维和三维评价,(iv)膜糖蛋白分析。在分离的I型胶原(Col-I)活化的血小板和粘附在Col-I或血管性血友病因子(VWF)涂层盖层上的血小板中评估血小板内信号传导。测定血浆中VWF抗原和ADAMTS-13的活性。结果患者PFA-100闭合时间明显缩短。CPA试验显示,当使用静脉血栓栓塞患者的血液时,血小板聚集物的大小显著增加。当暴露于静脉血栓栓塞患者的样本时,col - 1上的血小板粘附显示血小板覆盖面积增加,聚集体积增加。P-ZAP70/SYK72蛋白磷酸化水平在患者血小板中显著升高。静脉血栓栓塞患者血浆VWF明显升高。结论静脉血栓栓塞患者血小板在血流条件下表现出前黏附表型,可能与缩短PFA-100阻断时间有关。这种增强的粘附性可能是由于患者血小板内较高的ZAP70/SYK72磷酸化和血浆VWF增加所致。因此,原发性止血在静脉血栓栓塞的病理生理中起着重要的作用。
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