Kamath S, Blann A D, Chin B S P, Lanza F, Aleil B, Cazenave J P, Lip G Y H
Haemostasis Thrombosis and Vascular Biology Unit, University Department of Medicine, City Hospital, Birmingham, UK.
Eur Heart J. 2002 Nov;23(22):1788-95. doi: 10.1053/euhj.2002.3259.
Platelet function may be abnormal in patients with atrial fibrillation (AF) and could be related to abnormal thrombogenesis. The aim of this cross-sectional study was to investigate new aspects of platelet biology in AF, predominantly focusing on platelet activation and the effects of concomitant antiplatelet and anticoagulant therapy.
The study group of 238 patients were (i). 93 patients on no antithrombotic therapy, (ii). 60 patients taking 75-325 mg aspirin/day, and (iii). 85 patients on dose-adjusted warfarin (International Normalised Ratio [INR] range 2.0-3.0). Results were compared with those from 50 age- and sex-matched normal subjects. Platelet markers (plasma beta-thromboglobulin, soluble glycoprotein V [both ELISA]), coagulation markers (fibrin D-dimer [ELISA] and fibrinogen [Clauss]), and platelet aggregation in response to standard platelet agonists were studied.
beta-thromboglobulin (P=0.01), soluble glycoprotein V (P<0.001) and fibrin D-dimer (P=0.002) were higher in untreated AF patients compared to healthy controls. AF patients on warfarin had lower fibrin D-dimer (P<0.001) when compared to AF patients on no therapy. Plasma fibrinogen and platelet aggregation was no different between patients with AF and healthy controls. Aspirin use was associated with reduced platelet aggregation response to epinephrine (P=0.01), whilst patients established on warfarin had significantly lower plasma fibrin D-dimer levels.
AF patients exhibit changes in plasma markers of platelet function but no significant abnormalities of platelet aggregation. However, treatment with warfarin or aspirin failed to demonstrate any significant benefit on platelet activation, although warfarin use was associated with reduced thrombogenesis (fibrin D-dimer). We suggest that platelet activation may not play an important role in the pathogenesis of thromboembolism in AF.
心房颤动(AF)患者的血小板功能可能异常,且可能与异常血栓形成有关。这项横断面研究的目的是调查AF患者血小板生物学的新方面,主要关注血小板活化以及联合抗血小板和抗凝治疗的效果。
238例患者的研究组包括(i)93例未接受抗血栓治疗的患者,(ii)60例每天服用75 - 325mg阿司匹林的患者,以及(iii)85例接受剂量调整华法林治疗(国际标准化比值[INR]范围2.0 - 3.0)的患者。将结果与50例年龄和性别匹配的正常受试者的结果进行比较。研究了血小板标志物(血浆β - 血小板球蛋白、可溶性糖蛋白V[均采用酶联免疫吸附测定法])、凝血标志物(纤维蛋白D - 二聚体[酶联免疫吸附测定法]和纤维蛋白原[Clauss法])以及对标准血小板激动剂的血小板聚集情况。
与健康对照组相比,未治疗的AF患者的β - 血小板球蛋白(P = 0.01)、可溶性糖蛋白V(P <0.001)和纤维蛋白D - 二聚体(P = 0.002)更高。与未接受治疗的AF患者相比,接受华法林治疗的AF患者的纤维蛋白D - 二聚体更低(P <0.001)。AF患者与健康对照组之间血浆纤维蛋白原和血小板聚集无差异。使用阿司匹林与肾上腺素诱导的血小板聚集反应降低相关(P = 0.01),而接受华法林治疗的患者血浆纤维蛋白D - 二聚体水平显著更低。
AF患者表现出血小板功能血浆标志物变化,但血小板聚集无明显异常。然而,华法林或阿司匹林治疗未能显示对血小板活化有任何显著益处,尽管使用华法林与血栓形成减少(纤维蛋白D - 二聚体)相关。我们认为血小板活化可能在AF血栓栓塞发病机制中不起重要作用。
