Yano Yuichiro, Ohmori Tsukasa, Hoshide Satoshi, Madoiwa Seiji, Yamamoto Keiji, Katsuki Takaaki, Mitsuhashi Takeshi, Mimuro Jun, Shimada Kazuyuki, Kario Kazuomi, Sakata Yoichi
Division of Cardiovascular Medicine, Department of Medicine, Jichi Medical University School of Medicine, 3311-1 Yakushiji, Shimotsuke, Tochigi 329-0498, Japan.
Eur Heart J. 2008 Jul;29(14):1729-38. doi: 10.1093/eurheartj/ehn027. Epub 2008 Feb 12.
The aim of the study was to assess mechanisms and clinical backgrounds in order to determine residual platelet aggregability in dual antiplatelet therapy and to ascertain whether platelet aggregability is involved in systemic thrombogenicity.
A cross-sectional study was conducted in 85 consecutive patients who underwent dual antiplatelet therapy (aspirin and thienopyridine/cilostazol) after percutaneous coronary intervention (PCI). Although serum thromboxane B(2) and dephosphorylation of vasodilator-stimulated phosphoprotein were significantly abolished, the platelet aggregation tests showed inter-individual differences that could be partly explained by plasma glucose levels. Platelet aggregability was not related to other factors involved in thrombogenicity. Thrombin generation assessed by soluble fibrin was independently associated with total cholesterol (beta = 0.349, P < 0.001), brain natriuretic peptide (beta = 0.222, P = 0.018), and ankle-brachial index (beta = -0.330, P = 0.001). Plasminogen activator inhibitor-1 was associated with the apnea-hypopnea index (beta = 0.300, P = 0.006). E-selectin was correlated with diabetes mellitus (beta = 0.279, P = 0.008) and body mass index (beta = 0.323, P = 0.002).
Although dual antiplatelet therapy effectively inhibited its pharmacological targets, thrombin generation, inhibition of fibrinolytic activity, and endothelial dysfunction were determined by other clinical backgrounds. Our data suggested that some patients remain at risk of thrombotic complications after PCI and that these may benefit from anticoagulant treatment despite adequate dual antiplatelet therapy.
本研究旨在评估机制和临床背景,以确定双联抗血小板治疗中残余的血小板聚集性,并确定血小板聚集性是否与全身血栓形成有关。
对85例经皮冠状动脉介入治疗(PCI)后接受双联抗血小板治疗(阿司匹林和噻吩并吡啶/西洛他唑)的连续患者进行了横断面研究。尽管血清血栓素B2和血管舒张刺激磷蛋白的去磷酸化明显被抑制,但血小板聚集试验显示个体间存在差异,这部分可由血浆葡萄糖水平解释。血小板聚集性与血栓形成的其他因素无关。通过可溶性纤维蛋白评估的凝血酶生成与总胆固醇(β = 0.349,P < 0.001)、脑钠肽(β = 0.222,P = 0.018)和踝臂指数(β = -0.330,P = 0.001)独立相关。纤溶酶原激活物抑制剂-1与呼吸暂停低通气指数相关(β = 0.300,P = 0.006)。E-选择素与糖尿病(β = 0.279,P = 0.008)和体重指数(β = 0.323,P = 0.002)相关。
尽管双联抗血小板治疗有效抑制了其药理学靶点,但凝血酶生成、纤维蛋白溶解活性的抑制和内皮功能障碍由其他临床背景决定。我们的数据表明,一些患者在PCI后仍有血栓并发症的风险,尽管进行了充分的双联抗血小板治疗,但这些患者可能从抗凝治疗中获益。
