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首页> 外文期刊>Journal of cardiovascular translational research >Cigarette smoking and antiplatelet effects of aspirin monotherapy versus clopidogrel monotherapy in patients with atherosclerotic disease: Results of a prospective pharmacodynamic study
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Cigarette smoking and antiplatelet effects of aspirin monotherapy versus clopidogrel monotherapy in patients with atherosclerotic disease: Results of a prospective pharmacodynamic study

机译:阿司匹林单药治疗与氯吡格雷单药治疗动脉粥样硬化病患者的吸烟和抗血小板作用:前瞻性药效学研究的结果

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Smokers have a greater relative benefit of clopidogrel therapy compared with nonsmokers, likely attributed to its enhanced pharmacodynamic (PD) effects. However, to date, all PD studies have been conducted in patients on dual antiplatelet therapy with aspirin and clopidogrel, and it is unknown whether clopidogrel monotherapy can offer more effective antithrombotic effects compared with aspirin alone among smoking patients. Sixty aspirin-treated (81 mg/day) patients with vascular disease, classified as nonsmokers, light smokers, and heavy smokers according to cotinine serum levels, were enrolled. Patients were switched to clopidogrel (75 mg/day) monotherapy for 7-10 days. PD assessments were performed before and after switch by multiple electrode aggregometry (MEA) and kaolin-activated thromboelastography (TEG). Complete PD data were obtained in 57 patients (nonsmokers, n = 27; light smokers, n = 13; heavy smokers, n = 17). On treatment platelet reactivity following MEA, adenosine diphosphate (ADP) + prostaglandin E1 (PGE1) and thrombin receptor-activating peptide (TRAP) stimuli were significantly lower among heavy smokers following switch to clopidogrel. A significant inverse effect was observed with MEA arachidonic acid (ASPI), while neutral findings were shown with MEA collagen (COLL) stimulus. Thrombin and fibrin activity assessed by clot generation parameters were all nonsignificantly different but showed trends towards enhanced antithrombotic activity with clopidogrel among heavy smokers. In heavy smokers with vascular disease manifestations, clopidogrel is associated with enhanced platelet inhibitory effects, affecting purinergic and non-purinergic pathways, compared with aspirin as measured by MEA. Moreover, among smokers, clopidogrel offers trends towards enhanced effects on parameters of clot generation measured by TEG.
机译:与不吸烟者相比,吸烟者对氯吡格雷治疗的相对获益更大,这可能归因于其增强的药效学 (PD) 效应。然而,迄今为止,所有 PD 研究都是在阿司匹林和氯吡格雷双重抗血小板治疗的患者中进行的,目前尚不清楚氯吡格雷单药治疗是否能在吸烟患者中提供比单独使用阿司匹林更有效的抗血栓效果。纳入了60名接受阿司匹林治疗(81mg/天)的血管疾病患者,根据可替宁血清水平分为非吸烟者、轻度吸烟者和重度吸烟者。患者改用氯吡格雷(75 mg/天)单药治疗 7-10 天。通过多电极聚集法 (MEA) 和高岭土活化血栓弹力图 (TEG) 在切换前后进行 PD 评估。在 57 名患者(非吸烟者,n = 27;轻度吸烟者,n = 13;重度吸烟者,n = 17)中获得了完整的 PD 数据。在 MEA 后的治疗中,重度吸烟者在改用氯吡格雷后,二磷酸腺苷 (ADP) + 前列腺素 E1 (PGE1) 和凝血酶受体激活肽 (TRAP) 刺激显着降低。MEA花生四烯酸(ASPI)观察到显著的逆效应,而MEA胶原(COLL)刺激则显示出中性结果。通过凝块生成参数评估的凝血酶和纤维蛋白活性均无显著差异,但在重度吸烟者中显示出氯吡格雷的抗血栓活性增强的趋势。在有血管疾病表现的重度吸烟者中,与 MEA 测量的阿司匹林相比,氯吡格雷与增强的血小板抑制作用有关,影响嘌呤能和非嘌呤能通路。此外,在吸烟者中,氯吡格雷对TEG测量的凝块生成参数有增强影响的趋势。

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