Wang Kai, Zhou Xiaorong, Zhou Zhongmin, Tarakji Khaldoun, Carneiro Marcelo, Penn Marc S, Murray Daniel, Klein Allan, Humphries Robert G, Turner Jonathan, Thomas James D, Topol Eric J, Lincoff A Michael
Department of Cardiovascular Medicine, The Cleveland Clinic Foundation, Cleveland, OH 44195, USA.
Arterioscler Thromb Vasc Biol. 2003 Feb 1;23(2):357-62. doi: 10.1161/01.atv.0000052669.50791.0b.
Reperfusion therapy for myocardial infarction is limited by a significant reocclusion rate and less optimal myocardial tissue perfusion due to excessive platelet accumulation and recruitment at the sites of vascular injury. We assessed the influence of a selective P2Y(12)-receptor antagonist (AR-C69931MX), in conjunction with thrombolytic therapy, on the prevention of platelet aggregation and thrombus formation.
A canine coronary electrolytic injury thrombosis model was used. Tissue-type plasminogen activator (t-PA; 1 mg/kg in phase I, 0.5 mg/kg in phase II in the AR-C69931MX group, and 1 mg/kg in the placebo group in phase I and II) was administered 30 minutes after thrombus formation; either saline or AR-C69931MX (4 micro g x kg(-1) x min(-1)) was given to all animals intravenously 10 minutes before t-PA administration for a total of 2 hours. All animals received heparin (80 U/kg) as an intravenous bolus followed by a continuous infusion of 17 U x kg(-1) x h(-1). Myocardial tissue perfusion was evaluated by use of the colored microsphere technique and real-time myocardial contrast echocardiography. The incidences of reocclusion and cyclic flow variation were significantly decreased in the AR-C69931MX group (P<0.05). Myocardial tissue flow with AR-C69931MX treatment improved significantly at 20 and 120 minutes after reflow, whereas tissue flow with placebo remained at a level similar to that during occlusion (P<0.05).
The adjunctive administration of AR-C69931MX blocked ADP-mediated platelet aggregation and recruitment and prevented platelet-mediated thrombosis, resulting in prolongation of reperfusion time and a decrease in reocclusion and cyclic flow variations. Importantly, myocardial tissue perfusion was significantly improved in the P2Y(12) antagonist group.
心肌梗死的再灌注治疗受到显著再闭塞率的限制,并且由于血管损伤部位血小板过度聚集和募集,心肌组织灌注不太理想。我们评估了一种选择性P2Y(12)受体拮抗剂(AR-C69931MX)与溶栓治疗联合应用对预防血小板聚集和血栓形成的影响。
采用犬冠状动脉电解损伤血栓形成模型。血栓形成30分钟后给予组织型纤溶酶原激活剂(t-PA;AR-C69931MX组I期为1mg/kg,II期为0.5mg/kg,安慰剂组I期和II期均为1mg/kg);在给予t-PA前10分钟,所有动物静脉注射生理盐水或AR-C69931MX(4μg·kg⁻¹·min⁻¹),共2小时。所有动物静脉推注肝素(80U/kg),随后持续输注17U·kg⁻¹·h⁻¹。采用彩色微球技术和实时心肌对比超声心动图评估心肌组织灌注。AR-C69931MX组的再闭塞和循环血流变化发生率显著降低(P<0.05)。AR-C69931MX治疗后,再灌注20分钟和120分钟时心肌组织血流显著改善,而安慰剂组的组织血流仍维持在与闭塞期间相似的水平(P<0.05)。
AR-C69931MX的辅助给药可阻断ADP介导的血小板聚集和募集,预防血小板介导的血栓形成,从而延长再灌注时间,降低再闭塞和循环血流变化。重要的是,P2Y(12)拮抗剂组的心肌组织灌注显著改善。
