口服西美洛非班对犬动脉血栓形成的保护作用:与阿司匹林联合使用时活性增强。
Protective effect of oral xemilofiban in arterial thrombosis in dogs: increased activity in combination with aspirin.
作者信息
Frederick L G, Suleymanov O D, Szalony J A, Taite B B, Salyers A K, King L W, Feigen L P, Nicholson N S
机构信息
Thrombosis Research Department, Searle, Skokie, Ill, USA.
出版信息
Circulation. 1998 Aug 25;98(8):813-20. doi: 10.1161/01.cir.98.8.813.
BACKGROUND
Inhibition of platelet aggregation by preventing the binding of fibrinogen to glycoprotein (GP) IIb/IIIa on activated platelets results in antithrombotic activity. We report on the antithrombotic effect of xemilofiban (SC-54684A), an oral GP IIb/IIIa antagonist, administered alone or with aspirin (ASA) in an acute thrombosis model.
METHODS AND RESULTS
Conscious dogs were treated with xemilofiban (1.25, 2.5, 5.0, or 6 mg/kg, n=6); low-dose (LD, 81 mg) ASA, n=7; high-dose (HD, 162 mg) ASA, n=6; xemilofibran 1.25 mg/kg plus LD ASA, n=6; xemilofibran 1.25 mg/kg plus HD ASA, n=6; or placebo, n=7. Dogs were anesthetized 60 minutes later, and the effects of the treatments were evaluated after electrolytic injury (250 microA for 180 minutes) in the left circumflex coronary artery. Bleeding time (BT) was assessed in a separate study. Incidence of thrombosis was reduced (P<0.05) by xemilofiban > or =2.5 mg/kg, HD ASA, or xemilofiban 1.25 mg/kg plus HD ASA compared with placebo. Xemilofiban > or =2.5 mg/kg or xemilofiban 1.25 mg/kg plus HD ASA significantly increased time to occlusion, inhibited ex vivo platelet aggregation to collagen >90%, and prevented or decreased (P<0.05) cyclic flow variations (CFVs) compared with placebo. BT was increased (P<0.05) with xemilofiban > or =2.5 mg/kg but not with xemilofiban 1.25 mg/kg plus HD ASA.
CONCLUSIONS
Xemilofiban > or =2.5 mg/kg, HD ASA, or xemilofiban 1.25 mg/kg plus HD ASA significantly reduced the incidence of thrombosis. These doses of xemilofiban or xemilofiban 1.25 mg/kg plus HD ASA increased time to occlusion, inhibited ex vivo platelet aggregation by >90%, and prevented or reduced CFVs. Xemilofiban > or =2.5 mg/kg but not xemilofiban 1.25 mg/kg plus HD ASA significantly increased BT.
背景
通过阻止纤维蛋白原与活化血小板上的糖蛋白(GP)IIb/IIIa结合来抑制血小板聚集可产生抗血栓活性。我们报告了口服GP IIb/IIIa拮抗剂西美洛非班(SC - 54684A)单独或与阿司匹林(ASA)联合应用于急性血栓形成模型中的抗血栓作用。
方法与结果
清醒犬分别接受西美洛非班(1.25、2.5、5.0或6 mg/kg,n = 6);低剂量(LD,81 mg)ASA,n = 7;高剂量(HD,162 mg)ASA,n = 6;西美洛非班1.25 mg/kg加LD ASA,n = 6;西美洛非班1.25 mg/kg加HD ASA,n = 6;或安慰剂,n = 7治疗。60分钟后对犬进行麻醉,在左回旋冠状动脉进行电解损伤(250微安,持续180分钟)后评估治疗效果。在另一项研究中评估出血时间(BT)。与安慰剂相比,西美洛非班≥2.5 mg/kg、HD ASA或西美洛非班1.25 mg/kg加HD ASA可降低血栓形成发生率(P<0.05)。与安慰剂相比,西美洛非班≥2.5 mg/kg或西美洛非班1.25 mg/kg加HD ASA可显著延长闭塞时间,抑制体外血小板对胶原的聚集>90%,并预防或减少(P<0.05)周期性血流变化(CFV)。西美洛非班≥2.5 mg/kg可使BT延长(P<0.05),但西美洛非班1.25 mg/kg加HD ASA则不会。
结论
西美洛非班≥2.5 mg/kg、HD ASA或西美洛非班1.25 mg/kg加HD ASA可显著降低血栓形成发生率。这些剂量的西美洛非班或西美洛非班1.25 mg/kg加HD ASA可延长闭塞时间,抑制体外血小板聚集>90%,并预防或减少CFV。西美洛非班≥2.5 mg/kg可显著延长BT,但西美洛非班1.25 mg/kg加HD ASA则不会。
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