Rebello S S, Bentley R G, Morgan S R, Kasiewski C J, Chu V, Perrone M H, Leadley R J
Cardiovascular Biology, Aventis Pharmaceuticals, Collegeville, Pennsylvania, U.S.A.
Br J Pharmacol. 2001 Aug;133(7):1190-8. doi: 10.1038/sj.bjp.0704182.
We compared the antithrombotic efficacy of a potent factor Xa inhibitor, FXV673, to heparin and RPR109891, a GPIIb/IIIa antagonist, when used as adjunctive therapy in a canine model of rt-PA-induced coronary thrombolysis. Thrombus formation was induced by electrolytic injury to stenosed coronary artery. After thrombotic occlusion, a 135 min infusion of saline (n=8), FXV673 (10, 30 or 100 microg kg(-1)+1, 3, or 10 microg kg(-1) min(-1), respectively; n=8 per dose), heparin (60 u kg(-1)+0.7 u kg(-1) min(-1), n=8), or RPR109891 (30 microg kg(-1)+0.45 microg kg(-1) min(-1), n=8), was initiated. Aspirin (5 mg kg(-1), i.v.) was administered to all animals. Fifteen minutes after the start of drug infusion, rt-PA was administered (100 microg kg(-1)+20 microg kg(-1) min(-1) for 60 min). The incidence of reperfusion in the high dose FXV673 (8/8, 100%) was significantly greater than that in the heparin group (4/8, 50%), with a trend to faster reperfusion (23+/-5 min for FXV673 versus 41+/-11 min for heparin). Only 2/8 (25%) of the vessels reoccluded in the high dose FXV673 group, compared to 4/4 (100%) and 5/5 (100%) vessels in the heparin and RPR109891 groups, respectively (P<0.05). Throughout the protocol, blood flow was higher in the FXV673 treated group compared to other groups. FXV673 enhanced vessel patency in a dose-dependent manner. Compared to vehicle and heparin groups, the thrombus mass was decreased by 60% in the high dose FXV673. FXV673, heparin and RPR109891 increased the bleeding time by 2.7, 1.7 and 4 fold, and APTT by 2.8, 2.7 and 1.2 fold, respectively. In conclusion, FXV673 is more effective than heparin and at least as effective as RPR109891 when used as an adjunct during rt-PA-induced coronary thrombolysis.
我们比较了强效Xa因子抑制剂FXV673与肝素以及糖蛋白IIb/IIIa拮抗剂RPR109891在犬rt-PA诱导的冠状动脉溶栓模型中作为辅助治疗时的抗血栓形成疗效。通过对狭窄冠状动脉进行电解损伤诱导血栓形成。血栓形成闭塞后,开始输注135分钟的生理盐水(n = 8)、FXV673(分别为10、30或100μg kg⁻¹ + 1、3或10μg kg⁻¹ min⁻¹;每个剂量n = 8)、肝素(60 U kg⁻¹ + 0.7 U kg⁻¹ min⁻¹,n = 8)或RPR109891(30μg kg⁻¹ + 0.45μg kg⁻¹ min⁻¹,n = 8)。所有动物均静脉注射阿司匹林(5 mg kg⁻¹)。药物输注开始15分钟后,给予rt-PA(100μg kg⁻¹ + 20μg kg⁻¹ min⁻¹,持续60分钟)。高剂量FXV673组的再灌注发生率(8/8,100%)显著高于肝素组(4/8,50%),且有再灌注更快的趋势(FXV673为23±5分钟,肝素为41±11分钟)。高剂量FXV673组只有2/8(25%)的血管再次闭塞,而肝素组和RPR109891组分别为4/4(100%)和5/5(100%)的血管再次闭塞(P<0.05)。在整个实验过程中,FXV673治疗组的血流高于其他组。FXV673以剂量依赖的方式增强血管通畅性。与溶剂组和肝素组相比,高剂量FXV673组的血栓质量减少了60%。FXV673、肝素和RPR109891分别使出血时间增加2.7倍、1.7倍和4倍,使活化部分凝血活酶时间(APTT)增加2.8倍、2.7倍和1.2倍。总之,在rt-PA诱导的冠状动脉溶栓过程中作为辅助用药时,FXV673比肝素更有效且至少与RPR109891一样有效。
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