Finkle C D, St Pierre A, Leblond L, Deschenes I, DiMaio J, Winocour P D
BioChem Therapeutic Inc., Laval, Quebec, Canada.
Thromb Haemost. 1998 Feb;79(2):431-8.
Current clinical use of heparin as an antithrombotic agent is limited by suboptimal efficacy and safety considerations. Thrombin's central role in thrombosis makes it an attractive target to develop more effective and safer antithrombotic agents. BCH-2763 is a novel, potent (Ki: 0.11 nM), low molecular weight (1.51 kDa), bivalent direct thrombin inhibitor. The antithrombotic efficacy of BCH-2763 in vivo following i.v. bolus plus infusion in rats was compared in arterial and venous thrombosis models with two other bivalent direct thrombin inhibitors, r-hirudin and hirulog, with two catalytic site-directed thrombin inhibitors, inogatran and argatroban, and with heparin. In vivo efficacy was related to inhibition in vitro of fibrin clot formation, thrombin-induced aggregation of rat or human washed platelets and activity of free and plasma clot-bound thrombin. All the direct thrombin inhibitors were effective on both arterial and venous thrombosis at markedly lower fold aPTT increases than heparin. The antithrombotic doses of all inhibitors against venous thrombosis were less than against arterial thrombosis. The rank order of potency based on doses (mg/kg/h) required for full efficacy against arterial thrombosis was BCH-2763 (1.2) > inogatran (1.5) > r-hirudin (1.8) > hirulog (3.3) > argatroban (> 3.0); heparin required a markedly higher dose (5.7). In venous thrombosis the doses required for full efficacy were substantially lower for the bivalent (BCH-2763: 0.12; r-hirudin: 0.12; hirulog: 0.18) than for the catalytic site-directed (inogatran: 0.48; argatroban: 0.90) thrombin inhibitors; the dose required for heparin was 0.19. All the direct thrombin inhibitors caused similar shifts in aPTT at doses required to inhibit arterial thrombosis, but BCH-2763 inhibited venous thrombosis at lower aPTT fold increases. In vivo antithrombotic efficacy of direct thrombin inhibitors correlated with their inhibitory activity in vitro against fibrin clot formation and platelet aggregation. In contrast to heparin, all the direct thrombin inhibitors inhibited plasma clot-bound thrombin, but the relative IC50s did not correlate with their antithrombotic efficacy. In summary, direct thrombin inhibitors are more effective than heparin in inhibiting arterial and venous thrombosis in rats with less aPTT increases. BCH-2763 is effective at lower doses than the other direct thrombin inhibitors and for venous thrombosis at a smaller aPTT increase. BCH-2763 may offer an improved therapeutic index in the treatment of thromboembolic complications over heparin and other direct thrombin inhibitors.
肝素作为抗血栓药物目前的临床应用受到疗效欠佳和安全性方面考虑的限制。凝血酶在血栓形成中起核心作用,这使其成为开发更有效、更安全抗血栓药物的一个有吸引力的靶点。BCH - 2763是一种新型、强效(Ki:0.11 nM)、低分子量(1.51 kDa)的二价直接凝血酶抑制剂。在大鼠动脉和静脉血栓形成模型中,将静脉推注加输注BCH - 2763后的体内抗血栓疗效与另外两种二价直接凝血酶抑制剂重组水蛭素和水蛭肽、两种催化位点定向凝血酶抑制剂伊诺加群和阿加曲班以及肝素进行了比较。体内疗效与体外对纤维蛋白凝块形成的抑制、凝血酶诱导的大鼠或人洗涤血小板聚集以及游离和血浆凝块结合凝血酶的活性有关。所有直接凝血酶抑制剂在明显低于肝素的活化部分凝血活酶时间(aPTT)增加值倍数时,对动脉和静脉血栓形成均有效。所有抑制剂抗静脉血栓形成的抗血栓剂量均低于抗动脉血栓形成的剂量。基于完全抑制动脉血栓形成所需剂量(mg/kg/h)的效力排序为:BCH - 2763(1.2)>伊诺加群(1.5)>重组水蛭素(1.8)>水蛭肽(3.3)>阿加曲班(>3.0);肝素需要明显更高的剂量(5.7)。在静脉血栓形成中,二价(BCH - 2763:0.12;重组水蛭素:0.12;水蛭肽:0.18)凝血酶抑制剂完全起效所需剂量明显低于催化位点定向(伊诺加群:0.48;阿加曲班:0.90)凝血酶抑制剂;肝素所需剂量为0.19。所有直接凝血酶抑制剂在抑制动脉血栓形成所需剂量下引起的aPTT变化相似,但BCH - 2763在较低的aPTT增加值倍数下抑制静脉血栓形成。直接凝血酶抑制剂的体内抗血栓疗效与其体外对纤维蛋白凝块形成和血小板聚集的抑制活性相关。与肝素不同,所有直接凝血酶抑制剂均抑制血浆凝块结合凝血酶,但其相对半数抑制浓度(IC50)与抗血栓疗效不相关。总之,直接凝血酶抑制剂在抑制大鼠动脉和静脉血栓形成方面比肝素更有效,且aPTT增加值更小。BCH - 2763在低于其他直接凝血酶抑制剂的剂量下有效,且对静脉血栓形成时aPTT增加值更小。与肝素及其他直接凝血酶抑制剂相比,BCH - 2763在治疗血栓栓塞并发症方面可能具有更好的治疗指数。
