口服直接因子Xa抑制剂利伐沙班(BAY 59-7939)治疗近端深静脉血栓形成:ODIXa-DVT(急性症状性深静脉血栓形成患者口服直接因子Xa抑制剂BAY 59-7939)研究
Treatment of proximal deep-vein thrombosis with the oral direct factor Xa inhibitor rivaroxaban (BAY 59-7939): the ODIXa-DVT (Oral Direct Factor Xa Inhibitor BAY 59-7939 in Patients With Acute Symptomatic Deep-Vein Thrombosis) study.
作者信息
Agnelli Giancarlo, Gallus Alexander, Goldhaber Samuel Z, Haas Sylvia, Huisman Menno V, Hull Russel D, Kakkar Ajay K, Misselwitz Frank, Schellong Sebastian
机构信息
Division of Internal and Cardiovascular Medicine, University of Perugia, Ospedale S. Maria della Misericordia, Perugia, Italy.
出版信息
Circulation. 2007 Jul 10;116(2):180-7. doi: 10.1161/CIRCULATIONAHA.106.668020. Epub 2007 Jun 18.
BACKGROUND
An effective and safe oral anticoagulant that needs no monitoring for dose adjustment is urgently needed for the treatment of diseases that require long-term anticoagulation. Rivaroxaban (BAY 59-7939) is an oral direct factor Xa inhibitor currently under clinical development.
METHODS AND RESULTS
This randomized, parallel-group phase II trial in patients with proximal deep-vein thrombosis explored the efficacy and safety of rivaroxaban 10, 20, or 30 mg BID or 40 mg once daily compared with enoxaparin 1 mg/kg BID followed by vitamin K antagonist. Each treatment was administered for 12 weeks. The primary efficacy end point was an improvement in thrombotic burden at day 21 (assessed by quantitative compression ultrasonography; > or = 4-point improvement in thrombus score) without recurrent symptomatic venous thromboembolism or venous thromboembolism-related death. The primary safety end point was major bleeding during 12 weeks of treatment. Outcomes were adjudicated centrally without knowledge of treatment allocation. The primary efficacy end point was achieved in 53 (53.0%) of 100, 58 (59.2%) of 98, 62 (56.9%) of 109, and 49 (43.8%) of 112 patients receiving rivaroxaban 10, 20, or 30 mg BID or 40 mg once daily, respectively, compared with 50 (45.9%) of 109 patients treated with enoxaparin/vitamin K antagonist. There was no significant trend in the dose-response relationship between rivaroxaban BID and the primary efficacy end point (P=0.67). Major bleeding was observed in 1.7%, 1.7%, 3.3%, and 1.7% of patients receiving rivaroxaban 10, 20, or 30 mg BID or 40 mg once daily, respectively. There were no major bleeding events with enoxaparin/vitamin K antagonist.
CONCLUSIONS
Results of this proof-of-concept and dose-finding study support phase III evaluation of the orally active direct factor Xa inhibitor rivaroxaban, because efficacy and safety were apparent in the treatment of proximal deep-vein thrombosis across a 3-fold range of fixed daily dosing.
背景
对于需要长期抗凝治疗的疾病,迫切需要一种有效且安全、无需监测剂量调整的口服抗凝剂。利伐沙班(BAY 59 - 7939)是一种目前正在进行临床开发的口服直接Xa因子抑制剂。
方法与结果
这项针对近端深静脉血栓形成患者的随机、平行组II期试验,探讨了利伐沙班每日两次10mg、20mg或30mg或每日一次40mg与依诺肝素每日两次1mg/kg随后使用维生素K拮抗剂相比的疗效和安全性。每种治疗均持续12周。主要疗效终点是在第21天时血栓负荷的改善(通过定量压迫超声评估;血栓评分改善≥4分),且无复发性症状性静脉血栓栓塞或静脉血栓栓塞相关死亡。主要安全终点是治疗12周期间的大出血。结局由中心判定,且不知晓治疗分配情况。接受利伐沙班每日两次10mg、20mg或30mg或每日一次40mg治疗的患者中,分别有100例中的53例(53.0%)、98例中的58例(59.2%)、109例中的62例(56.9%)和112例中的49例(43.8%)达到主要疗效终点,而接受依诺肝素/维生素K拮抗剂治疗的109例患者中有50例(45.9%)达到该终点。利伐沙班每日两次给药与主要疗效终点之间的剂量 - 反应关系无显著趋势(P = 0.67)。接受利伐沙班每日两次10mg、20mg或30mg或每日一次40mg治疗的患者中,大出血发生率分别为1.7%、1.7%、3.3%和1.7%。依诺肝素/维生素K拮抗剂组未发生大出血事件。
结论
这项概念验证和剂量探索研究的结果支持对口服活性直接Xa因子抑制剂利伐沙班进行III期评估,因为在每日固定剂量3倍范围内治疗近端深静脉血栓形成时,其疗效和安全性均很明显。
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