双盲、安慰剂对照的 II 期研究显示蛋白酶激活受体 1 拮抗剂 E5555(atopaxar)在急性冠状动脉综合征或高危冠状动脉疾病的日本患者中的疗效。
Double-blind, placebo-controlled Phase II studies of the protease-activated receptor 1 antagonist E5555 (atopaxar) in Japanese patients with acute coronary syndrome or high-risk coronary artery disease.
机构信息
Department of Medicine (Cardiology), Tokai University School of Medicine, Isehara, Kanagawa 259-1143, Japan.
出版信息
Eur Heart J. 2010 Nov;31(21):2601-13. doi: 10.1093/eurheartj/ehq320. Epub 2010 Aug 30.
AIMS
Two multicentre, randomized, double-blind, placebo-controlled Phase II studies assessed the safety and efficacy of the oral protease-activated receptor 1 (PAR-1) antagonist E5555 in addition to standard therapy in Japanese patients with acute coronary syndrome (ACS) or high-risk coronary artery disease (CAD).
METHODS AND RESULTS
Patients with ACS (n = 241) or high-risk CAD (n = 263) received E5555 (50, 100, or 200 mg) or placebo once daily for 12 (ACS patients) or 24 weeks (CAD patients). The incidence of TIMI major, minor, and minimal bleeds requiring medical attention was similar in the placebo and combined E5555 (atopaxar) groups (ACS: 6.6% placebo vs. 5.0% E5555; CAD: 1.5% placebo vs. 1.5% E5555). There were no TIMI major bleeds and three CURE major bleeds (two with placebo; one with 100 mg E5555). There was a numerical increase in 'any' TIMI bleeding with the E5555 200 mg dose (ACS: 16.4% placebo vs. 23.0% E5555, P = 0.398; CAD: 4.5% placebo vs. 13.2% E5555, P = 0.081). The rate of major cardiovascular adverse events in the combined E5555 group was not different from placebo (ACS: 6.6% placebo vs. 5.0% E5555, P = 0.73; CAD: 4.5% placebo vs. 1.0% E5555, P = 0.066). There was a statistically significant dose-dependent increase in liver function abnormalities and QTcF with E5555. At trough dosing levels in both populations, mean inhibition of platelet aggregation was > 90% with 100 and 200 mg E5555, and 20-60% with 50 mg E5555.
CONCLUSION
E5555 (50, 100, and 200 mg) did not increase clinically significant bleeding, although there was a higher rate of any TIMI bleeding with the highest two doses. All doses tested achieved a significant level of platelet inhibition. There was a significant dose-dependent increase in liver function abnormalities and QTcF. Although further study is needed, PAR-1 antagonism may have the potential to be a novel pathway for platelet inhibition to add on to the current standard of care therapy.
目的
两项多中心、随机、双盲、安慰剂对照的 2 期研究评估了口服蛋白酶激活受体 1(PAR-1)拮抗剂 E5555 联合标准治疗在日本急性冠脉综合征(ACS)或高危冠状动脉疾病(CAD)患者中的安全性和疗效。
方法和结果
ACS 患者(n=241)或高危 CAD 患者(n=263)接受 E5555(50、100 或 200mg)或安慰剂,每日一次,持续 12 周(ACS 患者)或 24 周(CAD 患者)。安慰剂和联合 E5555( atopaxar)组的 TIMI 主要、次要和最小出血需要医学关注的发生率相似(ACS:安慰剂 6.6% vs. E5555 5.0%;CAD:安慰剂 1.5% vs. E5555 1.5%)。无 TIMI 主要出血,CURE 主要出血 3 例(安慰剂 2 例;100mg E5555 1 例)。E5555 200mg 剂量组“任何”TIMI 出血发生率呈数值增加(ACS:安慰剂 16.4% vs. E5555 23.0%,P=0.398;CAD:安慰剂 4.5% vs. E5555 13.2%,P=0.081)。联合 E5555 组主要心血管不良事件发生率与安慰剂无差异(ACS:安慰剂 6.6% vs. E5555 5.0%,P=0.73;CAD:安慰剂 4.5% vs. E5555 1.0%,P=0.066)。E5555 可引起肝功能异常和 QTcF 呈剂量依赖性增加。在两个人群的谷浓度水平,100mg 和 200mg E5555 可使血小板聚集抑制率>90%,50mg E5555 可使血小板聚集抑制率 20-60%。
结论
E5555(50、100 和 200mg)并未增加临床显著出血,尽管最高两剂量组任何 TIMI 出血发生率较高。所有测试剂量均实现了显著的血小板抑制水平。肝功能异常和 QTcF 呈剂量依赖性增加。尽管还需要进一步研究,但 PAR-1 拮抗剂可能具有成为除当前标准治疗外的血小板抑制新途径的潜力。
Zotero 插件