Kubitza Dagmar, Mueck Wolfgang, Becka Michael
Clinical Pharmacology, Pharmacometry, Bayer HealthCare AG, Wuppertal, Germany.
Drug Saf. 2008;31(1):67-77. doi: 10.2165/00002018-200831010-00006.
Rivaroxaban (BAY 59-7939) is a novel, oral, direct Factor Xa inhibitor in advanced clinical development for the prevention and treatment of thromboembolic disorders. Unwanted pro-arrhythmic effects are a common reason for drugs failing to gain regulatory approval; these properties can be detected by assessing the effect of the drug on the QT interval.
This study was performed, in accordance with International Conference on Harmonisation (ICH) E14 guidance, to assess whether rivaroxaban prolongs the QT interval.
This was a prospective, randomized, double-blind, double-dummy, four-way crossover study.
The study was conducted at a clinical pharmacology research unit.
Healthy male and female subjects (n = 54) aged > or =50 years were enrolled and remained in the study unit for 3 days for each treatment. Of these, 50 patients were eligible for the QT analysis.
Subjects received single oral doses of rivaroxaban 45 mg or 15 mg, moxifloxacin 400 mg (positive control), or placebo.
Multiple ECGs were taken at frequent intervals after drug administration, and the QT interval was measured manually under blinded conditions at a central laboratory. The Fridericia correction formula (QTcF) was used to correct the QT interval for heart rate. The primary outcome was the effect of rivaroxaban or moxifloxacin on the placebo-subtracted QTcF 3 hours after administration. The frequency of outlying QTcF values and the tolerability of the treatments were also assessed.
All treatments were well tolerated and had no effect on heart rate. Moxifloxacin established the required assay sensitivity; placebo-subtracted QTcF 3 hours after moxifloxacin administration was prolonged by 9.77 ms (95% CI 7.39, 12.15). Placebo-subtracted QTcF values 3 hours after rivaroxaban administration were -0.91 ms (95% CI -3.33, 1.52) and -1.83 ms (95% CI -4.19, 0.54) with rivaroxaban 45 mg and 15 mg, respectively. QTcF was not prolonged with rivaroxaban at any time, and the frequency of outlying results with rivaroxaban and placebo was similar.
This thorough QT study, which was performed in accordance with ICH E14 guidelines, shows that rivaroxaban does not prolong the QTc interval. Therefore, the potential of rivaroxaban for the prevention and treatment of thromboembolic disorders, including chronic cardiovascular disorders, can be investigated in appropriate clinical studies without the need for intensive monitoring of the QTc interval.
利伐沙班(BAY 59 - 7939)是一种新型口服直接凝血因子Xa抑制剂,正处于预防和治疗血栓栓塞性疾病的晚期临床开发阶段。不良的促心律失常作用是药物未能获得监管批准的常见原因;这些特性可通过评估药物对QT间期的影响来检测。
根据国际协调会议(ICH)E14指南进行本研究,以评估利伐沙班是否会延长QT间期。
这是一项前瞻性、随机、双盲、双模拟、四交叉研究。
研究在临床药理学研究单位进行。
年龄≥50岁的健康男性和女性受试者(n = 54)入组,每种治疗在研究单位停留3天。其中,50例患者符合QT分析条件。
受试者单次口服45 mg或15 mg利伐沙班、400 mg莫西沙星(阳性对照)或安慰剂。
给药后频繁采集多份心电图,在中心实验室的盲态条件下人工测量QT间期。采用弗里德里西亚校正公式(QTcF)校正心率对QT间期的影响。主要观察指标是给药后3小时利伐沙班或莫西沙星对减去安慰剂后的QTcF的影响。还评估了QTcF异常值的频率和治疗的耐受性。
所有治疗耐受性良好,对心率无影响。莫西沙星确立了所需的检测灵敏度;给药后3小时莫西沙星减去安慰剂后的QTcF延长了9.77 ms(95%CI 7.39, 12.15)。利伐沙班45 mg和15 mg给药后3小时减去安慰剂后的QTcF值分别为 - 0.91 ms(95%CI - 3.33, 1.52)和 - 1.83 ms(95%CI - 4.19, 0.54)。利伐沙班在任何时候均未使QTcF延长,利伐沙班和安慰剂的异常结果频率相似。
这项按照ICH E14指南进行的全面QT研究表明,利伐沙班不会延长QTc间期。因此,在适当的临床研究中可以对利伐沙班预防和治疗血栓栓塞性疾病(包括慢性心血管疾病)的潜力进行研究,而无需对QTc间期进行密集监测。
