Kim Sung-Doo, Kang Wonku, Lee Hae Won, Park Dae Jin, Ahn Ju Hee, Kim Mi Jin, Kim Eun Young, Kim Sung Wuk, Nam Hee Sook, Na Hye Jung, Yoon Young-Ran
Clinical Trial Center, Kyungpook National University Hospital, Jung-gu, Daegu, Republic of Korea.
Clin Ther. 2009 Apr;31(4):793-803. doi: 10.1016/j.clinthera.2009.04.017.
Clopidogrel, a potent antiplatelet agent, reduces the risk for thrombotic events in patients with atherothrombotic diseases. Clopidogrel is marketed primarily as a bisulfate salt. A different salt preparation of clopidogrel, clopidogrel besylate, has been developed and might provide an additional treatment option for patients.
The aim of this study was to compare the pharmacokinetic, pharmacodynamic, and tolerability profiles of clopidogrel besylate with those of clopidogrel bisulfate to determine bioequivalence for the purposes of marketing approval.
A randomized, open-label, 2-period, single- and multiple-dose, comparative crossover study was conducted in healthy Korean male subjects. The subjects received either clopidogrel bisulfate or clopidogrel besylate as a single 300-mg oral loading dose (day 1) followed by a 75-mg/d (once daily) maintenance dose on days 2 to 6. After a 15-day washout period, subjects were administered the alternative salt preparation according to the same protocol. The plasma concentrations of clopidogrel and its primary metabolite (SR26334) were assessed using high-performance liquid chromatography/tandem mass spectrometry after administration of the loading dose. The platelet aggregation response to 10-mumol/L adenosine diphosphate was measured using turbidometric aggregometry during the single- and multiple-dosing periods and at steady state (day 6). Tolerability was monitored using physical examination, including vital sign measurements, and laboratory analysis.
Forty-four subjects were enrolled and completed the study (mean [SD] age, 24.3 [2.7] years; weight, 70.0 [8.2] kg). The mean values for C(max), T(max), and AUC(0-t) with clopidogrel (parent drug) of clopidogrel besylate (5.2 ng/mL, 0.9 hour, and 10.1 ng/mL/h, respectively) were similar to those with clopidogrel bisulfate (5.4 ng/mL, 0.9 hour, and 10.3 ng/mL/h). The mean values for Cmax, AUC(0-t), and AUC(0-infinity) with the SR26334 of clopidogrel besylate (10.9 microg/mL, 38.8 microg/mL/h, and 43.0 microg/mL/h, respectively) were not significantly different from those with the SR26334 of clopidogrel bisulfate (11.9 microg/mL, 40.6 microg/mL/h, and 43.8 microg/mL/h). The mean values for maximal antiplatelet effect (Emax) and area under the time-effect curve (AUEC) with the 2 clopidogrel salt preparations were as follows: clopidogrel besylate, 58.8 h . % and 4299.1 h . % inhibition, respectively; and clopidogrel bisulfate, 61.7 h . % and 4406.9 h . % inhibition; these differences were not statistically significant. The 90% CIs for the ratios of the log-transformed C(max), AUC, E(max), and AUEC values were within the predetermined bioequivalence range of 80% to 125%. Three adverse events (6.8%) were reported during the study and included abdominal discomfort (1 subject [2.3%] in the group that received clopidogrel bisulfate), easy fatigability (1 subject [2.3%] immediately before administration of loading dose of clopidogrel besylate), and thrombocytopenia (1 subject [2.3%] in the group receiving the clopidogrel bisulfate). All adverse events were transient and mild.
In these healthy Korean male subjects, the differences in the pharmacokinetic and pharmacodynamic properties between the 2 clopidogrel salt preparations did not reach statistical significance and met the regulatory requirements for bioequivalence. Both preparations were well tolerated.
氯吡格雷是一种强效抗血小板药物,可降低动脉粥样硬化血栓形成疾病患者发生血栓事件的风险。氯吡格雷主要以硫酸氢盐形式上市。已开发出氯吡格雷的另一种盐制剂——氯吡格雷苯磺酸盐,它可能为患者提供更多治疗选择。
本研究旨在比较氯吡格雷苯磺酸盐与氯吡格雷硫酸氢盐的药代动力学、药效学和耐受性特征,以确定其生物等效性,用于上市批准。
在健康韩国男性受试者中进行了一项随机、开放标签、两周期、单剂量和多剂量的比较交叉研究。受试者接受一次300mg口服负荷剂量(第1天)的氯吡格雷硫酸氢盐或氯吡格雷苯磺酸盐,随后在第2至6天接受75mg/d(每日一次)的维持剂量。经过15天的洗脱期后,受试者按照相同方案服用另一种盐制剂。在给予负荷剂量后,使用高效液相色谱/串联质谱法评估氯吡格雷及其主要代谢物(SR26334)的血浆浓度。在单剂量和多剂量给药期间以及稳态(第6天),使用比浊法血小板聚集测定法测量血小板对10μmol/L二磷酸腺苷的聚集反应。通过体格检查(包括生命体征测量)和实验室分析监测耐受性。
44名受试者入组并完成研究(平均[标准差]年龄,24.3[2.7]岁;体重,70.0[8.2]kg)。氯吡格雷苯磺酸盐(母体药物)的C(max)、T(max)和AUC(0-t)的平均值(分别为5.2ng/mL、0.9小时和10.1ng/mL/h)与氯吡格雷硫酸氢盐(5.4ng/mL、0.9小时和10.3ng/mL/h)相似。氯吡格雷苯磺酸盐的SR26334的Cmax、AUC(0-t)和AUC(0-∞)的平均值(分别为10.9μg/mL、38.8μg/mL/h和43.0μg/mL/h)与氯吡格雷硫酸氢盐的SR26334(11.9μg/mL、40.6μg/mL/h和43.8μg/mL/h)无显著差异。两种氯吡格雷盐制剂的最大抗血小板效应(Emax)和时间-效应曲线下面积(AUEC)的平均值如下:氯吡格雷苯磺酸盐分别为58.8h·%和4299.1h·%抑制率;氯吡格雷硫酸氢盐分别为61.7h·%和4406.9h·%抑制率;这些差异无统计学意义。对数转换后的C(max)、AUC、E(max)和AUEC值的比值的90%置信区间在预定的生物等效性范围80%至125%内。研究期间报告了3例不良事件(6.8%),包括腹部不适(接受氯吡格雷硫酸氢盐组1例受试者[2.3%])、易疲劳(在给予氯吡格雷苯磺酸盐负荷剂量前1例受试者[2.3%])和血小板减少症(接受氯吡格雷硫酸氢盐组1例受试者[2.3%])。所有不良事件均为短暂且轻微的。
在这些健康韩国男性受试者中,两种氯吡格雷盐制剂的药代动力学和药效学特性差异无统计学意义,符合生物等效性的监管要求。两种制剂耐受性良好。
