Clinical Trials Management Division, Korea Food and Drug Administration, Seoul, Korea.
Clin Ther. 2009 Nov;31(11):2712-21. doi: 10.1016/j.clinthera.2009.11.010.
Rebamipide is a quinolinone-derived gastroprotective agent approved in Korea for the treatment of gastric ulcers, acute gastritis, and exacerbated chronic gastritis.
The aims of this study were to evaluate the pharmacokinetics and bioequivalence of a reference (branded) and test (generic) formulation of rebamipide 100-mg tablets in healthy Korean male volunteers for the purposes of generic substitution and to evaluate the relationship between genetic polymorphisms in the ABCB1 gene (exons 21 and 26) and rebamipide pharmacokinetics.
This study had a 2-period crossover design, with a 7-day washout between formulations. Healthy Korean male volunteers were randomly assigned to receive a single 100-mg dose of the test or reference formulation, administered with 240 mL of water after a 12-hour overnight fast. Serum concentrations of rebamipide up to 12 hours after administration were determined using a validated HPLC method with fluorescence detection. Vital signs (temperature, blood pressure, and heart rate) were measured before and after dosing in both periods. Adverse events were monitored by clinic staff on the days of study drug administration and were recorded for up to 1 week after the last dose of study medication. Pharmacokinetic parameters were determined using a noncompartmental method. The formulations were considered bioequivalent if the log-transformed ratios of AUC(0-t), AUC(0-infinity)), and C(max) were within the predetermined bioequivalence range (80%-125%) established by the US Food and Drug Administration and Korean legislation. The in vitro dissolution profiles of the 2 formulations were examined, and the influence on rebamipide pharmacokinetics of genetic polymorphisms in the ABCB1 gene (P-glycoprotein) was investigated.
Thirty healthy Korean male volunteers (mean [SD] age, 22.97 [1.67] years [range, 20-27 years]; height, 174.56 [6.27] cm [range, 159.1-184.8 cm]; and weight, 69.44 [8.32] kg [range, 54.7-90.2 kg]) were enrolled in and completed the study. No adverse events were reported. The 2 formulations had comparable in vitro dissolution profiles. The mean AUC(0-t) for the test and reference formulations was 831.09 (329.52) and 903.46 (419.17) ng/mL/h, respectively; the AUC(0-infinity) was 851.68 (332.62) and 923.58 (423.21) ng/mL/h; the C(max) was 218.12 (93.90) and 220.57 (107.48) ng/mL; the T(max) was 2.05 (1.15) and 2.10 (0.76) hours; and the t((1/2)) was 1.96 (0.52) and 1.93 (0.49) hours. No significant sequence, subject, formulation, or period effects were detected for any pharmacokinetic parameter. The point estimates for AUC(0-t), AUC(0-infinity), and C(max) were 0.95 (90% CI, 0.84-1.06), 0.95 (90% CI, 0.84-1.06), and 1.01 (90% CI, 0.89-1.15), respectively, satisfying the criterion for bioequivalence. There was no statistically significant difference in T(max). No significant differences in rebamipide AUC(0-t), AUC(0-infinity), or C(max) were found among the ABCB1 2677 GG, GT, or TT groups, or among the ABCB1 3435 CC, CT, or TT groups. There was no evidence that genetic polymorphisms in the ABCB1 gene influenced the pharmacokinetics of rebamipide.
The results of this study in healthy Korean male volunteers suggest that the 2 rebamipide 100-mg tablet formulations administered in the fasted state met the regulatory criterion for bioequivalence. There was no evidence that rebamipide pharmacokinetic parameters were influenced by genetic polymorphisms in the ABCB1 gene (exons 21 and 26). ClinicalTrials.gov identifier: .
瑞巴派特是一种喹诺酮类胃黏膜保护剂,在韩国被批准用于治疗胃溃疡、急性胃炎和加重的慢性胃炎。
本研究旨在评估健康韩国男性志愿者中瑞巴派特 100mg 片剂参比制剂(品牌药)和受试制剂(仿制药)的药代动力学特征和生物等效性,以实现仿制药替代,并评估 ABCB1 基因(外显子 21 和 26)的遗传多态性与瑞巴派特药代动力学之间的关系。
该研究采用 2 期交叉设计,两种制剂之间有 7 天的洗脱期。健康的韩国男性志愿者被随机分配,空腹状态下单次口服受试或参比制剂 100mg,用 240ml 水送服。给药后 12 小时内,采用经验证的 HPLC 荧光检测法测定血清中瑞巴派特的浓度。在两个周期中,在给药前后测量生命体征(体温、血压和心率)。在给药日,临床工作人员监测不良事件,并在最后一次服药后 1 周内记录不良事件。采用非房室模型法计算药代动力学参数。如果 AUC(0-t)、AUC(0-∞)和 Cmax 的对数比值在由美国食品药品监督管理局和韩国法规规定的 80%-125%的预定生物等效性范围内,则认为两种制剂具有生物等效性。考察了两种制剂的体外溶出度,并研究了 ABCB1 基因(P-糖蛋白)遗传多态性对瑞巴派特药代动力学的影响。
30 名健康的韩国男性志愿者(平均[标准差]年龄,22.97[1.67]岁[范围,20-27 岁];身高,174.56[6.27]cm[范围,159.1-184.8cm];体重,69.44[8.32]kg[范围,54.7-90.2kg])参与并完成了这项研究。没有报告不良事件。两种制剂具有相似的体外溶出度特征。受试制剂和参比制剂的 AUC(0-t)平均值分别为 831.09(329.52)和 903.46(419.17)ng/ml/h,AUC(0-∞)分别为 851.68(332.62)和 923.58(423.21)ng/ml/h,Cmax 分别为 218.12(93.90)和 220.57(107.48)ng/ml,Tmax 分别为 2.05(1.15)和 2.10(0.76)小时,t1/2 分别为 1.96(0.52)和 1.93(0.49)小时。任何药代动力学参数均未检测到显著的序列、受试者、制剂或周期效应。AUC(0-t)、AUC(0-∞)和 Cmax 的点估计值分别为 0.95(90%CI,0.84-1.06)、0.95(90%CI,0.84-1.06)和 1.01(90%CI,0.89-1.15),满足生物等效性标准。Tmax 无统计学差异。ABCB1 2677 GG、GT 或 TT 组和 ABCB1 3435 CC、CT 或 TT 组之间,瑞巴派特 AUC(0-t)、AUC(0-∞)或 Cmax 无显著差异。没有证据表明 ABCB1 基因的遗传多态性影响瑞巴派特的药代动力学。
本研究在健康的韩国男性志愿者中表明,空腹状态下口服两种瑞巴派特 100mg 片剂制剂符合监管标准的生物等效性。没有证据表明 ABCB1 基因(外显子 21 和 26)的遗传多态性影响瑞巴派特的药代动力学参数。临床试验注册编号:。
