Thudium Karen, Gallo Jorge, Bouillaud Emmanuel, Sachs Carolin, Eddy Simantini, Cheung Wing
Novartis Pharmaceuticals Corporation, East Hanover, NJ, USA.
Novartis Pharma AG, Basel, Switzerland.
Clin Pharmacol. 2015 Jan 22;7:11-7. doi: 10.2147/CPAA.S73472. eCollection 2015.
The mammalian target of rapamycin (mTOR) inhibitor everolimus has a well-established pharmacokinetics profile. We conducted a randomized, single-center, open-label, two-sequence, two-period crossover study of healthy volunteers to assess the relative bioavailability of everolimus administered as one 5 mg tablet or five 1 mg tablets.
Subjects were randomized 1:1 to receive everolimus dosed as one 5 mg tablet or as five 1 mg tablets on day 1, followed by a washout period on days 8-14 and then the opposite formulation on day 15. Blood sampling for pharmacokinetic evaluation was performed at prespecified time points, with 17 samples taken for each treatment period. Primary variables for evaluation of relative bioavailability were area under the concentration-time curve from time zero to infinity (AUCinf) and maximum blood concentration (Cmax). Safety was assessed by reporting the incidence of adverse events (AEs).
Twenty-two participants received everolimus as one 5 mg tablet followed by five 1 mg tablets (n=11) or the opposite sequence (n=11). The Cmax of five 1 mg tablets was 48% higher than that of one 5 mg tablet (geometric mean ratio, 1.48; 90% confidence interval [CI], 1.35-1.62). AUCinf was similar (geometric mean ratio, 1.08; 90% CI, 1.02-1.16), as were the extent of absorption and the distribution and elimination kinetics. AEs, all grade 1 or 2, were observed in 54.5% of subjects.
Although the extent of absorption was similar, the Cmax of five 1 mg tablets was higher than that of one 5 mg tablet, suggesting these formulations lead to different peak blood concentrations and are not interchangeable at the dose tested.
雷帕霉素哺乳动物靶点(mTOR)抑制剂依维莫司具有已明确的药代动力学特征。我们对健康志愿者进行了一项随机、单中心、开放标签、双序列、双周期交叉研究,以评估服用1片5 mg片剂或5片1 mg片剂的依维莫司的相对生物利用度。
受试者按1:1随机分组,在第1天接受1片5 mg片剂或5片1 mg片剂剂量的依维莫司,随后在第8 - 14天为洗脱期,然后在第15天接受相反的剂型。在预定时间点进行血样采集以进行药代动力学评估,每个治疗周期采集17个样本。评估相对生物利用度的主要变量为从时间零点至无穷大的浓度 - 时间曲线下面积(AUCinf)和最大血药浓度(Cmax)。通过报告不良事件(AE)的发生率来评估安全性。
22名参与者接受了依维莫司,其中11名先服用1片5 mg片剂,后服用5片1 mg片剂,另外11名接受相反顺序。5片1 mg片剂的Cmax比1片5 mg片剂高48%(几何平均比值,1.48;90%置信区间[CI],1.35 - 1.62)。AUCinf相似(几何平均比值,1.08;90% CI,1.02 - 1.16),吸收程度以及分布和消除动力学也相似。54.5%的受试者观察到AE,均为1级或2级。
尽管吸收程度相似,但5片1 mg片剂的Cmax高于1片5 mg片剂,表明这些剂型导致不同的血药峰值浓度,在所测试剂量下不可互换。
