Wilner K D, Tensfeldt T G, Baris B, Smolarek T A, Turncliff R Z, Colburn W A, Hansen R A
Department of Clinical Research, Pfizer Central Research, Groton, CT 06340, USA.
Br J Clin Pharmacol. 2000;49 Suppl 1(Suppl 1):15S-20S. doi: 10.1046/j.1365-2125.2000.00148.x.
To compare the pharmacokinetics of ziprasidone in healthy young (18-45 years) men and women, and healthy elderly (> or = 65 years) men and women.
Eight young men, 11 young women, 8 elderly men and 8 elderly women were given oral ziprasidone 40 mg day(-1), in two evenly divided daily doses, for 7 days, followed by a single 20 mg dose on day 8. Serum samples were collected immediately before the morning dose on days 1-8, for up to 12 h after dosing on day 1 and for up to 96 h after dosing on day 8. The resulting data were used to derive pharmacokinetic parameters of ziprasidone in each age and gender group.
Steady-state serum concentrations of ziprasidone were achieved within 2-3 days. The steady-state pharmacokinetics of ziprasidone, determined 8 days after the initiation of treatment, were similar in the young men, elderly men and young women. Assessment of gender effects by analysis of variance revealed statistically significant differences in Cmax (85 vs. 69 ng ml(-1) and tmax (3.19 vs. 4.81 h) but no differences in AUC(0,12 h) or lambda(z). Assessment of age effects by analysis of variance revealed statistically significant differences in AUC(0,12 h) (560 vs. 465 ng ml(-1) h), Cmax (85 vs. 69 ng ml(-1) and lambda(z) (0.126 vs. 0.197 l h(-1) but no difference in tmax. Assessment of age and gender effects by analysis of covariance, with body weight as the covariate, did not reveal any significant differences. The mean t(1/2), z in the young men, young women, elderly men and elderly women were 3.1, 4.1, 5.7 and 5.3 h, respectively. Standard deviations of the means for the pharmacokinetic parameters for the elderly women tended to be large.
The influence of age and gender on the pharmacokinetics of ziprasidone is not clinically significant.
比较齐拉西酮在健康年轻(18 - 45岁)男性和女性以及健康老年(≥65岁)男性和女性中的药代动力学。
8名年轻男性、11名年轻女性、8名老年男性和8名老年女性每天口服齐拉西酮40 mg,分两次等量服用,共7天,然后在第8天单次服用20 mg剂量。在第1 - 8天早晨服药前立即采集血清样本,在第1天服药后长达12小时以及第8天服药后长达96小时采集样本。所得数据用于推导齐拉西酮在每个年龄和性别组中的药代动力学参数。
在2 - 3天内达到齐拉西酮的稳态血清浓度。在治疗开始8天后测定的齐拉西酮稳态药代动力学在年轻男性、老年男性和年轻女性中相似。通过方差分析评估性别效应显示,Cmax(85对69 ng/ml)和tmax(3.19对4.81小时)存在统计学显著差异,但AUC(0,12 h)或λz无差异。通过方差分析评估年龄效应显示,AUC(0,12 h)(560对465 ng/ml·h)、Cmax(85对69 ng/ml)和λz(0.126对0.197 l/h)存在统计学显著差异,但tmax无差异。以体重为协变量通过协方差分析评估年龄和性别效应未发现任何显著差异。年轻男性、年轻女性、老年男性和老年女性的平均t(1/2),z分别为3.1、4.1、5.7和5.3小时。老年女性药代动力学参数均值的标准差往往较大。
年龄和性别对齐拉西酮药代动力学的影响在临床上不显著。