Aweeka F, Jayesekara D, Horton M, Swan S, Lambrecht L, Wilner K D, Sherwood J, Anziano R J, Smolarek T A, Turncliff R Z
San Francisco General Hospital, CA 94110, USA.
Br J Clin Pharmacol. 2000;49 Suppl 1(Suppl 1):27S-33S. doi: 10.1046/j.1365-2125.2000.00150.x.
To assess whether renal impairment influences the pharmacokinetics of ziprasidone, and to determine whether ziprasidone is cleared via haemodialysis.
Thirty-nine subjects with varying degrees of renal impairment were enrolled into an open-label, multicentre, multiple-dose study and assigned to four groups according to their renal function: normal (group 1, creatinine clearance > 70 ml min(-1); mildly impaired (group 2, creatinine clearance 30-60 ml min(-1); moderately impaired (group 3, creatinine clearance 10-29 ml min(-1), and severely impaired (group 4, requiring haemodialysis three times-a-week). Subjects received ziprasidone 40 mg day(-1), given orally with food, as two divided daily doses for 7 days and a single 20 mg dose on the morning of day 8. Pharmacokinetic variables were determined from multiple venous blood samples collected on days 1 and 8 (haemodialysis day for subjects with severe renal impairment). Additional samples were collected from subjects with severe renal impairment on day 7 (nonhaemodialysis day).
On day 1 there were no statistically significant differences in the pharmacokinetics (AUC(0, 12 h), Cmax, tmax) of ziprasidone among subjects with normal renal function and those with mild, moderate and severe renal impairment. The AUC(0,12 h) and Cmax in subjects with mildly impaired renal function were statistically significantly greater than in those with moderately impaired renal function (P = 0.0163-0.0385). The mean AUC(0,12 h) was 272, 370, 250 and 297 ng ml(-1) h in groups 1, 2, 3 and 4, respectively. Corresponding mean Cmax values were 47, 61, 41 and 50 ng ml(-1) and corresponding mean tmax values were 5, 6, 5 and 5 h. On day 8 there were no statistically significant differences in the pharmacokinetics (AUC(0,12 h), Cmax, tmax, lambda(z), Fb) of ziprasidone among subjects with normal renal function and those with moderate or severe renal impairment. The AUC(0,12 h) in subjects with mild renal impairment was statistically significantly greater than those in the other three groups (P = 0.0025-0.0221), but this was not considered clinically significant. The mean AUC(0,12 h) were 446, 650, 389 and 427 ng ml(-1) h in groups 1, 2, 3 and 4, respectively. Corresponding mean Cmax values were 68, 93, 54 and 70 ng ml(-1), corresponding mean tmax values were 4, 5, 4 and 5 h and corresponding mean lambda(z) were 0.14, 0.11, 0.14 and 0.17 h(-1). The mean percentage Fb was 99.84-99.88% across all groups and the mean t(1/2),z ranged from 4.2 to 6.4 h. Comparison of the mean AUC(0,12 h) and Cmax values in subjects with severe renal impairment on day 7 with those on day 8 suggested that haemodialysis does not have a clinically significant effect on the pharmacokinetics of ziprasidone.
The findings of this study indicate that mild-to-moderate impairment of renal function does not result in clinically significant alteration of ziprasidone pharmacokinetics and therefore does not necessitate dose adjustment.
评估肾功能损害是否会影响齐拉西酮的药代动力学,并确定齐拉西酮是否通过血液透析清除。
39名不同程度肾功能损害的受试者被纳入一项开放标签、多中心、多剂量研究,并根据其肾功能分为四组:正常(第1组,肌酐清除率>70 ml·min⁻¹);轻度损害(第2组,肌酐清除率30 - 60 ml·min⁻¹);中度损害(第3组,肌酐清除率10 - 29 ml·min⁻¹);重度损害(第4组,每周需要进行3次血液透析)。受试者每天口服40 mg齐拉西酮,与食物同服,分两次给药,共7天,并在第8天早晨单次服用20 mg剂量。药代动力学变量通过在第1天和第8天(重度肾功能损害受试者的血液透析日)采集的多个静脉血样进行测定。重度肾功能损害的受试者在第7天(非血液透析日)采集额外样本。
第1天,肾功能正常、轻度、中度和重度肾功能损害的受试者之间,齐拉西酮的药代动力学(AUC(0, 12 h)、Cmax、tmax)无统计学显著差异。轻度肾功能损害受试者的AUC(0,12 h)和Cmax在统计学上显著高于中度肾功能损害受试者(P = 0.0163 - 0.0385)。第1组、第2组、第3组和第4组的平均AUC(0,12 h)分别为272、370、250和297 ng·ml⁻¹·h。相应的平均Cmax值分别为47、61、41和50 ng·ml⁻¹,相应的平均tmax值分别为5、6、5和5 h。第8天,肾功能正常、中度或重度肾功能损害的受试者之间,齐拉西酮的药代动力学(AUC(0,12 h)、Cmax、tmax、lambda(z)、Fb)无统计学显著差异。轻度肾功能损害受试者的AUC(0,12 h)在统计学上显著高于其他三组(P = 0.002\5 - 0.0221),但这在临床上不被认为具有显著意义。第1组、第2组、第3组和第4组的平均AUC(0,12 h)分别为446、650、389和427 ng·ml⁻¹·h。相应的平均Cmax值分别为68、93、54和70 ng·ml⁻¹,相应的平均tmax值分别为4、5、4和5 h,相应的平均lambda(z)分别为0.14、0.11、0.14和0.17 h⁻¹。所有组的平均Fb百分比为99.84 - 99.88%,平均t(1/2),z范围为4.2至6.4 h。重度肾功能损害受试者第7天与第8天的平均AUC(0,12 h)和Cmax值比较表明,血液透析对齐拉西酮的药代动力学没有临床上显著的影响。
本研究结果表明,轻至中度肾功能损害不会导致齐拉西酮药代动力学发生临床上显著的改变,因此无需调整剂量。
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