Gillies H C, Herriott D, Liang R, Ohashi K, Rogers H J, Harper P G
Br J Clin Pharmacol. 1987 Mar;23(3):303-10. doi: 10.1111/j.1365-2125.1987.tb03049.x.
The plasma pharmacokinetics of idarubicin (4-demethoxydaunorubicin) were studied in 20 patients with advanced malignant disease after intravenous (21 occasions) and oral (14 occasions) administration. Idarubicin plasma concentrations were measured by high performance liquid chromatography with fluorescence detection. Pharmacokinetic parameters calculated for the intravenous plasma drug concentration, time data revealed a terminal half-life of 12.9 +/- 6.0 h (mean +/- s.d.), clearance 98.7 +/- 47.3 1 h-1 m-2 and volume of distribution 1533 +/- 536 1 m-2. A bi-exponential equation corresponding to a two compartment open model best fitted the data. Half-life and clearance were not significantly different following oral administration. Bioavailability of oral idarubicin was 0.29 +/- 0.20 (mean +/- s.d.). There was a wide range of bioavailability between and within subjects. Plasma concentrations of idarubicinol (the only metabolite detected) rapidly exceeded those of the parent drug, and exposure to this metabolite was greater than to the parent drug. The mean half-life of idarubicinol was not significantly different after i.v. (63.1 +/- 28.2 h) and oral (45.8 +/- 16.0 h) administration. Much larger amounts of this metabolite were formed following the oral route of administration. This may have implications for the clinical use of this drug as idarubicinol may have appreciable cytotoxic activity.
对20例晚期恶性疾病患者在静脉注射(21次)和口服(14次)给药后进行了伊达比星(4-去甲氧基柔红霉素)的血浆药代动力学研究。采用高效液相色谱荧光检测法测定伊达比星血浆浓度。根据静脉血浆药物浓度、时间数据计算的药代动力学参数显示,终末半衰期为12.9±6.0小时(均值±标准差),清除率为98.7±47.3升/小时·平方米,分布容积为1533±536升/平方米。对应二室开放模型的双指数方程最能拟合数据。口服给药后半衰期和清除率无显著差异。口服伊达比星的生物利用度为0.29±0.20(均值±标准差)。受试者之间和受试者内部的生物利用度范围较宽。伊达比星醇(唯一检测到的代谢物)的血浆浓度迅速超过母体药物,且该代谢物的暴露量大于母体药物。静脉注射(63.1±28.2小时)和口服(45.8±16.0小时)给药后伊达比星醇的平均半衰期无显著差异。口服给药后形成的该代谢物量要大得多。这可能对该药物的临床应用有影响,因为伊达比星醇可能具有明显的细胞毒活性。
