Lee S D, Lee W I, Shim H J, Lee E D, Kim W B, Yang J, Kim C K, Lee M G
Research Laboratories, Dong-A Pharmaceutical Company Ltd, Yongin-Gun, Kyunggi-Do, South Korea.
J Clin Pharm Ther. 1996 Aug;21(4):201-13. doi: 10.1111/j.1365-2710.1996.tb01140.x.
The tissue distribution, and biliary and urinary excretion of four metabolites (M1-M4) of a new anthracycline antineoplastic agent (DA-125) were compared after single and multiple (7 consecutive days) intravenous (i.v.) administration to rats. The mean pharmacokinetic parameters of M1, such as area under the plasma concentration-time curve (AUC: 56.4 micrograms/ml vs. 69.0 micrograms min/ml), terminal half-life (t1/2: 3.51 h vs. 3.01 h), total body clearance (Cl: 70.9 ml/min/kg vs. 58.0 ml/min/kg), renal clearance (ClR: 0.193 ml/min/kg vs. 0.336 ml/min/kg) and nonrenal clearance (ClNR: 70.7 ml/min/kg vs. 57.7 ml/min/kg); of M2, such as plasma AUC (39.4 micrograms min/ml vs. 41.9 micrograms min/ ml), t1/2 (6.15 h vs. 7.34 h) and ClR (10.5 ml/min/ kg vs. 13.8 ml/min/kg); and of M4, such as plasma AUC (4.82 micrograms min/ml vs. 6.54 micrograms min/ml) and t1/2 (3.33 h vs 4.02 h), were comparable between single and multiple administrations of DA-125. M3 was detected in plasma for up to 1-5 min, and M3 and M4 were below the detection limit in 24-h urine after both single and multiple administrations of DA-125. M2 was the main metabolite of DA-125 excreted (among M1-M4) in 24-h urine after both single and multiple administrations of DA-125; approximately 12.3% and 20.1% (P < 0.01) of i.v. dosage (expressed in terms of DA-125) was excreted as M2 after single and multiple administrations of DA-125, respectively. Corresponding values for M1 were 0.326% and 0.694% (P < 0.05). The mean levels of M1 (229 micrograms vs. 175 micrograms) and M2 (1330 micrograms vs. 1120 micrograms) excreted in 24-h bile after single and multiple administrations of DA-125 were not significantly different; the percentages of i.v. dosage excreted in 24-h bile as M1 (expressed in terms of DA-125) were 4.83% and 3.58% after single and multiple administrations, respectively. The corresponding values for M2 were 27.8% and 22.5%. M3 and M4 were below the detection limit in 24-h bile after both single and multiple administrations of DA-125. Mean AUAts (area under the amount-time curves from time zero to last measurement time t) (or AUCts-area under the plasma concentration-time curves from time zero until the last measurement time t) of M1-M4 in each tissue after single and multiple administrations of DA-125 were also comparable except in the bone marrow and thymus. The data suggest that 7 consecutive days of i.v. administration of DA-125 (4 mg/kg) to rats does not lead to considerable accumulation of M1-M4 in the tissues, except in the bone marrow and thymus.
将一种新型蒽环类抗肿瘤药物(DA - 125)单次和多次(连续7天)静脉注射给大鼠后,比较了其四种代谢物(M1 - M4)的组织分布以及胆汁和尿液排泄情况。单次和多次给予DA - 125后,M1的平均药代动力学参数,如血浆浓度 - 时间曲线下面积(AUC:56.4微克/毫升对69.0微克·分钟/毫升)、末端半衰期(t1/2:3.51小时对3.01小时)、全身清除率(Cl:70.9毫升/分钟/千克对58.0毫升/分钟/千克)、肾清除率(ClR:0.193毫升/分钟/千克对0.336毫升/分钟/千克)和非肾清除率(ClNR:70.7毫升/分钟/千克对57.7毫升/分钟/千克);M2的平均药代动力学参数,如血浆AUC(39.4微克·分钟/毫升对41.9微克·分钟/毫升)、t1/2(6.15小时对7.34小时)和ClR(10.5毫升/分钟/千克对13.8毫升/分钟/千克);以及M4的平均药代动力学参数,如血浆AUC(4.82微克·分钟/毫升对6.54微克·分钟/毫升)和t1/2(3.33小时对4.02小时),两者具有可比性。单次和多次给予DA - 125后,血浆中M3可检测长达1 - 5分钟,24小时尿液中M3和M4低于检测限。单次和多次给予DA - 125后,M2是DA - 125在24小时尿液中排泄的主要代谢物(在M1 - M4中);单次和多次给予DA - 125后,分别约有12.3%和20.1%(P < 0.01)的静脉注射剂量(以DA - 125计)以M2形式排泄。M1的相应值为0.326%和0.694%(P < 0.05)。单次和多次给予DA - 125后,24小时胆汁中排泄的M1(229微克对175微克)和M2(1330微克对1120微克)的平均水平无显著差异;单次和多次给药后,24小时胆汁中以M1形式排泄的静脉注射剂量百分比(以DA - 125计)分别为4.83%和3.58%。M2的相应值为27.8%和22.5%。单次和多次给予DA - 125后,24小时胆汁中M3和M4低于检测限。单次和多次给予DA - 125后,除骨髓和胸腺外,各组织中M1 - M4的平均AUAts(从零时间到最后测量时间t的量 - 时间曲线下面积)(或AUCts - 从零时间到最后测量时间t的血浆浓度 - 时间曲线下面积)也具有可比性。数据表明,对大鼠连续7天静脉注射DA - 125(4毫克/千克)不会导致M1 - M4在组织中大量蓄积,骨髓和胸腺除外。
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