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动脉内顺二氨二氯铂(II)的临床药理学

Clinical pharmacology of intraarterial cis-diamminedichloroplatinum(II).

作者信息

Stewart D J, Benjamin R S, Zimmerman S, Caprioli R M, Wallace S, Chuang V, Calvo D, Samuels M, Bonura J, Loo T L

出版信息

Cancer Res. 1983 Feb;43(2):917-20.

PMID:6681533
Abstract

After intraarterial (30 patients) or i.v. (seven patients) administration of cis-diamminedichloroplatinum, X-ray fluorescence spectrometry was used to measure platinum concentrations in plasma and urine. Arteries infused included hepatic (seven patients), carotid (six patients), iliac (ten patients), brachial (three patients), and femoral (four patients). All patients received i.v. mannitol. Pharmacokinetic parameters after intraarterial administration were similar to those after i.v. administration, although differences existed for different intraarterial routes of administration. Mean for all patients combined were: Co, 2.67 +/- 0.97 (S.D.) microgram/ml; t1/2 beta, 71.1 +/- 26.6 hr; clearance, 0.72 +/- 0.25 liters/hr/sq m; total volume of distribution, 45.2 +/- 17.0 liters/sq m; C x t, 167 +/- 72 mg/hr/liter; and 24-hr urinary excretion, 20 +/- 10% of the administered dose. Intrahepatic infusion of the drug was associated with a significantly lower Co (1.88 +/- 0.50 g/ml) and C x t (140 +/- 25 mg hr/liter) and significantly higher clearance (0.91 +/- 0.24 liters/hr/sq m) and volume of distribution (67.6 +/- 4.6 liters/sq m) than administration by other routes, suggesting first pass extraction of drug by liver. In addition, an apparent minor late rise in serum platinum concentration may suggest enterohepatic recirculation of drug. High fluid intake was associated with a low Co and a high volume of distribution, consistent with expansion of the central compartment by fluids. Low serum albumin (less than 3.5 g/dl) was associated with significant shortening of the t1/2 beta (50.5 +/- 21.6 hr), suggesting that the amount of unbound filterable drug may possibly be higher in patients with low serum albumin concentrations. Plasma from veins draining an infused area has a higher Co and C x t during infusion than concurrent plasma from peripheral veins. Thus, intraarterial administration of cis-diamminedichloroplatinum results in increased drug exposure of tumor in the infused area without substantially decreasing exposure of systemic tumor.

摘要

在经动脉(30例患者)或静脉(7例患者)给予顺二氨二氯铂后,采用X射线荧光光谱法测定血浆和尿液中的铂浓度。输注的动脉包括肝动脉(7例患者)、颈动脉(6例患者)、髂动脉(10例患者)、肱动脉(3例患者)和股动脉(4例患者)。所有患者均接受静脉注射甘露醇。动脉内给药后的药代动力学参数与静脉给药后的相似,尽管不同动脉内给药途径存在差异。所有患者合并后的平均值为:初始浓度(Co),2.67±0.97(标准差)微克/毫升;β半衰期(t1/2β),71.1±26.6小时;清除率,0.72±0.25升/小时/平方米;分布总体积,45.2±17.0升/平方米;浓度-时间曲线下面积(C×t),167±72毫克/小时/升;24小时尿排泄量,占给药剂量的20±10%。与其他给药途径相比,肝内输注该药物时Co(1.88±0.50微克/毫升)和C×t(140±25毫克·小时/升)显著降低,清除率(0.91±0.24升/小时/平方米)和分布体积(67.6±4.6升/平方米)显著升高,提示肝脏对药物的首过提取作用。此外,血清铂浓度明显的轻微后期升高可能提示药物的肠肝循环。高液体摄入量与低Co和高分布体积相关,这与液体使中央室扩张一致。低血清白蛋白(低于3.5克/分升)与t1/2β显著缩短(50.5±21.6小时)相关,提示血清白蛋白浓度低的患者中未结合的可滤过药物量可能更高。在输注过程中,来自输注区域引流静脉的血浆中的Co和C×t高于同期外周静脉血浆。因此,经动脉给予顺二氨二氯铂可增加输注区域肿瘤的药物暴露,而不会显著降低全身肿瘤的暴露。

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