21天持续口服依托泊苷在实体瘤儿科患者中的药代动力学和药效学

Pharmacokinetics and pharmacodynamics of 21-day continuous oral etoposide in pediatric patients with solid tumors.

作者信息

Sonnichsen D S, Ribeiro R C, Luo X, Mathew P, Relling M V

机构信息

Pharmaceutical Department, St. Jude Children's Research Hospital, Memphis, TN 38105, USA.

出版信息

Clin Pharmacol Ther. 1995 Jul;58(1):99-107. doi: 10.1016/0009-9236(95)90077-2.

DOI:10.1016/0009-9236(95)90077-2

PMID:7628187

Abstract

PURPOSE

The objectives of this study were to determine etoposide pharmacokinetics during continuous low-dose oral administration to children with solid tumors and to evaluate the relationships between parameters of etoposide systemic exposure and toxicity.

PATIENTS AND METHODS

In this phase I study, children were administered oral etoposide (25 to 75 mg/m2/day) for 21 days as a diluted solution of the intravenous preparation, divided into three equal daily doses. Plasma pharmacokinetics were studied on day 1 of therapy in 18 children and again on day 21 in 14 of these children. Etoposide plasma concentration-time data were fitted to a first-order absorption, two-compartment model with use of bayesian estimation. Pharmacokinetic parameter estimates from day 1 were used to estimate steady-state etoposide systemic exposure in all children. Stepwise multivariate regression was used in an exploratory manner to determine patient, laboratory, or pharmacokinetic predictors of toxicity.

RESULTS

Although there was substantial intrapatient variability, there was no difference in the area under the concentration-time curve [AUC(0-8hr)] measured at day 21 compared with the steady-state AUC(0-8hr) estimated from day 1 pharmacokinetic parameters (p = 0.64). Degree of neutropenia was best predicted by the estimated duration that steady-state plasma etoposide concentrations were maintained above 1 microgram/ml (t > 1 microgram/ml) rather than peak plasma concentrations, AUC(0-8hr), dosage, or other patient characteristics. Assuming a bioavailability of the oral solution of approximately 50%, the median etoposide systemic clearance was 21.4 ml/min/m2, a value similar to clearance estimates after intravenous etoposide in pediatric populations.

CONCLUSION

We conclude that a parameter reflective of etoposide systemic exposure (t > 1 microgram/ml) correlates more strongly with neutropenia than does dosage or other patient characteristics.

摘要

目的

本研究的目的是确定依托泊苷在实体瘤患儿持续低剂量口服给药期间的药代动力学，并评估依托泊苷全身暴露参数与毒性之间的关系。

患者与方法

在这项I期研究中，患儿口服依托泊苷（25至75mg/m²/天），持续21天，采用静脉制剂的稀释溶液，分为每日3次等量剂量。在治疗第1天对18名患儿进行血浆药代动力学研究，其中14名患儿在第21天再次进行研究。依托泊苷血浆浓度-时间数据采用贝叶斯估计法拟合为一级吸收二室模型。第1天的药代动力学参数估计值用于估计所有患儿的依托泊苷稳态全身暴露量。采用逐步多元回归进行探索性分析，以确定毒性的患者、实验室或药代动力学预测因素。

结果

尽管患者个体差异较大，但第21天测得的浓度-时间曲线下面积[AUC(0-8hr)]与根据第1天药代动力学参数估计的稳态AUC(0-8hr)相比无差异（p = 0.64）。中性粒细胞减少的程度最好通过稳态血浆依托泊苷浓度维持在1μg/ml以上的估计持续时间（t > 1μg/ml）来预测，而不是血浆峰浓度、AUC(0-8hr)、剂量或其他患者特征。假设口服溶液的生物利用度约为50%，依托泊苷的中位全身清除率为21.4ml/min/m²，该值与儿科人群静脉注射依托泊苷后的清除率估计值相似。