卡铂
非金属
医学
药代动力学
加药
治疗药物监测
人口
肿瘤科
生殖细胞肿瘤
药理学
化疗
泌尿科
内科学
临床研究阶段
毒性
药品
多中心研究
分布(数学)
协变量
体表面积
外科
癌症
回顾性队列研究
曲线下面积
顺铂
卵巢癌
人口研究
作者
Sotheara Moeung,Christine Chevreau,Sophie Broutin,Jérôme Guitton,Bénédicte Lelièvre,Joseph Ciccolini,Christophe Massart,Aude Fléchon,R. Delva,Gwénaëlle Gravis,Jean‐Pierre Lotz,Jacques‐Olivier Bay,Marine Gross‐Goupil,Angélo Paci,Sabrina Marsili,Laurence Malard,Étienne Chatelut,Fabienne Thomas
标识
DOI:10.1158/1078-0432.ccr-17-1344
摘要
Abstract Purpose: We aimed to evaluate the performance of therapeutic drug monitoring (TDM) approach in controlling interpatient variability of carboplatin exposure (AUC) in patients treated with TI-CE high-dose chemotherapy for advanced germ cell tumors and to assess the possibility of using a formula-based dosing method as a possible alternative. Experimental Design: Eighty-nine patients receiving carboplatin for 3 consecutive days during 3 cycles were evaluable for pharmacokinetic study. Blood samples were taken on day 1 to determine the carboplatin clearance using a Bayesian approach (NONMEM 7.2) and to adjust the dose on day 3 to reach the target AUC of 24 mg.min/mL over 3 days. On days 2 and 3, samples were taken for retrospective assessment of the actual AUC. A population pharmacokinetic analysis was also performed on 58 patients using NONMEM to develop a covariate equation for carboplatin clearance prediction adapted for future TI-CE patients, and its performance was prospectively evaluated on the other 29 patients along with different methods of carboplatin clearance prediction. Results: The mean actual AUC was 24.4 mg.min/mL per cycle (22.4 and 26.8 for 10th and 90th percentiles, respectively). The new covariate equation [CL (mL/min) = 130.7 × (Scr/83)−0.826 × (BW/76)+0.907 × (Age/36)−0.223 with Scr in μmol/L, BW in kilograms, age in years] allows unbiased and more accurate prediction of carboplatin clearance compared with other equations. Conclusions: TDM allows controlling and reaching the target AUC. Alternatively, the new equation of carboplatin clearance prediction, better adapted to these young male patients, could be used if TDM cannot be implemented. Clin Cancer Res; 23(23); 7171–9. ©2017 AACR.
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