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多周期大剂量卡铂随后进行外周血干细胞输注的癌症患者的Ⅰ期药代动力学研究

Phase I pharmacokinetic study of multicycle high-dose carboplatin followed by peripheral-blood stem-cell infusion in patients with cancer.

作者信息

Johansen M J, Madden T, Mehra R C, Wood J G, Rondon G, Browne V, Newman R A, Champlin R E

机构信息

Department of Pharmacy, University of Texas M.D. Anderson Cancer Center, Houston, USA.

出版信息

J Clin Oncol. 1997 Apr;15(4):1481-91. doi: 10.1200/JCO.1997.15.4.1481.

Abstract

PURPOSE

To examine the feasibility of escalating carboplatin area under the concentration-time curve (AUC), using dose predictions based on individual estimates of drug clearance, in a phase I trial of multicycle carboplatin, paclitaxel, and cyclophosphamide chemotherapy with peripheral-blood stem-cell (PBSC) replacement.

PATIENTS AND METHODS

Forty-four patients (37 breast, seven ovarian) received 165 courses. Initial target carboplatin AUC was 10 mg/ml x min, with interpatient escalation in increments of 25%. Initial carboplatin dose estimates used creatinine clearance (CrCl) to estimate carboplatin clearance. Subsequent clearance and dose estimates were determined using a model incorporating Bayesian estimation and two measured carboplatin plasma ultrafiltrate concentrations.

RESULTS

Median clearance was 80.5 mL/min/m2 (range, 41.6 to 131.8). Carboplatin doses up to 2,440 mg/m2 per course were administered without major extramedullary toxicity. Doses varied 2.6-fold at each exposure level. Using the Bayesian model, AUC was predicted with a mean accuracy of 101.2% (83% using CrCl). Ninety-six of 117 courses were within 25% of the target AUC. This model was less biased (0.15 v -2.35 mg/mL x min) and more precise (2.76 v 3.52) in predicting AUC compared with one using CrCl. Hematologic recovery was not prolonged with increasing exposure. The carboplatin maximum-tolerated systemic exposure (MTSE) was 13.3 mg/mL x min (level five). The dose-limiting toxicity was cardiac toxicity, which occurred at dose levels six and seven.

CONCLUSION

Results demonstrate that (1) CrCl is a poor estimator of carboplatin clearance in this population, and (2) the use of a model incorporating limited sampling and Bayesian estimation improves the precision of carboplatin clearance estimation and is suitable for targeting carboplatin exposure in an ambulatory setting.

摘要

目的

在一项采用外周血干细胞(PBSC)置换的多周期卡铂、紫杉醇和环磷酰胺化疗的I期试验中,研究根据药物清除率的个体估计值进行剂量预测来提高卡铂浓度-时间曲线下面积(AUC)的可行性。

患者和方法

44例患者(37例乳腺癌,7例卵巢癌)接受了165个疗程的治疗。初始目标卡铂AUC为10mg/ml×min,患者间以25%的增量递增。初始卡铂剂量估计采用肌酐清除率(CrCl)来估计卡铂清除率。随后的清除率和剂量估计通过一个结合贝叶斯估计和两次测量的卡铂血浆超滤浓度的模型来确定。

结果

中位清除率为80.5mL/min/m²(范围41.6至131.8)。每个疗程给予高达2440mg/m²的卡铂剂量,无严重髓外毒性。在每个暴露水平下,剂量变化2.6倍。使用贝叶斯模型预测AUC的平均准确率为101.2%(使用CrCl时为83%)。117个疗程中有96个在目标AUC的25%范围内。与使用CrCl的模型相比,该模型在预测AUC时偏差较小(0.15对-2.35mg/mL×min)且更精确(2.76对3.52)。随着暴露增加,血液学恢复未延长。卡铂的最大耐受全身暴露(MTSE)为13.3mg/mL×min(五级)。剂量限制性毒性为心脏毒性,发生在六级和七级剂量水平。

结论

结果表明,(1)CrCl在此人群中是卡铂清除率的较差估计指标,(2)使用结合有限采样和贝叶斯估计的模型可提高卡铂清除率估计的精度,适用于在门诊环境中靶向卡铂暴露。

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