硫替派降低环磷酰胺的生物活化作用：高剂量化疗方案中的关键序列依赖性

Reduction of cyclophosphamide bioactivation by thioTEPA: critical sequence-dependency in high-dose chemotherapy regimens.

作者信息

Huitema A D, Kerbusch T, Tibben M M, Rodenhuis S, Beijnen J H

机构信息

Department of Pharmacy and Pharmacology, The Netherlands Cancer Institute/Slotervaart Hospital, Amsterdam.

出版信息

Cancer Chemother Pharmacol. 2000;46(2):119-27. doi: 10.1007/s002800000132.

DOI:10.1007/s002800000132

PMID:10972481

Abstract

PURPOSE

Cyclophosphamide and thioTEPA are frequently used simultaneously in high-dose chemotherapy regimens. During a pharmacokinetic study of 31 courses in 20 patients of cyclophosphamide and its activated metabolite 4-hydroxycyclophosphamide given in the combination cyclophosphamide thioTEPA carboplatin, a sharp decrease in 4-hydroxycyclophosphamide concentration was observed immediately after the start of the thioTEPA infusion. A drug-drug interaction was suspected. This putative interaction was investigated in this study.

METHODS

Possible sequence dependency, due to inhibition of the formation of 4-hydroxycyclophosphamide by thioTEPA, was investigated by altering the sequence of infusion in three patients (four courses) receiving high-dose chemotherapy with cyclophosphamide (1,000 or 1,500 mg/m2 per day), thioTEPA (80 or 120 mg/m2 per day) and carboplatin (265 or 400 mg/m2 per day) in short infusions for four consecutive days. The pharmacokinetics of cyclophosphamide and 4-hydroxycyclophosphamide were established. Possible inhibition of the metabolism of cyclophosphamide and thioTEPA was investigated in human microsomes.

RESULTS

A striking sequence dependency of the pharmacokinetics of 4-hydroxycyclophosphamide was observed. Administration of thioTEPA 1 h prior to cyclophosphamide resulted in decreased Cmax (-62%) and AUC (-26%) values of 4-hydroxycyclophosphamide compared to those of thioTEPA administered 1 h after cyclophosphamide. In human microsomes an inhibition of the conversion of cyclophosphamide to 4-hydroxycyclophosphamide by thioTEPA was observed at clinically relevant concentrations with an IC50 of 23 microM. No inhibition of the formation of TEPA by cyclophosphamide was observed.

CONCLUSIONS

ThioTEPA strongly inhibits the bioactivation of cyclophosphamide and this may decrease both efficacy and toxicity. Our results seriously question the practice of the simultaneous continuous infusion of cyclophosphamide and thioTEPA and suggest that the sequencing and scheduling of these two agents in high-dose chemotherapy regimens may be of critical importance.

摘要

目的

环磷酰胺和塞替派在高剂量化疗方案中经常同时使用。在一项对20名患者进行的31个疗程的药代动力学研究中，给予环磷酰胺、塞替派和卡铂联合用药，观察到在塞替派输注开始后，4-羟基环磷酰胺浓度立即急剧下降。怀疑存在药物相互作用。本研究对这种假定的相互作用进行了调查。

方法

通过改变三名接受高剂量化疗的患者（四个疗程）的输注顺序，研究塞替派对4-羟基环磷酰胺形成的抑制作用可能导致的序列依赖性。这三名患者连续四天接受短期输注，药物包括环磷酰胺（每天1000或1500mg/m²）、塞替派（每天80或120mg/m²）和卡铂（每天265或400mg/m²）。确定了环磷酰胺和4-羟基环磷酰胺的药代动力学。在人微粒体中研究了环磷酰胺和塞替派代谢可能受到的抑制作用。

结果

观察到4-羟基环磷酰胺药代动力学存在显著的序列依赖性。与环磷酰胺后1小时给予塞替派相比，塞替派在环磷酰胺前1小时给予导致4-羟基环磷酰胺的Cmax（-62%）和AUC（-26%）值降低。在人微粒体中，在临床相关浓度下观察到塞替派对环磷酰胺向4-羟基环磷酰胺转化的抑制作用，IC50为23μM。未观察到环磷酰胺对塞替派形成的抑制作用。