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伊立替康(CPT-11)的肠肝循环模型及胶质瘤患者体内代谢物的药代动力学

Enterohepatic recirculation model of irinotecan (CPT-11) and metabolite pharmacokinetics in patients with glioma.

作者信息

Younis Islam R, Malone Samuel, Friedman Henry S, Schaaf Larry J, Petros William P

机构信息

Department of Basic Pharmaceutical Sciences and Mary Babb Randolph Cancer Center, West Virginia University Health Sciences Center, Morgantown, WV 26506, USA.

出版信息

Cancer Chemother Pharmacol. 2009 Feb;63(3):517-24. doi: 10.1007/s00280-008-0769-8. Epub 2008 May 22.

DOI:10.1007/s00280-008-0769-8
PMID:18496691
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3914774/
Abstract

BACKGROUND

Enterohepatic recirculation of irinotecan and one of its metabolites, SN-38, has been observed in pharmacokinetic data sets from previous studies. A mathematical model that can incorporate this phenomenon was developed to describe the pharmacokinetics of irinotecan and its metabolites.

PATIENTS AND METHODS

A total of 32 patients with recurrent malignant glioma were treated with weekly intravenous administration of irinotecan at a dose of 125 mg/m(2). Plasma concentrations of irinotecan and its three major metabolites were determined. Pharmacokinetic models were developed and tested for simultaneous fit of parent drug and metabolites, including a recirculation component.

RESULTS

Rebound in the plasma concentration suggestive of enterohepatic recirculation at approximately 0.5-1 h post-infusion was observed in most irinotecan plasma concentration profiles, and in some plasma profiles of the SN-38 metabolite. A multi-compartment model containing a recirculation chain was developed to describe this process. The recirculation model was optimal in 22 of the 32 patients compared to the traditional model without the recirculation component.

CONCLUSION

A recirculation chain incorporated in a multi-compartment pharmacokinetic model of irinotecan and its metabolites appears to improve characterization of this drug's disposition in patients with glioma.

摘要

背景

在既往研究的药代动力学数据集中已观察到伊立替康及其代谢产物之一SN - 38的肠肝循环。开发了一种能够纳入该现象的数学模型,以描述伊立替康及其代谢产物的药代动力学。

患者与方法

总共32例复发性恶性胶质瘤患者接受每周一次静脉注射伊立替康治疗,剂量为125 mg/m²。测定伊立替康及其三种主要代谢产物的血浆浓度。开发并测试了药代动力学模型,以同时拟合母体药物和代谢产物,包括一个再循环成分。

结果

在大多数伊立替康血浆浓度曲线以及某些SN - 38代谢产物的血浆曲线中,观察到输注后约0.5 - 1小时出现提示肠肝循环的血浆浓度反弹。开发了一个包含再循环链的多室模型来描述这一过程。与没有再循环成分的传统模型相比,再循环模型在32例患者中的22例中表现最佳。

结论

纳入伊立替康及其代谢产物多室药代动力学模型中的再循环链似乎改善了该药物在胶质瘤患者体内处置情况的表征。

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