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通过体外过滤增强肝脏对阿霉素的摄取可避免全身给药时观察到的AUC呈剂量依赖性的非线性增加。

Augmentation of hepatic doxorubicin extraction with extracorporeal filtration avoids the dose-dependent, nonlinear increase in AUC observed with systemic administration.

作者信息

Sturgill M G, Brenner D E, August D A

机构信息

College of Pharmacy, Rutgers, The State University of New Jersey, USA.

出版信息

Cancer Chemother Pharmacol. 1998;41(3):193-200. doi: 10.1007/s002800050728.

DOI:10.1007/s002800050728
PMID:9443635
Abstract

PURPOSE

Regional therapy of primary or metastatic liver cancer with low hepatic extraction ratio drugs such as doxorubicin is constrained by development of systemic toxicity. To examine the effect of augmentation of hepatic drug extraction, a swine model of hepatic artery infusion (HAI) with minimally invasive hepatic venous isolation and hepatic venous drug extraction (HVDE) was developed to study the comparative pharmacokinetic profiles of regional and systemically administered doxorubicin.

METHODS

Doxorubicin 0.5-9 mg/kg was administered to 31 pigs over 90 min either by HAI with simultaneous HVDE or by standard systemic vein infusion. Systemic artery and hepatic vein plasma samples were collected periodically (0 to 240 min) for determination of doxorubicin concentrations by high-performance liquid chromatography. Pharmacokinetic profiles were modeled with PCNONLIN 4.2.

RESULTS

Concentration-time data were best described in all pigs by a two-compartment open model of elimination. Independent of the route of administration, AUC and Cmax values increased with dose. Mean systemic AUC and Cmax values were consistently lower with regional administration, with statistically significant decreases at the 0.5 and 3 mg/kg doses, whereas there was no relationship between hepatic vein parameters and route of administration. There was a linear relationship between mean systemic AUC values and dose in pigs receiving doxorubicin via HAI with HVDE, whereas mean systemic AUC values increased exponentially at doses of 5 mg/kg or above with systemic vein administration.

CONCLUSIONS

Administration of doxorubicin by HAI with simultaneous HVDE significantly decreases systemic exposure in comparison with standard systemic vein drug infusion, and may protect against nonlinear increases in exposure at higher doses.

摘要

目的

原发性或转移性肝癌的区域治疗采用低肝摄取率药物(如阿霉素)时,会受到全身毒性的限制。为了研究增强肝脏药物摄取的效果,建立了一种猪的肝动脉灌注(HAI)模型,采用微创肝静脉隔离和肝静脉药物提取(HVDE),以研究区域给药和全身给药阿霉素的比较药代动力学特征。

方法

将0.5 - 9mg/kg的阿霉素在90分钟内通过HAI联合HVDE或标准全身静脉输注给予31头猪。定期(0至240分钟)采集全身动脉和肝静脉血浆样本,通过高效液相色谱法测定阿霉素浓度。用药代动力学软件PCNONLIN 4.2对药代动力学特征进行建模。

结果

所有猪的浓度 - 时间数据均用二室开放消除模型进行最佳描述。与给药途径无关,AUC和Cmax值随剂量增加。区域给药时,全身AUC和Cmax的平均值始终较低,在0.5mg/kg和3mg/kg剂量时统计学上有显著降低,而肝静脉参数与给药途径之间无相关性。在接受HAI联合HVDE给予阿霉素的猪中,全身AUC平均值与剂量呈线性关系,而全身静脉给药时,剂量为5mg/kg或以上时全身AUC平均值呈指数增加。

结论

与标准全身静脉药物输注相比,HAI联合HVDE给予阿霉素可显著降低全身暴露,并可能防止高剂量时暴露的非线性增加。

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Augmentation of hepatic doxorubicin extraction with extracorporeal filtration avoids the dose-dependent, nonlinear increase in AUC observed with systemic administration.通过体外过滤增强肝脏对阿霉素的摄取可避免全身给药时观察到的AUC呈剂量依赖性的非线性增加。
Cancer Chemother Pharmacol. 1998;41(3):193-200. doi: 10.1007/s002800050728.
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