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在大鼠体内米托蒽醌的药代动力学和胆汁排泄。

Pharmacokinetics and biliary excretion of mitoxantrone in rats.

机构信息

Department of Pharmaceutical Sciences, School of Pharmacy and Pharmaceutical Sciences, University at Buffalo, State University of New York, Amherst, New York 14260-1200, USA.

出版信息

J Pharm Sci. 2010 May;99(5):2502-10. doi: 10.1002/jps.22011.

Abstract

The objective of this investigation was to compare the observed biliary clearance (CL(b)) and % of dose excreted in the bile (PD(b)) of mitoxantrone with the predicted values obtained from quantitative structure pharmacokinetic relationship (QSPKR) models. Blood and bile samples were collected from bile duct cannulated rats after an intravenous bolus dose of 0.5 or 2 mg/kg mitoxantrone, and the concentrations were measured by HPLC. Mitoxantrone plasma concentrations exhibited a tri-exponential profile with systemic clearance of 118 +/- 6.8 mL/min/kg. After dosing, 6.08 +/- 2.32% and 5.69 +/- 0.59% of the dose were excreted into bile in unchanged form after a 3-h collection. CL(b) was 7.20 +/- 4.54 and 7.46 +/- 0.62 mL/min/kg after the two doses. With the co-administration of 10 mg/kg GF-120918, a P-glycoprotein and BCRP inhibitor, PD(b) was reduced to 0.69 +/- 0.07%, suggesting that BCRP or P-glycoprotein may play an important role in the biliary elimination of mitoxantrone. Using QSPKR models developed for the biliary excretion of cations/neutral compounds in rats, CL(b) and PD(b) of mitoxantrone were predicted as 5.18 mL/min/kg and 7.21%, respectively, suggesting that the models could be used to predict the biliary excretion of mitoxantrone.

摘要

本研究旨在比较米托蒽醌的实际胆汁清除率(CL(b))和胆汁排泄率(PD(b))与定量构效关系(QSPKR)模型预测值。在胆管插管大鼠静脉推注 0.5 或 2mg/kg 米托蒽醌后,采集血样和胆汁样本,并用 HPLC 法测定浓度。米托蒽醌的血浆浓度呈三指数廓清特征,全身清除率为 118±6.8mL/min/kg。在 3 小时的采集时间内,原形药物 6.08±2.32%和 5.69±0.59%的剂量从胆汁中排泄。两个剂量的胆汁清除率分别为 7.20±4.54 和 7.46±0.62mL/min/kg。当给予 10mg/kg 的 GF-120918(一种 P-糖蛋白和 BCRP 抑制剂)时,PD(b)降低至 0.69±0.07%,表明 BCRP 或 P-糖蛋白可能在米托蒽醌的胆汁消除中发挥重要作用。使用大鼠胆汁排泄阳离子/中性化合物的 QSPKR 模型,预测米托蒽醌的 CL(b)和 PD(b)分别为 5.18mL/min/kg 和 7.21%,表明该模型可用于预测米托蒽醌的胆汁排泄。

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