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胺碘酮在高脂血症和模拟高脂餐大鼠模型中的药代动力学

Pharmacokinetics of Amiodarone in hyperlipidemic and simulated high fat-meal rat models.

作者信息

Shayeganpour Anooshirvan, Jun Andrew S, Brocks Dion R

机构信息

Faculty of Pharmacy and Pharmaceutical Sciences, University of Alberta, Edmonton, Alberta, Canada.

出版信息

Biopharm Drug Dispos. 2005 Sep;26(6):249-57. doi: 10.1002/bdd.457.

Abstract

The objective of this study was to examine the effect of a high fat meal and hyperlipidemia on the pharmacokinetic behavior of amiodarone. To evaluate these effects, single doses of amiodarone were administered to rats i.v. (25 mg/kg) or orally (50 mg/kg). Some rats were rendered hyperlipidemic by intraperitoneal doses of poloxamer 407 followed by amiodarone i.v. In other normolipidemic rats, amiodarone was administered i.v. in a fasted state or after the administration of 1% cholesterol in peanut oil. Amiodarone plasma concentrations were considerably (>11-fold) increased in hyperlipidemia. Substantial decreases were noted in the clearance, volume of distribution and unbound fraction (11.6, 23 and 24.7-fold, respectively) in plasma of hyperlipidemic rats. Oral lipid caused a significant increase in plasma AUC(0-infinity) (1.38-fold) and a significant decrease in clearance (1.5-fold) of amiodarone after intravenous doses. Oral consumption of 1% cholesterol in peanut oil significantly increased the plasma AUC (1.83-fold) and bioavailability of amiodarone (1.31-fold) after oral doses. In determining oral bioavailability of lipophilic drugs such as amiodarone in food effect studies, in addition to the increase in absorption of drugs, other factors such as a decrease in clearance due to increases in lipoprotein levels should be taken into account.

摘要

本研究的目的是考察高脂餐和高脂血症对胺碘酮药代动力学行为的影响。为评估这些影响,向大鼠静脉注射(25mg/kg)或口服(50mg/kg)单剂量的胺碘酮。部分大鼠通过腹腔注射泊洛沙姆407造成高脂血症,随后静脉注射胺碘酮。在其他血脂正常的大鼠中,在禁食状态下或在给予花生油中的1%胆固醇后静脉注射胺碘酮。高脂血症时胺碘酮血浆浓度显著升高(>11倍)。高脂血症大鼠血浆中的清除率、分布容积和游离分数分别大幅下降(分别为11.6、23和24.7倍)。口服脂质使静脉注射胺碘酮后的血浆AUC(0-无穷大)显著增加(1.38倍),清除率显著降低(1.5倍)。口服花生油中的1%胆固醇显著增加口服胺碘酮后的血浆AUC(1.83倍)和生物利用度(1.31倍)。在食物效应研究中确定亲脂性药物如胺碘酮的口服生物利用度时,除了药物吸收增加外,还应考虑其他因素,如脂蛋白水平升高导致清除率降低。

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