Poloxamer 407 诱导的大鼠高脂血症模型中达比加群的药代动力学。

IF 1.3 4区医学 Q4 PHARMACOLOGY & PHARMACY

Xenobiotica Pub Date : 2024-09-12 DOI:10.1080/00498254.2024.2404168

Ji Hyeon Kim,Eugene Baek,Hee Eun Kang

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引用次数: 0

摘要

据报道，实验性高脂血症（HL）动物模型的药代动力学发生了各种变化。为了评估 P-糖蛋白（P-gp）活性是否会影响 HL 大鼠的药代动力学，我们评估了口服达比加群酯（DABE）后达比加群的药代动力学；达比加群酯是达比加群的原药，也是众所周知的 P-gp 底物。静脉注射达比加群酯（1 毫克/千克）后，HL 大鼠和对照组大鼠表现出相似的血浆浓度-时间曲线下面积（AUC）、全身清除率（CL）和稳态分布容积（Vss）值。这表明达比加群在对照组大鼠和HL大鼠中的分布和消除情况相似。对照组大鼠和HL大鼠的肝脏和肠道P-gp蛋白水平没有显著差异。对照组大鼠和 HL 大鼠口服达比加群后的达比加群 AUC 值和绝对口服生物利用度 (F) 值相似。因此，与对照组大鼠相比，HL 大鼠肠道中的 P-gp 活性没有明显变化。高脂血症可能不会直接影响 P-gp 底物药物的口服吸收。

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The pharmacokinetics of dabigatran in a rat model of hyperlipidemia induced by poloxamer 407.

Various pharmacokinetic changes have been reported in experimental hyperlipidemic (HL) animal models. To evaluate whether P-glycoprotein (P-gp) activity was affected in HL rats, we assessed the pharmacokinetics of dabigatran after oral administration of dabigatran etexilate (DABE); this is a dabigatran prodrug and a well-known P-gp substrate.HL and control rats exhibited similar area under the plasma concentration-time curve (AUC), total body clearance (CL), and steady state volume of distribution (Vss) values following intravenous administration of dabigatran (1 mg/kg). This suggested that the distribution and elimination of dabigatran were similar in control and HL rats.The hepatic and intestinal P-gp protein levels did not differ significantly between control and HL rats. The dabigatran AUC and extent of absolute oral bioavailability (F) values were similar in control and HL rats following oral administration of DABE (10 mg/kg as dabigatran). Therefore, there was no apparent change in intestinal P-gp activity in HL rats compared to control rats.This study revealed no significant change in P-gp expression or activity in the intestine or liver of HL rats, and similar pharmacokinetics of dabigatran. Hyperlipidemia may not directly affect the oral absorption of P-gp substrate drugs.

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来源期刊

Xenobiotica 医学-毒理学

CiteScore

3.80

自引率

5.60%

发文量

审稿时长

2 months

期刊介绍： Xenobiotica covers seven main areas, including:General Xenobiochemistry, including in vitro studies concerned with the metabolism, disposition and excretion of drugs, and other xenobiotics, as well as the structure, function and regulation of associated enzymesClinical Pharmacokinetics and Metabolism, covering the pharmacokinetics and absorption, distribution, metabolism and excretion of drugs and other xenobiotics in manAnimal Pharmacokinetics and Metabolism, covering the pharmacokinetics, and absorption, distribution, metabolism and excretion of drugs and other xenobiotics in animalsPharmacogenetics, defined as the identification and functional characterisation of polymorphic genes that encode xenobiotic metabolising enzymes and transporters that may result in altered enzymatic, cellular and clinical responses to xenobioticsMolecular Toxicology, concerning the mechanisms of toxicity and the study of toxicology of xenobiotics at the molecular levelXenobiotic Transporters, concerned with all aspects of the carrier proteins involved in the movement of xenobiotics into and out of cells, and their impact on pharmacokinetic behaviour in animals and manTopics in Xenobiochemistry, in the form of reviews and commentaries are primarily intended to be a critical analysis of the issue, wherein the author offers opinions on the relevance of data or of a particular experimental approach or methodology