柚皮苷及其活性代谢产物柚皮素在大鼠、犬、人类体内的药代动力学与代谢以及种属差异
Pharmacokinetics and Metabolism of Naringin and Active Metabolite Naringenin in Rats, Dogs, Humans, and the Differences Between Species.
作者信息
Bai Yang, Peng Wei, Yang Cuiping, Zou Wei, Liu Menghua, Wu Hao, Fan Loudi, Li Peibo, Zeng Xuan, Su Weiwei
机构信息
Guangdong Engineering and Technology Research Center for Quality and Efficacy Re-evaluation of Post-Marketed Traditional Chinese Medicine, School of Life Sciences, Sun Yat-sen University, Guangzhou, China.
Guangdong Key Laboratory of Plant Resources, School of Life Sciences, Sun Yat-sen University, Guangzhou, China.
出版信息
Front Pharmacol. 2020 Mar 27;11:364. doi: 10.3389/fphar.2020.00364. eCollection 2020.
BACKGROUND
Pharmacokinetics provides a scientific basis for drug product design, dosage regimen planning, understanding the body's action on the drug, and relating the time course of the drug in the body to its pharmacodynamics and/or toxic effects. Recently, naringin, a natural flavonoid, was approved for clinical trials as a first-class new drug product by the China Food and Drug Administration, owing to its nonclinical efficacy in relieving cough, reducing sputum, and low toxicity. Previous reports focused on the pharmacokinetic studies of naringin or its active metabolite naringenin in rats, which were scattered and insufficient because naringin was coadministered with mixtures such as herbs, fruits, and other traditional medicines. The purpose of this study was to evaluate the pharmacokinetics and metabolism of naringin and naringenin, following oral and intravenous administration of naringin in rats, dogs, and humans, which can be beneficial for new drug development.
METHODS
Separate bioanalytical methods were developed and validated to determine the concentrations of naringin and its active metabolite naringenin in biological samples obtained from rats, dogs, and humans. Comprehensive nonclinical and clinical data were used to estimate the pharmacokinetic parameters of naringin and naringenin. Experiments included single-dose studies (oral and intravenous administration), multiple-dose studies, and an assessment of food-effects. Furthermore, the metabolism of naringin and naringenin was studied in rat and human liver and kidney microsomes. All biological samples were analyzed using liquid chromatography-tandem mass spectrometry.
RESULTS
The pharmacokinetic parameters of naringin and naringenin were calculated and the results show an insignificant influence of high-fat diet and insignificant accumulation of the drugs after multiple dosing. Twelve metabolites were detected in the liver and kidney microsomes of rats and humans; naringin metabolism was a complex process simultaneously catalyzed by multiple human enzymes. All evaluated species demonstrated differences in the pharmacokinetics and metabolism of naringin and naringenin.
CONCLUSION
The results can be used to design a dosage regimen, deepen understanding of mechanisms, and accelerate new drug development.
CLINICAL TRIAL REGISTRATION
http://www.chinadrugtrials.org.cn/eap/main, identifiers CTR20130704 and CTR20190127.
背景
药代动力学为药物产品设计、给药方案规划、理解机体对药物的作用以及将药物在体内的时程与其药效学和/或毒性效应相关联提供了科学依据。最近,天然黄酮类化合物柚皮苷因其在止咳、祛痰方面的非临床疗效以及低毒性,被中国食品药品监督管理总局批准作为一类新药进行临床试验。以往的报道主要集中在柚皮苷或其活性代谢产物柚皮素在大鼠体内的药代动力学研究,由于柚皮苷是与草药、水果和其他传统药物等混合物共同给药,这些研究较为分散且不充分。本研究的目的是评估大鼠、犬和人类口服及静脉注射柚皮苷后柚皮苷和柚皮素的药代动力学及代谢情况,这有助于新药研发。
方法
开发并验证了单独的生物分析方法,以测定从大鼠、犬和人类获取的生物样品中柚皮苷及其活性代谢产物柚皮素的浓度。利用全面的非临床和临床数据来估算柚皮苷和柚皮素的药代动力学参数。实验包括单剂量研究(口服和静脉注射)、多剂量研究以及食物效应评估。此外,还在大鼠和人类肝、肾微粒体中研究了柚皮苷和柚皮素的代谢情况。所有生物样品均采用液相色谱 - 串联质谱法进行分析。
结果
计算了柚皮苷和柚皮素的药代动力学参数,结果表明高脂饮食对其影响不显著,多次给药后药物无明显蓄积。在大鼠和人类的肝、肾微粒体中检测到了12种代谢产物;柚皮苷的代谢是一个由多种人类酶同时催化的复杂过程。所有评估物种在柚皮苷和柚皮素的药代动力学及代谢方面均表现出差异。
结论
这些结果可用于设计给药方案、加深对作用机制的理解并加速新药研发。
临床试验注册
http://www.chinadrugtrials.org.cn/eap/main,标识符CTR20130704和CTR20190127。
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