Evaluation of metabolism and cytochrome P450 mediated interaction liabilities of naringenin

Mallik Samarla, Ramachandra Sangana
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Abstract

Naringenin is one of the major components of grapefruit juice. It has a broad spectrum of pharmacological activities, and many studies report that grapefruit juice inhibits cytochrome P450 (CYP) 3A4 leading to drug interactions. Naringenin was profiled through various in vitro studies like metabolic stability and glucuronidation in rat and human liver microsomes while, CYP inhibition using human liver microsomes. In addition, pharmacokinetic profiling was conducted upon intravenous (i.v.) and oral administration in rats. Naringenin undergoes both phase I and phase II metabolism in rat liver microsomes, and in human liver microsomes, it is predominantly metabolized by phase II. Glucuronidation which is addition (conjugation) of glucuronic acid to various functional groups is one of the major metabolic pathways of Naringenin. Naringenin, at 1.0 μM and 10.0 μM, did not elicit any appreciable inhibition of the 5 major CYP isoforms (CYP1A2, CYP3A4, CYP2C9, CYP2C19, and CYP2D6). Oral pharmacokinetic studies at 100, 300,and 1000 mg/kg dose and intravenous pharmacokinetic studies at 1 mg/kg dose were performed in male SD rats. Naringenin exhibited very short half-life (0.27 h) and rapid elimination (Clearance=110.65 mL/min/kg) after i.v. administration. There was saturation in Cmax and exposure beyond 100 mg/kg, and the absolute bioavailability was found to be ≤ 5% at the tested oral doses. This present experiment suggests that naringenin does not substantially inhibit CYP3A4 (or any of the tested five isoforms) isoforms per se. Given the minimal involvement of CYP enzymes in the metabolism of naringenin and minimal inhibition of CYP enzymes (IC50> 10 μM), the potential for drug-drug interactions involving CYP substrates and inhibitors is very minimal in humans.
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柚皮素代谢和细胞色素P450介导的相互作用的评价
柚皮素是葡萄柚汁的主要成分之一。它具有广泛的药理活性,许多研究报道葡萄柚汁抑制细胞色素P450 (CYP) 3A4导致药物相互作用。通过对柚皮素在大鼠和人肝微粒体中的代谢稳定性和葡萄糖醛酸化作用进行了体外研究,并利用人肝微粒体对CYP进行了抑制。此外,在大鼠静脉(i.v.)和口服给药时进行了药代动力学分析。柚皮素在大鼠肝微粒体中经历I期和II期代谢,在人肝微粒体中主要经历II期代谢。葡萄糖醛酸加(缀合)是柚皮素的主要代谢途径之一。柚皮素在1.0 μM和10.0 μM浓度下,对CYP1A2、CYP3A4、CYP2C9、CYP2C19和CYP2D6 5种主要CYP1A2、CYP3A4、CYP2D6亚型均无明显抑制作用。对雄性SD大鼠进行100mg /kg、300mg /kg和1000mg /kg剂量的口服药代动力学研究和1mg /kg剂量的静脉药代动力学研究。柚皮素的半衰期短(0.27 h),清除率(清除率=110.65 mL/min/kg)快。Cmax达到饱和,暴露量超过100 mg/kg时,绝对生物利用度≤5%。本实验表明,柚皮素本身并没有实质性地抑制CYP3A4(或任何测试的五种异构体)。鉴于CYP酶对柚皮素代谢的参与很小,并且对CYP酶的抑制很小(IC50> 10 μM),在人类中涉及CYP底物和抑制剂的药物-药物相互作用的可能性很小。
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0.00%
发文量
25
审稿时长
12 weeks
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