柑橘类黄酮苷元橙皮素和柚皮素在人体单次口服给药后的药代动力学。

Pharmacokinetics of the citrus flavanone aglycones hesperetin and naringenin after single oral administration in human subjects.

作者信息

Kanaze F I, Bounartzi M I, Georgarakis M, Niopas I

机构信息

Department of Pharmacy, Aristotle University of Thessaloniki, Thessaloniki, Greece.

出版信息

Eur J Clin Nutr. 2007 Apr;61(4):472-7. doi: 10.1038/sj.ejcn.1602543. Epub 2006 Oct 18.

DOI:10.1038/sj.ejcn.1602543

PMID:17047689

Abstract

BACKGROUND AND OBJECTIVE

Hesperetin and naringenin, the aglycones of the flavanone glycosides hesperidin and naringin, occur naturally in citrus fruits. They exert interesting pharmacological properties such as antioxidant, anti-inflammatory, blood lipid and cholesterol lowering and are considered to contribute to health benefits in humans. However, no information is available on the pharmacokinetics of the citrus flavanones hesperetin and naringenin after their oral administration to humans as pure aglycones. Therefore, the objective of the present investigation was the evaluation of the pharmacokinetic parameters of hesperetin and naringenin in plasma and urine, after their single oral administration in humans in the form of solid dispersion capsules, and also to improve the absorption rate of flavanones by using aglycones rather than the naturally occurring glycosides.

DESIGN

Six healthy volunteers received orally 135 mg of each compound, hesperetin and naringenin, under fasting conditions. Blood samples were collected at 14 different time points over a 12 h period. Urine was collected over 24 h, in five sequential timed intervals. Plasma and urine hesperetin and naringenin concentrations, after enzymatic hydrolysis of their conjugated forms, were measured using validated high-pressure liquid chromatography methods. Pharmacokinetic parameters for hesperetin and naringenin, such as C(max), T(max), AUC(0-t), AUC(0-infinity), CL/F, V/F, t(1/2), MRT, A(e), A(e)((0-24)), and R(max) were calculated from their plasma or urine concentrations.

RESULTS

Pharmacokinetic analysis showed that both hesperetin and naringenin were rapidly absorbed and their concentrations in plasma observed 20 min after dosing and reached a peak in 4.0 and 3.5 h, respectively. The mean peak plasma concentration (C(max)) for hesperetin and naringenin were 825.78+/-410.63 ng/ml (2731.8+/-1358.4 nmol/l) and 2009.51+/-770.82 ng/ml (7386.6+/-2833.4 nmol/l), respectively and the mean AUC(0-infinity) values were 4846.20+/-1675.99 ng h/ml and 9424.52+/-2960.52 ng h/ml for hesperetin and naringenin, respectively. The elimination half-life for hesperetin was found to be 3.05+/-0.91 h and for naringenin 2.31+/-0.40 h, respectively. The mean values of the relative cumulative urinary excretion, as percentage of the administered dose, for hesperetin and naringenin, were found to be 3.26+/-0.44 and 5.81+/-0.81%, respectively.

CONCLUSIONS

Oral administration of the flavanone aglycones, hesperetin and naringenin, lead to their rapid absorption as their conjugated forms. The cumulative urinary recovery data indicated low bioavailability for both flavanone aglycones, owing to extensive first-pass metabolism partly by cleavage of the C-ring by the enzymes of intestinal bacteria leading to degradation products such as phenolic acids.

摘要

背景与目的

橙皮素和柚皮素是黄酮糖苷类化合物橙皮苷和柚皮苷的苷元，天然存在于柑橘类水果中。它们具有抗氧化、抗炎、降血脂和胆固醇等有趣的药理特性，被认为对人类健康有益。然而，关于橙皮素和柚皮素作为纯苷元口服给药后在人体内的药代动力学信息尚无报道。因此，本研究的目的是评估橙皮素和柚皮素以固体分散体胶囊形式单次口服给药后在血浆和尿液中的药代动力学参数，并通过使用苷元而非天然存在的糖苷来提高黄酮类化合物的吸收率。

设计

6名健康志愿者在禁食条件下口服135mg的每种化合物，即橙皮素和柚皮素。在12小时内的14个不同时间点采集血样。在24小时内按五个连续的定时间隔收集尿液。使用经过验证的高压液相色谱法测定血浆和尿液中经酶水解其结合形式后的橙皮素和柚皮素浓度。根据血浆或尿液浓度计算橙皮素和柚皮素的药代动力学参数，如C(max)、T(max)、AUC(0-t)、AUC(0-∞)、CL/F、V/F、t(1/2)、MRT、A(e)、A(e)(0-24)和R(max)。

结果

药代动力学分析表明，橙皮素和柚皮素均迅速吸收，给药后20分钟在血浆中观察到其浓度，并分别在4.0小时和3.5小时达到峰值。橙皮素和柚皮素的平均血浆峰值浓度（C(max)）分别为825.78±410.63ng/ml（2731.8±1358.4nmol/l）和2009.51±770.82ng/ml（7386.6±2833.4nmol/l），橙皮素和柚皮素的平均AUC(0-∞)值分别为4846.20±1675.99ng h/ml和9424.52±2960.52ng h/ml。发现橙皮素的消除半衰期为3.05±0.91小时，柚皮素为2.31±0.40小时。橙皮素和柚皮素的相对累积尿排泄量占给药剂量的百分比的平均值分别为3.26±0.44和5.81±0.81%。