肝肠首过效应对五味子醇甲在大鼠体内生物利用度的影响

李宁; 沈璐; 牛丽君; 李卓; 邱志霞; 张德文

doi:10.14148/j.issn.1672-0482.2022.0228

肝肠首过效应对五味子醇甲在大鼠体内生物利用度的影响

Impact of Hepatic-Intestinal First-Pass Effect on the Bioavailability of Schizandrin in Rats

摘要

摘要:
目的以整体动物和肝肠首过代谢动物模型, 考察五味子主要活性成分五味子醇甲在体内外的处置过程, 探讨五味子醇甲低生物利用度的原因, 为五味子的现代化开发提供必要的数据支撑。
方法首先研究不同剂量的五味子醇甲在整体动物(大鼠)体内的药动学过程; 其后借助颈静脉和幽门静脉插管的首过代谢模型, 研究肝脏、肠道在五味子醇甲体内转化过程中的作用以及对其生物利用度的影响。
结果在清醒大鼠体内, 分别灌胃(i.g)给予10、20、50 mg · kg^-1五味子醇甲后, 五味子醇甲表现为吸收快(T_max, 0.37、0.44、0.33 h)、体内平均停留时间短(MRT_last, 1.74、1.65、1.27 h)、生物利用度较低(F, 12.0%, 11.0%, 9.35%)的药动学特性; 经i.g和十二指肠穿刺(i.d)给予20 mg · kg^-1五味子醇甲的血药浓度-时间曲线下面积相近(AUC_{0-4 h}，467.98 h · ng · mL^-1 vs 469.03 h · ng · mL^-1), 说明胃部首过效应对其生物利用度影响较小胃利用度(F_G)接近100%; 经i.d给予20 mg · kg^-1五味子醇甲后, 幽门静脉血中五味子醇甲的暴露量显著高于颈静脉中的暴露量(1 648.08 h · ng · mL^-1 vs 469.03 h · ng · mL^-1, P < 0.05), 以此估算肠道发生代谢的部分为78.47%;幽门静脉注射(i.p.v)给药后经颈静脉采血，五味子醇甲的系统暴露量低于静脉注射(i.v)给药后经颈静脉采血的系统暴露量(1 960.22 h · ng · mL^-1 vs 2 547.79 h · ng · mL^-1), 以此估算五味子醇甲摄取入肝脏发生代谢的部分为23.06%;综合肝脏利用度(F_h, 76.94%=1-23.06%)、肠道利用度(F_a × F_g, 21.53%=1-78.47%), 估算五味子醇甲的绝对生物利用度(F_t)为16.57%, 与i.g给药经颈静脉采血后计算的生物利用度(18.33%)接近; 在体外肝、肠微粒体体系中, 五味子醇甲发生明显的NADPH依赖的代谢。
结论肝肠首过代谢在很大程度上影响五味子醇甲的生物利用度, 而肠道代谢对五味子醇甲的首过代谢贡献程度更大, 对其绝对生物利用度的影响更大。

Abstract:
OBJECTIVES The pharmacokinetic analysis of schizandrin in rats were performed to investigate the potential impact of intestinal-hepatic first-pass effect on the low bioavailability of schizandrin from Schizandra sinensis Baill.
METHODS Firstly, the pharmacokinetic assay was carried out in rats following intravenous (i.v) or intragastric (i.g) administration at different dose levels (10, 20, 50 mg · kg^-1). Secondly, the jugular vein or pyloric vein cannulated rats model was established to study the specific role of intestine and liver on the schizandrin.
RESULTS Schizandrin was rapidly absorbed (T_max, 0.37, 0.44, 0.33 h), quickly eliminated with short mean resident time (MRT_last, 1.74, 1.65, 1.27 h) and low bioavailability (12.0%, 11.0%, 9.35%) in conscious rats treated with i.g administration 10, 20, 50 mg · kg^-1 of schizandrin. The systemic exposure to schizandrin was comparable (AUC_0-t, 467.98 vs 469.03 h · ng · mL^-1) after i.g or intraduodenal (i.d) puncture administration at 20 mg · kg^-1. This indicated the gastric effect to the metabolism of schizandrin was minor. Following i.d administration of schizandrin at 20 mg · kg^-1, the pre-systemic exposure to schizandrin in pyloric vein was higher than that in jugular vein (AUC_0-t, 1 648.08 vs 469.03 h · ng · mL^-1). The calculated intestinal metabolism was estimated at 78.47%; After intravenous administration via portal vein at 10 mg · kg^-1, the systemic exposure in jugular vein was a bit lower than that following intravenous via jugular vein at identical dose (AUC_0-t, 1 960.22 vs 2 547.79 h · ng · mL^-1), indicating the hepatic metabolism occupied 23.06%. Comprehensive consideration of intestinal (F_a × F_g, 21.53%) and hepatic (F_h, 76.94%) availability, the total bioavailability was estimated as 16.57% in cannulated rats, which was close to the value (18.33%) calculated from the i.g and i.v administration in anaesthetic rats. In the intestinal and hepatic microsomes incubation system, schizandrin was extensively degraded in the presence of NADPH.
CONCLUSIONS The intestinal-hepatic first-pass effect largely determines the bioavailability of schizandrin, while the intestine contributes in a larger extent.

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