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首页> 外文期刊>Planta medica: Natural products and medicinal plant research >In Vitro Metabolic Stability and Permeability of Gymnemagenin and Its In Vivo Pharmacokinetic Correlation in Rats - A Pilot Study
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In Vitro Metabolic Stability and Permeability of Gymnemagenin and Its In Vivo Pharmacokinetic Correlation in Rats - A Pilot Study

机译:Gymnemagenin在大鼠体内的体外代谢稳定性和通透性及其体内药代动力学相关性的初步研究

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摘要

Gymnema sylvestre is traditionally used for diabetes mellitus. A literature survey revealed very few reports, particularly on rat liver microsomal stability, caco-2 permeability and efflux concerns and its correlation with the bioavailability of gymnemagenin, an important component of G. sylvestre. Therefore, the objective of our study was to investigate the in vitro rat liver microsomal stability and caco-2 permeability along with the efflux of gymnemagenin and establish a probable correlation of these in vitro findings with pharmacokinetic parameters after oral and intravenous administration in rats. Rat liver microsomal stability studies to estimate the in vitro intrinsic half-life, clearance, and Caco-2 permeability after 21 days of culture to determine the apparent permeability from apical to basal and from basal to apical, and efflux ratio of gymnemagenin were performed using liquid chromatography-tandem mass spectrometry. A sensitive, robust bioanalytical method was validated and successfully applied to determine the plasma exposure of gymnemagenin. In vitro rat liver microsomal stability demonstrated that gymnemagenin metabolizes rapidly with a short apparent and intrinsic half-life (similar to 7min) and high intrinsic clearance, i.e., 190.08 mu L/min/mg of microsomes. The results of the Caco-2 study indicated a poor permeability (1.31x10(-6)cm/sec) with a very high efflux ratio. The pharmacokinetic study revealed poor oral bioavailability (similar to 14%) of gymnemagenin and it was found to have a short half-life and a high clearance in rats. Our in vitro findings indicated low metabolic stability and poor Caco-2 permeability with high efflux, which might have a role in the observed poor oral bioavailability in rats.
机译:匙藤传统上用于糖尿病。文献调查显示很少有报道,特别是关于大鼠肝微粒体稳定性,caco-2通透性和外排问题及其与匙ne藤碱(,草的重要组成部分)生物利用度的相关性。因此,我们的研究目的是研究大鼠裸鼠体内的微粒体稳定性和caco-2的通透性以及裸心菌素的外排作用,并确定这些口服的发现与大鼠口服和静脉内给药后的药代动力学参数之间可能的相关性。使用大鼠肝微粒体稳定性研究来评估培养21天后的体外固有半衰期,清除率和Caco-2渗透性,从而确定从根尖到基底以及从基尖到根尖的表观渗透性,以及使用Gymnemagenin的流出比液相色谱-串联质谱。灵敏,稳健的生物分析方法已经过验证,并成功应用于确定裸心菌素的血浆暴露。体外大鼠肝脏微粒体稳定性表明,裸子草碱素代谢迅速,具有短的表观和固有半衰期(类似于7分钟)和高固有清除率,即190.08μL / min / mg的微粒体。 Caco-2研究的结果表明,渗透率很低(1.31x10(-6)cm / sec),具有很高的流出率。药代动力学研究表明,裸心精原的口服生物利用度较差(接近14%),并且发现半衰期短,大鼠清除率高。我们的体外研究结果表明,新陈代谢的稳定性较低,Caco-2的通透性较差,但流出量较高,这可能与观察到的大鼠口服生物利用度差有关。

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