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首页> 外文期刊>Journal of Analytical Methods in Chemistry >Metabolite Profiling, Pharmacokinetics, and In Vitro Glucuronidation of Icaritin in Rats by Ultra-Performance Liquid Chromatography Coupled with Mass Spectrometry
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Metabolite Profiling, Pharmacokinetics, and In Vitro Glucuronidation of Icaritin in Rats by Ultra-Performance Liquid Chromatography Coupled with Mass Spectrometry

机译:通过超高效液相色谱法与质谱相偶联,代谢物分析,药代动力学和大鼠ICARITIN的体外葡糖醛糖化

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摘要

Icaritin is a naturally bioactive flavonoid with several significant effects. This study aimed to clarify the metabolite profiling, pharmacokinetics, and glucuronidation of icaritin in rats. An ultra-performance liquid chromatography coupled with mass spectrometry (UPLC-MS) assay was developed and validated for qualitative and quantitative analysis of icaritin. Glucuronidation rates were determined by incubating icaritin with uridine diphosphate glucuronic acid-(UDPGA-) supplemented microsomes. Kinetic parameters were derived by appropriate model fitting. A total of 30 metabolites were identified or tentatively characterized in rat biosamples based on retention times and characteristic fragmentations, following proposed metabolic pathway which was summarized. Additionally, the pharmacokinetics parameters were investigated after oral administration of icaritin. Moreover, icaritin glucuronidation in rat liver microsomes was efficient with CLint (the intrinsic clearance) values of 1.12 and 1.56 mL/min/mg for icaritin-3-O-glucuronide and icaritin-7-O-glucuronide, respectively. Similarly, the CLint values of icaritin-3-O-glucuronide and icaritin-7-O-glucuronide in rat intestine microsomes (RIM) were 1.45 and 0.86 mL/min/mg, respectively. Taken altogether, dehydrogenation at isopentenyl group and glycosylation and glucuronidation at the aglycone were main biotransformation process in vivo. The general tendency was that icaritin was transformed to glucuronide conjugates to be excreted from rat organism. In conclusion, these results would improve our understanding of metabolic fate of icaritin in vivo.
机译:炼素是一种天然生物活性的黄酮,具有几种显着效果。本研究旨在阐明大鼠Icaritin的代谢物分析,药代动力学和葡萄糖醛。偶联与质谱(UPLC-MS)测定偶联的超高性能液相色谱法,并验证了伊加洛汀的定性和定量分析。通过用尿苷二磷酸葡糖醛酸 - (UDPGA-)补充微粒体孵育icaritin来确定血糖抑制率。通过适当的模型配件来源的动力学参数。在基于保留时间和特征碎片的大鼠生物素中鉴定了30种代谢物,其鉴定了大鼠生物素,并进行了总结的代谢途径。另外,在口服乙素施用后研究了药代动力学参数。此外,在大鼠肝微粒体中炼素血糖尿糖苷分别为icaritin-3-O-葡糖苷和伊加洛汀-7-o-葡糖醛酸的克林(内在清除)值为1.12和1.56ml / min / mg。类似地,大鼠肠微粒体(RIM)中icAritin-3-O-葡糖尿醛酸和icaritin-7-O-葡糖醛酸的克林特值分别为1.45和0.86ml / min / mg。在异戊烯基和糖糖基化和糖糖基化的脱氢方中得到脱氢,糖苷的糖醛酸在体内是主要的生物转化过程。一般趋势是将伊加洛汀转化为葡糖醛酸官缀合物,以从大鼠生物体排出。总之,这些结果将改善我们对体内伊拉特汀代谢命运的理解。

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    Zhengzhou Univ Dept Pharm Affiliated Hosp 1 Zhengzhou 450052 Henan Peoples R China;

    Zhengzhou Univ Dept Pharm Affiliated Hosp 1 Zhengzhou 450052 Henan Peoples R China;

    Zhengzhou Univ Dept Pharm Affiliated Hosp 1 Zhengzhou 450052 Henan Peoples R China;

    Zhengzhou Univ Dept Pharm Affiliated Hosp 1 Zhengzhou 450052 Henan Peoples R China;

    Zhengzhou Univ Dept Pharm Affiliated Hosp 1 Zhengzhou 450052 Henan Peoples R China;

    Zhengzhou Univ Dept Pharm Affiliated Hosp 1 Zhengzhou 450052 Henan Peoples R China;

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  • 正文语种 eng
  • 中图分类 分析化学;
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