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Comparative pharmacokinetics of major bioactive components from Puerariae Radix-Gastrodiae Rhizome extracts and their intestinal absorption in rats

机译:葛根菌岩石毒素根瘤菌提取物的主要生物活性成分的比较药代动力学及其大鼠肠道吸收

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Puerariae Radix (PR) and Gastrodiae Rhizome (GR) is frequently used in traditional herbal formulas to treat cardio-cerebral vascular diseases due to their synergistic effects. In this study, to elucidate the action mechanism of PR-GR in vivo, a simple and reliable ultra-performance liquid chromatography tandem mass spectrometry (UPLC-MS/MS) method for simultaneous determination of nine bioactive ingredients from PR-GR in plasma was developed and applied to a comparative pharmacokinetic study following oral administration of PR, GR, and PR-GR aqueous extracts in rats. The effect of GR on the absorption of components of PR was also investigated by single-pass intestinal perfusion study. Results showed that comparing to the single herbs, PR-GR extract significantly increased the systemic exposure of puerarin, 3'-hydroxypuerarin, 3'-methoxypuerarin, 6 ''-O-xylo-sylpuerarin, daidzin, genistein, and gastrodin. Moreover, the intestinal absorption of puerarin and daidzin could be improved by GR extract and inhibitors of P-glycoprotein and multidrug resistanceassociated protein 2, respectively. These results indicate that the combination of PR and GR increases the levels of their bioactive ingredients exposed in the blood, and GR increases the absorption of ingredients of PR may by inhibition of the efflux mediated by P-glycoprotein and multidrug resistanceassociated protein 2. This is the first report for the pharmacokinetics and intestinal absorption of PR-GR, which may explain their synergetic effects in the treatment of circulatory systematic diseases and provide a meaningful insight for their clinical applications.
机译:葛根菌(PR)和胃毒素根茎(GR)经常用于传统的草药公式,以治疗心肌血管疾病,由于其协同效应。在该研究中,为了阐明体内PR-GR的作用机理,简单可靠的超级性能液相色谱串联质谱(UPLC-MS / MS)方法,用于同时测定来自PR-GR的血浆中的九种生物活性成分在大鼠PR,GR和PR-GR含水提取物之后开发和应用于对比药代动力学研究。通过单通过肠道灌注研究还研究了GR对PR组分的吸收的影响。结果表明,与单一草药相比,PR-GR提取物显着提高了葛根素,3'-羟基脲,3'-甲氧基因素,6''-Xylo-sylpuerarin,Daidzin,Genistein和Gastrodin的全身暴露。此外,P-糖蛋白和多药抗性抑制蛋白2的GR提取物和抑制剂可以改善葛根素和Daidzin的肠道吸收。这些结果表明,PR和GR的组合增加了血液中暴露的生物活性成分的水平,GR增加了PR的成分可以通过抑制由p-糖蛋白和多药抗性抑制蛋白2介导的流出来增加。这是PR-GR的药代动力学和肠道吸收的第一个报告,可以解释它们在治疗循环系统疾病中的协同作用,并为其临床应用提供有意义的见解。

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