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Studies on metabolism and pharmacological effect of active constituents of a Tibetan herbal medicine, Halenia elliptica.

机译:藏草药哈勒氏菌(Halenia elliptica)有效成分的代谢和药理作用研究。

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摘要

Halenia elliptica D. Don belongs to Gentianaceae family. It is often used as part of a traditional Tibetan medicine to treat hepatitis. In the present investigation, six major xanthone components were isolated and identified from Halenia elliptica. An HPLC/DAD/APCI/MS method was developed and validated for the quantitative analysis of these xanthones, including 1-hydroxy-2,3,5-trimethoxy-xanthone (HM-1), 1-hydroxy-2,3,4,7-tetramethoxy- xanthone (HM-2), 1-hydroxy-2,3,4,5-tetramethoxy-xanthone (HM-3), 1,7- dihydroxy-2,3,4,5-tetramethoxy-xanthone (HM-4), 1,5-dihydroxy-2,3-dimethoxy-xanthone (HM-5) and 1-0-[beta-D-xylopyranosyl-(1-6)-beta-D-glucopyranosyl]-2,3,5-trimethoxy-xanthone (HM-2-10). All the xanthones aglycons caused vasodilation in the coronary artery pre-contracted with 1 muM 5-HT, but the xanthone glycoside had no effect. HM-1 was one of the most abundant xanthones with the most potent vasorelaxant activity.;The metabolism and pharmacokinetics of HM-1 displayed biphasic elimination kinetics, with an elimination half-life of 60.4 +/- 4.2 min. Four other Phase I metabolites were isolated and identified as demethylated products in vitro. HM-1 was metabolised to HM-5 in the liver. Biliary excretion studies showed that both HM-1 and the metabolite (HM-5) underwent extensive phase II conjugation to form glucuronides and sulfates. Tissue distribution studies showed that HM-1 was widely distributed to different organs. Collection of urine and faeces over 24 h showed that 10.88% of dose was excreted from urine and 1.91% of dose via faeces.;With HM-5 being one of the major in vivo metabolites of HM-1, the effect of HM-5 has been studied on rat coronary artery and compared to HM-1. HM-5-mediated vasorelaxant effect was mediated through opening of potassium channel (TEA, 4-AP) and altering intracellular calcium by partial inhibition of Ca2+ influx through L-type voltage-operated Ca 2+ channels and intracellular Ca2+ stores.;Taken together, in spite of the pharmacokinetics results showed that HM-1 was rapidly and widely distributed to tissues after intravenous administration in rats, with conjugation to being the major metabolic pathway in vivo, both HM-1 and its active metabolite (HM-5) show that they are important pharmacological agents with potentially useful therapeutic indications.;Mechanisms of the vasorelaxant effect of HM-1 were investigated. HM-1 showed a potent vasorelaxant activity on rat coronary artery involved both an endothelium-dependent mechanism involving NO and an endothelium-independent mechanism by inhibiting Ca2+ influx through L-type voltage-operated Ca2+ channels.
机译:椭圆形Halenia elliptica D. Don属于龙胆科。它经常被用作传统藏药治疗肝炎的一部分。在本研究中,从椭圆形哈雷氏菌中分离并鉴定了六种主要的蒽酮成分。建立了HPLC / DAD / APCI / MS方法并验证了这些杂吨的定量分析,包括1-羟基-2,3,5-三甲氧基-蒽酮(HM-1),1-羟基-2,3,4 ,7-四甲氧基-x吨酮(HM-2),1-羟基-2,3,4,5-四甲氧基-an吨酮(HM-3),1,7-二羟基-2,3,4,5-四甲氧基-an吨酮(HM-4),1,5-二羟基-2,3-二甲氧基-an吨酮(HM-5)和1-0- [β-D-吡喃吡喃糖基-(1-6)-β-D-吡喃吡喃糖基] -2 ,3,5-三甲氧基-黄酮(HM-2-10)。所有的人参酮糖苷配基都在与1μM5-HT预收缩的冠状动脉中引起血管舒张,但x吨酮苷没有作用。 HM-1是最丰富的氧杂蒽酮之一,具有最强的血管舒张活性。HM-1的代谢和药代动力学表现出双相消除动力学,消除半衰期为60.4 +/- 4.2分钟。分离了其他四种I期代谢物,并在体外鉴定为脱甲基产物。 HM-1在肝脏中代谢为HM-5。胆汁排泄研究表明,HM-1和代谢产物(HM-5)均经历了广泛的II期结合,形成了葡糖醛酸和硫酸盐。组织分布研究表明,HM-1广泛分布于不同器官。超过24小时的尿液和粪便收集表明,尿液通过粪便排泄了10.88%的剂量,而粪便则为1.91%。; HM-5是HM-1的主要体内代谢产物之一,HM-5的作用已经在大鼠冠状动脉上进行了研究,并与HM-1进行了比较。 HM-5介导的血管舒张作用是通过打开钾离子通道(TEA,4-AP)以及通过部分抑制通过L型电压操纵的Ca 2+通道和细胞内Ca2 +储存的Ca2 +流入来改变细胞内钙而介导的。 ,尽管药代动力学结果表明,HM-1在大鼠静脉内给药后迅速并广泛分布在组织中,并结合为体内的主要代谢途径,但HM-1及其活性代谢物(HM-5)均显示;它们是具有潜在有用治疗适应症的重要药理学药物。;研究了HM-1血管舒张作用的机制。 HM-1对大鼠冠状动脉具有有效的血管舒张活性,涉及通过NO介导的内皮依赖性机制和通过L型电压操纵的Ca2 +通道抑制Ca2 +内流,从而引起内皮依赖性机制。

著录项

  • 作者

    Wang, Yan.;

  • 作者单位

    The Chinese University of Hong Kong (Hong Kong).;

  • 授予单位 The Chinese University of Hong Kong (Hong Kong).;
  • 学科 Health Sciences Pharmacology.
  • 学位 Ph.D.
  • 年度 2007
  • 页码 218 p.
  • 总页数 218
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类
  • 关键词

  • 入库时间 2022-08-17 11:39:44

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