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波耳定碱通过渗透和法尼酯X受体依赖性机制增强大鼠胆汁分泌。

Boldine enhances bile production in rats via osmotic and farnesoid X receptor dependent mechanisms.

作者信息

Cermanova Jolana, Kadova Zuzana, Zagorova Marie, Hroch Milos, Tomsik Pavel, Nachtigal Petr, Kudlackova Zdenka, Pavek Petr, Dubecka Michaela, Ceckova Martina, Staud Frantisek, Laho Tomas, Micuda Stanislav

机构信息

Department of Pharmacology, Charles University in Prague, Faculty of Medicine in Hradec Kralove, Czech Republic.

Department of Pharmacology, Charles University in Prague, Faculty of Medicine in Hradec Kralove, Czech Republic; Deparment of Pharmacology and Toxicology, Charles University in Prague, Faculty of Pharmacy in Hradec Kralove, Czech Republic.

出版信息

Toxicol Appl Pharmacol. 2015 May 15;285(1):12-22. doi: 10.1016/j.taap.2015.03.004. Epub 2015 Mar 12.

Abstract

Boldine, the major alkaloid from the Chilean Boldo tree, is used in traditional medicine to support bile production, but evidence to support this function is controversial. We analyzed the choleretic potential of boldine, including its molecular background. The acute- and long-term effects of boldine were evaluated in rats either during intravenous infusion or after 28-day oral treatment. Infusion of boldine instantly increased the bile flow 1.4-fold in healthy rats as well as in animals with Mrp2 deficiency or ethinylestradiol induced cholestasis. This effect was not associated with a corresponding increase in bile acid or glutathione biliary excretion, indicating that the effect is not related to stimulation of either bile acid dependent or independent mechanisms of bile formation and points to the osmotic activity of boldine itself. We subsequently analyzed bile production under conditions of changing biliary excretion of boldine after bolus intravenous administration and found strong correlations between both parameters. HPLC analysis showed that bile concentrations of boldine above 10 μM were required for induction of choleresis. Importantly, long-term pretreatment, when the bile collection study was performed 24-h after the last administration of boldine, also accelerated bile formation despite undetectable levels of the compound in bile. The effect paralleled upregulation of the Bsep transporter and increased biliary clearance of its substrates, bile acids. We consequently confirmed the ability of boldine to stimulate the Bsep transcriptional regulator, FXR receptor. In conclusion, our study clarified the mechanisms and circumstances surrounding the choleretic activity of boldine.

摘要

波耳定碱是智利波尔多树中的主要生物碱,在传统医学中用于促进胆汁分泌,但支持这一功能的证据存在争议。我们分析了波耳定碱的利胆潜力,包括其分子背景。在大鼠静脉输注期间或口服治疗28天后,评估了波耳定碱的急性和长期作用。在健康大鼠以及患有多药耐药相关蛋白2(Mrp2)缺乏症或乙炔雌二醇诱导胆汁淤积的动物中,输注波耳定碱可使胆汁流量立即增加1.4倍。这种作用与胆汁酸或谷胱甘肽胆汁排泄的相应增加无关,表明该作用与胆汁形成的胆汁酸依赖性或非依赖性机制的刺激无关,而是指向波耳定碱本身的渗透活性。我们随后分析了静脉推注波耳定碱后胆汁排泄变化条件下的胆汁生成情况,发现这两个参数之间存在很强的相关性。高效液相色谱分析表明,诱导利胆作用需要胆汁中波耳定碱浓度高于10μM。重要的是,在最后一次给予波耳定碱24小时后进行胆汁收集研究时,长期预处理也加速了胆汁形成,尽管胆汁中未检测到该化合物。这种作用与胆汁盐输出泵(Bsep)转运蛋白的上调及其底物胆汁酸的胆汁清除增加平行。因此,我们证实了波耳定碱刺激Bsep转录调节因子法尼醇X受体(FXR)的能力。总之,我们的研究阐明了波耳定碱利胆活性的机制和相关情况。

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