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大鼠体内通过微透析同步采集七叶亭的血液和胆汁样本。

Simultaneous blood and biliary sampling of esculetin by microdialysis in the rat.

作者信息

Tsai T H, Huang C T, Shum A Y, Chen C F

机构信息

Department of Pharmacology, National Research Institute of Chinese Medicine, Taipei, Taiwan.

出版信息

Life Sci. 1999;65(16):1647-55. doi: 10.1016/s0024-3205(99)00413-0.

Abstract

Biliary excretion and intestinal reabsorption in enterohepatic circulation play major dispositional roles for some drugs. To circumvent multiple blood sampling and interruption of enterohepatic circulation in conventional biliary cannulation, the present study utilized the minimally invasive sampling technique of microdialysis in pharmacokinetics and biliary excretion studies. Microdialysis probes were inserted into the jugular vein and bile duct in the anesthetized rat for simultaneous and continuous sampling following intravenous administration of esculetin, a bioactive coumarin derivative. Placements of the microdialysis probes were designed to minimize obstruction to normal flows of the body fluids. Separation and quantitation of esculetin in the dialysates were achieved using high performance liquid chromatography (HPLC) coupled to UV detection. The results indicated higher drug concentrations in the bile than in the blood, suggesting active biliary excretion. The study also provided an example of successful application of in vivo microdialysis as an interesting and feasible alternative for pharmacokinetics and biliary drug excretion studies.

摘要

肝肠循环中的胆汁排泄和肠道重吸收对某些药物起着主要的处置作用。为了避免在传统胆管插管中进行多次采血以及中断肝肠循环,本研究在药代动力学和胆汁排泄研究中采用了微创微透析采样技术。在麻醉大鼠的颈静脉和胆管中插入微透析探针,以便在静脉注射生物活性香豆素衍生物七叶亭后进行同步连续采样。微透析探针的放置旨在尽量减少对体液正常流动的阻碍。使用与紫外检测联用的高效液相色谱法(HPLC)对透析液中的七叶亭进行分离和定量。结果表明胆汁中的药物浓度高于血液中的药物浓度,提示存在主动胆汁排泄。该研究还提供了一个成功应用体内微透析的实例,作为药代动力学和胆汁药物排泄研究中一种有趣且可行的替代方法。

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