评价胆汁淤积大鼠转运蛋白和p -糖蛋白的调节及其对地高辛清除的影响。

Parker Giroux, Patrick B Kyle, Chalet Tan, Joseph D Edwards, Michael J Nowicki, Hua Liu
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引用次数: 1

摘要

背景:心脏和肝脏功能在多方面的关系中交织在一起。涉及其中一种的病理过程可能通过多种机制影响另一种,包括血液动力学和膜运输效应。目的:了解肝外胆汁淤积对地高辛膜转运蛋白调控的影响及其对地高辛清除率的影响。方法:选取12只成年大鼠;建立基线肝脏和肾脏实验室值和地高辛药代动力学(PK)研究,然后均匀分为两组进行胆管结扎(BDL)或假手术。重复7 d后,完成地高辛PK研究,取组织样品,采用定量western blot和实时聚合酶链反应检测细胞膜转运蛋白的表达。使用SigmaStat 3.5分析数据。同一实验组术前、术后均值比较采用配对t检验,sham组与BDL组均值比较采用独立t检验。结果:BDL大鼠地高辛清除率降低,肝功能受损,但肾功能未见损害。BDL导致肝脏和肾脏多药耐药1表达显著上调,小肠多药耐药1表达显著下调。BDL后,有机阴离子转运多肽(OATP)1A4在肝脏中表达上调,在肠道中表达下调。BDL后肾脏OATP4C1表达明显升高。结论:地高辛的细胞膜转运蛋白在肝外胆汁淤积中受到调节。这些调节有利于增加地高辛在肾脏中的排泄,减少其从肠道的吸收,以补偿由于胆汁淤积而减少的地高辛清除率。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Evaluating the regulation of transporter proteins and P-glycoprotein in rats with cholestasis and its implication for digoxin clearance.

Evaluating the regulation of transporter proteins and P-glycoprotein in rats with cholestasis and its implication for digoxin clearance.

Evaluating the regulation of transporter proteins and P-glycoprotein in rats with cholestasis and its implication for digoxin clearance.

Evaluating the regulation of transporter proteins and P-glycoprotein in rats with cholestasis and its implication for digoxin clearance.

Background: Cardiac and hepatic functionality are intertwined in a multifaceted relationship. Pathologic processes involving one may affect the other through a variety of mechanisms, including hemodynamic and membrane transport effects.

Aim: To better understand the effect of extrahepatic cholestasis on regulations of membrane transporters involving digoxin and its implication for digoxin clearance.

Methods: Twelve adult rats were included in this study; baseline hepatic and renal laboratory values and digoxin pharmacokinetic (PK) studies were established before evenly dividing them into two groups to undergo bile duct ligation (BDL) or a sham procedure. After 7 d repeat digoxin PK studies were completed and tissue samples were taken to determine the expressions of cell membrane transport proteins by quantitative western blot and real-time polymerase chain reaction. Data were analyzed using SigmaStat 3.5. Means between pre-surgery and post-surgery in the same experimental group were compared by paired t-test, while independent t-test was employed to compare the means between sham and BDL groups.

Results: Digoxin clearance was decreased and liver function, but not renal function, was impaired in BDL rats. BDL resulted in significant up-regulation of multidrug resistance 1 expression in the liver and kidney and its down-regulation in the small intestine. Organic anion transporting polypeptides (OATP)1A4 was up-regulated in the liver but down-regulated in intestine after BDL. OATP4C1 expression was markedly increased in the kidney following BDL.

Conclusion: The results suggest that cell membrane transporters of digoxin are regulated during extrahepatic cholestasis. These regulations are favorable for increasing digoxin excretion in the kidney and decreasing its absorption from the intestine to compensate for reduced digoxin clearance due to cholestasis.

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