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药物性胆汁淤积的最新研究进展:机制及理化性质和药代动力学参数研究。

An updated review on drug-induced cholestasis: mechanisms and investigation of physicochemical properties and pharmacokinetic parameters.

机构信息

Division of Pharmacotherapy and Experimental Therapeutics, UNC Eshelman School of Pharmacy, University of North Carolina at Chapel Hill, Chapel Hill, North Carolina 27599, USA.

出版信息

J Pharm Sci. 2013 Sep;102(9):3037-57. doi: 10.1002/jps.23584. Epub 2013 May 7.

Abstract

Drug-induced cholestasis is an important form of acquired liver disease and is associated with significant morbidity and mortality. Bile acids are key signaling molecules, but they can exert toxic responses when they accumulate in hepatocytes. This review focuses on the physiological mechanisms of drug-induced cholestasis associated with altered bile acid homeostasis due to direct (e.g., bile acid transporter inhibition) or indirect (e.g., activation of nuclear receptors, altered function/expression of bile acid transporters) processes. Mechanistic information about the effects of a drug on bile acid homeostasis is important when evaluating the cholestatic potential of a compound, but experimental data often are not available. The relationship between physicochemical properties, pharmacokinetic parameters, and inhibition of the bile salt export pump among 77 cholestatic drugs with different pathophysiological mechanisms of cholestasis (i.e., impaired formation of bile vs. physical obstruction of bile flow) was investigated. The utility of in silico models to obtain mechanistic information about the impact of compounds on bile acid homeostasis to aid in predicting the cholestatic potential of drugs is highlighted.

摘要

药物性胆汁淤积是一种重要的获得性肝病形式,与显著的发病率和死亡率相关。胆汁酸是关键的信号分子,但当它们在肝细胞中积累时,会产生毒性反应。本综述重点介绍了由于直接(例如,胆汁酸转运蛋白抑制)或间接(例如,核受体激活,胆汁酸转运蛋白功能/表达改变)过程导致胆汁酸动态平衡改变而与药物相关的胆汁淤积的生理机制。在评估化合物的胆汁淤积潜力时,了解药物对胆汁酸动态平衡的影响的机制信息很重要,但通常无法获得实验数据。研究了 77 种具有不同胆汁淤积病理生理学机制(即胆汁形成受损与胆汁流动的物理阻塞)的胆汁淤积药物的理化性质、药代动力学参数和胆汁盐输出泵抑制之间的关系。强调了使用计算模型获得关于化合物对胆汁酸动态平衡影响的机制信息,以帮助预测药物的胆汁淤积潜力的实用性。

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