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药物代谢中P-糖蛋白与细胞色素P450 3A之间的功能相互作用。

Functional interactions between P-glycoprotein and CYP3A in drug metabolism.

作者信息

Christians Uwe, Schmitz Volker, Haschke Manuel

机构信息

University of Colorado Health Sciences Center, Clinical Research & Development, Department of Anesthesiology, Denver, Colorado 80262, USA.

出版信息

Expert Opin Drug Metab Toxicol. 2005 Dec;1(4):641-54. doi: 10.1517/17425255.1.4.641.

Abstract

The interaction between drug-metabolising enzymes and active transporters is an emerging concept in pharmacokinetics. In the gut mucosa, P-glycoprotein and cytochrome P450 (CYP)3A functionally interact in three ways: i) drugs are repeatedly taken up and pumped out of the enterocytes by P-glycoprotein, thus increasing the probability of drugs being metabolised; ii) P-glycoprotein keeps intracellular drug concentrations within the linear range of the metabolising capacity of CYP3A; and iii) P-glycoprotein transports drug metabolites formed in the mucosa back into the gut lumen. In comparison with the gut mucosa, in hepatocytes the spatial sequence of CYP3A and P-glycoprotein is reversed, resulting in different effects when the activity of one or both are changed. CYP3A and P-glycoprotein are both regulated by nuclear receptors such as the pregnane X receptor (PXR). There is significant genetic variability of CYP3A, P-glycoprotein and PXR and their expression and activity is dependent on coadministered drugs, herbs, food, age, hormonal status and disease. Future pharmacogenomic and pharmacokinetic studies will have to take all three components into account to allow for valid conclusions.

摘要

药物代谢酶与活性转运体之间的相互作用是药代动力学中一个新兴的概念。在肠道黏膜中,P-糖蛋白和细胞色素P450(CYP)3A通过三种方式发生功能相互作用:i)药物被P-糖蛋白反复摄取并泵出肠细胞,从而增加药物被代谢的可能性;ii)P-糖蛋白使细胞内药物浓度保持在CYP3A代谢能力的线性范围内;iii)P-糖蛋白将在黏膜中形成的药物代谢产物转运回肠腔。与肠道黏膜相比,在肝细胞中CYP3A和P-糖蛋白的空间顺序相反,当其中一种或两种的活性发生变化时会产生不同的影响。CYP3A和P-糖蛋白均受孕烷X受体(PXR)等核受体的调节。CYP3A、P-糖蛋白和PXR存在显著的基因变异性,它们的表达和活性取决于同时服用的药物、草药、食物、年龄、激素状态和疾病。未来的药物基因组学和药代动力学研究必须将这三个因素都考虑在内,才能得出有效的结论。

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