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芳烃受体、孕烷X受体以及组成型雄甾烷受体对人类药物代谢酶和结合转运体的协同调节

Coordinate regulation of human drug-metabolizing enzymes, and conjugate transporters by the Ah receptor, pregnane X receptor and constitutive androstane receptor.

作者信息

Köhle Christoph, Bock Karl Walter

机构信息

Department of Toxicology, Institute of Pharmacology and Toxicology, University of Tübingen, Tübingen, Germany.

出版信息

Biochem Pharmacol. 2009 Feb 15;77(4):689-99. doi: 10.1016/j.bcp.2008.05.020. Epub 2008 Jul 5.

Abstract

Coordinate regulation of Phase I and II drug-metabolizing enzymes and conjugate transporters by nuclear receptors suggests that these proteins evolved to an integrated biotransformation system. Two major groups of ligand-activated nuclear receptors/xenosensors evolved: the Ah receptor (activated by aryl hydrocarbons and drugs such as omeprazole) and type 2 steroid receptors such as PXR and CAR, activated by drugs such as rifampicin, carbamazepin and phenytoin. It is increasingly recognized that there is considerable cross-talk between these xenosensors. Therefore, an attempt was made to discuss biotransformation by the Ah receptor together with that of PXR and CAR. Due to considerable species differences the emphasis is on human biotransformation. Agonists coordinately induce biotransformation due to common xenosensor-binding response elements in the regulatory region of target genes. However, whereas different groups of xenobiotics appear to more selectively stimulate CYPs (Phase I), their regulatory control largely converged in modulating Phase II metabolism and transport. Biotransformation appears to be tightly controlled to achieve efficient homeostasis of endobiotics and detoxification of dietary phytochemicals, but nuclear receptor agonists may also lead to potentially harmful drug interactions.

摘要

核受体对I相和II相药物代谢酶及结合转运体的协调调节表明,这些蛋白质进化为一个整合的生物转化系统。配体激活的核受体/异生素感受器主要进化出两大类:芳烃受体(由芳基烃和药物如奥美拉唑激活)和2型类固醇受体,如孕烷X受体(PXR)和组成型雄烷受体(CAR),由利福平、卡马西平和苯妥英等药物激活。人们越来越认识到这些异生素感受器之间存在大量的相互作用。因此,本文尝试将芳烃受体与PXR和CAR的生物转化进行讨论。由于存在显著的物种差异,重点在于人类生物转化。激动剂通过靶基因调控区域中共同的异生素感受器结合反应元件来协调诱导生物转化。然而,不同组的异生素似乎更有选择性地刺激细胞色素P450(CYP,I相),但其调控在调节II相代谢和转运方面基本趋同。生物转化似乎受到严格控制,以实现内源性物质的有效稳态和膳食植物化学物质的解毒,但核受体激动剂也可能导致潜在有害的药物相互作用。

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