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首页> 外文期刊>Basic & clinical pharmacology & toxicology. >Cytochrome P450 Induction and Xeno‐Sensing Receptors Pregnane X Receptor, Constitutive Androstane Receptor, Aryl Hydrocarbon Receptor and Peroxisome Proliferator‐Activated Receptor α at the Crossroads of Toxicokinetics and Toxicodynamics
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Cytochrome P450 Induction and Xeno‐Sensing Receptors Pregnane X Receptor, Constitutive Androstane Receptor, Aryl Hydrocarbon Receptor and Peroxisome Proliferator‐Activated Receptor α at the Crossroads of Toxicokinetics and Toxicodynamics

机译:细胞色素P450诱导和异诺感测受体妊娠X受体,组成型腺甾烷受体,芳基烃受体和过氧化物体增殖剂活化受体α在毒物动脉管性和毒性学的十字路口中

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摘要

Abstract Pregnane X receptor ( PXR ), constitutive androstane receptor ( CAR ), aryl hydrocarbon receptor ( AHR ) and peroxisome proliferator‐activated receptor α ( PPAR α) are ligand‐activated transcription factors that regulate expression of many xenobiotic‐metabolizing enzymes including several cytochrome P450 ( CYP ) enzymes. Many xenobiotics induce CYP enzymes through these intracellular receptors and consequently affect toxicokinetics and possible metabolic activation of the receptor ligands and other xenobiotics utilizing similar metabolic pathways. However, it is now apparent that the xenobiotic receptors regulate also many endogenous functions and signalling pathways, and xenobiotic exposure thus may dysregulate an array of fundamental cell functions. This MiniReview surveys and discusses the multifaceted roles of xenobiotic receptors, for which CYP induction may serve as the first alert and possibly a biomarker for exposure to xenobiotics. With the current emergence of the adverse outcome pathway ( AOP ) concept, these receptors are being and will be assigned as molecular initiating events or key events in numerous discrete toxicity pathways.
机译:摘要妊娠X受体(PXR),组成芳烃受体(AHR),芳基烃受体(AHR)和过氧化物体增殖物激活受体α(PPARα)是调节许多异丙酸代谢酶的表达,包括几种细胞色素的配体活化转录因子P450(CYP)酶。许多异种症通过这些细胞内受体诱导CYP酶,因此影响受体配体的可能代谢激活和使用类似的代谢途径。然而,现在显而易见的是,异卵菌受体也调节许多内源性功能和信号通路,并且异卵暴露可能使一系列基本细胞功能失调。这种Minieview调查并讨论了异种症受体的多方面作用,其中CYP诱导可以作为第一个警报,并且可能是用于暴露于异种症的生物标志物。随着当前出现的不良结果途径(AOP)概念,存在这些受体,并将被分配为许多离散毒性途径中的分子启动事件或关键事件。

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