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Metabolism-Disrupting Chemicals and the Constitutive Androstane Receptor CAR

机译:代谢破坏化学品和组成型androstane受体汽车

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摘要

During the last two decades, the constitutive androstane receptor (CAR; NR1I3) has emerged as a master activator of drug- and xenobiotic-metabolizing enzymes and transporters that govern the clearance of both exogenous and endogenous small molecules. Recent studies indicate that CAR participates, together with other nuclear receptors (NRs) and transcription factors, in regulation of hepatic glucose and lipid metabolism, hepatocyte communication, proliferation and toxicity, and liver tumor development in rodents. Endocrine-disrupting chemicals (EDCs) constitute a wide range of persistent organic compounds that have been associated with aberrations of hormone-dependent physiological processes. Their adverse health effects include metabolic alterations such as diabetes, obesity, and fatty liver disease in animal models and humans exposed to EDCs. As numerous xenobiotics can activate CAR, its role in EDC-elicited adverse metabolic effects has gained much interest. Here, we review the key features and mechanisms of CAR as a xenobiotic-sensing receptor, species differences and selectivity of CAR ligands, contribution of CAR to regulation hepatic metabolism, and evidence for CAR-dependent EDC action therein.
机译:在过去的二十年中,组成型androstane受体(汽车; NR1I3)已成为药物和异丙酸的母体活化剂,其用于治理外源性和内源性小分子的间隙的转运蛋白。最近的研究表明,CAR参与,与其他核受体(保护区)和转录因子,肝葡萄糖和脂质代谢,肝细胞通讯,增殖和毒性,和肝肿瘤发展的啮齿类动物的调控在一起。内分泌破坏化学品(EDC)构成了与激素依赖性生理过程的像差有关的持久性有机化合物。它们的不良健康影响包括动物模型和暴露于EDC的动物模型和人类的糖尿病,肥胖和脂肪肝疾病的代谢改变。由于众多的异卵虫可以激活汽车,其在EDC引发的不良代谢效应中的作用已经获得了很多兴趣。在这里,我们审查汽车作为Xenobiotic感应受体的关键特征和机制,汽车配体的物种差异和选择性,汽车调节肝脏代谢的贡献,以及其中的汽车依赖性EDC行动的证据。

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