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Evolution and Function of the NR1I Nuclear Hormone Receptor Subfamily (VDR PXR and CAR) with Respect to Metabolism of Xenobiotics and Endogenous Compounds

机译:NR1I核激素受体亚家族(VDRPXR和CAR)在异源生物和内源性化合物代谢方面的进化和功能

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摘要

The NR1I subfamily of nuclear hormone receptors includes the 1,25-(OH)2-vitamin D3 receptor (VDR; NR1I1), pregnane X receptor (PXR; NR1I2), and constitutive androstane receptor (CAR; NR1I3). PXR and VDR are found in diverse vertebrates from fish to mammals while CAR is restricted to mammals. Current evidence suggests that the CAR gene arose from a duplication of an ancestral PXR gene, and that PXR and VDR arose from duplication of an ancestral gene, represented now by a single gene in the invertebrate Ciona intestinalis. Aside from the high-affinity effects of 1,25-(OH)2-vitamin D3 on VDRs, the NR1I subfamily members are functionally united by the ability to bind potentially toxic endogenous compounds with low affinity and initiate changes in gene expression that lead to enhanced metabolism and elimination (e.g., induction of cytochrome P450 3A4 expression in humans). The detoxification role of VDR seems limited to sensing high concentrations of certain toxic bile salts, such as lithocholic acid, whereas PXR and CAR have the ability to recognize structurally diverse compounds. PXR and CAR show the highest degree of cross-species variation in the ligand-binding domain of the entire vertebrate nuclear hormone receptor superfamily, suggesting adaptation to species-specific ligands. This review examines the insights that phylogenetic and experimental studies provide into the function of VDR, PXR, and CAR, and how the functions of these receptors have expanded to evolutionary advantage in humans and other animals.
机译:核激素受体的NR1I亚家族包括1,25-(OH)2-维生素D3受体(VDR; NR1I1),孕烷X受体(PXR; NR1I2)和组成型雄烷烃受体(CAR; NR1I3)。 PXR和VDR存在于从鱼类到哺乳动物的各种脊椎动物中,而CAR仅限于哺乳动物。目前的证据表明,CAR基因起源于祖先的PXR基因的重复,而PXR和VDR起源于祖先的基因的重复,而现在无脊椎动物Ciona intestinalis的单个基因代表了这一点。除了1,25-(OH)2-维生素D3对VDR具有高亲和力以外,NR1I亚家族成员还具有以低亲和力结合潜在毒性内源性化合物并引发基因表达变化的能力,从而在功能上实现了统一增强新陈代谢和消除作用(例如,诱导人类细胞色素P450 3A4表达)。 VDR的排毒作用似乎仅限于检测高浓度的某些有毒胆汁盐,例如石胆酸,而PXR和CAR具有识别结构多样的化合物的能力。 PXR和CAR在整个脊椎动物核激素受体超家族的配体结合域中显示出最高程度的跨物种变异,表明对物种特异性配体的适应性。这篇综述检查了系统发育和实验研究对VDR,PXR和CAR的功能提供的见解,以及这些受体的功能如何扩展到人类和其他动物的进化优势。

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