孕烷X受体
法尼甾体X受体
胆酸
胆酸
化学
骨化三醇受体
脱氧胆酸
鹅去氧胆酸
核受体
乙酰化
雄激素受体
胆汁酸
受体
生物化学
G蛋白偶联胆汁酸受体
基因
转录因子
作者
Alejandro Carazo,Lucie Hyršová,Ján Dušek,Hana Chodounská,Alžbeta Horvátová,Karel Berka,Václav Bazgier,Hongying Gan‐Schreier,Waleé Chamulitrat,Eva Kudová,Petr Pávek
标识
DOI:10.1016/j.toxlet.2016.11.013
摘要
The Pregnane X (PXR), Vitamin D (VDR) and Farnesoid X (FXR) nuclear receptors have been shown to be receptors of bile acids controlling their detoxification or synthesis. Chenodeoxycholic (CDCA) and lithocholic (LCA) acids are ligands of FXR and VDR, respectively, whereas 3-keto and acetylated derivates of LCA have been described as ligands for all three receptors. In this study, we hypothesized that oxidation or acetylation at position 3, 7 and 12 of bile acids DCA (deoxycholic acid), LCA, CA (cholic acid), and CDCA by detoxification enzymes or microbiome may have an effect on the interactions with bile acid nuclear receptors. We employed reporter gene assays in HepG2 cells, the TR-FRET assay with recombinant PXR and RT-PCR to study the effects of acetylated and keto bile acids on the nuclear receptors activation and their target gene expression in differentiated hepatic HepaRG cells. We demonstrate that the DCA 3,12-diacetate and CA 3,7,12-triacetate derivatives are ligands of PXR and DCA 3,12-diacetate induces PXR target genes such as CYP3A4, CYP2B6 and ABCB1/MDR1. In conclusion, we found that acetylated DCA and CA are potent ligands of PXR. Whether the acetylated bile acid derivatives are novel endogenous ligands of PXR with detoxification or physiological functions should be further studied in ongoing experiments.
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