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. 2014 Jul 7;5(4):373–385. doi: 10.3945/an.114.005868

TABLE 1.

Food ligands of nuclear receptors and influence on epigenetic regulation1

Food compound Metabolic/epigenetic effects
ER
 Genistein, daidzein, equol Potent activators of ERβ and ERα promoters through regulation of DNMT expression and enhanced HAT activity (122)
 Resveratrol Increases ER promoter methylation and inhibits HDAC (150)
 EGCG Induces chromatin remodeling by altering histone acetylation and methylation status leading to ER reactivation (47)
 I3C Disrupts interaction between ERα and Sp1 on promoter of the hTERT gene (151)
AR
 EGCG Lowers AR acetylation and activation by inhibiting HAT activity (152)
 DIM Reverses epigenetic silencing of miR-34a in prostate cancer, inducing inactivation of the AR (153)
AhR
 Resveratrol Prevents BRCA-1 promoter hypermethylation and silencing (49, 126)
 EGCG Inhibits binding of AhR to XRE in endothelial cells (154); directly inhibits DNMT by binding to catalytic subunit (122)
 DIM, I3C Abrogate dioxin-induced recruitment of AhR and AcH4 to the COX-2 promoter (35)
 Quercetin, kaempferol, genistein, daidzein, apigenin Inhibit AhR binding to XRE of target genes, such as CYP1A1 (123)
PPARα/γ
 Resveratrol Activates PPARs in vitro and in vivo leading to reduced COX-2 expression (155)
PPARα
 Eicosanoids Regulate β-oxidation genes in liver; inhibit NF-κB transcription in heart (156)
PPARγ
 Arachidonic acid Increases adipocyte differentiation in brown adipose tissue (156)
 Genistein Promotes adipogenesis at concentrations >1 μmol/L through mechanisms involving downregulation of ER-mediated transcription (156)
 Daidzein and equol Activate PPARγ at lower concentrations than genistein (157)
 CLA Inhibits adipogenesis and inflammation, promotes osteoblastogenesis (158)
PPARβ/δ
 PUFAs Increase FA oxidation (156)
 PGs Lower TGs and free FA amounts in adipose tissue (156)
RXR
 9-cis RA Binding to an NR partner (e.g., FXR, LXR, PPAR, RAR, TR, or VDR) promotes recruitment of cofactors and HATs that lead to transcriptional activation (159)
 Lithocholic acid
 Phytanic acid
VDR
 Vitamin D Binding to VDR influences recruitment of coactivators or repressors and transcription of target genes (160162)
 Curcumin Activates heterodimer formation with RXR and recruitment of coactivator SRC-1 (163)
FXR
 BAs Increase interaction with NCoA6 (LXXLL motif) (126)
 EGCG Inhibits recruitment of coactivator SRC-2 to FXR and transcription of target genes in the intestine (7)
LXR
 Resveratrol Increases RNA polymerase recruitment to the LXR promoter (164)
 EGCG Reduces expression of LXR in 3T3-LI liver cells (165)
 Genistein Increases promoter activity in rat liver, leading to insulin sensitization and improved lipid homeostasis (166)
1

AcH4, acetylated histone-4; AhR, aromatic hydrocarbon receptor; AR, androgen receptor; BA, bile acid; BRCA-1, breast cancer-1; COX-2, cyclooxygenase-2; CYP1A1, cytochrome P450, family 1, subfamily A, polypeptide 1; DIM, diindolylmethane; DNMT, DNA methyltransferase; EGCG, epigallocatechin 3-O-gallate; ER, estrogen receptor; FXR, farnesoid X receptor; HAT, histone acetyltransferase; HDAC, histone deacetylase; hTERT, human telomerase reverse transcriptase; I3C, indole-3-carbinol; LXR, liver X receptor; LXXLL, L indicates leucine and X indicates any amino acid; miR-34a, microRNA-34a; NCoA6, nuclear receptor coactivator 6; NR, nuclear receptor; RA, retinoic acid; RAR, retinoic acid receptor; RXR, retinoid X receptor; Sp1, specificity protein 1; SRC-1, steroid receptor coactivator-1; SRC-2, SRC-1, steroid receptor coactivator-2; TR, thyroid receptor; VDR, vitamin D receptor; XRE, xenobiotic response element.