Hepatic Aryl Hydrocarbon Receptor Attenuates Fibroblast Growth Factor 21 Expression

May 27, 2016The Journal of biological chemistry

Liver Aryl Hydrocarbon Receptor Reduces Levels of Fibroblast Growth Factor 21

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Abstract

Non-fasted hepatocyte-targeted AHR knock-out mice exhibit a 4-fold increase in hepatic Fgf21 expression compared to the congenic parental strain.

  • AHR is involved in regulating hepatic Fgf21 expression.
  • Agonist activation of AHR reduces hepatic Fgf21 expression during fasting.
  • AHR binds to specific elements in the Fgf21 promoter that overlap with binding sites for other regulatory proteins.
  • Agonist-activated AHR impairs the activity of PPARα, ChREBP, and CREBH in promoting Fgf21 expression.
  • Effects of AHR activation on FGF21 expression were also observed in primary human hepatocytes, suggesting broader relevance.

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