Litcius/Paper detail

Nuclear receptor phosphorylation in xenobiotic signal transduction

Masahiko Negishi, Kaoru Kobayashi, Tsutomu Sakuma, Tatsuya Sueyoshi

2020Journal of Biological Chemistry52 citationsDOIOpen Access PDF

Abstract

genes. Inevitably, both nuclear receptors have been investigated as ligand-activated nuclear receptors by identifying and characterizing xenobiotics and therapeutics that directly bind CAR and/or PXR to activate them. However, PB, which does not bind CAR directly, presented an alternative research avenue for an indirect ligand-mediated nuclear receptor activation mechanism: phosphorylation-mediated signal regulation. This review summarizes phosphorylation-based mechanisms utilized by xenobiotics to elicit cell signaling. First, the review presents how PB activates CAR (and other nuclear receptors) through a conserved phosphorylation motif located between two zinc fingers within its DNA-binding domain. PB-regulated phosphorylation at this motif enables nuclear receptors to form communication networks, integrating their functions. Next, the review discusses xenobiotic-induced PXR activation in the absence of the conserved DNA-binding domain phosphorylation motif. In this case, phosphorylation occurs at a motif located within the ligand-binding domain to transduce cell signaling that regulates hepatic energy metabolism. Finally, the review delves into the implications of xenobiotic-induced signaling through phosphorylation in disease development and progression.

Topics & Concepts

Pregnane X receptorConstitutive androstane receptorNuclear receptorPELP-1PhosphorylationCell biologySignal transductionXenobioticBiologyReceptorBiochemistryTranscription factorGeneEnzymePharmacogenetics and Drug MetabolismDrug Transport and Resistance MechanismsHormonal Regulation and Hypertension