Wnt/beta-catenin Signaling Activates and Determines Hepatic Zonal Expression of Glutathione S-transferases in Mouse Liver

Overview

Journal Toxicol Sci

Publisher Oxford University Press

Specialty Toxicology

Date 2010 Feb 2

PMID 20118494

Citations 26

Authors

Stefanie Giera

Albert Braeuning

Christoph Kohle

Wilfried Bursch

Ute Metzger

Albrecht Buchmann

Michael Schwarz

Affiliations

Soon will be listed here.

Abstract

Glutathione S-transferases (GSTs) play an essential role in the elimination of xenobiotic-derived electrophilic metabolites and also catalyze certain steps in the conversion of endogenous molecules. Their expression is controlled by different transcription factors, such as the antioxidant-activated Nrf2 or the constitutive androstane receptor. Here, we show that the Wnt/beta-catenin pathway is also involved in the transcriptional regulation of GSTs: GSTm2, GSTm3, and GSTm6 are overexpressed in mouse hepatomas with activating Ctnnb1 (encoding beta-catenin) mutations and in transgenic hepatocytes expressing activated beta-catenin. Inversely, GSTm expression is reduced in mice with hepatocyte-specific knock out of Ctnnb1. Activation of beta-catenin-dependent signaling stimulates GSTm expression in vitro. Activation of beta-catenin in mouse hepatoma cells activates GSTm3 promoter-driven reporter activity, independently of beta-catenin/T-cell factor sites, via a retinoid X receptor-binding site. By contrast, GSTm expression is inhibited upon Ras activation in mouse liver tumors and transgenic hepatocytes. Recent studies by different groups have shown that beta-catenin-dependent signaling is involved in the transcriptional control of "perivenous" expression of various cytochrome P450s in mouse liver, whereas Ras signaling was hypothesized to antagonize the perivenous hepatocyte phenotype. In synopsis with our present results, it now appears that the Wnt/beta-catenin pathway functions as a master regulator of the expression of both phase I and phase II drug-metabolizing enzymes in perivenous hepatocytes from mouse liver.

Citing Articles

Loss of β-catenin reveals a role for glutathione in regulating oxidative stress during cholestatic liver disease.

Balogun O, Shao D, Carson M, King T, Kosar K, Zhang R Hepatol Commun. 2024; 8(7.

PMID: 38967587 PMC: 11227358. DOI: 10.1097/HC9.0000000000000485.

Phylogenetic inference from single-cell RNA-seq data.

Liu X, Griffiths J, Bishara I, Liu J, Bild A, Chang J Sci Rep. 2023; 13(1):12854.

PMID: 37553438 PMC: 10409753. DOI: 10.1038/s41598-023-39995-6.

DiProspero T, Brown L, Fachko T, Lockett M Drug Metab Dispos. 2022; 50(8).

PMID: 35701181 PMC: 9341261. DOI: 10.1124/dmd.122.000870.

Role and Regulation of Wnt/β-Catenin in Hepatic Perivenous Zonation and Physiological Homeostasis.

Goel C, Monga S, Nejak-Bowen K Am J Pathol. 2021; 192(1):4-17.

PMID: 34924168 PMC: 8747012. DOI: 10.1016/j.ajpath.2021.09.007.

Wnt-Independent and Wnt-Dependent Effects of APC Loss on the Chemotherapeutic Response.

Stefanski C, Prosperi J Int J Mol Sci. 2020; 21(21).

PMID: 33105836 PMC: 7660076. DOI: 10.3390/ijms21217844.