Peli3 Ablation Ameliorates Acetaminophen-induced Liver Injury Through Inhibition of GSK3β Phosphorylation and Mitochondrial Translocation

Overview

Journal Exp Mol Med

Specialties Biochemistry
Molecular Biology

Date 2023 May 31

PMID 37258579

Authors

Jaewon Lee

Jihoon Ha

Jun-Hyeong Kim

Dongyeob Seo

Minbeom Kim

Yerin Lee

Seong Shil Park

Dahee Choi

Jin Seok Park

Young Jae Lee

Siyoung Yang

Kyung-Min Yang

Su Myung Jung

Suntaek Hong

Seung-Hoi Koo

Yong-Soo Bae

Seong-Jin Kim

Seok Hee Park

Affiliations

Soon will be listed here.

Abstract

The signaling pathways governing acetaminophen (APAP)-induced liver injury have been extensively studied. However, little is known about the ubiquitin-modifying enzymes needed for the regulation of APAP-induced liver injury. Here, we examined whether the Pellino3 protein, which has E3 ligase activity, is needed for APAP-induced liver injury and subsequently explored its molecular mechanism. Whole-body Peli3 knockout (KO) and adenovirus-mediated Peli3 knockdown (KD) mice showed reduced levels of centrilobular cell death, infiltration of immune cells, and biomarkers of liver injury, such as alanine aminotransferase (ALT) and aspartate aminotransferase (AST), upon APAP treatment compared to wild-type (WT) mice. Peli3 deficiency in primary hepatocytes decreased mitochondrial and lysosomal damage and reduced the mitochondrial reactive oxygen species (ROS) levels. In addition, the levels of phosphorylation at serine 9 in the cytoplasm and mitochondrial translocation of GSK3β were decreased in primary hepatocytes obtained from Peli3 KO mice, and these reductions were accompanied by decreases in JNK phosphorylation and mitochondrial translocation. Pellino3 bound more strongly to GSK3β compared with JNK1 and JNK2 and induced the lysine 63 (K63)-mediated polyubiquitination of GSK3β. In rescue experiments, the ectopic expression of wild-type Pellino3 in Peli3 KO hepatocytes restored the mitochondrial translocation of GSK3β, but this restoration was not obtained with expression of a catalytically inactive mutant of Pellino3. These findings are the first to suggest a mechanistic link between Pellino3 and APAP-induced liver injury through the modulation of GSK3β polyubiquitination.

Citing Articles

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