Litcius/Paper detail

Interaction between dual specificity phosphatase-1 and cullin-1 attenuates alcohol-related liver disease by restoring p62-mediated mitophagy

Ruibin Li, Zhe Dai, Xiaoman Liu, Chunling Wang, Jia Huang, Ting Xin, Ying Tong, Yijin Wang

2023International Journal of Biological Sciences19 citationsDOIOpen Access PDF

Abstract

) mice showed resistance to alcohol-mediated hepatic dysfunction, as evidenced by decreased AST/ALT activity, improved alcohol metabolism, and suppressed liver fibrosis, inflammation, and oxidative stress. Functional experiments demonstrated that DUSP1 overexpression prevents alcohol-mediated mitochondrial damage in hepatocytes through restoring mitophagy. Accordingly, pharmacological blockade of mitophagy abolished the hepatoprotective actions of DUSP1. Molecular assays showed that DUSP1 binds cytosolic CUL1 and prevents its translocation to the nucleus. Importantly, CUL1 silencing restored the transcription of p62 and Parkin, resulting in mitophagy activation, and sustained mitochondrial integrity and hepatocyte function upon alcohol stress. These results indicate that alcohol-mediated DUSP1 downregulation interrupts DUSP1/CUL1 interaction, leading to CUL1 nuclear translocation and mitophagy inhibition via transcriptional repression of p62 and Parkin. Thus, targeting the DUSP1/CUL1/p62 axis will be a key approach to restore hepatic mitophagy as well as alleviate symptoms of ALD.

Topics & Concepts

MitophagyCullinParkinUbiquitin ligasePINK1Cell biologyChemistryMitochondrionBiologyUbiquitinBiochemistryAutophagyInternal medicineMedicineGeneApoptosisParkinson's diseaseDiseaseAlcohol Consumption and Health EffectsLipid metabolism and biosynthesisCancer, Hypoxia, and Metabolism