Modulatory effects of CNNM4 on protein- l -isoaspartyl- O -methyltransferase repair function during alcohol-induced hepatic damage.

Fecha de publicación: 19/11/2024 Fecha Ahead of Print: 01/11/2024

Autores de IIS La Fe

Ramiro Jover Atienza

Autor

Participantes ajenos a IIS La Fe

Gonzalez-Recio, Irene
Goikoetxea-Usandizaga, Naroa
Rejano-Gordillo, Claudia M
Conter, Carolina
Rodriguez Agudo, Ruben
Serrano-Macia, Marina
Zapata-Pavas, Leidy Estefania
Pena-Sanfelix, Patricia
Azkargorta, Mikel
Elortza, Felix
Herranz, Jose Maria
Guillamon Thiery, Alex
Guerra-Ruiz, Armando Raul
Galicia-Garcia, Unai
Martin, Cesar
Schaeper, Ute
Delgado, Teresa C
Diaz-Moreno, Irene
Diaz Quintana, Antonio
Buccella, Daniela
Nogueiras, Ruben
Argemi, JosepMaria
Avila, Matias A
Gratacos-Gines, Jordi
Iruzubieta, Paula
Pose, Elisa
Bataller, Ramon
Crespo, Javier
Martinez-Cruz, Luis Alfonso
Martinez-Chantar, Maria Luz

Grupos

Hepatología experimental y Trasplante hepático

Investigador Principal

Laia Tolosa Pardo
Unidad Mixta de Investigación en Hepatología Experimental

Investigador Principal

Ramiro Jover Atienza

Abstract

BACKGROUND AND AIMS: Alcohol-associated liver disease (ALD) is a leading cause of liver-related mortality worldwide, with limited treatment options beyond abstinence and liver transplantation. Chronic alcohol consumption has been linked to magnesium (Mg 2+ ) deficiency, which can influence liver disease progression. The mechanisms underlying Mg 2+ homeostasis dysregulation in ALD remain elusive. This study aimed to investigate the role of the Mg 2+ transporter Cyclin M4 (CNNM4) in ALD by analyzing its expression patterns in patients with ALD and preclinical animal models. APPROACH AND RESULTS: In this study, CNNM4 is upregulated in the liver of both patients with ALD and animal models. CNNM4 overexpression triggers Mg 2+ homeostasis dysregulation, linked to ALD progression. We propose a novel therapeutic approach for ALD treatment using N -acetylgalactosamine silencing RNA technology to specifically modulate Cnnm4 expression in the liver, improving mitochondrial function and alleviating endoplasmic reticulum stress. Notably, silencing Cnnm4 restores protein isoaspartyl methyltransferase (PCMT1) activity, essential for repairing ethanol-induced protein damage. Enhancing mitochondrial activity through Cnnm4-dependent mechanisms increases S -adenosylmethionine levels, crucial for PCMT1 function, highlighting the interconnected roles of mitochondrial health and protein homeostasis in ALD treatment. CONCLUSIONS: These findings shed light on the dysregulation of Mg 2+ homeostasis in ALD, providing a promising therapeutic approach targeting CNNM4. N -acetylgalactosamine si Cnnm4 therapy boosts the repair processes of ethanol-damaged proteins through the upregulation of PCMT1 activity.