Hydroxycitrate delays early mortality in mice and promotes muscle regeneration while inducing a rich hepatic energetic status

Author:

Espadas Isabel1,Cáliz‐Molina María Ángeles1,López‐Fernández‐Sobrino Raúl1,Panadero‐Morón Concepción1,Sola‐García Alejandro1,Soriano‐Navarro Mario2,Martínez‐Force Enrique3ORCID,Venegas‐Calerón Mónica3,Salas Joaquin J.3,Martín Franz14,Gauthier Benoit R.14,Alfaro‐Cervelló Clara5,Martí‐Aguado David67,Capilla‐González Vivian1,Martín‐Montalvo Alejandro14ORCID

Affiliation:

1. Andalusian Molecular Biology and Regenerative Medicine Centre‐CABIMER Universidad de Sevilla‐CSIC‐Universidad Pablo de Olavide Seville Spain

2. Electron Microscopy Core Facility, Centro de Investigación Príncipe Felipe (CIPF) Valencia Spain

3. Instituto de la Grasa (CSIC) Universidad Pablo de Olavide Sevilla Spain

4. Biomedical Research Network on Diabetes and Related Metabolic Diseases‐CIBERDEM Instituto de Salud Carlos III Madrid Spain

5. Pathology Department, INCLIVA Health Research Institute, Clinic University Hospital University of Valencia Valencia Spain

6. Digestive Disease Department, Clinic University Hospital INCLIVA Health Research Institute Valencia Spain

7. Division of Gastroenterology, Hepatology and Nutrition Center for Liver Diseases

Abstract

AbstractATP citrate lyase (ACLY) inhibitors have the potential of modulating central processes in protein, carbohydrate, and lipid metabolism, which can have relevant physiological consequences in aging and age‐related diseases. Here, we show that hepatic phospho‐active ACLY correlates with overweight and Model for End‐stage Liver Disease score in humans. Wild‐type mice treated chronically with the ACLY inhibitor potassium hydroxycitrate exhibited delayed early mortality. In AML12 hepatocyte cultures, the ACLY inhibitors potassium hydroxycitrate, SB‐204990, and bempedoic acid fostered lipid accumulation, which was also observed in the liver of healthy‐fed mice treated with potassium hydroxycitrate. Analysis of soleus tissue indicated that potassium hydroxycitrate produced the modulation of wound healing processes. In vivo, potassium hydroxycitrate modulated locomotor function toward increased wire hang performance and reduced rotarod performance in healthy‐fed mice, and improved locomotion in mice exposed to cardiotoxin‐induced muscle atrophy. Our findings implicate ACLY and ACLY inhibitors in different aspects of aging and muscle regeneration.

Funder

Junta de Andalucía

Instituto de Salud Carlos III

Ministerio de Ciencia e Innovación

Publisher

Wiley

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