Skip to main content

Skeletal muscle action of estrogen receptor α is critical for the maintenance of mitochondrial function and metabolic homeostasis in females.

Citation
Ribas, V., et al. “Skeletal Muscle Action Of Estrogen Receptor Α Is Critical For The Maintenance Of Mitochondrial Function And Metabolic Homeostasis In Females.”. Science Translational Medicine, p. 334ra54.
Center UCSD-UCLA
Featured
Author Vicent Ribas, Brian G Drew, Zhenqi Zhou, Jennifer Phun, Nareg Y Kalajian, Teo Soleymani, Pedram Daraei, Kevin Widjaja, Jonathan Wanagat, Thomas Q de Aguiar Vallim, Amy H Fluitt, Steven Bensinger, Thuc Le, Caius Radu, Julian P Whitelegge, Simon W Beaven, Peter Tontonoz, Aldons J Lusis, Brian W Parks, Laurent Vergnes, Karen Reue, Harpreet Singh, Jean C Bopassa, Ligia Toro, Enrico Stefani, Matthew J Watt, Simon Schenk, Thorbjorn Akerstrom, Meghan Kelly, Bente K Pedersen, Sylvia C Hewitt, Kenneth S Korach, Andrea L Hevener
Abstract

Impaired estrogen receptor α (ERα) action promotes obesity and metabolic dysfunction in humans and mice; however, the mechanisms underlying these phenotypes remain unknown. Considering that skeletal muscle is a primary tissue responsible for glucose disposal and oxidative metabolism, we established that reduced ERα expression in muscle is associated with glucose intolerance and adiposity in women and female mice. To test this relationship, we generated muscle-specific ERα knockout (MERKO) mice. Impaired glucose homeostasis and increased adiposity were paralleled by diminished muscle oxidative metabolism and bioactive lipid accumulation in MERKO mice. Aberrant mitochondrial morphology, overproduction of reactive oxygen species, and impairment in basal and stress-induced mitochondrial fission dynamics, driven by imbalanced protein kinase A-regulator of calcineurin 1-calcineurin signaling through dynamin-related protein 1, tracked with reduced oxidative metabolism in MERKO muscle. Although muscle mitochondrial DNA (mtDNA) abundance was similar between the genotypes, ERα deficiency diminished mtDNA turnover by a balanced reduction in mtDNA replication and degradation. Our findings indicate the retention of dysfunctional mitochondria in MERKO muscle and implicate ERα in the preservation of mitochondrial health and insulin sensitivity as a defense against metabolic disease in women.

Year of Publication
2016
Journal
Science translational medicine
Volume
8
Issue
334
Number of Pages
334ra54
Date Published
04/2016
ISSN Number
1946-6242
DOI
10.1126/scitranslmed.aad3815
Alternate Journal
Sci Transl Med
PMID
27075628
PMCID
PMC4934679
Download citation