The human OPA1delTTAG mutation induces premature age-related systemic neurodegeneration in mouse

Emmanuelle Sarzi; Claire Angebault; Marie Seveno; Naïg Gueguen; Benjamin Chaix; Guy Bielicki; Nathalie Boddaert; Anne-Laure Mausset-Bonnefont; Chantal Cazevieille; Valérie Rigau; Jean-Pierre Renou; Jing Wang; Cécile Delettre; Philippe Brabet; Jean-Luc Puel; Christian P Hamel; Pascal Reynier; Guy Lenaers

doi:10.1093/brain/aws303

The human OPA1delTTAG mutation induces premature age-related systemic neurodegeneration in mouse

Brain. 2012 Dec;135(Pt 12):3599-613. doi: 10.1093/brain/aws303.

Authors

Emmanuelle Sarzi¹, Claire Angebault, Marie Seveno, Naïg Gueguen, Benjamin Chaix, Guy Bielicki, Nathalie Boddaert, Anne-Laure Mausset-Bonnefont, Chantal Cazevieille, Valérie Rigau, Jean-Pierre Renou, Jing Wang, Cécile Delettre, Philippe Brabet, Jean-Luc Puel, Christian P Hamel, Pascal Reynier, Guy Lenaers

Affiliation

¹ Institut des Neurosciences de Montpellier, INSERM U1051, Université Montpellier I et II CHU St Eloi, 80, rue Auguste Fliche, 34091 Montpellier Cedex 5, France.

PMID: 23250881
DOI: 10.1093/brain/aws303

Abstract

Dominant optic atrophy is a rare inherited optic nerve degeneration caused by mutations in the mitochondrial fusion gene OPA1. Recently, the clinical spectrum of dominant optic atrophy has been extended to frequent syndromic forms, exhibiting various degrees of neurological and muscle impairments frequently found in mitochondrial diseases. Although characterized by a specific loss of retinal ganglion cells, the pathophysiology of dominant optic atrophy is still poorly understood. We generated an Opa1 mouse model carrying the recurrent Opa1(delTTAG) mutation, which is found in 30% of all patients with dominant optic atrophy. We show that this mouse displays a multi-systemic poly-degenerative phenotype, with a presentation associating signs of visual failure, deafness, encephalomyopathy, peripheral neuropathy, ataxia and cardiomyopathy. Moreover, we found premature age-related axonal and myelin degenerations, increased autophagy and mitophagy and mitochondrial supercomplex instability preceding degeneration and cell death. Thus, these results support the concept that Opa1 protects against neuronal degeneration and opens new perspectives for the exploration and the treatment of mitochondrial diseases.

MeSH terms

Acoustic Stimulation
Age Factors
Aging, Premature / genetics
Animals
Aspartic Acid / analogs & derivatives
Aspartic Acid / metabolism
Chi-Square Distribution
Creatine / metabolism
Disease Models, Animal
Disease Progression
Electron Transport Chain Complex Proteins / metabolism
Electron Transport Complex IV / metabolism
Electroretinography
Evoked Potentials, Auditory, Brain Stem / genetics
Evoked Potentials, Visual / genetics
GTP Phosphohydrolases / genetics*
Gene Expression Regulation / genetics*
Glycolysis / genetics
Humans
Lactic Acid / metabolism
Locomotion / genetics
Magnetic Resonance Imaging
Magnetic Resonance Spectroscopy
Membrane Proteins / metabolism
Mice
Mice, Inbred C57BL
Mice, Transgenic
Mitochondrial Diseases / complications
Mitochondrial Diseases / genetics*
Muscle, Skeletal / pathology
Muscle, Skeletal / ultrastructure
Nervous System / pathology
Nervous System / ultrastructure
Optic Atrophy, Autosomal Dominant / genetics*
Optic Atrophy, Autosomal Dominant / pathology
Optic Atrophy, Autosomal Dominant / physiopathology*
Optic Atrophy, Autosomal Dominant / rehabilitation
Optic Nerve / pathology
Optic Nerve / physiopathology
Optic Nerve / ultrastructure
Phenotype
Physical Conditioning, Animal
Psychoacoustics
Psychomotor Performance / physiology
Reaction Time / genetics
Retina / pathology
Retina / physiopathology
Retina / ultrastructure
Retinal Ganglion Cells / pathology
Sequence Deletion / genetics*

Substances

Electron Transport Chain Complex Proteins
Membrane Proteins
Aspartic Acid
Lactic Acid
N-acetylaspartate
Electron Transport Complex IV
GTP Phosphohydrolases
OPA1 protein, human
Creatine