Microglia mitochondrial complex I deficiency during development induces glial dysfunction and early lethality.
Bella Mora-RomeroNicolas Capelo-CarrascoJuan José Pérez-MorenoMaría I Alvarez-VergaraLaura Trujillo-EstradaCarmen Romero-MolinaEmilio Martinez-MarquezNoelia Morano-CatalanMarisa VizueteJosé López-BarneoJose Luis Nieto-GonzalezPablo Garcia-Junco-ClementeJavier VitoricaAntonia GutierrezDavid MaciasAlicia E Rosales-NievesAlberto PascualPublished in: Nature metabolism (2024)
Primary mitochondrial diseases (PMDs) are associated with pediatric neurological disorders and are traditionally related to oxidative phosphorylation system (OXPHOS) defects in neurons. Interestingly, both PMD mouse models and patients with PMD show gliosis, and pharmacological depletion of microglia, the innate immune cells of the brain, ameliorates multiple symptoms in a mouse model. Given that microglia activation correlates with the expression of OXPHOS genes, we studied whether OXPHOS deficits in microglia may contribute to PMDs. We first observed that the metabolic rewiring associated with microglia stimulation in vitro (via IL-33 or TAU treatment) was partially changed by complex I (CI) inhibition (via rotenone treatment). In vivo, we generated a mouse model deficient for CI activity in microglia (MGcCI). MGcCI microglia showed metabolic rewiring and gradual transcriptional activation, which led to hypertrophy and dysfunction in juvenile (1-month-old) and adult (3-month-old) stages, respectively. MGcCI mice presented widespread reactive astrocytes, a decrease of synaptic markers accompanied by an increased number of parvalbumin neurons, a behavioral deficit characterized by prolonged periods of immobility, loss of weight and premature death that was partially rescued by pharmacologic depletion of microglia. Our data demonstrate that microglia development depends on mitochondrial CI and suggest a direct microglial contribution to PMDs.
Keyphrases
- inflammatory response
- neuropathic pain
- mouse model
- oxidative stress
- spinal cord
- lipopolysaccharide induced
- immune response
- poor prognosis
- body mass index
- gene expression
- traumatic brain injury
- machine learning
- type diabetes
- long non coding rna
- combination therapy
- brain injury
- adipose tissue
- big data
- binding protein
- artificial intelligence
- subarachnoid hemorrhage
- protein kinase