LOSS OF DJ-1 AND PARKIN IN PARKINSON’S DISEASE OLIGODENDROCYTES INDUCES OXIDATIVE STRESS AND IMPAIRS DIFFERENTIATION AND MYELINATION
Biomedical Center (BMC), Faculty of Medicine, LMU Munich
Presentation
Date TBA
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Poster Board
PS03-08AM-064
Poster
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To explore a potential causal role for OLs in PD aetiology, we generated PD patient-derived and CRISPR-engineered OLs from induced pluripotent stem cells (iPSCs) with loss of the PD-linked genes DJ-1 or parkin. In these cells, we uncovered reduced differentiation into both early and mature OLs, accompanied by oxidative stress and mitochondrial dysfunction, which was reversible upon correction of the DJ-1 mutation. Analysis of PD patient brain tissue confirmed decreased myelination, and transplantation of DJ-1-deficient OLs into ex vivo mouse brain slices likewise resulted in impaired myelination capacity. Collectively, our study shows how PD-associated mutations compromise OL functionality by affecting maturation, cellular stress responses, and myelin formation. These findings highlight a critical contribution of OLs to PD pathology, and suggest that restoring OL function may offer new therapeutic avenues for PD.
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