mitoTALEN reduces the mutant mtDNA load in neurons

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Abstract

Mutations within mtDNA frequently give rise to severe encephalopathies. Given that a majority of these mtDNA defects exist in a heteroplasmic state, we harnessed the precision of mitochondrial-targeted TALEN (mitoTALEN) to selectively eliminate mutant mtDNA within the CNS of a murine model harboring a heteroplasmic mutation in the mitochondrial tRNA alanine gene (m.5024C>T). This targeted approach was accomplished by the use of AAV-PHP.eB and a neuron-specific synapsin promoter for effective neuronal delivery and expression of mitoTALEN. We found that most CNS regions were effectively transduced and showed a significant reduction in mutant mtDNA. This reduction was accompanied by an increase in mitochondrial tRNA alanine levels, which are drastically reduced by the m.5024C>T mutation. These results showed that mitochondrial-targeted gene editing can be effective in reducing CNS-mutant mtDNA in vivo, paving the way for clinical trials in patients with mitochondrial encephalopathies.

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Bacman, S. R., Barrera-Paez, J. D., Pinto, M., Van Booven, D., Stewart, J. B., Griswold, A. J., & Moraes, C. T. (2024). mitoTALEN reduces the mutant mtDNA load in neurons. Molecular Therapy Nucleic Acids, 35(1). https://doi.org/10.1016/j.omtn.2024.102132

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