Journal
FRONTIERS IN AGING NEUROSCIENCE
Volume 13, Issue -, Pages -Publisher
FRONTIERS MEDIA SA
DOI: 10.3389/fnagi.2021.751742
Keywords
topoisomerase; DNA cleavage complexes; TDP1; TDP2; neurodegeneration
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Funding
- CPRIT award [RR170010]
- Welch Foundation [I-1960-201803324]
- NIMH [R01MH120132]
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The nervous system is susceptible to genomic instability and mutations in DNA damage response factors can lead to neurological disorders. The main sources and mechanisms of DNA damage relevant to neuronal dysfunction are not well understood. Topoisomerase-mediated DNA damage may be a significant underlying source of neuronal dysfunction.
The nervous system is vulnerable to genomic instability and mutations in DNA damage response factors lead to numerous developmental and progressive neurological disorders. Despite this, the sources and mechanisms of DNA damage that are most relevant to the development of neuronal dysfunction are poorly understood. The identification of primarily neurological abnormalities in patients with mutations in TDP1 and TDP2 suggest that topoisomerase-mediated DNA damage could be an important underlying source of neuronal dysfunction. Here we review the potential sources of topoisomerase-induced DNA damage in neurons, describe the cellular mechanisms that have evolved to repair such damage, and discuss the importance of these repair mechanisms for preventing neurological disorders.
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