AI Article Synopsis
- Mutations in the POLG gene, responsible for making POLγA, lead to various disorders due to mitochondrial DNA instability.
- Researchers created a mouse model with a common POLG mutation (A449T) that hinders DNA binding and synthesis, resulting in issues with mitochondrial function.
- The study reveals that POLγB stabilizes POLγA and prevents its degradation, suggesting that managing POLγA turnover could be a potential strategy for treatment development.
Article Abstract
Mutations in POLG, encoding POLγA, the catalytic subunit of the mitochondrial DNA polymerase, cause a spectrum of disorders characterized by mtDNA instability. However, the molecular pathogenesis of POLG-related diseases is poorly understood and efficient treatments are missing. Here, we generate the PolgA449T/A449T mouse model, which reproduces the A467T change, the most common human recessive mutation of POLG. We show that the mouse A449T mutation impairs DNA binding and mtDNA synthesis activities of POLγ, leading to a stalling phenotype. Most importantly, the A449T mutation also strongly impairs interactions with POLγB, the accessory subunit of the POLγ holoenzyme. This allows the free POLγA to become a substrate for LONP1 protease degradation, leading to dramatically reduced levels of POLγA in A449T mouse tissues. Therefore, in addition to its role as a processivity factor, POLγB acts to stabilize POLγA and to prevent LONP1-dependent degradation. Notably, we validated this mechanism for other disease-associated mutations affecting the interaction between the two POLγ subunits. We suggest that targeting POLγA turnover can be exploited as a target for the development of future therapies.
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| http://www.ncbi.nlm.nih.gov/pmc/articles/PMC8136776 | PMC |
| http://dx.doi.org/10.1093/nar/gkab282 | DOI Listing |
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