Impact of ribonucleotide incorporation by DNA polymerases β and λ on oxidative base excision repair
Impact of ribonucleotide incorporation by DNA polymerases β and λ on oxidative base excision repair
AbstractOxidative stress is a very frequent source of DNA damage. Many cellular DNA polymerases (Pols) can incorporate ribonucleotides (rNMPs) during DNA synthesis. However, whether oxidative stress-triggered DNA repair synthesis contributes to genomic rNMPs incorporation is so far not fully understood. Human specialized Pols β and λ are the important enzymes involved in the oxidative stress tolerance, acting both in base excision repair and in translesion synthesis past the very frequent oxidative lesion 7,8-dihydro-8-oxoguanine (8-oxo-G). We found that Pol β, to a greater extent than Pol λ can incorporate rNMPs opposite normal bases or 8-oxo-G, and with a different fidelity. Further, the incorporation of rNMPs opposite 8-oxo-G delays repair by DNA glycosylases. Studies in Pol β- and λ-deficient cell extracts suggest that Pol β levels can greatly affect rNMP incorporation opposite oxidative DNA lesions.
- National Research Council Italy
- University of Zurich Switzerland
- National Research Council Sri Lanka
- ETH Zurich Switzerland
Guanine, DNA Repair, Science, Q, Ribonucleotides, Article, Cell Line, DNA Glycosylases, Mice, Oxidative Stress, Animals, Humans, DNA polymerases beta and lambda, DNA Polymerase beta, DNA Damage
Guanine, DNA Repair, Science, Q, Ribonucleotides, Article, Cell Line, DNA Glycosylases, Mice, Oxidative Stress, Animals, Humans, DNA polymerases beta and lambda, DNA Polymerase beta, DNA Damage
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