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Ligation of newly replicated DNA controls the timing of DNA mismatch repair

Curr Biol. 2021-01; 
Gloria X Reyes, Anna Kolodziejczak, Lovely Jael Paul Solomon Devakumar, Takashi Kubota, Richard D Kolodner, Christopher D Putnam, Hans Hombauer
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摘要

Mismatch repair (MMR) safeguards genome stability through recognition and excision of DNA replication errors. How eukaryotic MMR targets the newly replicated strand in?vivo has not been established. MMR reactions reconstituted in?vitro are directed to the strand containing a preexisting nick or gap, suggesting that strand discontinuities could act as discrimination signals. Another candidate is the proliferating cell nuclear antigen (PCNA) that is loaded at replication forks and is required for the activation of Mlh1-Pms1 endonuclease. Here, we discovered that overexpression of DNA ligase I (Cdc9) in Saccharomyces cerevisiae causes elevated mutation rates and increased chromatin-bound PCNA levels and accumula... More

關鍵詞

Cdc9, DNA ligase I, DNA ligase I overexpression, DNA replication fidelity, DNA replication-associated nicks, MMR, MMR strand discrimination signal, ligation Okazaki fragments, mismatch repair, mutation accumulation
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