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. 2025 Oct 2;188(20):5735-5747.e15.
doi: 10.1016/j.cell.2025.07.003. Epub 2025 Jul 29.

DNA mutagenesis driven by transcription factor competition with mismatch repair

Wei Zhu  1 Yuning Zhang  2 Harshit Sahay  2 Hana Wasserman  2 Ariel Afek  3 Jonathan Williams  4 Samantha Shaltz  4 Caitlin Johnson  5 Kyle Pinheiro  6 David M MacAlpine  7 Keith R Weninger  8 Dorothy A Erie  5 Sue Jinks-Robertson  9 Raluca Gordân  10
Affiliations

DNA mutagenesis driven by transcription factor competition with mismatch repair

Wei Zhu et al. Cell. .

Abstract

Despite the remarkable fidelity of eukaryotic DNA replication, nucleotide misincorporation errors occur in every replication cycle, generating mutations that drive genetic diseases and genome evolution. Here, we show that transcription factor (TF) proteins, key players in gene regulation, can increase mutagenesis from replication errors by directly competing with the recognition of DNA mismatches by MutSα, the primary initiator of eukaryotic mismatch repair (MMR). We demonstrate this TF-induced mutagenesis mechanism using a yeast genetic assay that quantifies the accumulation of mutations in TF binding sites. Analyses of human cancer mutations recapitulate the trends observed in yeast, with mutations arising from MYC-bound mismatches being enriched in MMR-proficient cells. These findings implicate TF-MMR competition as a critical determinant of somatic hypermutation at TF binding sites in cancer. Furthermore, our results provide a molecular mechanism for the higher-than-expected rate of rare genetic variants at TF binding sites, with important implications for regulatory DNA evolution.

Keywords: DNA mismatch repair; DNA mutagenesis; DNA replication errors; MutSα; competition with mismatch repair; hypermutation; mutation patterns; mutations in transcription factor binding sites; transcription factors.

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Conflict of interest statement

Declaration of interests The authors declare no competing interests.

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