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High-resolution mapping of DNA alkylation damage and base excision repair at yeast transcription factor binding sites

Authors :
Smitha Sivapragasam
Mingrui Duan
Gregory M.K. Poon
Jacob S. Antony
John J. Wyrick
John M. Hinz
Jenna Ulibarri
Peng Mao
Publication Year :
2021
Publisher :
Cold Spring Harbor Laboratory, 2021.

Abstract

DNA base damage arises frequently in living cells and needs to be removed by base excision repair (BER) to prevent mutagenesis and genome instability. Both the formation and repair of base damage occur in chromatin and are conceivably affected by DNA-binding proteins such as transcription factors (TFs). However, to what extent TF binding affects base damage distribution and BER in cells is unclear. Here, we used a genome-wide damage mapping method, N-methylpurine-sequencing (NMP-seq), to characterize alkylation damage distribution and BER at TF binding sites in yeast cells treated with the alkylating agent methyl methanesulfonate (MMS). Our data shows that alkylation damage formation was mainly suppressed at the binding sites of yeast TFs Abf1 and Reb1, but individual hotspots with elevated damage levels were also found. Additionally, Abf1 and Reb1 binding strongly inhibits BER in vivo and in vitro, causing slow repair both within the core motif and its adjacent DNA. The observed effects are caused by the TF-DNA interaction, because damage formation and BER can be restored by depletion of Abf1 or Reb1 protein from the nucleus. Thus, our data reveal that TF binding significantly modulates alkylation base damage formation and inhibits repair by the BER pathway. The interplay between base damage formation and BER may play an important role in affecting mutation frequency in gene regulatory regions.

Details

Database :
OpenAIRE
Accession number :
edsair.doi...........f0a2673bf9b0b94a24dce873dc11a2de
Full Text :
https://doi.org/10.1101/2021.09.24.461700