Serine-linked PARP1 auto-modification controls PARP inhibitor response
- Evgeniia Prokhorova
- Florian Zobel
- Rebecca Smith
- Siham Zentout
- Ian Gibbs-Seymour
- Kira Schützenhofer
- Alessandra Peters
- Joséphine Groslambert
- Valentina Zorzini
- Thomas Agnew
- John Brognard
- Michael L. Nielsen
- Dragana Ahel
- Sébastien Huet
- Marcin J. Suskiewicz
- Ivan Ahel
Publication date
July 2021
DOI Publisher
Springer Science and Business Media LLC Journal
Nature CommunicationsAbstract
PARP inhibitors function by trapping PARP1 protein on DNA breaks, which has cytotoxic consequences to cancer cells. Here the authors identify three serine residues within PARP1 as key sites whose efficient HPF1-dependent modification counters PARP1 trapping and contributes to inhibitor tolerance
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