E2F1-Associated Purine Synthesis Pathway Is a Major Component of the MET-DNA Damage Response Network.

Michaela Poliaková Turan Rahel Riedo Matúš Medo Chiara Pozzato Manja Friese-Hamim Jonas Paul Koch Si'Ana A Coggins Qun Li Baek Kim Joachim Albers Daniel Matthias Aebersold Nicola Zamboni Yitzhak Zimmer Michaela Medová

Published in: Cancer research communications (2024)

Maintenance of genome stability prevents disease and affiliates with growth factor receptor tyrosine kinases. We identified de novo purine synthesis as a pathway in which key enzymatic players are regulated through MET receptor and whose depletion via MET targeting explains MET inhibition-associated formation of DNA double-strand breaks. The mechanistic importance of MET inhibition-dependent E2F1 downregulation for interference with DNA integrity has translational implications for MET-targeting-based treatment of malignancies.

Keyphrases

tyrosine kinase
growth factor
dna damage response
circulating tumor
cancer therapy
cell free
cell proliferation
single molecule
signaling pathway
transcription factor
dna damage
dna repair
nucleic acid
binding protein