1313361-51-1Relevant articles and documents
Discovery of dihydroisoquinolinone derivatives as novel inhibitors of the p53-MDM2 interaction with a distinct binding mode
Gessier, Fran?ois,Kallen, Joerg,Jacoby, Edgar,Chène, Patrick,Stachyra-Valat, Thérèse,Ruetz, Stephan,Jeay, Sébastien,Holzer, Philipp,Masuya, Keiichi,Furet, Pascal
, p. 3621 - 3625 (2015/08/11)
Blocking the interaction between the p53 tumor suppressor and its regulatory protein MDM2 is a promising therapeutic concept under current investigation in oncology drug research. We report here the discovery of the first representatives of a new class of small molecule inhibitors of this protein-protein interaction: the dihydroisoquinolinones. Starting from an initial hit identified by virtual screening, a derivatization program has resulted in compound 11, a low nanomolar inhibitor of the p53-MDM2 interaction showing significant cellular activity. Initially based on a binding mode hypothesis, this effort was then guided by a X-ray co-crystal structure of MDM2 in complex with one of the synthesized analogs. The X-ray structure revealed an unprecedented binding mode for p53-MDM2 inhibitors.