| Literature DB >> 26267534 |
Ana Herrero1, Adán Pinto1, Paula Colón-Bolea1, Berta Casar1, Mary Jones2, Lorena Agudo-Ibáñez1, Rebeca Vidal3, Stephan P Tenbaum4, Paolo Nuciforo4, Elsa M Valdizán3, Zoltan Horvath5, Laszlo Orfi6, Antonio Pineda-Lucena7, Emilie Bony8, Gyorgy Keri9, Germán Rivas10, Angel Pazos3, Rafael Gozalbes11, Héctor G Palmer4, Adam Hurlstone12, Piero Crespo13.
Abstract
Nearly 50% of human malignancies exhibit unregulated RAS-ERK signaling; inhibiting it is a valid strategy for antineoplastic intervention. Upon activation, ERK dimerize, which is essential for ERK extranuclear, but not for nuclear, signaling. Here, we describe a small molecule inhibitor for ERK dimerization that, without affecting ERK phosphorylation, forestalls tumorigenesis driven by RAS-ERK pathway oncogenes. This compound is unaffected by resistance mechanisms that hamper classical RAS-ERK pathway inhibitors. Thus, ERK dimerization inhibitors provide the proof of principle for two understudied concepts in cancer therapy: (1) the blockade of sub-localization-specific sub-signals, rather than total signals, as a means of impeding oncogenic RAS-ERK signaling and (2) targeting regulatory protein-protein interactions, rather than catalytic activities, as an approach for producing effective antitumor agents.Entities:
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Year: 2015 PMID: 26267534 DOI: 10.1016/j.ccell.2015.07.001
Source DB: PubMed Journal: Cancer Cell ISSN: 1535-6108 Impact factor: 31.743