posted on 2016-11-07, 11:51authored byS. J. Heidorn, C. Milagre, S. Whittaker, A. Nourry, I. Niculescu Duvas, I. Dhomen, Jahan Hussain, J. S. Reis Filho, C. J. Springer, Catrin Pritchard, R. Marais
We describe a mechanism of tumorigenesis mediated by kinase-dead BRAF in the presence of oncogenic RAS. We show that drugs that selectively inhibit BRAF drive RAS-dependent BRAF binding to CRAF, CRAF activation, and MEK–ERK signaling. This does not occur when oncogenic BRAF is inhibited, demonstrating that BRAF inhibition per se does not drive pathway activation; it only occurs when BRAF is inhibited in the presence of oncogenic RAS. Kinase-dead BRAF mimics the effects of the BRAF-selective drugs and kinase-dead Braf and oncogenic Ras cooperate to induce melanoma in mice. Our data reveal another paradigm of BRAF-mediated signaling that promotes tumor progression. They highlight the importance of understanding pathway signaling in clinical practice and of genotyping tumors prior to administering BRAF-selective drugs, to identify patients who are likely to respond and also to identify patients who may experience adverse effects.
Funding
The Institute of Cancer Research, Cancer Research UK (C107/A10433), and
the Wellcome Trust (080333/Z/06/Z) funded this work. J.S.R.-F. is funded in
part by Breakthrough Breast Cancer. We acknowledge NHS funding to the
NIHR Biomedical Research Centre.
History
Citation
Cell, 2010, 140 (2), pp. 209-221
Author affiliation
/Organisation/COLLEGE OF MEDICINE, BIOLOGICAL SCIENCES AND PSYCHOLOGY/School of Medicine/Department of Cancer Studies and Molecular Medicine
Supplemental Information includes Extended Experimental Procedures, four
figures, and three tables and can be found with this article online at doi:
10.1016/j.cell.2009.12.040.