Nilotinib and MEK inhibitors induce synthetic lethality through paradoxical activation of RAF in drug-resistant chronic myeloid leukemia
| Data(s) |
2011
|
|---|---|
| Resumo |
We show that imatinib, nilotinib, and dasatinib possess weak off-target activity against RAF and, therefore, drive paradoxical activation of BRAF and CRAF in a RAS-dependent manner. Critically, because RAS is activated by BCR-ABL, in drug-resistant chronic myeloid leukemia (CML) cells, RAS activity persists in the presence of these drugs, driving paradoxical activation of BRAF, CRAF, MEK, and ERK, and leading to an unexpected dependency on the pathway. Consequently, nilotinib synergizes with MEK inhibitors to kill drug-resistant CML cells and block tumor growth in mice. Thus, we show that imatinib, nilotinib, and dasatinib drive paradoxical RAF/MEK/ERK pathway activation and have uncovered a synthetic lethal interaction that can be used to kill drug-resistant CML cells in vitro and in vivo. |
| Identificador | |
| Publicador |
Cell Press |
| Relação |
DOI:10.1016/j.ccr.2011.11.004 Packer, Leisl M., Rana, Sareena, Hayward, Robert, O'Hare, Thomas, Eide, Christopher A., Rebocho, Ana, Heidorn, Sonja, Zabriskie, Matthew S., Niculescu-Duvaz, Ion, Druker, Brian J., Springer, Caroline, & Marais, Richard (2011) Nilotinib and MEK inhibitors induce synthetic lethality through paradoxical activation of RAF in drug-resistant chronic myeloid leukemia. Cancer Cell, 20(6), pp. 715-727. |
| Fonte |
School of Biomedical Sciences; Faculty of Health; Institute of Health and Biomedical Innovation |
| Palavras-Chave | #110100 MEDICAL BIOCHEMISTRY AND METABOLOMICS #111205 Chemotherapy #2 (2 chloro 4 iodoanilino) n cyclopropylmethoxy 3,4 difluorobenzamide; B Raf kinase; dasatinib; imatinib; mitogen activated protein kinase; mitogen activated protein kinase kinase; nilotinib; Ras protein; animal experiment; animal model; article; chronic |
| Tipo |
Journal Article |
