|
|||||
|
|
Acquired resistance to BRAF inhibitors mediated by a RAF kinase switch in melanoma can be overcome by cotargeting MEK and IGF-1R/PI3K |
|
| Authors: | Villanueva Jessie Vultur Adina Lee John T Somasundaram Rajasekharan Fukunaga-Kalabis Mizuho Cipolla Angela K Wubbenhorst Bradley Xu Xiaowei Gimotty Phyllis A Kee Damien Santiago-Walker Ademi E Letrero Richard D'Andrea Kurt Pushparajan Anitha Hayden James E Brown Kimberly Dahlman Laquerre Sylvie McArthur Grant A Sosman Jeffrey A Nathanson Katherine L Herlyn Meenhard |
| Affiliation: | The Wistar Institute, Philadelphia, PA 19104, USA. |
| Abstract: | BRAF is an attractive target for melanoma drug development. However, resistance to BRAF inhibitors is a significant clinical challenge. We describe a model of resistance to BRAF inhibitors developed by chronic treatment of BRAF(V)???(E) melanoma cells with the BRAF inhibitor SB-590885; these cells are cross-resistant to other BRAF-selective inhibitors. Resistance involves flexible switching among the three RAF isoforms, underscoring the ability of melanoma cells to adapt to pharmacological challenges. IGF-1R/PI3K signaling was enhanced in resistant melanomas, and combined treatment with IGF-1R/PI3K and MEK inhibitors induced death of BRAF inhibitor-resistant cells. Increased IGF-1R and pAKT levels in a post-relapse human tumor sample are consistent with a role for IGF-1R/PI3K-dependent survival in the development of resistance to BRAF inhibitors. |
| Keywords: | |
| 本文献已被 PubMed 等数据库收录! | |