| Literature DB >> 31618628 |
Thomas Botton1, Eric Talevich2, Vivek Kumar Mishra2, Tongwu Zhang3, A Hunter Shain2, Céline Berquet2, Alexander Gagnon2, Robert L Judson4, Robert Ballotti5, Antoni Ribas6, Meenhard Herlyn7, Stéphane Rocchi5, Kevin M Brown3, Nicholas K Hayward8, Iwei Yeh2, Boris C Bastian9.
Abstract
BRAF fusions are detected in numerous neoplasms, but their clinical management remains unresolved. We identified six melanoma lines harboring BRAF fusions representative of the clinical cases reported in the literature. Their unexpected heterogeneous responses to RAF and MEK inhibitors could be categorized upon specific features of the fusion kinases. Higher expression level correlated with resistance, and fusion partners containing a dimerization domain promoted paradoxical activation of the mitogen-activated protein kinase (MAPK) pathway and hyperproliferation in response to first- and second-generation RAF inhibitors. By contrast, next-generation αC-IN/DFG-OUT RAF inhibitors blunted paradoxical activation across all lines and had their therapeutic efficacy further increased in vitro and in vivo by combination with MEK inhibitors, opening perspectives in the clinical management of tumors harboring BRAF fusions.Entities:
Keywords: BRAF fusion; MEK inhibitor; RAF inhibitor; kinase; melanoma; paradoxical activation; pre-clinical; rearrangement; sequencing; translocation
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Year: 2019 PMID: 31618628 PMCID: PMC6939448 DOI: 10.1016/j.celrep.2019.09.009
Source DB: PubMed Journal: Cell Rep Impact factor: 9.423