Identification of PLX4032-resistance mechanisms and implications for novel RAF inhibitors

نویسندگان

  • Jaehyuk Choi
  • Sean F Landrette
  • Tiffany Wang
  • Perry Evans
  • Antonella Bacchiocchi
  • Robert Bjornson
  • Elaine Cheng
  • Amy L Stiegler
  • Symon Gathiaka
  • Orlando Acevedo
  • Titus J Boggon
  • Michael Krauthammer
  • Ruth Halaban
  • Tian Xu
چکیده

BRAF inhibitors improve melanoma patient survival, but resistance invariably develops. Here we report the discovery of a novel BRAF mutation that confers resistance to PLX4032 employing whole-exome sequencing of drug-resistant BRAF(V600K) melanoma cells. We further describe a new screening approach, a genome-wide piggyBac mutagenesis screen that revealed clinically relevant aberrations (N-terminal BRAF truncations and CRAF overexpression). The novel BRAF mutation, a Leu505 to His substitution (BRAF(L505H) ), is the first resistance-conferring second-site mutation identified in BRAF mutant cells. The mutation replaces a small nonpolar amino acid at the BRAF-PLX4032 interface with a larger polar residue. Moreover, we show that BRAF(L505H) , found in human prostate cancer, is itself a MAPK-activating, PLX4032-resistant oncogenic mutation. Lastly, we demonstrate that the PLX4032-resistant melanoma cells are sensitive to novel, next-generation BRAF inhibitors, especially the 'paradox-blocker' PLX8394, supporting its use in clinical trials for treatment of melanoma patients with BRAF-mutations.

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عنوان ژورنال:

دوره 27  شماره 

صفحات  -

تاریخ انتشار 2014