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An Acquired Vulnerability of Drug-Resistant Melanoma with Therapeutic Potential.

Liqin Wang ,
Rodrigo Leite de Oliveira ,
Sanne Huijberts ,
Evert Bosdriesz ,
Nora Pencheva ,
Diede Brunen ,
Astrid Bosma ,
Ji-Ying Song ,
John Zevenhoven ,
G Tjitske Los-de Vries ,
Hugo Horlings ,
Bastiaan Nuijen ,
Jos H Beijnen ,
Jan H M Schellens ,
Rene Bernards

Abstract

BRAF(V600E) mutant melanomas treated with inhibitors of the BRAF and MEK kinases almost invariably develop resistance that is frequently caused by reactivation of the mitogen activated protein kinase (MAPK) pathway. To identify novel treatment options for such patients, we searched for acquired vulnerabilities of MAPK inhibitor-resistant melanomas. We find that resistance to BRAF+MEK inhibitors is associated with increased levels of reactive oxygen species (ROS). Subsequent treatment with the histone deacetylase inhibitor vorinostat suppresses SLC7A11, leading to a lethal increase in the already-elevated levels of ROS in drug-resistant cells. This causes selective apoptotic death of only the drug-resistant tumor cells. Consistently, treatment of BRAF inhibitor-resistant melanoma with vorinostat in mice results in dramatic tumor regression. In a study in patients with advanced BRAF+MEK inhibitor-resistant melanoma, we find that vorinostat can selectively ablate drug-resistant tumor cells, providing clinical proof of concept for the novel therapy identified here.

More about this publication

Cell

Volume 173
Issue nr. 6
Pages 1413-1425.e14
Publication date 31-05-2018

Full text links

Publisher website (DOI) 10.1016/j.cell.2018.04.012
Europe PubMed Central 29754815
Pubmed 29754815

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