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Parallel in vivo and in vitro melanoma RNAi dropout screens reveal synthetic lethality between hypoxia and DNA damage response inhibition.

Patricia A Possik ,
Judith Müller ,
Carmen Gerlach ,
Juliana C N Kenski ,
Xinyao Huang ,
Aida Shahrabi ,
Oscar Krijgsman ,
Ji-Ying Song ,
Marjon A Smit ,
Bram Gerritsen ,
Cor Lieftink ,
Kristel Kemper ,
Magali Michaut ,
Roderick L Beijersbergen ,
Lodewyk Wessels ,
Ton N Schumacher ,
Daniel S Peeper

Abstract

To identify factors preferentially necessary for driving tumor expansion, we performed parallel in vitro and in vivo negative-selection short hairpin RNA (shRNA) screens. Melanoma cells harboring shRNAs targeting several DNA damage response (DDR) kinases had a greater selective disadvantage in vivo than in vitro, indicating an essential contribution of these factors during tumor expansion. In growing tumors, DDR kinases were activated following hypoxia. Correspondingly, depletion or pharmacologic inhibition of DDR kinases was toxic to melanoma cells, including those that were resistant to BRAF inhibitor, and this could be enhanced by angiogenesis blockade. These results reveal that hypoxia sensitizes melanomas to targeted inhibition of the DDR and illustrate the utility of in vivo shRNA dropout screens for the identification of pharmacologically tractable targets.

More about this publication

Cell reports

Volume 9
Issue nr. 4
Pages 1375-86
Publication date 20-11-2014

Full text links

Publisher website (DOI) 10.1016/j.celrep.2014.10.024
Europe PubMed Central 25456132
Pubmed 25456132

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