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Kelly, Gemma L; Grabow, Stephanie; Glaser, Stefan P; Fitzsimmons, Leah; Aubrey, Brandon J; Okamoto, Toru; Valente, Liz J; Robati, Mikara; Tai, Lin; Fairlie, W Douglas; Lee, Erinna F; Lindstrom, Mikael S; Wiman, Klas G; Huang, David C S; Bouillet, Philippe; Rowe, Martin; Rickinson, Alan B; Herold, Marco J; Strasser, Andreas
Genes & development, 2014-Jan-01, 2014-01-01, 20140101, 2014, Letnik: 28, Številka: 1Journal Article
The transcriptional regulator c-MYC is abnormally overexpressed in many human cancers. Evasion from apoptosis is critical for cancer development, particularly c-MYC-driven cancers. We explored which anti-apoptotic BCL-2 family member (expressed under endogenous regulation) is essential to sustain c-MYC-driven lymphoma growth to reveal which should be targeted for cancer therapy. Remarkably, inducible Cre-mediated deletion of even a single Mcl-1 allele substantially impaired the growth of c-MYC-driven mouse lymphomas. Mutations in p53 could diminish but not obviate the dependency of c-MYC-driven mouse lymphomas on MCL-1. Importantly, targeting of MCL-1 killed c-MYC-driven human Burkitt lymphoma cells, even those bearing mutations in p53. Given that loss of one allele of Mcl-1 is well tolerated in healthy tissues, our results suggest that therapeutic targeting of MCL-1 would be an attractive therapeutic strategy for MYC-driven cancers.
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in: SICRIS
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