| Literature DB >> 25216638 |
Ramona Rudalska1, Daniel Dauch1, Thomas Longerich2, Katherine McJunkin3, Torsten Wuestefeld4, Tae-Won Kang5, Anja Hohmeyer5, Marina Pesic4, Josef Leibold4, Anne von Thun6, Peter Schirmacher2, Johannes Zuber7, Karl-Heinz Weiss8, Scott Powers9, Nisar P Malek10, Martin Eilers6, Bence Sipos11, Scott W Lowe12, Robert Geffers13, Stefan Laufer14, Lars Zender5.
Abstract
In solid tumors, resistance to therapy inevitably develops upon treatment with cytotoxic drugs or molecularly targeted therapies. Here, we describe a system that enables pooled shRNA screening directly in mouse hepatocellular carcinomas (HCC) in vivo to identify genes likely to be involved in therapy resistance. Using a focused shRNA library targeting genes located within focal genomic amplifications of human HCC, we screened for genes whose inhibition increased the therapeutic efficacy of the multikinase inhibitor sorafenib. Both shRNA-mediated and pharmacological silencing of Mapk14 (p38α) were found to sensitize mouse HCC to sorafenib therapy and prolong survival by abrogating Mapk14-dependent activation of Mek-Erk and Atf2 signaling. Elevated Mapk14-Atf2 signaling predicted poor response to sorafenib therapy in human HCC, and sorafenib resistance of p-Mapk14-expressing HCC cells could be reverted by silencing Mapk14. Our results suggest that a combination of sorafenib and Mapk14 blockade is a promising approach to overcoming therapy resistance of human HCC.Entities:
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Year: 2014 PMID: 25216638 PMCID: PMC4587571 DOI: 10.1038/nm.3679
Source DB: PubMed Journal: Nat Med ISSN: 1078-8956 Impact factor: 53.440