Genome-wide CRISPR-Cas9 screens identify mechanisms of BET bromodomain inhibitor sensitivity

被引:7
作者
Estoppey, David [1 ]
Schutzius, Gabi [1 ]
Kolter, Christian [1 ]
Salathe, Adrian [1 ]
Wunderlin, Tiffany [1 ]
Meyer, Amandine [1 ]
Nigsch, Florian [1 ]
Bouwmeester, Tewis [1 ]
Hoepfner, Dominic [1 ]
Kirkland, Susan [1 ]
机构
[1] Novartis Inst Biomed Res, CH-4056 Basel, Switzerland
来源
ISCIENCE | 2021年 / 24卷 / 11期
关键词
HUMAN-CELLS; SELECTIVE-INHIBITION; SYNTHETIC LETHAL; MANGANESE; CANCER; MAPK; ABNORMALITIES; EXPRESSION; PACLITAXEL; RESISTANCE;
D O I
10.1016/j.isci.2021.103323
中图分类号
O [数理科学和化学]; P [天文学、地球科学]; Q [生物科学]; N [自然科学总论];
学科分类号
07 ; 0710 ; 09 ;
摘要
BET bromodomain inhibitors hold promise as therapeutic agents in diverse indications, but their clinical progression has been challenging and none have received regulatory approval. Early clinical trials in cancer have shown heterogeneous clinical responses, development of resistance, and adverse events. Increased understanding of their mechanism(s) of action and identification of biomarkers are needed to identify appropriate indication(s) and achieve efficacious dosing. Using genome-wide CRISPR-Cas9 screens at different concentrations, we report molecular mechanisms defining cellular responses to BET inhibitors, some of which appear specific to a single compound concentration. We identify multiple transcrirgonal regulators and mTOR pathway members as key determinants of JQ1 sensitivity and two Ca2+/Mn2+ transporters, ATP2C1 and TMEM165, as key determinants of JQ1 resistance. Our study reveals new molecular mediators of BET bromodomain inhibitor effects, suggests the involvement of manganese, and provides a rich resource for discovery of biomarkers and targets for combination therapies.
引用
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页数:24
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