| Literature DB >> 24584072 |
Birgit Knoechel1, Justine E Roderick2, Kaylyn E Williamson3, Jiang Zhu3, Jens G Lohr4, Matthew J Cotton3, Shawn M Gillespie3, Daniel Fernandez5, Manching Ku6, Hongfang Wang7, Federica Piccioni8, Serena J Silver8, Mohit Jain9, Daniel Pearson10, Michael J Kluk7, Christopher J Ott11, Leonard D Shultz12, Michael A Brehm13, Dale L Greiner13, Alejandro Gutierrez14, Kimberly Stegmaier14, Andrew L Kung14, David E Root8, James E Bradner4, Jon C Aster7, Michelle A Kelliher15, Bradley E Bernstein3.
Abstract
The identification of activating NOTCH1 mutations in T cell acute lymphoblastic leukemia (T-ALL) led to clinical testing of γ-secretase inhibitors (GSIs) that prevent NOTCH1 activation. However, responses to these inhibitors have been transient, suggesting that resistance limits their clinical efficacy. Here we modeled T-ALL resistance, identifying GSI-tolerant 'persister' cells that expand in the absence of NOTCH1 signaling. Rare persisters are already present in naive T-ALL populations, and the reversibility of their phenotype suggests an epigenetic mechanism. Relative to GSI-sensitive cells, persister cells activate distinct signaling and transcriptional programs and exhibit chromatin compaction. A knockdown screen identified chromatin regulators essential for persister viability, including BRD4. BRD4 binds enhancers near critical T-ALL genes, including MYC and BCL2. The BRD4 inhibitor JQ1 downregulates expression of these targets and induces growth arrest and apoptosis in persister cells, at doses well tolerated by GSI-sensitive cells. Consistently, the GSI-JQ1 combination was found to be effective against primary human leukemias in vivo. Our findings establish a role for epigenetic heterogeneity in leukemia resistance that may be addressed by incorporating epigenetic modulators in combination therapy.Entities:
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Year: 2014 PMID: 24584072 PMCID: PMC4086945 DOI: 10.1038/ng.2913
Source DB: PubMed Journal: Nat Genet ISSN: 1061-4036 Impact factor: 38.330