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BPTF is required for c-MYC transcriptional activity and in vivo tumorigenesis.


ABSTRACT: c-MYC oncogene is deregulated in most human tumours. Histone marks associated with transcriptionally active genes define high-affinity c-MYC targets. The mechanisms involved in their recognition by c-MYC are unknown. Here we report that c-MYC interacts with BPTF, a core subunit of the NURF chromatin-remodelling complex. BPTF is required for the activation of the full c-MYC transcriptional programme in fibroblasts. BPTF knockdown leads to decreased c-MYC recruitment to DNA and changes in chromatin accessibility. In Bptf-null MEFs, BPTF is necessary for c-MYC-driven proliferation, G1-S progression and replication stress, but not for c-MYC-driven apoptosis. Bioinformatics analyses unveil that BPTF levels correlate positively with c-MYC-driven transcriptional signatures. In vivo, Bptf inactivation in pre-neoplastic pancreatic acinar cells significantly delays tumour development and extends survival. Our findings uncover BPTF as a crucial c-MYC co-factor required for its biological activity and suggest that the BPTF-c-MYC axis is a potential therapeutic target in cancer.

SUBMITTER: Richart L 

PROVIDER: S-EPMC4728380 | biostudies-literature | 2016 Jan

REPOSITORIES: biostudies-literature

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BPTF is required for c-MYC transcriptional activity and in vivo tumorigenesis.

Richart Laia L   Carrillo-de Santa Pau Enrique E   Río-Machín Ana A   de Andrés Mónica P MP   Cigudosa Juan C JC   Lobo Víctor J Sánchez-Arévalo VJS   Real Francisco X FX  

Nature communications 20160105


c-MYC oncogene is deregulated in most human tumours. Histone marks associated with transcriptionally active genes define high-affinity c-MYC targets. The mechanisms involved in their recognition by c-MYC are unknown. Here we report that c-MYC interacts with BPTF, a core subunit of the NURF chromatin-remodelling complex. BPTF is required for the activation of the full c-MYC transcriptional programme in fibroblasts. BPTF knockdown leads to decreased c-MYC recruitment to DNA and changes in chromati  ...[more]

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