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A novel phosphatidylinositol 3-kinase (PI3K) inhibitor directs a potent FOXO-dependent, p53-independent cell cycle arrest phenotype characterized by the differential induction of a subset of FOXO-regulated genes

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dc.contributor.authorHill, Richard
dc.contributor.authorKalathur, Ravi Kiran Reddy
dc.contributor.authorCallejas, Sergio
dc.contributor.authorColaço, Laura
dc.contributor.authorBrandão, Ricardo
dc.contributor.authorSerelde, Beatriz
dc.contributor.authorCebriá, Antonio
dc.contributor.authorBlanco-Aparicio, Carmen
dc.contributor.authorPastor Fernandez, Joaquin
dc.contributor.authorFutschik, Matthias
dc.contributor.authorDopazo, Ana
dc.contributor.authorLink, Wolfgang
dc.contributor.funderFundação para a Ciência e Tecnologia (Portugal)
dc.date.accessioned2019-04-29T08:06:56Z
dc.date.available2019-04-29T08:06:56Z
dc.date.issued2014-12-09
dc.description.abstractINTRODUCTION: The activation of the phosphoinositide 3-kinase (PI3K)/AKT signalling pathway is one the most frequent genetic events in breast cancer, consequently the development of PI3K inhibitors has attracted much attention. Here we evaluate the effect of PI3K inhibition on global gene expression in breast cancer cells. METHODS: We used a range of methodologies that include in silico compound analysis, in vitro kinase assays, cell invasion assays, proliferation assays, genome-wide transcription studies (Agilent Technologies full genome arrays), gene set enrichment analysis, quantitative real-time PCR, immunoblotting in addition to chromatin immunoprecipitation. RESULTS: We defined the physico-chemical and the biological properties of ETP-45658, a novel potent PI3K inhibitor. We demonstrated that ETP-45658 potently inhibited cell proliferation within a broad range of human cancer cells, most potently suppressing the growth of breast cancer cells via inhibiting cell cycle. We show that this response is Forkhead box O (FOXO) protein dependent and p53 independent. Our genome-wide microarray analysis revealed that the cell cycle was the most affected biological process after exposure to ETP-45658 (or our control PI3K inhibitor PI-103), that despite the multiple transcription factors that are regulated by the PI3K/AKT signalling cascade, only the binding sites for FOXO transcription factors were significantly enriched and only a subset of all FOXO-dependent genes were induced. This disparity in gene transcription was not due to differential FOXO promoter recruitment. CONCLUSIONS: The constitutive activation of PI3Ks and thus the exclusion of FOXO transcription factors from the nucleus is a key feature of breast cancer. Our results presented here highlight that PI3K inhibition activates specific FOXO-dependent genes that mediate cell cycle arrest in breast cancer cells.es_ES
dc.description.peerreviewedes_ES
dc.description.sponsorshipR Hill is the recipient of a Fundação para a Ciência e a Tecnologia (FCT) 2012 research grant n° SFRH/BPD/84634/2012. R Kalathur is the recipient of a Fundação para a Ciência e a Tecnologia (FCT) research grant n° SFRH/BPD/70718/2010. We thank B. Vogelstein (Johns Hopkins University, Baltimore, USA) for our [p53−/−] HCT116 cell line.es_ES
dc.format.number6es_ES
dc.format.page482es_ES
dc.format.volume16es_ES
dc.identifier.citationBreast Cancer Res. 2014; 16(6):482es_ES
dc.identifier.doi10.1186/s13058-014-0482-yes_ES
dc.identifier.e-issn1465-542Xes_ES
dc.identifier.issn1465-542Xes_ES
dc.identifier.journalBreast cancer research : BCRes_ES
dc.identifier.pubmedID25488803es_ES
dc.identifier.urihttp://hdl.handle.net/20.500.12105/7524
dc.language.isoenges_ES
dc.publisherBioMed Central (BMC)
dc.relation.publisherversionhttps://doi.org/10.1186/s13058-014-0482-yes_ES
dc.repisalud.institucionCNICes_ES
dc.repisalud.orgCNICCNIC::Unidades técnicas::Genómicaes_ES
dc.rights.accessRightsopen accesses_ES
dc.rights.licenseAtribución 4.0 Internacional*
dc.rights.urihttp://creativecommons.org/licenses/by/4.0/*
dc.subject.meshCell Cycle Checkpointses_ES
dc.subject.meshCell Line, Tumores_ES
dc.subject.meshCell Proliferationes_ES
dc.subject.meshComputer Simulationes_ES
dc.subject.meshFemalees_ES
dc.subject.meshForkhead Transcription Factorses_ES
dc.subject.meshHCT116 Cellses_ES
dc.subject.meshHumanses_ES
dc.subject.meshIn Vitro Techniqueses_ES
dc.subject.meshMCF-7 Cellses_ES
dc.subject.meshPhosphatidylinositol 3-Kinasees_ES
dc.subject.meshProto-Oncogene Proteins c-aktes_ES
dc.subject.meshPyrazoleses_ES
dc.subject.meshPyrimidineses_ES
dc.subject.meshReal-Time Polymerase Chain Reactiones_ES
dc.subject.meshSignal Transductiones_ES
dc.subject.meshAdenocarcinomaes_ES
dc.subject.meshBreast Neoplasmses_ES
dc.titleA novel phosphatidylinositol 3-kinase (PI3K) inhibitor directs a potent FOXO-dependent, p53-independent cell cycle arrest phenotype characterized by the differential induction of a subset of FOXO-regulated geneses_ES
dc.typejournal articlees_ES
dc.type.hasVersionVoRes_ES
dspace.entity.typePublication
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