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dc.contributor.authorFernández Calero, Tamara-
dc.contributor.authorDavyt Borthagaray, Marcos-
dc.contributor.authorPerelmuter, Karen-
dc.contributor.authorChalar, Cora-
dc.contributor.authorBampi, G.-
dc.contributor.authorPersson, H.-
dc.contributor.authorTosar Rovira, Juan Pablo-
dc.contributor.authorHafstað, V.-
dc.contributor.authorNaya Monteverde, Hugo Mario-
dc.contributor.authorRovira, Carlos-
dc.contributor.authorBollati-Fogolín, Mariela-
dc.contributor.authorEhrlich, Ricardo-
dc.contributor.authorFlouriot, Gilles-
dc.contributor.authorIgnatova, Z.-
dc.contributor.authorMarín Gutiérrez, Mónica-
dc.date.accessioned2022-05-31T13:08:04Z-
dc.date.available2022-05-31T13:08:04Z-
dc.date.issued2020-
dc.identifier.citationFernández-Calero, T, Davyt Borthagaray, M, Perelmuter, K, [y otros] "Fine-tuning the metabolic rewiring and adaptation of translational machinery during an epithelial-mesenchymal transition in breast cancer cells". Cancer and Metabolism. [en línea] 2020, 8: 8. 20 h. DOI: 10.1186/s40170-020-00216-7es
dc.identifier.issn2049-3002-
dc.identifier.urihttps://hdl.handle.net/20.500.12008/31741-
dc.description.abstractBackground: During breast cancer progression, the epithelial to mesenchymal transition has been associated with metastasis and endocrine therapy resistance; however, the underlying mechanisms remain elusive. To gain insight into this process, we studied the transition undergone by MCF7-derived cells, which is driven by the constitutive nuclear expression of a MKL1 variant devoid of the actin-binding domain (MKL1 ΔN200). We characterized the adaptive changes that occur during the MKL1-induced cellular model and focused on regulation of translation machinery and metabolic adaptation. Methods: We performed a genome-wide analysis at the transcriptional and translational level using ribosome profiling complemented with RNA-Seq and analyzed the expression of components of the translation machinery and enzymes involved in energy metabolism. NGS data were correlated with metabolomic measurements and quantification of specific mRNAs extracted from polysomes and western blots. Results: Our results reveal the expression profiles of a luminal to basal-like state in accordance with an epithelial to mesenchymal transition. During the transition, the synthesis of ribosomal proteins and that of many translational factors was upregulated. This overexpression of the translational machinery appears to be regulated at the translational level. Our results indicate an increase of ribosome biogenesis and translation activity. We detected an extensive metabolic rewiring occurring in an already “Warburg-like” context, in which enzyme isoform switches and metabolic shunts indicate a crucial role of HIF-1α along with other master regulatory factors. Furthermore, we detected a decrease in the expression of enzymes involved in ribonucleotide synthesis from the pentose phosphate pathway. During this transition, cells increase in size, downregulate genes associated with proliferation, and strongly upregulate expression of cytoskeletal and extracellular matrix genes.Conclusions: Our study reveals multiple regulatory events associated with metabolic and translational machinery adaptation during an epithelial mesenchymal-like transition process. During this major cellular transition, cells achieve a new homeostatic state ensuring their survival. This work shows that ribosome profiling complemented with RNA-Seq is a powerful approach to unveil in-depth global adaptive cellular responses and the interconnection among regulatory circuits, which will be helpful for identification of new therapeutic targetses
dc.format.extent20 h.es
dc.format.mimetypeapplication/pdfes
dc.language.isoenes
dc.publisherBMCes
dc.relation.ispartofCancer and Metabolism, 2020, 8: 8es
dc.rightsLas obras depositadas en el Repositorio se rigen por la Ordenanza de los Derechos de la Propiedad Intelectual de la Universidad de la República.(Res. Nº 91 de C.D.C. de 8/III/1994 – D.O. 7/IV/1994) y por la Ordenanza del Repositorio Abierto de la Universidad de la República (Res. Nº 16 de C.D.C. de 07/10/2014)es
dc.subjectBreast canceres
dc.subjectEMTes
dc.subjectLuminal to basal transitiones
dc.subjectMKL1/actin signaling pathwayes
dc.subjectMetabolism adaptationes
dc.subjectTranslation machineryes
dc.subjectRibosome profilinges
dc.subjectBreast cancer stem cellses
dc.titleFine-tuning the metabolic rewiring and adaptation of translational machinery during an epithelial-mesenchymal transition in breast cancer cellses
dc.typeArtículoes
dc.contributor.filiacionFernández Calero Tamara, Universidad de la República (Uruguay). Facultad de Ciencias. Instituto de Biología.-
dc.contributor.filiacionDavyt Borthagaray Marcos, Universidad de la República (Uruguay). Facultad de Ciencias. Instituto de Biología.-
dc.contributor.filiacionPerelmuter Karen, Instituto Pasteur (Montevideo).-
dc.contributor.filiacionChalar Cora, Universidad de la República (Uruguay). Facultad de Ciencias. Instituto de Biología.-
dc.contributor.filiacionBampi G.-
dc.contributor.filiacionPersson H.-
dc.contributor.filiacionTosar Rovira Juan Pablo, IUniversidad de la República (Uruguay). Facultad de Ciencias. Instituto de Biología.-
dc.contributor.filiacionHafstað V.-
dc.contributor.filiacionNaya Monteverde Hugo Mario, Instituto Pasteur (Montevideo).-
dc.contributor.filiacionRovira Carlos-
dc.contributor.filiacionBollati-Fogolín Mariela, InstitutoPasteur (Montevideo).-
dc.contributor.filiacionEhrlich Ricardo, Universidad de la República (Uruguay). Facultad de Ciencias. Instituto de Biología.-
dc.contributor.filiacionFlouriot Gilles-
dc.contributor.filiacionIgnatova Z.-
dc.contributor.filiacionMarín Gutiérrez Mónica, Universidad de la República (Uruguay). Facultad de Ciencias. Instituto de Biología.-
dc.rights.licenceLicencia Creative Commons Atribución (CC - By 4.0)es
dc.identifier.doi10.1186/s40170-020-00216-7-
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