CTBP1 and metabolic syndrome induce an mRNA and miRNA expression profile critical for breast cancer progression and metastasis

Metastatic breast cancer (BrCa) is still one of the main causes of cancer death in women. Metabolic syndrome (MeS), a risk factor for BrCa, is associated to high grade tumors, increased metastasis and recurrence of this disease. C-terminal binding protein 1 (CTBP1) is a co-repressor of tumor suppres...

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Autores principales: Farré, Paula L., Scalise, Georgina D., Duca, Rocío B., Dalton, Guillermo N., Massillo, Cintia, Porretti, Juliana, Graña, Karen, Gardner, Kevin, De Luca, Paola, De Siervi, Adriana
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Impact Journals LLC 2018
Materias:
Research Paper
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5862620/
https://www.ncbi.nlm.nih.gov/pubmed/29568399
http://dx.doi.org/10.18632/oncotarget.24486
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author Farré, Paula L.
Scalise, Georgina D.
Duca, Rocío B.
Dalton, Guillermo N.
Massillo, Cintia
Porretti, Juliana
Graña, Karen
Gardner, Kevin
De Luca, Paola
De Siervi, Adriana
author_facet Farré, Paula L.
Scalise, Georgina D.
Duca, Rocío B.
Dalton, Guillermo N.
Massillo, Cintia
Porretti, Juliana
Graña, Karen
Gardner, Kevin
De Luca, Paola
De Siervi, Adriana
author_sort Farré, Paula L.
collection PubMed
description Metastatic breast cancer (BrCa) is still one of the main causes of cancer death in women. Metabolic syndrome (MeS), a risk factor for BrCa, is associated to high grade tumors, increased metastasis and recurrence of this disease. C-terminal binding protein 1 (CTBP1) is a co-repressor of tumor suppressor genes that is activated by low NAD(+)/NADH ratio. Previously, we demonstrated that CTBP1 hyperactivation by MeS increased tumor growth in MDA-MB-231-derived xenografts regulating several genes and miRNAs. In this work, our aim was to elucidate the role of CTBP1 and MeS in BrCa metastasis. We found that CTBP1 protein diminished adhesion while increased migration of triple negative BrCa cells. CTBP1 and MeS modulated the expression of multiple genes (ITGB4, ITGB6, PRSS2, COL17A1 and FABP4) and miRNAs (miR-378a-3p, miR-146a-5p, let-7e-3p, miR-381-5p, miR-194-5p, miR-494-3p) involved in BrCa progression of MDA-MB-231-derived xenografts. Furthermore, we demonstrated that MeS increased lung micrometastasis and liver neoplastic disease in mice. CTBP1 hyperactivation seems to be critical for MeS effect on BrCa metastasis since CTBP1 depletion completely impaired the detection of circulating tumor cells. Our results highlight CTBP1 and MeS impact on BrCa progression positioning them as key properties to be considered for BrCa patient prognosis and management.
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spelling pubmed-58626202018-03-22 CTBP1 and metabolic syndrome induce an mRNA and miRNA expression profile critical for breast cancer progression and metastasis Farré, Paula L. Scalise, Georgina D. Duca, Rocío B. Dalton, Guillermo N. Massillo, Cintia Porretti, Juliana Graña, Karen Gardner, Kevin De Luca, Paola De Siervi, Adriana Oncotarget Research Paper Metastatic breast cancer (BrCa) is still one of the main causes of cancer death in women. Metabolic syndrome (MeS), a risk factor for BrCa, is associated to high grade tumors, increased metastasis and recurrence of this disease. C-terminal binding protein 1 (CTBP1) is a co-repressor of tumor suppressor genes that is activated by low NAD(+)/NADH ratio. Previously, we demonstrated that CTBP1 hyperactivation by MeS increased tumor growth in MDA-MB-231-derived xenografts regulating several genes and miRNAs. In this work, our aim was to elucidate the role of CTBP1 and MeS in BrCa metastasis. We found that CTBP1 protein diminished adhesion while increased migration of triple negative BrCa cells. CTBP1 and MeS modulated the expression of multiple genes (ITGB4, ITGB6, PRSS2, COL17A1 and FABP4) and miRNAs (miR-378a-3p, miR-146a-5p, let-7e-3p, miR-381-5p, miR-194-5p, miR-494-3p) involved in BrCa progression of MDA-MB-231-derived xenografts. Furthermore, we demonstrated that MeS increased lung micrometastasis and liver neoplastic disease in mice. CTBP1 hyperactivation seems to be critical for MeS effect on BrCa metastasis since CTBP1 depletion completely impaired the detection of circulating tumor cells. Our results highlight CTBP1 and MeS impact on BrCa progression positioning them as key properties to be considered for BrCa patient prognosis and management. Impact Journals LLC 2018-02-13 /pmc/articles/PMC5862620/ /pubmed/29568399 http://dx.doi.org/10.18632/oncotarget.24486 Text en Copyright: © 2018 Farré et al. http://creativecommons.org/licenses/by/3.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/3.0/) 3.0 (CC BY 3.0), which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
spellingShingle Research Paper
Farré, Paula L.
Scalise, Georgina D.
Duca, Rocío B.
Dalton, Guillermo N.
Massillo, Cintia
Porretti, Juliana
Graña, Karen
Gardner, Kevin
De Luca, Paola
De Siervi, Adriana
CTBP1 and metabolic syndrome induce an mRNA and miRNA expression profile critical for breast cancer progression and metastasis
title CTBP1 and metabolic syndrome induce an mRNA and miRNA expression profile critical for breast cancer progression and metastasis
title_full CTBP1 and metabolic syndrome induce an mRNA and miRNA expression profile critical for breast cancer progression and metastasis
title_fullStr CTBP1 and metabolic syndrome induce an mRNA and miRNA expression profile critical for breast cancer progression and metastasis
title_full_unstemmed CTBP1 and metabolic syndrome induce an mRNA and miRNA expression profile critical for breast cancer progression and metastasis
title_short CTBP1 and metabolic syndrome induce an mRNA and miRNA expression profile critical for breast cancer progression and metastasis
title_sort ctbp1 and metabolic syndrome induce an mrna and mirna expression profile critical for breast cancer progression and metastasis
topic Research Paper
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5862620/
https://www.ncbi.nlm.nih.gov/pubmed/29568399
http://dx.doi.org/10.18632/oncotarget.24486
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