Mitochondrial biogenesis is required for the anchorage-independent survival and propagation of stem-like cancer cells

Here, we show that new mitochondrial biogenesis is required for the anchorage independent survival and propagation of cancer stem-like cells (CSCs). More specifically, we used the drug XCT790 as an investigational tool, as it functions as a specific inhibitor of the ERRα-PGC1 signaling pathway, whic...

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Autores principales: De Luca, Arianna, Fiorillo, Marco, Peiris-Pagès, Maria, Ozsvari, Bela, Smith, Duncan L., Sanchez-Alvarez, Rosa, Martinez-Outschoorn, Ubaldo E., Cappello, Anna Rita, Pezzi, Vincenzo, Lisanti, Michael P., Sotgia, Federica
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Impact Journals LLC 2015
Materias:
Priority Research Paper
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4558115/
https://www.ncbi.nlm.nih.gov/pubmed/26087310
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author De Luca, Arianna
Fiorillo, Marco
Peiris-Pagès, Maria
Ozsvari, Bela
Smith, Duncan L.
Sanchez-Alvarez, Rosa
Martinez-Outschoorn, Ubaldo E.
Cappello, Anna Rita
Pezzi, Vincenzo
Lisanti, Michael P.
Sotgia, Federica
author_facet De Luca, Arianna
Fiorillo, Marco
Peiris-Pagès, Maria
Ozsvari, Bela
Smith, Duncan L.
Sanchez-Alvarez, Rosa
Martinez-Outschoorn, Ubaldo E.
Cappello, Anna Rita
Pezzi, Vincenzo
Lisanti, Michael P.
Sotgia, Federica
author_sort De Luca, Arianna
collection PubMed
description Here, we show that new mitochondrial biogenesis is required for the anchorage independent survival and propagation of cancer stem-like cells (CSCs). More specifically, we used the drug XCT790 as an investigational tool, as it functions as a specific inhibitor of the ERRα-PGC1 signaling pathway, which governs mitochondrial biogenesis. Interestingly, our results directly demonstrate that XCT790 efficiently blocks both the survival and propagation of tumor initiating stem-like cells (TICs), using the MCF7 cell line as a model system. Mechanistically, we show that XCT790 suppresses the activity of several independent signaling pathways that are normally required for the survival of CSCs, such as Sonic hedgehog, TGFβ-SMAD, STAT3, and Wnt signaling. We also show that XCT790 markedly reduces oxidative mitochondrial metabolism (OXPHOS) and that XCT790-mediated inhibition of CSC propagation can be prevented or reversed by Acetyl-L-Carnitine (ALCAR), a mitochondrial fuel. Consistent with our findings, over-expression of ERRα significantly enhances the efficiency of mammosphere formation, which can be blocked by treatment with mitochondrial inhibitors. Similarly, mammosphere formation augmented by FOXM1, a downstream target of Wnt/β-catenin signaling, can also be blocked by treatment with three different classes of mitochondrial inhibitors (XCT790, oligomycin A, or doxycycline). In this context, our unbiased proteomics analysis reveals that FOXM1 drives the expression of >90 protein targets associated with mitochondrial biogenesis, glycolysis, the EMT and protein synthesis in MCF7 cells, processes which are characteristic of an anabolic CSC phenotype. Finally, doxycycline is an FDA-approved antibiotic, which is very well-tolerated in patients. As such, doxycycline could be re-purposed clinically as a ‘safe’ mitochondrial inhibitor, to target FOXM1 and mitochondrial biogenesis in CSCs, to prevent tumor recurrence and distant metastasis, thereby avoiding patient relapse.
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spelling pubmed-45581152015-09-09 Mitochondrial biogenesis is required for the anchorage-independent survival and propagation of stem-like cancer cells De Luca, Arianna Fiorillo, Marco Peiris-Pagès, Maria Ozsvari, Bela Smith, Duncan L. Sanchez-Alvarez, Rosa Martinez-Outschoorn, Ubaldo E. Cappello, Anna Rita Pezzi, Vincenzo Lisanti, Michael P. Sotgia, Federica Oncotarget Priority Research Paper Here, we show that new mitochondrial biogenesis is required for the anchorage independent survival and propagation of cancer stem-like cells (CSCs). More specifically, we used the drug XCT790 as an investigational tool, as it functions as a specific inhibitor of the ERRα-PGC1 signaling pathway, which governs mitochondrial biogenesis. Interestingly, our results directly demonstrate that XCT790 efficiently blocks both the survival and propagation of tumor initiating stem-like cells (TICs), using the MCF7 cell line as a model system. Mechanistically, we show that XCT790 suppresses the activity of several independent signaling pathways that are normally required for the survival of CSCs, such as Sonic hedgehog, TGFβ-SMAD, STAT3, and Wnt signaling. We also show that XCT790 markedly reduces oxidative mitochondrial metabolism (OXPHOS) and that XCT790-mediated inhibition of CSC propagation can be prevented or reversed by Acetyl-L-Carnitine (ALCAR), a mitochondrial fuel. Consistent with our findings, over-expression of ERRα significantly enhances the efficiency of mammosphere formation, which can be blocked by treatment with mitochondrial inhibitors. Similarly, mammosphere formation augmented by FOXM1, a downstream target of Wnt/β-catenin signaling, can also be blocked by treatment with three different classes of mitochondrial inhibitors (XCT790, oligomycin A, or doxycycline). In this context, our unbiased proteomics analysis reveals that FOXM1 drives the expression of >90 protein targets associated with mitochondrial biogenesis, glycolysis, the EMT and protein synthesis in MCF7 cells, processes which are characteristic of an anabolic CSC phenotype. Finally, doxycycline is an FDA-approved antibiotic, which is very well-tolerated in patients. As such, doxycycline could be re-purposed clinically as a ‘safe’ mitochondrial inhibitor, to target FOXM1 and mitochondrial biogenesis in CSCs, to prevent tumor recurrence and distant metastasis, thereby avoiding patient relapse. Impact Journals LLC 2015-06-09 /pmc/articles/PMC4558115/ /pubmed/26087310 Text en Copyright: © 2015 De Luca et al. http://creativecommons.org/licenses/by/2.5/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
spellingShingle Priority Research Paper
De Luca, Arianna
Fiorillo, Marco
Peiris-Pagès, Maria
Ozsvari, Bela
Smith, Duncan L.
Sanchez-Alvarez, Rosa
Martinez-Outschoorn, Ubaldo E.
Cappello, Anna Rita
Pezzi, Vincenzo
Lisanti, Michael P.
Sotgia, Federica
Mitochondrial biogenesis is required for the anchorage-independent survival and propagation of stem-like cancer cells
title Mitochondrial biogenesis is required for the anchorage-independent survival and propagation of stem-like cancer cells
title_full Mitochondrial biogenesis is required for the anchorage-independent survival and propagation of stem-like cancer cells
title_fullStr Mitochondrial biogenesis is required for the anchorage-independent survival and propagation of stem-like cancer cells
title_full_unstemmed Mitochondrial biogenesis is required for the anchorage-independent survival and propagation of stem-like cancer cells
title_short Mitochondrial biogenesis is required for the anchorage-independent survival and propagation of stem-like cancer cells
title_sort mitochondrial biogenesis is required for the anchorage-independent survival and propagation of stem-like cancer cells
topic Priority Research Paper
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4558115/
https://www.ncbi.nlm.nih.gov/pubmed/26087310
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