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Therapeutic potential of the metabolic modulator phenformin in targeting the stem cell compartment in melanoma

Melanoma is the most dangerous and treatment-resistant skin cancer. Tumor resistance and recurrence are due to the persistence in the patient of aggressive cells with stem cell features, the cancer stem cells (CSC). Recent evidences have shown that CSC display a distinct metabolic profile as compare...

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Autores principales: Petrachi, Tiziana, Romagnani, Alessandra, Albini, Adriana, Longo, Caterina, Argenziano, Giuseppe, Grisendi, Giulia, Dominici, Massimo, Ciarrocchi, Alessia, Dallaglio, Katiuscia
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Impact Journals LLC 2016
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5351679/
https://www.ncbi.nlm.nih.gov/pubmed/28036292
http://dx.doi.org/10.18632/oncotarget.14321
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author Petrachi, Tiziana
Romagnani, Alessandra
Albini, Adriana
Longo, Caterina
Argenziano, Giuseppe
Grisendi, Giulia
Dominici, Massimo
Ciarrocchi, Alessia
Dallaglio, Katiuscia
author_facet Petrachi, Tiziana
Romagnani, Alessandra
Albini, Adriana
Longo, Caterina
Argenziano, Giuseppe
Grisendi, Giulia
Dominici, Massimo
Ciarrocchi, Alessia
Dallaglio, Katiuscia
author_sort Petrachi, Tiziana
collection PubMed
description Melanoma is the most dangerous and treatment-resistant skin cancer. Tumor resistance and recurrence are due to the persistence in the patient of aggressive cells with stem cell features, the cancer stem cells (CSC). Recent evidences have shown that CSC display a distinct metabolic profile as compared to tumor bulk population: a promising anti-tumor strategy is therefore to target specific metabolic pathways driving CSC behavior. Biguanides (metformin and phenformin) are anti-diabetic drugs able to perturb cellular metabolism and displaying anti-cancer activity. However, their ability to target the CSC compartment in melanoma is not known. Here we show that phenformin, but not metformin, strongly reduces melanoma cell viability, growth and invasion in both 2D and 3D (spheroids) models. While phenformin decreases melanoma CSC markers expression and the levels of the pro-survival factor MITF, MITF overexpression fails to prevent phenformin effects. Phenformin significantly reduces cell viability in melanoma by targeting both CSC (ALDH(high)) and non-CSC cells and by significantly reducing the number of viable cells in ALDH(high) and ALDH(low)-derived spheroids. Consistently, phenformin reduces melanoma cell viability and growth independently from SOX2 levels. Our results show that phenformin is able to affect both CSC and non-CSC melanoma cell viability and growth and suggests its potential use as anti-cancer therapy in melanoma.
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spelling pubmed-53516792017-04-13 Therapeutic potential of the metabolic modulator phenformin in targeting the stem cell compartment in melanoma Petrachi, Tiziana Romagnani, Alessandra Albini, Adriana Longo, Caterina Argenziano, Giuseppe Grisendi, Giulia Dominici, Massimo Ciarrocchi, Alessia Dallaglio, Katiuscia Oncotarget Research Paper Melanoma is the most dangerous and treatment-resistant skin cancer. Tumor resistance and recurrence are due to the persistence in the patient of aggressive cells with stem cell features, the cancer stem cells (CSC). Recent evidences have shown that CSC display a distinct metabolic profile as compared to tumor bulk population: a promising anti-tumor strategy is therefore to target specific metabolic pathways driving CSC behavior. Biguanides (metformin and phenformin) are anti-diabetic drugs able to perturb cellular metabolism and displaying anti-cancer activity. However, their ability to target the CSC compartment in melanoma is not known. Here we show that phenformin, but not metformin, strongly reduces melanoma cell viability, growth and invasion in both 2D and 3D (spheroids) models. While phenformin decreases melanoma CSC markers expression and the levels of the pro-survival factor MITF, MITF overexpression fails to prevent phenformin effects. Phenformin significantly reduces cell viability in melanoma by targeting both CSC (ALDH(high)) and non-CSC cells and by significantly reducing the number of viable cells in ALDH(high) and ALDH(low)-derived spheroids. Consistently, phenformin reduces melanoma cell viability and growth independently from SOX2 levels. Our results show that phenformin is able to affect both CSC and non-CSC melanoma cell viability and growth and suggests its potential use as anti-cancer therapy in melanoma. Impact Journals LLC 2016-12-28 /pmc/articles/PMC5351679/ /pubmed/28036292 http://dx.doi.org/10.18632/oncotarget.14321 Text en Copyright: © 2017 Petrachi 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, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
spellingShingle Research Paper
Petrachi, Tiziana
Romagnani, Alessandra
Albini, Adriana
Longo, Caterina
Argenziano, Giuseppe
Grisendi, Giulia
Dominici, Massimo
Ciarrocchi, Alessia
Dallaglio, Katiuscia
Therapeutic potential of the metabolic modulator phenformin in targeting the stem cell compartment in melanoma
title Therapeutic potential of the metabolic modulator phenformin in targeting the stem cell compartment in melanoma
title_full Therapeutic potential of the metabolic modulator phenformin in targeting the stem cell compartment in melanoma
title_fullStr Therapeutic potential of the metabolic modulator phenformin in targeting the stem cell compartment in melanoma
title_full_unstemmed Therapeutic potential of the metabolic modulator phenformin in targeting the stem cell compartment in melanoma
title_short Therapeutic potential of the metabolic modulator phenformin in targeting the stem cell compartment in melanoma
title_sort therapeutic potential of the metabolic modulator phenformin in targeting the stem cell compartment in melanoma
topic Research Paper
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5351679/
https://www.ncbi.nlm.nih.gov/pubmed/28036292
http://dx.doi.org/10.18632/oncotarget.14321
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