AurkA inhibitors enhance the effects of B-RAF and MEK inhibitors in melanoma treatment

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BACKGROUND: Aurora kinase A (AurkA) is over-expressed in melanoma and its inhibition has been observed to limit tumor growth, suggesting a potential role in melanoma treatment. METHODS: A human melanoma cell line with the B-RAF (V600E) mutation (A375mel) was exposed to B-RAF inhibitor (GSK2118436),...

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Autores principales: Caputo, Emilia, Miceli, Roberta, Motti, Maria Letizia, Taté, Rosarita, Fratangelo, Federica, Botti, Gerardo, Mozzillo, Nicola, Carriero, Maria Vincenza, Cavalcanti, Ernesta, Palmieri, Giuseppe, Ciliberto, Gennaro, Pirozzi, Giuseppe, Ascierto, Paolo Antonio
Formato: Online Artículo Texto
Lenguaje:English
Publicado: BioMed Central 2014
Materias:
Research
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4237855/
https://www.ncbi.nlm.nih.gov/pubmed/25074438
http://dx.doi.org/10.1186/s12967-014-0216-z
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author Caputo, Emilia
Miceli, Roberta
Motti, Maria Letizia
Taté, Rosarita
Fratangelo, Federica
Botti, Gerardo
Mozzillo, Nicola
Carriero, Maria Vincenza
Cavalcanti, Ernesta
Palmieri, Giuseppe
Ciliberto, Gennaro
Pirozzi, Giuseppe
Ascierto, Paolo Antonio
author_facet Caputo, Emilia
Miceli, Roberta
Motti, Maria Letizia
Taté, Rosarita
Fratangelo, Federica
Botti, Gerardo
Mozzillo, Nicola
Carriero, Maria Vincenza
Cavalcanti, Ernesta
Palmieri, Giuseppe
Ciliberto, Gennaro
Pirozzi, Giuseppe
Ascierto, Paolo Antonio
author_sort Caputo, Emilia
collection PubMed
description BACKGROUND: Aurora kinase A (AurkA) is over-expressed in melanoma and its inhibition has been observed to limit tumor growth, suggesting a potential role in melanoma treatment. METHODS: A human melanoma cell line with the B-RAF (V600E) mutation (A375mel) was exposed to B-RAF inhibitor (GSK2118436), MEK inhibitor (GSK1120212) and AurkA inhibitor (MLN8054) as single agents or in various combinations (BRAF plus AurkA inhibitor, MEK plus AurkA inhibitor or triple combination BRAF plus MEK plus AurkA inhibitor). Cell proliferation was assessed using xCELLigence technology. Total protein extracts were examined for p53 and c-Myc protein expression by Western blot analysis. Drug anti-tumor effects were further assessed using a 3D-human melanoma skin reconstruction model, in which tissues were incubated with serum-free medium containing control, B-RAF plus MEK inhibitor, MEK plus AurkA inhibitor or the triple combination. RESULTS: AurkA inhibitor plus B-RAF inhibitor, AurkA inhibitor plus MEK inhibitor or triple combination had a markedly greater anti-proliferative effect on A375 (BRAFV600E) melanoma cells than single agents. In the 3D human skin model, the triple combination had a greater anti-tumor effect at the epidermal/dermal junction than control or either double combination. However, S-100 and Ki-67 positively stained spindle-shaped cells were detected in the dermal stratum, suggesting the presence of alive and proliferating melanoma cells. CONCLUSIONS: These findings provide new prospects for melanoma research, including combined B-RAF/AurkA inhibition for B-RAF mutated melanomas and MEK/AurkA inhibitor combination for patients without B-RAF mutations. Moreover, for the first time, we have shown that a B-RAF, MEK and AurkA inhibitor triple drug combination offers increased efficacy against melanoma cell growth and might be considered as a potential treatment strategy for enhancing clinical response in melanoma. However, although this triple drug combination was more effective at the epidermal/dermal junction, the suggested presence of alive and proliferating melanoma cells in the dermal stratum could result in drug resistance and disease recurrence. Molecular characterization of these dermal cells may be critical for the development of novel therapeutic strategies.
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spelling pubmed-42378552014-11-21 AurkA inhibitors enhance the effects of B-RAF and MEK inhibitors in melanoma treatment Caputo, Emilia Miceli, Roberta Motti, Maria Letizia Taté, Rosarita Fratangelo, Federica Botti, Gerardo Mozzillo, Nicola Carriero, Maria Vincenza Cavalcanti, Ernesta Palmieri, Giuseppe Ciliberto, Gennaro Pirozzi, Giuseppe Ascierto, Paolo Antonio J Transl Med Research BACKGROUND: Aurora kinase A (AurkA) is over-expressed in melanoma and its inhibition has been observed to limit tumor growth, suggesting a potential role in melanoma treatment. METHODS: A human melanoma cell line with the B-RAF (V600E) mutation (A375mel) was exposed to B-RAF inhibitor (GSK2118436), MEK inhibitor (GSK1120212) and AurkA inhibitor (MLN8054) as single agents or in various combinations (BRAF plus AurkA inhibitor, MEK plus AurkA inhibitor or triple combination BRAF plus MEK plus AurkA inhibitor). Cell proliferation was assessed using xCELLigence technology. Total protein extracts were examined for p53 and c-Myc protein expression by Western blot analysis. Drug anti-tumor effects were further assessed using a 3D-human melanoma skin reconstruction model, in which tissues were incubated with serum-free medium containing control, B-RAF plus MEK inhibitor, MEK plus AurkA inhibitor or the triple combination. RESULTS: AurkA inhibitor plus B-RAF inhibitor, AurkA inhibitor plus MEK inhibitor or triple combination had a markedly greater anti-proliferative effect on A375 (BRAFV600E) melanoma cells than single agents. In the 3D human skin model, the triple combination had a greater anti-tumor effect at the epidermal/dermal junction than control or either double combination. However, S-100 and Ki-67 positively stained spindle-shaped cells were detected in the dermal stratum, suggesting the presence of alive and proliferating melanoma cells. CONCLUSIONS: These findings provide new prospects for melanoma research, including combined B-RAF/AurkA inhibition for B-RAF mutated melanomas and MEK/AurkA inhibitor combination for patients without B-RAF mutations. Moreover, for the first time, we have shown that a B-RAF, MEK and AurkA inhibitor triple drug combination offers increased efficacy against melanoma cell growth and might be considered as a potential treatment strategy for enhancing clinical response in melanoma. However, although this triple drug combination was more effective at the epidermal/dermal junction, the suggested presence of alive and proliferating melanoma cells in the dermal stratum could result in drug resistance and disease recurrence. Molecular characterization of these dermal cells may be critical for the development of novel therapeutic strategies. BioMed Central 2014-07-31 /pmc/articles/PMC4237855/ /pubmed/25074438 http://dx.doi.org/10.1186/s12967-014-0216-z Text en Copyright © 2014 Caputo et al.; licensee BioMed Central Ltd. http://creativecommons.org/licenses/by/4.0 This is an Open Access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/4.0), which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly credited. The Creative Commons Public Domain Dedication waiver (http://creativecommons.org/publicdomain/zero/1.0/) applies to the data made available in this article, unless otherwise stated.
spellingShingle Research
Caputo, Emilia
Miceli, Roberta
Motti, Maria Letizia
Taté, Rosarita
Fratangelo, Federica
Botti, Gerardo
Mozzillo, Nicola
Carriero, Maria Vincenza
Cavalcanti, Ernesta
Palmieri, Giuseppe
Ciliberto, Gennaro
Pirozzi, Giuseppe
Ascierto, Paolo Antonio
AurkA inhibitors enhance the effects of B-RAF and MEK inhibitors in melanoma treatment
title AurkA inhibitors enhance the effects of B-RAF and MEK inhibitors in melanoma treatment
title_full AurkA inhibitors enhance the effects of B-RAF and MEK inhibitors in melanoma treatment
title_fullStr AurkA inhibitors enhance the effects of B-RAF and MEK inhibitors in melanoma treatment
title_full_unstemmed AurkA inhibitors enhance the effects of B-RAF and MEK inhibitors in melanoma treatment
title_short AurkA inhibitors enhance the effects of B-RAF and MEK inhibitors in melanoma treatment
title_sort aurka inhibitors enhance the effects of b-raf and mek inhibitors in melanoma treatment
topic Research
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4237855/
https://www.ncbi.nlm.nih.gov/pubmed/25074438
http://dx.doi.org/10.1186/s12967-014-0216-z
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