Pharmacological activation of TRPV4 produces immediate cell damage and induction of apoptosis in human melanoma cells and HaCaT keratinocytes

BACKGROUND: TRPV4 channels are calcium-permeable cation channels that are activated by several physicochemical stimuli. Accordingly, TRPV4 channels have been implicated in the regulation of osmosensing, mechanotransduction, thermosensation, and epithelial/endothelial barrier functions. Whether TRPV4...

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Autores principales: Olivan-Viguera, Aida, Garcia-Otin, Angel Luis, Lozano-Gerona, Javier, Abarca-Lachen, Edgar, Garcia-Malinis, Ana J., Hamilton, Kirk L., Gilaberte, Yolanda, Pueyo, Esther, Köhler, Ralf
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2018
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Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5749757/
https://www.ncbi.nlm.nih.gov/pubmed/29293584
http://dx.doi.org/10.1371/journal.pone.0190307
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author Olivan-Viguera, Aida
Garcia-Otin, Angel Luis
Lozano-Gerona, Javier
Abarca-Lachen, Edgar
Garcia-Malinis, Ana J.
Hamilton, Kirk L.
Gilaberte, Yolanda
Pueyo, Esther
Köhler, Ralf
author_facet Olivan-Viguera, Aida
Garcia-Otin, Angel Luis
Lozano-Gerona, Javier
Abarca-Lachen, Edgar
Garcia-Malinis, Ana J.
Hamilton, Kirk L.
Gilaberte, Yolanda
Pueyo, Esther
Köhler, Ralf
author_sort Olivan-Viguera, Aida
collection PubMed
description BACKGROUND: TRPV4 channels are calcium-permeable cation channels that are activated by several physicochemical stimuli. Accordingly, TRPV4 channels have been implicated in the regulation of osmosensing, mechanotransduction, thermosensation, and epithelial/endothelial barrier functions. Whether TRPV4 is also mechanistically implicated in melanoma cell proliferation is not clear. Here, we hypothesized that TRPV4 is expressed in human melanoma and that pharmacological activation interferes with cell proliferation. METHODOLOGY/PRINCIPAL FINDINGS: TRPV4 functions were studied in melanoma cell lines (A375, SK-MEL-28, MKTBR), immortalized non-cancer keratinocytes (HaCaT), and murine 3T3 fibroblasts by patch-clamp, qRT-PCR, intracellular calcium measurements, cell proliferation, and flow cytometric assays of apoptosis and cell cycle. The selective TRPV4-activator, GSK1016790A, elicited non-selective cation currents with TRPV4-typical current-voltage-relationship in all cell lines. GSK1016790A-induced currents were blocked by the TRPV4-blocker, HC067047. TRPV4 mRNA expression was demonstrated by qRT-PCR. In A375 cells, TRPV4 activation was frequently paralleled by co-activation of calcium/calmodulin-regulated KCa3.1 channels. Light microscopy showed that TRPV4-activation produced rapid cellular disarrangement, nuclear densification, and detachment of a large fraction of all melanoma cell lines and HaCaT cells. TRPV4-activation induced apoptosis and drastically inhibited A375 and HaCaT proliferation that could be partially prevented by HC067047. CONCLUSIONS/SIGNIFICANCE: Our study showed that TRPV4 channels were functionally expressed in human melanoma cell lines and in human keratinocytes. Pharmacological TRPV4 activation in human melanoma cells and keratinocytes caused severe cellular disarrangement, necrosis and apoptosis. Pharmacological targeting of TRPV4 could be an alternative or adjuvant therapeutic strategy to treat melanoma progression and other proliferative skin disorders.
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spelling pubmed-57497572018-01-26 Pharmacological activation of TRPV4 produces immediate cell damage and induction of apoptosis in human melanoma cells and HaCaT keratinocytes Olivan-Viguera, Aida Garcia-Otin, Angel Luis Lozano-Gerona, Javier Abarca-Lachen, Edgar Garcia-Malinis, Ana J. Hamilton, Kirk L. Gilaberte, Yolanda Pueyo, Esther Köhler, Ralf PLoS One Research Article BACKGROUND: TRPV4 channels are calcium-permeable cation channels that are activated by several physicochemical stimuli. Accordingly, TRPV4 channels have been implicated in the regulation of osmosensing, mechanotransduction, thermosensation, and epithelial/endothelial barrier functions. Whether TRPV4 is also mechanistically implicated in melanoma cell proliferation is not clear. Here, we hypothesized that TRPV4 is expressed in human melanoma and that pharmacological activation interferes with cell proliferation. METHODOLOGY/PRINCIPAL FINDINGS: TRPV4 functions were studied in melanoma cell lines (A375, SK-MEL-28, MKTBR), immortalized non-cancer keratinocytes (HaCaT), and murine 3T3 fibroblasts by patch-clamp, qRT-PCR, intracellular calcium measurements, cell proliferation, and flow cytometric assays of apoptosis and cell cycle. The selective TRPV4-activator, GSK1016790A, elicited non-selective cation currents with TRPV4-typical current-voltage-relationship in all cell lines. GSK1016790A-induced currents were blocked by the TRPV4-blocker, HC067047. TRPV4 mRNA expression was demonstrated by qRT-PCR. In A375 cells, TRPV4 activation was frequently paralleled by co-activation of calcium/calmodulin-regulated KCa3.1 channels. Light microscopy showed that TRPV4-activation produced rapid cellular disarrangement, nuclear densification, and detachment of a large fraction of all melanoma cell lines and HaCaT cells. TRPV4-activation induced apoptosis and drastically inhibited A375 and HaCaT proliferation that could be partially prevented by HC067047. CONCLUSIONS/SIGNIFICANCE: Our study showed that TRPV4 channels were functionally expressed in human melanoma cell lines and in human keratinocytes. Pharmacological TRPV4 activation in human melanoma cells and keratinocytes caused severe cellular disarrangement, necrosis and apoptosis. Pharmacological targeting of TRPV4 could be an alternative or adjuvant therapeutic strategy to treat melanoma progression and other proliferative skin disorders. Public Library of Science 2018-01-02 /pmc/articles/PMC5749757/ /pubmed/29293584 http://dx.doi.org/10.1371/journal.pone.0190307 Text en © 2018 Olivan-Viguera et al 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 author and source are credited.
spellingShingle Research Article
Olivan-Viguera, Aida
Garcia-Otin, Angel Luis
Lozano-Gerona, Javier
Abarca-Lachen, Edgar
Garcia-Malinis, Ana J.
Hamilton, Kirk L.
Gilaberte, Yolanda
Pueyo, Esther
Köhler, Ralf
Pharmacological activation of TRPV4 produces immediate cell damage and induction of apoptosis in human melanoma cells and HaCaT keratinocytes
title Pharmacological activation of TRPV4 produces immediate cell damage and induction of apoptosis in human melanoma cells and HaCaT keratinocytes
title_full Pharmacological activation of TRPV4 produces immediate cell damage and induction of apoptosis in human melanoma cells and HaCaT keratinocytes
title_fullStr Pharmacological activation of TRPV4 produces immediate cell damage and induction of apoptosis in human melanoma cells and HaCaT keratinocytes
title_full_unstemmed Pharmacological activation of TRPV4 produces immediate cell damage and induction of apoptosis in human melanoma cells and HaCaT keratinocytes
title_short Pharmacological activation of TRPV4 produces immediate cell damage and induction of apoptosis in human melanoma cells and HaCaT keratinocytes
title_sort pharmacological activation of trpv4 produces immediate cell damage and induction of apoptosis in human melanoma cells and hacat keratinocytes
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5749757/
https://www.ncbi.nlm.nih.gov/pubmed/29293584
http://dx.doi.org/10.1371/journal.pone.0190307
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