Pharmacological targeting of the mitochondrial calcium-dependent potassium channel KCa3.1 triggers cell death and reduces tumor growth and metastasis in vivo

Ion channels are non-conventional, druggable oncological targets. The intermediate-conductance calcium-dependent potassium channel (K(Ca)3.1) is highly expressed in the plasma membrane and in the inner mitochondrial membrane (mitoK(Ca)3.1) of various cancer cell lines. The role mitoK(Ca)3.1 plays in...

Descripción completa

Detalles Bibliográficos
Autores principales: Bachmann, Magdalena, Rossa, Andrea, Varanita, Tatiana, Fioretti, Bernard, Biasutto, Lucia, Milenkovic, Stefan, Checchetto, Vanessa, Peruzzo, Roberta, Ahmad, Syed A., Patel, Sameer H., Lukowski, Robert, Edwards, Michael J., Ceccarelli, Matteo, Gulbins, Erich, Zoratti, Mario, Mattarei, Andrea, Szabo, Ildiko
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Nature Publishing Group UK 2022
Materias:
Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9768205/
https://www.ncbi.nlm.nih.gov/pubmed/36539400
http://dx.doi.org/10.1038/s41419-022-05463-8
_version_ 1784854116158144512
author Bachmann, Magdalena
Rossa, Andrea
Varanita, Tatiana
Fioretti, Bernard
Biasutto, Lucia
Milenkovic, Stefan
Checchetto, Vanessa
Peruzzo, Roberta
Ahmad, Syed A.
Patel, Sameer H.
Lukowski, Robert
Edwards, Michael J.
Ceccarelli, Matteo
Gulbins, Erich
Zoratti, Mario
Mattarei, Andrea
Szabo, Ildiko
author_facet Bachmann, Magdalena
Rossa, Andrea
Varanita, Tatiana
Fioretti, Bernard
Biasutto, Lucia
Milenkovic, Stefan
Checchetto, Vanessa
Peruzzo, Roberta
Ahmad, Syed A.
Patel, Sameer H.
Lukowski, Robert
Edwards, Michael J.
Ceccarelli, Matteo
Gulbins, Erich
Zoratti, Mario
Mattarei, Andrea
Szabo, Ildiko
author_sort Bachmann, Magdalena
collection PubMed
description Ion channels are non-conventional, druggable oncological targets. The intermediate-conductance calcium-dependent potassium channel (K(Ca)3.1) is highly expressed in the plasma membrane and in the inner mitochondrial membrane (mitoK(Ca)3.1) of various cancer cell lines. The role mitoK(Ca)3.1 plays in cancer cells is still undefined. Here we report the synthesis and characterization of two mitochondria-targeted novel derivatives of a high-affinity K(Ca)3.1 antagonist, TRAM-34, which retain the ability to block channel activity. The effects of these drugs were tested in melanoma, pancreatic ductal adenocarcinoma and breast cancer lines, as well as in vivo in two orthotopic models. We show that the mitochondria-targeted TRAM-34 derivatives induce release of mitochondrial reactive oxygen species, rapid depolarization of the mitochondrial membrane, fragmentation of the mitochondrial network. They trigger cancer cell death with an EC(50) in the µM range, depending on channel expression. In contrast, inhibition of the plasma membrane K(Ca)3.1 by membrane-impermeant Maurotoxin is without effect, indicating a specific role of mitoK(Ca)3.1 in determining cell fate. At sub-lethal concentrations, pharmacological targeting of mitoK(Ca)3.1 significantly reduced cancer cell migration by enhancing production of mitochondrial reactive oxygen species and nuclear factor-κB (NF-κB) activation, and by downregulating expression of Bcl-2 Nineteen kD-Interacting Protein (BNIP-3) and of Rho GTPase CDC-42. This signaling cascade finally leads to cytoskeletal reorganization and impaired migration. Overexpression of BNIP-3 or pharmacological modulation of NF-κB and CDC-42 prevented the migration-reducing effect of mitoTRAM-34. In orthotopic models of melanoma and pancreatic ductal adenocarcinoma, the tumors at sacrifice were 60% smaller in treated versus untreated animals. Metastasis of melanoma cells to lymph nodes was also drastically reduced. No signs of toxicity were observed. In summary, our results identify mitochondrial K(Ca)3.1 as an unexpected player in cancer cell migration and show that its pharmacological targeting is efficient against both tumor growth and metastatic spread in vivo.
format Online
Article
Text
id pubmed-9768205
institution National Center for Biotechnology Information
language English
publishDate 2022
publisher Nature Publishing Group UK
record_format MEDLINE/PubMed
spelling pubmed-97682052022-12-22 Pharmacological targeting of the mitochondrial calcium-dependent potassium channel KCa3.1 triggers cell death and reduces tumor growth and metastasis in vivo Bachmann, Magdalena Rossa, Andrea Varanita, Tatiana Fioretti, Bernard Biasutto, Lucia Milenkovic, Stefan Checchetto, Vanessa Peruzzo, Roberta Ahmad, Syed A. Patel, Sameer H. Lukowski, Robert Edwards, Michael J. Ceccarelli, Matteo Gulbins, Erich Zoratti, Mario Mattarei, Andrea Szabo, Ildiko Cell Death Dis Article Ion channels are non-conventional, druggable oncological targets. The intermediate-conductance calcium-dependent potassium channel (K(Ca)3.1) is highly expressed in the plasma membrane and in the inner mitochondrial membrane (mitoK(Ca)3.1) of various cancer cell lines. The role mitoK(Ca)3.1 plays in cancer cells is still undefined. Here we report the synthesis and characterization of two mitochondria-targeted novel derivatives of a high-affinity K(Ca)3.1 antagonist, TRAM-34, which retain the ability to block channel activity. The effects of these drugs were tested in melanoma, pancreatic ductal adenocarcinoma and breast cancer lines, as well as in vivo in two orthotopic models. We show that the mitochondria-targeted TRAM-34 derivatives induce release of mitochondrial reactive oxygen species, rapid depolarization of the mitochondrial membrane, fragmentation of the mitochondrial network. They trigger cancer cell death with an EC(50) in the µM range, depending on channel expression. In contrast, inhibition of the plasma membrane K(Ca)3.1 by membrane-impermeant Maurotoxin is without effect, indicating a specific role of mitoK(Ca)3.1 in determining cell fate. At sub-lethal concentrations, pharmacological targeting of mitoK(Ca)3.1 significantly reduced cancer cell migration by enhancing production of mitochondrial reactive oxygen species and nuclear factor-κB (NF-κB) activation, and by downregulating expression of Bcl-2 Nineteen kD-Interacting Protein (BNIP-3) and of Rho GTPase CDC-42. This signaling cascade finally leads to cytoskeletal reorganization and impaired migration. Overexpression of BNIP-3 or pharmacological modulation of NF-κB and CDC-42 prevented the migration-reducing effect of mitoTRAM-34. In orthotopic models of melanoma and pancreatic ductal adenocarcinoma, the tumors at sacrifice were 60% smaller in treated versus untreated animals. Metastasis of melanoma cells to lymph nodes was also drastically reduced. No signs of toxicity were observed. In summary, our results identify mitochondrial K(Ca)3.1 as an unexpected player in cancer cell migration and show that its pharmacological targeting is efficient against both tumor growth and metastatic spread in vivo. Nature Publishing Group UK 2022-12-20 /pmc/articles/PMC9768205/ /pubmed/36539400 http://dx.doi.org/10.1038/s41419-022-05463-8 Text en © The Author(s) 2022 https://creativecommons.org/licenses/by/4.0/Open Access This article is licensed under a Creative Commons Attribution 4.0 International License, which permits use, sharing, adaptation, distribution and reproduction in any medium or format, as long as you give appropriate credit to the original author(s) and the source, provide a link to the Creative Commons license, and indicate if changes were made. The images or other third party material in this article are included in the article’s Creative Commons license, unless indicated otherwise in a credit line to the material. If material is not included in the article’s Creative Commons license and your intended use is not permitted by statutory regulation or exceeds the permitted use, you will need to obtain permission directly from the copyright holder. To view a copy of this license, visit http://creativecommons.org/licenses/by/4.0/ (https://creativecommons.org/licenses/by/4.0/) .
spellingShingle Article
Bachmann, Magdalena
Rossa, Andrea
Varanita, Tatiana
Fioretti, Bernard
Biasutto, Lucia
Milenkovic, Stefan
Checchetto, Vanessa
Peruzzo, Roberta
Ahmad, Syed A.
Patel, Sameer H.
Lukowski, Robert
Edwards, Michael J.
Ceccarelli, Matteo
Gulbins, Erich
Zoratti, Mario
Mattarei, Andrea
Szabo, Ildiko
Pharmacological targeting of the mitochondrial calcium-dependent potassium channel KCa3.1 triggers cell death and reduces tumor growth and metastasis in vivo
title Pharmacological targeting of the mitochondrial calcium-dependent potassium channel KCa3.1 triggers cell death and reduces tumor growth and metastasis in vivo
title_full Pharmacological targeting of the mitochondrial calcium-dependent potassium channel KCa3.1 triggers cell death and reduces tumor growth and metastasis in vivo
title_fullStr Pharmacological targeting of the mitochondrial calcium-dependent potassium channel KCa3.1 triggers cell death and reduces tumor growth and metastasis in vivo
title_full_unstemmed Pharmacological targeting of the mitochondrial calcium-dependent potassium channel KCa3.1 triggers cell death and reduces tumor growth and metastasis in vivo
title_short Pharmacological targeting of the mitochondrial calcium-dependent potassium channel KCa3.1 triggers cell death and reduces tumor growth and metastasis in vivo
title_sort pharmacological targeting of the mitochondrial calcium-dependent potassium channel kca3.1 triggers cell death and reduces tumor growth and metastasis in vivo
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9768205/
https://www.ncbi.nlm.nih.gov/pubmed/36539400
http://dx.doi.org/10.1038/s41419-022-05463-8
work_keys_str_mv AT bachmannmagdalena pharmacologicaltargetingofthemitochondrialcalciumdependentpotassiumchannelkca31triggerscelldeathandreducestumorgrowthandmetastasisinvivo
AT rossaandrea pharmacologicaltargetingofthemitochondrialcalciumdependentpotassiumchannelkca31triggerscelldeathandreducestumorgrowthandmetastasisinvivo
AT varanitatatiana pharmacologicaltargetingofthemitochondrialcalciumdependentpotassiumchannelkca31triggerscelldeathandreducestumorgrowthandmetastasisinvivo
AT fiorettibernard pharmacologicaltargetingofthemitochondrialcalciumdependentpotassiumchannelkca31triggerscelldeathandreducestumorgrowthandmetastasisinvivo
AT biasuttolucia pharmacologicaltargetingofthemitochondrialcalciumdependentpotassiumchannelkca31triggerscelldeathandreducestumorgrowthandmetastasisinvivo
AT milenkovicstefan pharmacologicaltargetingofthemitochondrialcalciumdependentpotassiumchannelkca31triggerscelldeathandreducestumorgrowthandmetastasisinvivo
AT checchettovanessa pharmacologicaltargetingofthemitochondrialcalciumdependentpotassiumchannelkca31triggerscelldeathandreducestumorgrowthandmetastasisinvivo
AT peruzzoroberta pharmacologicaltargetingofthemitochondrialcalciumdependentpotassiumchannelkca31triggerscelldeathandreducestumorgrowthandmetastasisinvivo
AT ahmadsyeda pharmacologicaltargetingofthemitochondrialcalciumdependentpotassiumchannelkca31triggerscelldeathandreducestumorgrowthandmetastasisinvivo
AT patelsameerh pharmacologicaltargetingofthemitochondrialcalciumdependentpotassiumchannelkca31triggerscelldeathandreducestumorgrowthandmetastasisinvivo
AT lukowskirobert pharmacologicaltargetingofthemitochondrialcalciumdependentpotassiumchannelkca31triggerscelldeathandreducestumorgrowthandmetastasisinvivo
AT edwardsmichaelj pharmacologicaltargetingofthemitochondrialcalciumdependentpotassiumchannelkca31triggerscelldeathandreducestumorgrowthandmetastasisinvivo
AT ceccarellimatteo pharmacologicaltargetingofthemitochondrialcalciumdependentpotassiumchannelkca31triggerscelldeathandreducestumorgrowthandmetastasisinvivo
AT gulbinserich pharmacologicaltargetingofthemitochondrialcalciumdependentpotassiumchannelkca31triggerscelldeathandreducestumorgrowthandmetastasisinvivo
AT zorattimario pharmacologicaltargetingofthemitochondrialcalciumdependentpotassiumchannelkca31triggerscelldeathandreducestumorgrowthandmetastasisinvivo
AT mattareiandrea pharmacologicaltargetingofthemitochondrialcalciumdependentpotassiumchannelkca31triggerscelldeathandreducestumorgrowthandmetastasisinvivo
AT szaboildiko pharmacologicaltargetingofthemitochondrialcalciumdependentpotassiumchannelkca31triggerscelldeathandreducestumorgrowthandmetastasisinvivo

Ejemplares similares