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Switch of Voltage-Gated K(+) Channel Expression in the Plasma Membrane of Chondrogenic Cells Affects Cytosolic Ca(2+)-Oscillations and Cartilage Formation

BACKGROUND: Understanding the key elements of signaling of chondroprogenitor cells at the earliest steps of differentiation may substantially improve our opportunities for the application of mesenchymal stem cells in cartilage tissue engineering, which is a promising approach of regenerative therapy...

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Autores principales: Varga, Zoltan, Juhász, Tamás, Matta, Csaba, Fodor, János, Katona, Éva, Bartok, Adam, Oláh, Tamás, Sebe, Attila, Csernoch, László, Panyi, Gyorgy, Zákány, Róza
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2011
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3221679/
https://www.ncbi.nlm.nih.gov/pubmed/22132179
http://dx.doi.org/10.1371/journal.pone.0027957
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author Varga, Zoltan
Juhász, Tamás
Matta, Csaba
Fodor, János
Katona, Éva
Bartok, Adam
Oláh, Tamás
Sebe, Attila
Csernoch, László
Panyi, Gyorgy
Zákány, Róza
author_facet Varga, Zoltan
Juhász, Tamás
Matta, Csaba
Fodor, János
Katona, Éva
Bartok, Adam
Oláh, Tamás
Sebe, Attila
Csernoch, László
Panyi, Gyorgy
Zákány, Róza
author_sort Varga, Zoltan
collection PubMed
description BACKGROUND: Understanding the key elements of signaling of chondroprogenitor cells at the earliest steps of differentiation may substantially improve our opportunities for the application of mesenchymal stem cells in cartilage tissue engineering, which is a promising approach of regenerative therapy of joint diseases. Ion channels, membrane potential and Ca(2+)-signaling are important regulators of cell proliferation and differentiation. Our aim was to identify such plasma membrane ion channels involved in signaling during chondrogenesis, which may serve as specific molecular targets for influencing chondrogenic differentiation and ultimately cartilage formation. METHODOLOGY/PRINCIPAL FINDINGS: Using patch-clamp, RT-PCR and Western-blot experiments, we found that chondrogenic cells in primary micromass cell cultures obtained from embryonic chicken limb buds expressed voltage-gated Na(V)1.4, K(V)1.1, K(V)1.3 and K(V)4.1 channels, although K(V)1.3 was not detectable in the plasma membrane. Tetrodotoxin (TTX), the inhibitor of Na(V)1.4 channels, had no effect on cartilage formation. In contrast, presence of 20 mM of the K(+) channel blocker tetraethyl-ammonium (TEA) during the time-window of the final commitment of chondrogenic cells reduced K(V) currents (to 27±3% of control), cell proliferation (thymidine incorporation: to 39±4.4% of control), expression of cartilage-specific genes and consequently, cartilage formation (metachromasia: to 18.0±6.4% of control) and also depolarized the membrane potential (by 9.3±2.1 mV). High-frequency Ca(2+)-oscillations were also suppressed by 10 mM TEA (confocal microscopy: frequency to 8.5±2.6% of the control). Peak expression of TEA-sensitive K(V)1.1 in the plasma membrane overlapped with this period. Application of TEA to differentiated chondrocytes, mainly expressing the TEA-insensitive K(V)4.1 did not affect cartilage formation. CONCLUSIONS/SIGNIFICANCE: These data demonstrate that the differentiation and proliferation of chondrogenic cells depend on rapid Ca(2+)-oscillations, which are modulated by K(V)-driven membrane potential changes. K(V)1.1 function seems especially critical during the final commitment period. We show the critical role of voltage-gated cation channels in the differentiation of non-excitable cells with potential therapeutic use.
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spelling pubmed-32216792011-11-30 Switch of Voltage-Gated K(+) Channel Expression in the Plasma Membrane of Chondrogenic Cells Affects Cytosolic Ca(2+)-Oscillations and Cartilage Formation Varga, Zoltan Juhász, Tamás Matta, Csaba Fodor, János Katona, Éva Bartok, Adam Oláh, Tamás Sebe, Attila Csernoch, László Panyi, Gyorgy Zákány, Róza PLoS One Research Article BACKGROUND: Understanding the key elements of signaling of chondroprogenitor cells at the earliest steps of differentiation may substantially improve our opportunities for the application of mesenchymal stem cells in cartilage tissue engineering, which is a promising approach of regenerative therapy of joint diseases. Ion channels, membrane potential and Ca(2+)-signaling are important regulators of cell proliferation and differentiation. Our aim was to identify such plasma membrane ion channels involved in signaling during chondrogenesis, which may serve as specific molecular targets for influencing chondrogenic differentiation and ultimately cartilage formation. METHODOLOGY/PRINCIPAL FINDINGS: Using patch-clamp, RT-PCR and Western-blot experiments, we found that chondrogenic cells in primary micromass cell cultures obtained from embryonic chicken limb buds expressed voltage-gated Na(V)1.4, K(V)1.1, K(V)1.3 and K(V)4.1 channels, although K(V)1.3 was not detectable in the plasma membrane. Tetrodotoxin (TTX), the inhibitor of Na(V)1.4 channels, had no effect on cartilage formation. In contrast, presence of 20 mM of the K(+) channel blocker tetraethyl-ammonium (TEA) during the time-window of the final commitment of chondrogenic cells reduced K(V) currents (to 27±3% of control), cell proliferation (thymidine incorporation: to 39±4.4% of control), expression of cartilage-specific genes and consequently, cartilage formation (metachromasia: to 18.0±6.4% of control) and also depolarized the membrane potential (by 9.3±2.1 mV). High-frequency Ca(2+)-oscillations were also suppressed by 10 mM TEA (confocal microscopy: frequency to 8.5±2.6% of the control). Peak expression of TEA-sensitive K(V)1.1 in the plasma membrane overlapped with this period. Application of TEA to differentiated chondrocytes, mainly expressing the TEA-insensitive K(V)4.1 did not affect cartilage formation. CONCLUSIONS/SIGNIFICANCE: These data demonstrate that the differentiation and proliferation of chondrogenic cells depend on rapid Ca(2+)-oscillations, which are modulated by K(V)-driven membrane potential changes. K(V)1.1 function seems especially critical during the final commitment period. We show the critical role of voltage-gated cation channels in the differentiation of non-excitable cells with potential therapeutic use. Public Library of Science 2011-11-21 /pmc/articles/PMC3221679/ /pubmed/22132179 http://dx.doi.org/10.1371/journal.pone.0027957 Text en Varga 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, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Varga, Zoltan
Juhász, Tamás
Matta, Csaba
Fodor, János
Katona, Éva
Bartok, Adam
Oláh, Tamás
Sebe, Attila
Csernoch, László
Panyi, Gyorgy
Zákány, Róza
Switch of Voltage-Gated K(+) Channel Expression in the Plasma Membrane of Chondrogenic Cells Affects Cytosolic Ca(2+)-Oscillations and Cartilage Formation
title Switch of Voltage-Gated K(+) Channel Expression in the Plasma Membrane of Chondrogenic Cells Affects Cytosolic Ca(2+)-Oscillations and Cartilage Formation
title_full Switch of Voltage-Gated K(+) Channel Expression in the Plasma Membrane of Chondrogenic Cells Affects Cytosolic Ca(2+)-Oscillations and Cartilage Formation
title_fullStr Switch of Voltage-Gated K(+) Channel Expression in the Plasma Membrane of Chondrogenic Cells Affects Cytosolic Ca(2+)-Oscillations and Cartilage Formation
title_full_unstemmed Switch of Voltage-Gated K(+) Channel Expression in the Plasma Membrane of Chondrogenic Cells Affects Cytosolic Ca(2+)-Oscillations and Cartilage Formation
title_short Switch of Voltage-Gated K(+) Channel Expression in the Plasma Membrane of Chondrogenic Cells Affects Cytosolic Ca(2+)-Oscillations and Cartilage Formation
title_sort switch of voltage-gated k(+) channel expression in the plasma membrane of chondrogenic cells affects cytosolic ca(2+)-oscillations and cartilage formation
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3221679/
https://www.ncbi.nlm.nih.gov/pubmed/22132179
http://dx.doi.org/10.1371/journal.pone.0027957
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