Dihydropyridine Receptors as Voltage Sensors for a Depolarization-evoked, IP(3)R-mediated, Slow Calcium Signal in Skeletal Muscle Cells

The dihydropyridine receptor (DHPR), normally a voltage-dependent calcium channel, functions in skeletal muscle essentially as a voltage sensor, triggering intracellular calcium release for excitation-contraction coupling. In addition to this fast calcium release, via ryanodine receptor (RYR) channe...

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Autores principales: Araya, Roberto, Liberona, José L., Cárdenas, J. César, Riveros, Nora, Estrada, Manuel, Powell, Jeanne A., Carrasco, M. Angélica, Jaimovich, Enrique
Formato: Texto
Lenguaje:English
Publicado: The Rockefeller University Press 2003
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Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2217318/
https://www.ncbi.nlm.nih.gov/pubmed/12508050
http://dx.doi.org/10.1085/jgp.20028671
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author Araya, Roberto
Liberona, José L.
Cárdenas, J. César
Riveros, Nora
Estrada, Manuel
Powell, Jeanne A.
Carrasco, M. Angélica
Jaimovich, Enrique
author_facet Araya, Roberto
Liberona, José L.
Cárdenas, J. César
Riveros, Nora
Estrada, Manuel
Powell, Jeanne A.
Carrasco, M. Angélica
Jaimovich, Enrique
author_sort Araya, Roberto
collection PubMed
description The dihydropyridine receptor (DHPR), normally a voltage-dependent calcium channel, functions in skeletal muscle essentially as a voltage sensor, triggering intracellular calcium release for excitation-contraction coupling. In addition to this fast calcium release, via ryanodine receptor (RYR) channels, depolarization of skeletal myotubes evokes slow calcium waves, unrelated to contraction, that involve the cell nucleus (Jaimovich, E., R. Reyes, J.L. Liberona, and J.A. Powell. 2000. Am. J. Physiol. Cell Physiol. 278:C998–C1010). We tested the hypothesis that DHPR may also be the voltage sensor for these slow calcium signals. In cultures of primary rat myotubes, 10 μM nifedipine (a DHPR inhibitor) completely blocked the slow calcium (fluo-3-fluorescence) transient after 47 mM K(+) depolarization and only partially reduced the fast Ca(2+) signal. Dysgenic myotubes from the GLT cell line, which do not express the α(1) subunit of the DHPR, did not show either type of calcium transient following depolarization. After transfection of the α(1) DNA into the GLT cells, K(+) depolarization induced slow calcium transients that were similar to those present in normal C(2)C(12) and normal NLT cell lines. Slow calcium transients in transfected cells were blocked by nifedipine as well as by the G protein inhibitor, pertussis toxin, but not by ryanodine, the RYR inhibitor. Since slow Ca(2+) transients appear to be mediated by IP(3), we measured the increase of IP(3) mass after K(+) depolarization. The IP(3) transient seen in control cells was inhibited by nifedipine and was absent in nontransfected dysgenic cells, but α(1)-transfected cells recovered the depolarization-induced IP(3) transient. In normal myotubes, 10 μM nifedipine, but not ryanodine, inhibited c-jun and c-fos mRNA increase after K(+) depolarization. These results suggest a role for DHPR-mediated calcium signals in regulation of early gene expression. A model of excitation-transcription coupling is presented in which both G proteins and IP(3) appear as important downstream mediators after sensing of depolarization by DHPR.
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spelling pubmed-22173182008-04-16 Dihydropyridine Receptors as Voltage Sensors for a Depolarization-evoked, IP(3)R-mediated, Slow Calcium Signal in Skeletal Muscle Cells Araya, Roberto Liberona, José L. Cárdenas, J. César Riveros, Nora Estrada, Manuel Powell, Jeanne A. Carrasco, M. Angélica Jaimovich, Enrique J Gen Physiol Article The dihydropyridine receptor (DHPR), normally a voltage-dependent calcium channel, functions in skeletal muscle essentially as a voltage sensor, triggering intracellular calcium release for excitation-contraction coupling. In addition to this fast calcium release, via ryanodine receptor (RYR) channels, depolarization of skeletal myotubes evokes slow calcium waves, unrelated to contraction, that involve the cell nucleus (Jaimovich, E., R. Reyes, J.L. Liberona, and J.A. Powell. 2000. Am. J. Physiol. Cell Physiol. 278:C998–C1010). We tested the hypothesis that DHPR may also be the voltage sensor for these slow calcium signals. In cultures of primary rat myotubes, 10 μM nifedipine (a DHPR inhibitor) completely blocked the slow calcium (fluo-3-fluorescence) transient after 47 mM K(+) depolarization and only partially reduced the fast Ca(2+) signal. Dysgenic myotubes from the GLT cell line, which do not express the α(1) subunit of the DHPR, did not show either type of calcium transient following depolarization. After transfection of the α(1) DNA into the GLT cells, K(+) depolarization induced slow calcium transients that were similar to those present in normal C(2)C(12) and normal NLT cell lines. Slow calcium transients in transfected cells were blocked by nifedipine as well as by the G protein inhibitor, pertussis toxin, but not by ryanodine, the RYR inhibitor. Since slow Ca(2+) transients appear to be mediated by IP(3), we measured the increase of IP(3) mass after K(+) depolarization. The IP(3) transient seen in control cells was inhibited by nifedipine and was absent in nontransfected dysgenic cells, but α(1)-transfected cells recovered the depolarization-induced IP(3) transient. In normal myotubes, 10 μM nifedipine, but not ryanodine, inhibited c-jun and c-fos mRNA increase after K(+) depolarization. These results suggest a role for DHPR-mediated calcium signals in regulation of early gene expression. A model of excitation-transcription coupling is presented in which both G proteins and IP(3) appear as important downstream mediators after sensing of depolarization by DHPR. The Rockefeller University Press 2003-01 /pmc/articles/PMC2217318/ /pubmed/12508050 http://dx.doi.org/10.1085/jgp.20028671 Text en Copyright © 2003, The Rockefeller University Press This article is distributed under the terms of an Attribution–Noncommercial–Share Alike–No Mirror Sites license for the first six months after the publication date (see http://www.rupress.org/terms). After six months it is available under a Creative Commons License (Attribution–Noncommercial–Share Alike 4.0 Unported license, as described at http://creativecommons.org/licenses/by-nc-sa/4.0/).
spellingShingle Article
Araya, Roberto
Liberona, José L.
Cárdenas, J. César
Riveros, Nora
Estrada, Manuel
Powell, Jeanne A.
Carrasco, M. Angélica
Jaimovich, Enrique
Dihydropyridine Receptors as Voltage Sensors for a Depolarization-evoked, IP(3)R-mediated, Slow Calcium Signal in Skeletal Muscle Cells
title Dihydropyridine Receptors as Voltage Sensors for a Depolarization-evoked, IP(3)R-mediated, Slow Calcium Signal in Skeletal Muscle Cells
title_full Dihydropyridine Receptors as Voltage Sensors for a Depolarization-evoked, IP(3)R-mediated, Slow Calcium Signal in Skeletal Muscle Cells
title_fullStr Dihydropyridine Receptors as Voltage Sensors for a Depolarization-evoked, IP(3)R-mediated, Slow Calcium Signal in Skeletal Muscle Cells
title_full_unstemmed Dihydropyridine Receptors as Voltage Sensors for a Depolarization-evoked, IP(3)R-mediated, Slow Calcium Signal in Skeletal Muscle Cells
title_short Dihydropyridine Receptors as Voltage Sensors for a Depolarization-evoked, IP(3)R-mediated, Slow Calcium Signal in Skeletal Muscle Cells
title_sort dihydropyridine receptors as voltage sensors for a depolarization-evoked, ip(3)r-mediated, slow calcium signal in skeletal muscle cells
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2217318/
https://www.ncbi.nlm.nih.gov/pubmed/12508050
http://dx.doi.org/10.1085/jgp.20028671
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