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Ca(2+)-sparks constitute elementary building blocks for global Ca(2+)-signals in myocytes of retinal arterioles

Spontaneous Ca(2+)-events were imaged in myocytes within intact retinal arterioles (diameter <40 μm) freshly isolated from rat eyes. Ca(2+)-sparks were often observed to spread across the width of these small cells, and could summate to produce prolonged Ca(2+)-oscillations and contraction. Appli...

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Autores principales: Tumelty, James, Scholfield, Norman, Stewart, Michael, Curtis, Tim, McGeown, Graham
Formato: Texto
Lenguaje:English
Publicado: Elsevier 2007
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2638024/
https://www.ncbi.nlm.nih.gov/pubmed/17027081
http://dx.doi.org/10.1016/j.ceca.2006.08.005
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author Tumelty, James
Scholfield, Norman
Stewart, Michael
Curtis, Tim
McGeown, Graham
author_facet Tumelty, James
Scholfield, Norman
Stewart, Michael
Curtis, Tim
McGeown, Graham
author_sort Tumelty, James
collection PubMed
description Spontaneous Ca(2+)-events were imaged in myocytes within intact retinal arterioles (diameter <40 μm) freshly isolated from rat eyes. Ca(2+)-sparks were often observed to spread across the width of these small cells, and could summate to produce prolonged Ca(2+)-oscillations and contraction. Application of cyclopiazonic acid (20 μM) transiently increased spark frequency and oscillation amplitude, but inhibited both sparks and oscillations within 60 s. Both ryanodine (100 μM) and tetracaine (100 μM) reduced the frequency of sparks and oscillations, while tetracaine also reduced oscillation amplitude. None of these interventions affected spark amplitude. Nifedipine, which blocks store filling independently of any action on L-type Ca(2+)-channels in these cells, reduced the frequency and amplitude of both sparks and oscillations. Removal of external [Ca(2+)] (1 mM EGTA) also reduced the frequency of sparks and oscillations but these reductions were slower in onset than those in the presence of tetracaine or cyclopiazonic acid. Cyclopiazonic acid, nifedipine and low external [Ca(2+)] all reduced SR loading, as indicated by the amplitude of caffeine evoked Ca(2+)-transients. This study demonstrates for the first time that spontaneous Ca(2+)-events in small arterioles of the eye result from activation of ryanodine receptors in the SR and suggests that this activation is not tightly coupled to Ca(2+)-influx. The data also supports a model in which Ca(2+)-sparks act as building blocks for more prolonged, global Ca(2+)-signals.
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spelling pubmed-26380242009-02-11 Ca(2+)-sparks constitute elementary building blocks for global Ca(2+)-signals in myocytes of retinal arterioles Tumelty, James Scholfield, Norman Stewart, Michael Curtis, Tim McGeown, Graham Cell Calcium Article Spontaneous Ca(2+)-events were imaged in myocytes within intact retinal arterioles (diameter <40 μm) freshly isolated from rat eyes. Ca(2+)-sparks were often observed to spread across the width of these small cells, and could summate to produce prolonged Ca(2+)-oscillations and contraction. Application of cyclopiazonic acid (20 μM) transiently increased spark frequency and oscillation amplitude, but inhibited both sparks and oscillations within 60 s. Both ryanodine (100 μM) and tetracaine (100 μM) reduced the frequency of sparks and oscillations, while tetracaine also reduced oscillation amplitude. None of these interventions affected spark amplitude. Nifedipine, which blocks store filling independently of any action on L-type Ca(2+)-channels in these cells, reduced the frequency and amplitude of both sparks and oscillations. Removal of external [Ca(2+)] (1 mM EGTA) also reduced the frequency of sparks and oscillations but these reductions were slower in onset than those in the presence of tetracaine or cyclopiazonic acid. Cyclopiazonic acid, nifedipine and low external [Ca(2+)] all reduced SR loading, as indicated by the amplitude of caffeine evoked Ca(2+)-transients. This study demonstrates for the first time that spontaneous Ca(2+)-events in small arterioles of the eye result from activation of ryanodine receptors in the SR and suggests that this activation is not tightly coupled to Ca(2+)-influx. The data also supports a model in which Ca(2+)-sparks act as building blocks for more prolonged, global Ca(2+)-signals. Elsevier 2007-05 /pmc/articles/PMC2638024/ /pubmed/17027081 http://dx.doi.org/10.1016/j.ceca.2006.08.005 Text en © 2007 Elsevier Ltd. https://creativecommons.org/licenses/by/3.0/ Open Access under CC BY 3.0 (https://creativecommons.org/licenses/by/3.0/) license
spellingShingle Article
Tumelty, James
Scholfield, Norman
Stewart, Michael
Curtis, Tim
McGeown, Graham
Ca(2+)-sparks constitute elementary building blocks for global Ca(2+)-signals in myocytes of retinal arterioles
title Ca(2+)-sparks constitute elementary building blocks for global Ca(2+)-signals in myocytes of retinal arterioles
title_full Ca(2+)-sparks constitute elementary building blocks for global Ca(2+)-signals in myocytes of retinal arterioles
title_fullStr Ca(2+)-sparks constitute elementary building blocks for global Ca(2+)-signals in myocytes of retinal arterioles
title_full_unstemmed Ca(2+)-sparks constitute elementary building blocks for global Ca(2+)-signals in myocytes of retinal arterioles
title_short Ca(2+)-sparks constitute elementary building blocks for global Ca(2+)-signals in myocytes of retinal arterioles
title_sort ca(2+)-sparks constitute elementary building blocks for global ca(2+)-signals in myocytes of retinal arterioles
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2638024/
https://www.ncbi.nlm.nih.gov/pubmed/17027081
http://dx.doi.org/10.1016/j.ceca.2006.08.005
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