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Ultradian Cortisol Pulsatility Encodes a Distinct, Biologically Important Signal

CONTEXT: Cortisol is released in ultradian pulses. The biological relevance of the resulting fluctuating cortisol concentration has not been explored. OBJECTIVE: Determination of the biological consequences of ultradian cortisol pulsatility. DESIGN: A novel flow through cell culture system was devel...

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Autores principales: McMaster, Andrew, Jangani, Maryam, Sommer, Paula, Han, Namshik, Brass, Andy, Beesley, Stephen, Lu, Weiqun, Berry, Andrew, Loudon, Andrew, Donn, Rachelle, Ray, David W.
Formato: Texto
Lenguaje:English
Publicado: Public Library of Science 2011
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3022879/
https://www.ncbi.nlm.nih.gov/pubmed/21267416
http://dx.doi.org/10.1371/journal.pone.0015766
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author McMaster, Andrew
Jangani, Maryam
Sommer, Paula
Han, Namshik
Brass, Andy
Beesley, Stephen
Lu, Weiqun
Berry, Andrew
Loudon, Andrew
Donn, Rachelle
Ray, David W.
author_facet McMaster, Andrew
Jangani, Maryam
Sommer, Paula
Han, Namshik
Brass, Andy
Beesley, Stephen
Lu, Weiqun
Berry, Andrew
Loudon, Andrew
Donn, Rachelle
Ray, David W.
author_sort McMaster, Andrew
collection PubMed
description CONTEXT: Cortisol is released in ultradian pulses. The biological relevance of the resulting fluctuating cortisol concentration has not been explored. OBJECTIVE: Determination of the biological consequences of ultradian cortisol pulsatility. DESIGN: A novel flow through cell culture system was developed to deliver ultradian pulsed or continuous cortisol to cells. The effects of cortisol dynamics on cell proliferation and survival, and on gene expression were determined. In addition, effects on glucocorticoid receptor (GR) expression levels and phosphorylation, as a potential mediator, were measured. RESULTS: Pulsatile cortisol caused a significant reduction in cell survival compared to continuous exposure of the same cumulative dose, due to increased apoptosis. Comprehensive analysis of the transcriptome response by microarray identified genes with a differential response to pulsatile versus continuous glucocorticoid delivery. These were confirmed with qRT-PCR. Several transcription factor binding sites were enriched in these differentially regulated target genes, including CCAAT-displacement protein (CDP). A CDP regulated reporter gene (MMTV-luc) was, as predicted, also differentially regulated by pulsatile compared to continuous cortisol delivery. Importantly there was no effect of cortisol delivery kinetics on either GR expression, or activation (GR phosphoSer(211)). CONCLUSIONS: Cortisol oscillations exert important effects on target cell gene expression, and phenotype. This is not due to differences in cumulative cortisol exposure, or either expression, or activation of the GR. This suggests a novel means to regulate GR function.
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spelling pubmed-30228792011-01-25 Ultradian Cortisol Pulsatility Encodes a Distinct, Biologically Important Signal McMaster, Andrew Jangani, Maryam Sommer, Paula Han, Namshik Brass, Andy Beesley, Stephen Lu, Weiqun Berry, Andrew Loudon, Andrew Donn, Rachelle Ray, David W. PLoS One Research Article CONTEXT: Cortisol is released in ultradian pulses. The biological relevance of the resulting fluctuating cortisol concentration has not been explored. OBJECTIVE: Determination of the biological consequences of ultradian cortisol pulsatility. DESIGN: A novel flow through cell culture system was developed to deliver ultradian pulsed or continuous cortisol to cells. The effects of cortisol dynamics on cell proliferation and survival, and on gene expression were determined. In addition, effects on glucocorticoid receptor (GR) expression levels and phosphorylation, as a potential mediator, were measured. RESULTS: Pulsatile cortisol caused a significant reduction in cell survival compared to continuous exposure of the same cumulative dose, due to increased apoptosis. Comprehensive analysis of the transcriptome response by microarray identified genes with a differential response to pulsatile versus continuous glucocorticoid delivery. These were confirmed with qRT-PCR. Several transcription factor binding sites were enriched in these differentially regulated target genes, including CCAAT-displacement protein (CDP). A CDP regulated reporter gene (MMTV-luc) was, as predicted, also differentially regulated by pulsatile compared to continuous cortisol delivery. Importantly there was no effect of cortisol delivery kinetics on either GR expression, or activation (GR phosphoSer(211)). CONCLUSIONS: Cortisol oscillations exert important effects on target cell gene expression, and phenotype. This is not due to differences in cumulative cortisol exposure, or either expression, or activation of the GR. This suggests a novel means to regulate GR function. Public Library of Science 2011-01-18 /pmc/articles/PMC3022879/ /pubmed/21267416 http://dx.doi.org/10.1371/journal.pone.0015766 Text en McMaster 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
McMaster, Andrew
Jangani, Maryam
Sommer, Paula
Han, Namshik
Brass, Andy
Beesley, Stephen
Lu, Weiqun
Berry, Andrew
Loudon, Andrew
Donn, Rachelle
Ray, David W.
Ultradian Cortisol Pulsatility Encodes a Distinct, Biologically Important Signal
title Ultradian Cortisol Pulsatility Encodes a Distinct, Biologically Important Signal
title_full Ultradian Cortisol Pulsatility Encodes a Distinct, Biologically Important Signal
title_fullStr Ultradian Cortisol Pulsatility Encodes a Distinct, Biologically Important Signal
title_full_unstemmed Ultradian Cortisol Pulsatility Encodes a Distinct, Biologically Important Signal
title_short Ultradian Cortisol Pulsatility Encodes a Distinct, Biologically Important Signal
title_sort ultradian cortisol pulsatility encodes a distinct, biologically important signal
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3022879/
https://www.ncbi.nlm.nih.gov/pubmed/21267416
http://dx.doi.org/10.1371/journal.pone.0015766
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