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The in vivo regulation of heart rate in the murine sinoatrial node by stimulatory and inhibitory heterotrimeric G proteins

Reciprocal physiological modulation of heart rate is controlled by the sympathetic and parasympathetic systems acting on the sinoatrial (SA) node. However, there is little direct in vivo work examining the role of stimulatory and inhibitory G protein signaling in the SA node. Thus, we designed a stu...

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Autores principales: Sebastian, Sonia, Ang, Richard, Abramowitz, Joel, Weinstein, Lee S., Chen, Min, Ludwig, Andreas, Birnbaumer, Lutz, Tinker, Andrew
Formato: Online Artículo Texto
Lenguaje:English
Publicado: American Physiological Society 2013
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4073991/
https://www.ncbi.nlm.nih.gov/pubmed/23697798
http://dx.doi.org/10.1152/ajpregu.00037.2013
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author Sebastian, Sonia
Ang, Richard
Abramowitz, Joel
Weinstein, Lee S.
Chen, Min
Ludwig, Andreas
Birnbaumer, Lutz
Tinker, Andrew
author_facet Sebastian, Sonia
Ang, Richard
Abramowitz, Joel
Weinstein, Lee S.
Chen, Min
Ludwig, Andreas
Birnbaumer, Lutz
Tinker, Andrew
author_sort Sebastian, Sonia
collection PubMed
description Reciprocal physiological modulation of heart rate is controlled by the sympathetic and parasympathetic systems acting on the sinoatrial (SA) node. However, there is little direct in vivo work examining the role of stimulatory and inhibitory G protein signaling in the SA node. Thus, we designed a study to examine the role of the stimulatory (Gαs) and inhibitory G protein (Gαi2) in in vivo heart rate regulation in the SA node in the mouse. We studied mice with conditional deletion of Gαs and Gαi2 in the conduction system using cre-loxP technology. We crossed mice in which cre recombinase expression was driven by a tamoxifen-inducible conduction system-specific construct with “Gαs floxed” and “Gαi2 floxed” mice. We studied the heart rate responses of adult mice compared with littermate controls by using radiotelemetry before and after administration of tamoxifen. The mice with conditional deletion of Gαs and Gαi2 had a loss of diurnal variation and were bradycardic or tachycardic, respectively, in the daytime. In mice with conditional deletion of Gαs, there was a selective loss of low-frequency power, while with deletion of Gαi2, there was a loss of high-frequency power in power spectral analysis of heart rate variability. There was no evidence of pathological arrhythmia. Pharmacological modulation of heart rate by isoprenaline was impaired in the Gαs mice, but a muscarinic agonist was still able to slow the heart rate in Gαi2 mice. We conclude that Gαs- and Gαi2-mediated signaling in the sinoatrial node is important in the reciprocal regulation of heart rate through the autonomic nervous system.
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spelling pubmed-40739912014-08-01 The in vivo regulation of heart rate in the murine sinoatrial node by stimulatory and inhibitory heterotrimeric G proteins Sebastian, Sonia Ang, Richard Abramowitz, Joel Weinstein, Lee S. Chen, Min Ludwig, Andreas Birnbaumer, Lutz Tinker, Andrew Am J Physiol Regul Integr Comp Physiol Cardiovascular and Renal Integration Reciprocal physiological modulation of heart rate is controlled by the sympathetic and parasympathetic systems acting on the sinoatrial (SA) node. However, there is little direct in vivo work examining the role of stimulatory and inhibitory G protein signaling in the SA node. Thus, we designed a study to examine the role of the stimulatory (Gαs) and inhibitory G protein (Gαi2) in in vivo heart rate regulation in the SA node in the mouse. We studied mice with conditional deletion of Gαs and Gαi2 in the conduction system using cre-loxP technology. We crossed mice in which cre recombinase expression was driven by a tamoxifen-inducible conduction system-specific construct with “Gαs floxed” and “Gαi2 floxed” mice. We studied the heart rate responses of adult mice compared with littermate controls by using radiotelemetry before and after administration of tamoxifen. The mice with conditional deletion of Gαs and Gαi2 had a loss of diurnal variation and were bradycardic or tachycardic, respectively, in the daytime. In mice with conditional deletion of Gαs, there was a selective loss of low-frequency power, while with deletion of Gαi2, there was a loss of high-frequency power in power spectral analysis of heart rate variability. There was no evidence of pathological arrhythmia. Pharmacological modulation of heart rate by isoprenaline was impaired in the Gαs mice, but a muscarinic agonist was still able to slow the heart rate in Gαi2 mice. We conclude that Gαs- and Gαi2-mediated signaling in the sinoatrial node is important in the reciprocal regulation of heart rate through the autonomic nervous system. American Physiological Society 2013-05-22 2013-08-15 /pmc/articles/PMC4073991/ /pubmed/23697798 http://dx.doi.org/10.1152/ajpregu.00037.2013 Text en Licensed under Creative Commons Attribution CC-BY 3.0 (http://creativecommons.org/licenses/by/3.0/deed.en_US) : the American Physiological Society.
spellingShingle Cardiovascular and Renal Integration
Sebastian, Sonia
Ang, Richard
Abramowitz, Joel
Weinstein, Lee S.
Chen, Min
Ludwig, Andreas
Birnbaumer, Lutz
Tinker, Andrew
The in vivo regulation of heart rate in the murine sinoatrial node by stimulatory and inhibitory heterotrimeric G proteins
title The in vivo regulation of heart rate in the murine sinoatrial node by stimulatory and inhibitory heterotrimeric G proteins
title_full The in vivo regulation of heart rate in the murine sinoatrial node by stimulatory and inhibitory heterotrimeric G proteins
title_fullStr The in vivo regulation of heart rate in the murine sinoatrial node by stimulatory and inhibitory heterotrimeric G proteins
title_full_unstemmed The in vivo regulation of heart rate in the murine sinoatrial node by stimulatory and inhibitory heterotrimeric G proteins
title_short The in vivo regulation of heart rate in the murine sinoatrial node by stimulatory and inhibitory heterotrimeric G proteins
title_sort in vivo regulation of heart rate in the murine sinoatrial node by stimulatory and inhibitory heterotrimeric g proteins
topic Cardiovascular and Renal Integration
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4073991/
https://www.ncbi.nlm.nih.gov/pubmed/23697798
http://dx.doi.org/10.1152/ajpregu.00037.2013
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