GRK2 blockade with βARKct is essential for cardiac β(2)-adrenergic receptor signaling towards increased contractility

BACKGROUND: β(1)- and β(2)–adrenergic receptors (ARs) play distinct roles in the heart, e.g. β(1)AR is pro-contractile and pro-apoptotic but β(2)AR anti-apoptotic and only weakly pro-contractile. G protein coupled receptor kinase (GRK)-2 desensitizes and opposes βAR pro-contractile signaling by phos...

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Autores principales: Salazar, Norma C, Vallejos, Ximena, Siryk, Ashley, Rengo, Giuseppe, Cannavo, Alessandro, Liccardo, Daniela, De Lucia, Claudio, Gao, Erhe, Leosco, Dario, Koch, Walter J, Lymperopoulos, Anastasios
Formato: Online Artículo Texto
Lenguaje:English
Publicado: BioMed Central 2013
Materias:
Research
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3846709/
https://www.ncbi.nlm.nih.gov/pubmed/23984976
http://dx.doi.org/10.1186/1478-811X-11-64
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author Salazar, Norma C
Vallejos, Ximena
Siryk, Ashley
Rengo, Giuseppe
Cannavo, Alessandro
Liccardo, Daniela
De Lucia, Claudio
Gao, Erhe
Leosco, Dario
Koch, Walter J
Lymperopoulos, Anastasios
author_facet Salazar, Norma C
Vallejos, Ximena
Siryk, Ashley
Rengo, Giuseppe
Cannavo, Alessandro
Liccardo, Daniela
De Lucia, Claudio
Gao, Erhe
Leosco, Dario
Koch, Walter J
Lymperopoulos, Anastasios
author_sort Salazar, Norma C
collection PubMed
description BACKGROUND: β(1)- and β(2)–adrenergic receptors (ARs) play distinct roles in the heart, e.g. β(1)AR is pro-contractile and pro-apoptotic but β(2)AR anti-apoptotic and only weakly pro-contractile. G protein coupled receptor kinase (GRK)-2 desensitizes and opposes βAR pro-contractile signaling by phosphorylating the receptor and inducing beta-arrestin (βarr) binding. We posited herein that GRK2 blockade might enhance the pro-contractile signaling of the β(2)AR subtype in the heart. We tested the effects of cardiac-targeted GRK2 inhibition in vivo exclusively on β(2)AR signaling under normal conditions and in heart failure (HF). RESULTS: We crossed β(1)AR knockout (B1KO) mice with cardiac-specific transgenic mice expressing the βARKct, a known GRK2 inhibitor, and studied the offspring under normal conditions and in post-myocardial infarction (MI). βARKct expression in vivo proved essential for β(2)AR-dependent contractile function, as β(2)AR stimulation with isoproterenol fails to increase contractility in either healthy or post-MI B1KO mice and it only does so in the presence of βARKct. The main underlying mechanism for this is blockade of the interaction of phosphodiesterase (PDE) type 4D with the cardiac β(2)AR, which is normally mediated by the actions of GRK2 and βarrs on the receptor. The molecular “brake” that PDE4D poses on β(2)AR signaling to contractility stimulation is thus “released”. Regarding the other beneficial functions of cardiac β(2)AR, βARKct increased overall survival of the post-MI B1KO mice progressing to HF, via a decrease in cardiac apoptosis and an increase in wound healing-associated inflammation early (at 24 hrs) post-MI. However, these effects disappear by 4 weeks post-MI, and, in their place, upregulation of the other major GRK in the heart, GRK5, is observed. CONCLUSIONS: GRK2 inhibition in vivo with βARKct is absolutely essential for cardiac β(2)AR pro-contractile signaling and function. In addition, β(2)AR anti-apoptotic signaling in post-MI HF is augmented by βARKct, although this effect is short-lived.
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spelling pubmed-38467092013-12-03 GRK2 blockade with βARKct is essential for cardiac β(2)-adrenergic receptor signaling towards increased contractility Salazar, Norma C Vallejos, Ximena Siryk, Ashley Rengo, Giuseppe Cannavo, Alessandro Liccardo, Daniela De Lucia, Claudio Gao, Erhe Leosco, Dario Koch, Walter J Lymperopoulos, Anastasios Cell Commun Signal Research BACKGROUND: β(1)- and β(2)–adrenergic receptors (ARs) play distinct roles in the heart, e.g. β(1)AR is pro-contractile and pro-apoptotic but β(2)AR anti-apoptotic and only weakly pro-contractile. G protein coupled receptor kinase (GRK)-2 desensitizes and opposes βAR pro-contractile signaling by phosphorylating the receptor and inducing beta-arrestin (βarr) binding. We posited herein that GRK2 blockade might enhance the pro-contractile signaling of the β(2)AR subtype in the heart. We tested the effects of cardiac-targeted GRK2 inhibition in vivo exclusively on β(2)AR signaling under normal conditions and in heart failure (HF). RESULTS: We crossed β(1)AR knockout (B1KO) mice with cardiac-specific transgenic mice expressing the βARKct, a known GRK2 inhibitor, and studied the offspring under normal conditions and in post-myocardial infarction (MI). βARKct expression in vivo proved essential for β(2)AR-dependent contractile function, as β(2)AR stimulation with isoproterenol fails to increase contractility in either healthy or post-MI B1KO mice and it only does so in the presence of βARKct. The main underlying mechanism for this is blockade of the interaction of phosphodiesterase (PDE) type 4D with the cardiac β(2)AR, which is normally mediated by the actions of GRK2 and βarrs on the receptor. The molecular “brake” that PDE4D poses on β(2)AR signaling to contractility stimulation is thus “released”. Regarding the other beneficial functions of cardiac β(2)AR, βARKct increased overall survival of the post-MI B1KO mice progressing to HF, via a decrease in cardiac apoptosis and an increase in wound healing-associated inflammation early (at 24 hrs) post-MI. However, these effects disappear by 4 weeks post-MI, and, in their place, upregulation of the other major GRK in the heart, GRK5, is observed. CONCLUSIONS: GRK2 inhibition in vivo with βARKct is absolutely essential for cardiac β(2)AR pro-contractile signaling and function. In addition, β(2)AR anti-apoptotic signaling in post-MI HF is augmented by βARKct, although this effect is short-lived. BioMed Central 2013-08-28 /pmc/articles/PMC3846709/ /pubmed/23984976 http://dx.doi.org/10.1186/1478-811X-11-64 Text en Copyright © 2013 Salazar et al.; licensee BioMed Central Ltd. http://creativecommons.org/licenses/by/2.0 This is an Open Access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/2.0), which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Research
Salazar, Norma C
Vallejos, Ximena
Siryk, Ashley
Rengo, Giuseppe
Cannavo, Alessandro
Liccardo, Daniela
De Lucia, Claudio
Gao, Erhe
Leosco, Dario
Koch, Walter J
Lymperopoulos, Anastasios
GRK2 blockade with βARKct is essential for cardiac β(2)-adrenergic receptor signaling towards increased contractility
title GRK2 blockade with βARKct is essential for cardiac β(2)-adrenergic receptor signaling towards increased contractility
title_full GRK2 blockade with βARKct is essential for cardiac β(2)-adrenergic receptor signaling towards increased contractility
title_fullStr GRK2 blockade with βARKct is essential for cardiac β(2)-adrenergic receptor signaling towards increased contractility
title_full_unstemmed GRK2 blockade with βARKct is essential for cardiac β(2)-adrenergic receptor signaling towards increased contractility
title_short GRK2 blockade with βARKct is essential for cardiac β(2)-adrenergic receptor signaling towards increased contractility
title_sort grk2 blockade with βarkct is essential for cardiac β(2)-adrenergic receptor signaling towards increased contractility
topic Research
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3846709/
https://www.ncbi.nlm.nih.gov/pubmed/23984976
http://dx.doi.org/10.1186/1478-811X-11-64
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