Comparative analyses of downstream signal transduction targets modulated after activation of the AT(1) receptor by two β-arrestin-biased agonists

G protein-coupled receptors (GPCRs) are involved in essentially all physiological processes in mammals. The classical GPCR signal transduction mechanism occurs by coupling to G protein, but it has recently been demonstrated that interaction with β-arrestins leads to activation of pathways that are i...

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Autores principales: Santos, Geisa A., Duarte, Diego A., Parreiras-e-Silva, Lucas T., Teixeira, Felipe R., Silva-Rocha, Rafael, Oliveira, Eduardo B., Bouvier, Michel, Costa-Neto, Claudio M.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2015
Materias:
Pharmacology
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4486767/
https://www.ncbi.nlm.nih.gov/pubmed/26191004
http://dx.doi.org/10.3389/fphar.2015.00131
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author Santos, Geisa A.
Duarte, Diego A.
Parreiras-e-Silva, Lucas T.
Teixeira, Felipe R.
Silva-Rocha, Rafael
Oliveira, Eduardo B.
Bouvier, Michel
Costa-Neto, Claudio M.
author_facet Santos, Geisa A.
Duarte, Diego A.
Parreiras-e-Silva, Lucas T.
Teixeira, Felipe R.
Silva-Rocha, Rafael
Oliveira, Eduardo B.
Bouvier, Michel
Costa-Neto, Claudio M.
author_sort Santos, Geisa A.
collection PubMed
description G protein-coupled receptors (GPCRs) are involved in essentially all physiological processes in mammals. The classical GPCR signal transduction mechanism occurs by coupling to G protein, but it has recently been demonstrated that interaction with β-arrestins leads to activation of pathways that are independent of the G protein pathway. Also, it has been reported that some ligands can preferentially activate one of these signaling pathways; being therefore called biased agonists for G protein or β-arrestin pathways. The angiotensin II (AngII) AT(1) receptor is a prototype GPCR in the study of biased agonism due to the existence of well-known β-arrestin-biased agonists, such as [Sar(1), Ile(4), Ile(8)]-AngII (SII), and [Sar(1), D-Ala(8)]-AngII (TRV027). The aim of this study was to comparatively analyze the two above mentioned β-arrestin-biased agonists on downstream phosphorylation events and gene expression profiles. Our data reveal that activation of AT(1) receptor by each ligand led to a diversity of activation profiles that is far broader than that expected from a simple dichotomy between “G protein-dependent” and “β-arrestin-dependent” signaling. We observed clusters of activation profiles common to AngII, SII, and TRV027, as well as downstream effector activation that are unique to AngII, SII, or TRV027. Analyses of β-arrestin conformational changes after AT(1) receptor stimulation with SII or TRV027 suggests that the observed differences could account, at least partially, for the diversity of modulated targets observed. Our data reveal that, although the categorization “G protein-dependent” vs. “β-arrestin-dependent” signaling can be of pharmacological relevance, broader analyses of signaling pathways and downstream targets are necessary to generate an accurate activation profile for a given ligand. This may bring relevant information for drug development, as it may allow more refined comparison of drugs with similar mechanism of action and effects, but with distinct side effects.
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spelling pubmed-44867672015-07-17 Comparative analyses of downstream signal transduction targets modulated after activation of the AT(1) receptor by two β-arrestin-biased agonists Santos, Geisa A. Duarte, Diego A. Parreiras-e-Silva, Lucas T. Teixeira, Felipe R. Silva-Rocha, Rafael Oliveira, Eduardo B. Bouvier, Michel Costa-Neto, Claudio M. Front Pharmacol Pharmacology G protein-coupled receptors (GPCRs) are involved in essentially all physiological processes in mammals. The classical GPCR signal transduction mechanism occurs by coupling to G protein, but it has recently been demonstrated that interaction with β-arrestins leads to activation of pathways that are independent of the G protein pathway. Also, it has been reported that some ligands can preferentially activate one of these signaling pathways; being therefore called biased agonists for G protein or β-arrestin pathways. The angiotensin II (AngII) AT(1) receptor is a prototype GPCR in the study of biased agonism due to the existence of well-known β-arrestin-biased agonists, such as [Sar(1), Ile(4), Ile(8)]-AngII (SII), and [Sar(1), D-Ala(8)]-AngII (TRV027). The aim of this study was to comparatively analyze the two above mentioned β-arrestin-biased agonists on downstream phosphorylation events and gene expression profiles. Our data reveal that activation of AT(1) receptor by each ligand led to a diversity of activation profiles that is far broader than that expected from a simple dichotomy between “G protein-dependent” and “β-arrestin-dependent” signaling. We observed clusters of activation profiles common to AngII, SII, and TRV027, as well as downstream effector activation that are unique to AngII, SII, or TRV027. Analyses of β-arrestin conformational changes after AT(1) receptor stimulation with SII or TRV027 suggests that the observed differences could account, at least partially, for the diversity of modulated targets observed. Our data reveal that, although the categorization “G protein-dependent” vs. “β-arrestin-dependent” signaling can be of pharmacological relevance, broader analyses of signaling pathways and downstream targets are necessary to generate an accurate activation profile for a given ligand. This may bring relevant information for drug development, as it may allow more refined comparison of drugs with similar mechanism of action and effects, but with distinct side effects. Frontiers Media S.A. 2015-07-01 /pmc/articles/PMC4486767/ /pubmed/26191004 http://dx.doi.org/10.3389/fphar.2015.00131 Text en Copyright © 2015 Santos, Duarte, Parreiras-e-Silva, Teixeira, Silva-Rocha, Oliveira, Bouvier and Costa-Neto. http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) or licensor are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.
spellingShingle Pharmacology
Santos, Geisa A.
Duarte, Diego A.
Parreiras-e-Silva, Lucas T.
Teixeira, Felipe R.
Silva-Rocha, Rafael
Oliveira, Eduardo B.
Bouvier, Michel
Costa-Neto, Claudio M.
Comparative analyses of downstream signal transduction targets modulated after activation of the AT(1) receptor by two β-arrestin-biased agonists
title Comparative analyses of downstream signal transduction targets modulated after activation of the AT(1) receptor by two β-arrestin-biased agonists
title_full Comparative analyses of downstream signal transduction targets modulated after activation of the AT(1) receptor by two β-arrestin-biased agonists
title_fullStr Comparative analyses of downstream signal transduction targets modulated after activation of the AT(1) receptor by two β-arrestin-biased agonists
title_full_unstemmed Comparative analyses of downstream signal transduction targets modulated after activation of the AT(1) receptor by two β-arrestin-biased agonists
title_short Comparative analyses of downstream signal transduction targets modulated after activation of the AT(1) receptor by two β-arrestin-biased agonists
title_sort comparative analyses of downstream signal transduction targets modulated after activation of the at(1) receptor by two β-arrestin-biased agonists
topic Pharmacology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4486767/
https://www.ncbi.nlm.nih.gov/pubmed/26191004
http://dx.doi.org/10.3389/fphar.2015.00131
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