Isoproterenol Acts as a Biased Agonist of the Alpha-1A-Adrenoceptor that Selectively Activates the MAPK/ERK Pathway

The α(1A)-AR is thought to couple predominantly to the Gα(q)/PLC pathway and lead to phosphoinositide hydrolysis and calcium mobilization, although certain agonists acting at this receptor have been reported to trigger activation of arachidonic acid formation and MAPK pathways. For several G protein...

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Autores principales: Copik, Alicja. J., Baldys, Aleksander, Nguyen, Khanh, Sahdeo, Sunil, Ho, Hoangdung, Kosaka, Alan, Dietrich, Paul J., Fitch, Bill, Raymond, John R., Ford, Anthony P. D. W., Button, Donald, Milla, Marcos E.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2015
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4301629/
https://www.ncbi.nlm.nih.gov/pubmed/25606852
http://dx.doi.org/10.1371/journal.pone.0115701
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author Copik, Alicja. J.
Baldys, Aleksander
Nguyen, Khanh
Sahdeo, Sunil
Ho, Hoangdung
Kosaka, Alan
Dietrich, Paul J.
Fitch, Bill
Raymond, John R.
Ford, Anthony P. D. W.
Button, Donald
Milla, Marcos E.
author_facet Copik, Alicja. J.
Baldys, Aleksander
Nguyen, Khanh
Sahdeo, Sunil
Ho, Hoangdung
Kosaka, Alan
Dietrich, Paul J.
Fitch, Bill
Raymond, John R.
Ford, Anthony P. D. W.
Button, Donald
Milla, Marcos E.
author_sort Copik, Alicja. J.
collection PubMed
description The α(1A)-AR is thought to couple predominantly to the Gα(q)/PLC pathway and lead to phosphoinositide hydrolysis and calcium mobilization, although certain agonists acting at this receptor have been reported to trigger activation of arachidonic acid formation and MAPK pathways. For several G protein-coupled receptors (GPCRs) agonists can manifest a bias for activation of particular effector signaling output, i.e. not all agonists of a given GPCR generate responses through utilization of the same signaling cascade(s). Previous work with Gα(q) coupling-defective variants of α(1A)-AR, as well as a combination of Ca(2+) channel blockers, uncovered cross-talk between α(1A)-AR and β(2)-AR that leads to potentiation of a Gα(q)-independent signaling cascade in response to α(1A)-AR activation. We hypothesized that molecules exist that act as biased agonists to selectively activate this pathway. In this report, isoproterenol (Iso), typically viewed as β-AR-selective agonist, was examined with respect to activation of α(1A)-AR. α(1A)-AR selective antagonists were used to specifically block Iso evoked signaling in different cellular backgrounds and confirm its action at α(1A)-AR. Iso induced signaling at α(1A)-AR was further interrogated by probing steps along the Gα(q) /PLC, Gα(s) and MAPK/ERK pathways. In HEK-293/EBNA cells transiently transduced with α(1A)-AR, and CHO_α(1A)-AR stable cells, Iso evoked low potency ERK activity as well as Ca(2+) mobilization that could be blocked by α(1A)-AR selective antagonists. The kinetics of Iso induced Ca(2+) transients differed from typical Gα(q)- mediated Ca(2+) mobilization, lacking both the fast IP(3)R mediated response and the sustained phase of Ca(2+) re-entry. Moreover, no inositol phosphate (IP) accumulation could be detected in either cell line after stimulation with Iso, but activation was accompanied by receptor internalization. Data are presented that indicate that Iso represents a novel type of α(1A)-AR partial agonist with signaling bias toward MAPK/ERK signaling cascade that is likely independent of coupling to Gα(q).
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spelling pubmed-43016292015-01-30 Isoproterenol Acts as a Biased Agonist of the Alpha-1A-Adrenoceptor that Selectively Activates the MAPK/ERK Pathway Copik, Alicja. J. Baldys, Aleksander Nguyen, Khanh Sahdeo, Sunil Ho, Hoangdung Kosaka, Alan Dietrich, Paul J. Fitch, Bill Raymond, John R. Ford, Anthony P. D. W. Button, Donald Milla, Marcos E. PLoS One Research Article The α(1A)-AR is thought to couple predominantly to the Gα(q)/PLC pathway and lead to phosphoinositide hydrolysis and calcium mobilization, although certain agonists acting at this receptor have been reported to trigger activation of arachidonic acid formation and MAPK pathways. For several G protein-coupled receptors (GPCRs) agonists can manifest a bias for activation of particular effector signaling output, i.e. not all agonists of a given GPCR generate responses through utilization of the same signaling cascade(s). Previous work with Gα(q) coupling-defective variants of α(1A)-AR, as well as a combination of Ca(2+) channel blockers, uncovered cross-talk between α(1A)-AR and β(2)-AR that leads to potentiation of a Gα(q)-independent signaling cascade in response to α(1A)-AR activation. We hypothesized that molecules exist that act as biased agonists to selectively activate this pathway. In this report, isoproterenol (Iso), typically viewed as β-AR-selective agonist, was examined with respect to activation of α(1A)-AR. α(1A)-AR selective antagonists were used to specifically block Iso evoked signaling in different cellular backgrounds and confirm its action at α(1A)-AR. Iso induced signaling at α(1A)-AR was further interrogated by probing steps along the Gα(q) /PLC, Gα(s) and MAPK/ERK pathways. In HEK-293/EBNA cells transiently transduced with α(1A)-AR, and CHO_α(1A)-AR stable cells, Iso evoked low potency ERK activity as well as Ca(2+) mobilization that could be blocked by α(1A)-AR selective antagonists. The kinetics of Iso induced Ca(2+) transients differed from typical Gα(q)- mediated Ca(2+) mobilization, lacking both the fast IP(3)R mediated response and the sustained phase of Ca(2+) re-entry. Moreover, no inositol phosphate (IP) accumulation could be detected in either cell line after stimulation with Iso, but activation was accompanied by receptor internalization. Data are presented that indicate that Iso represents a novel type of α(1A)-AR partial agonist with signaling bias toward MAPK/ERK signaling cascade that is likely independent of coupling to Gα(q). Public Library of Science 2015-01-21 /pmc/articles/PMC4301629/ /pubmed/25606852 http://dx.doi.org/10.1371/journal.pone.0115701 Text en https://creativecommons.org/publicdomain/zero/1.0/ This is an open-access article distributed under the terms of the Creative Commons Public Domain declaration, which stipulates that, once placed in the public domain, this work may be freely reproduced, distributed, transmitted, modified, built upon, or otherwise used by anyone for any lawful purpose.
spellingShingle Research Article
Copik, Alicja. J.
Baldys, Aleksander
Nguyen, Khanh
Sahdeo, Sunil
Ho, Hoangdung
Kosaka, Alan
Dietrich, Paul J.
Fitch, Bill
Raymond, John R.
Ford, Anthony P. D. W.
Button, Donald
Milla, Marcos E.
Isoproterenol Acts as a Biased Agonist of the Alpha-1A-Adrenoceptor that Selectively Activates the MAPK/ERK Pathway
title Isoproterenol Acts as a Biased Agonist of the Alpha-1A-Adrenoceptor that Selectively Activates the MAPK/ERK Pathway
title_full Isoproterenol Acts as a Biased Agonist of the Alpha-1A-Adrenoceptor that Selectively Activates the MAPK/ERK Pathway
title_fullStr Isoproterenol Acts as a Biased Agonist of the Alpha-1A-Adrenoceptor that Selectively Activates the MAPK/ERK Pathway
title_full_unstemmed Isoproterenol Acts as a Biased Agonist of the Alpha-1A-Adrenoceptor that Selectively Activates the MAPK/ERK Pathway
title_short Isoproterenol Acts as a Biased Agonist of the Alpha-1A-Adrenoceptor that Selectively Activates the MAPK/ERK Pathway
title_sort isoproterenol acts as a biased agonist of the alpha-1a-adrenoceptor that selectively activates the mapk/erk pathway
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4301629/
https://www.ncbi.nlm.nih.gov/pubmed/25606852
http://dx.doi.org/10.1371/journal.pone.0115701
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