Insulin Inhibits Cardiac Contractility by Inducing a G(i)-Biased β(2)-Adrenergic Signaling in Hearts

Insulin and adrenergic stimulation are two divergent regulatory systems that may interact under certain pathophysiological circumstances. Here, we characterized a complex consisting of insulin receptor (IR) and β(2)-adrenergic receptor (β(2)AR) in the heart. The IR/β(2)AR complex undergoes dynamic d...

Descripción completa

Detalles Bibliográficos
Autores principales: Fu, Qin, Xu, Bing, Liu, Yongming, Parikh, Dippal, Li, Jing, Li, Ying, Zhang, Yuan, Riehle, Christian, Zhu, Yi, Rawlings, Tenley, Shi, Qian, Clark, Richard B., Chen, Xiongwen, Abel, E. Dale, Xiang, Yang K.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: American Diabetes Association 2014
Materias:
Signal Transduction
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4113065/
https://www.ncbi.nlm.nih.gov/pubmed/24677713
http://dx.doi.org/10.2337/db13-1763
_version_ 1782328242579963904
author Fu, Qin
Xu, Bing
Liu, Yongming
Parikh, Dippal
Li, Jing
Li, Ying
Zhang, Yuan
Riehle, Christian
Zhu, Yi
Rawlings, Tenley
Shi, Qian
Clark, Richard B.
Chen, Xiongwen
Abel, E. Dale
Xiang, Yang K.
author_facet Fu, Qin
Xu, Bing
Liu, Yongming
Parikh, Dippal
Li, Jing
Li, Ying
Zhang, Yuan
Riehle, Christian
Zhu, Yi
Rawlings, Tenley
Shi, Qian
Clark, Richard B.
Chen, Xiongwen
Abel, E. Dale
Xiang, Yang K.
author_sort Fu, Qin
collection PubMed
description Insulin and adrenergic stimulation are two divergent regulatory systems that may interact under certain pathophysiological circumstances. Here, we characterized a complex consisting of insulin receptor (IR) and β(2)-adrenergic receptor (β(2)AR) in the heart. The IR/β(2)AR complex undergoes dynamic dissociation under diverse conditions such as Langendorff perfusions of hearts with insulin or after euglycemic-hyperinsulinemic clamps in vivo. Activation of IR with insulin induces protein kinase A (PKA) and G-protein receptor kinase 2 (GRK2) phosphorylation of the β(2)AR, which promotes β(2)AR coupling to the inhibitory G-protein, G(i). The insulin-induced phosphorylation of β(2)AR is dependent on IRS1 and IRS2. After insulin pretreatment, the activated β(2)AR-G(i) signaling effectively attenuates cAMP/PKA activity after β-adrenergic stimulation in cardiomyocytes and consequently inhibits PKA phosphorylation of phospholamban and contractile responses in myocytes in vitro and in Langendorff perfused hearts. These data indicate that increased IR signaling, as occurs in hyperinsulinemic states, may directly impair βAR-regulated cardiac contractility. This β(2)AR-dependent IR and βAR signaling cross-talk offers a molecular basis for the broad interaction between these signaling cascades in the heart and other tissues or organs that may contribute to the pathophysiology of metabolic and cardiovascular dysfunction in insulin-resistant states.
format Online
Article
Text
id pubmed-4113065
institution National Center for Biotechnology Information
language English
publishDate 2014
publisher American Diabetes Association
record_format MEDLINE/PubMed
spelling pubmed-41130652015-08-01 Insulin Inhibits Cardiac Contractility by Inducing a G(i)-Biased β(2)-Adrenergic Signaling in Hearts Fu, Qin Xu, Bing Liu, Yongming Parikh, Dippal Li, Jing Li, Ying Zhang, Yuan Riehle, Christian Zhu, Yi Rawlings, Tenley Shi, Qian Clark, Richard B. Chen, Xiongwen Abel, E. Dale Xiang, Yang K. Diabetes Signal Transduction Insulin and adrenergic stimulation are two divergent regulatory systems that may interact under certain pathophysiological circumstances. Here, we characterized a complex consisting of insulin receptor (IR) and β(2)-adrenergic receptor (β(2)AR) in the heart. The IR/β(2)AR complex undergoes dynamic dissociation under diverse conditions such as Langendorff perfusions of hearts with insulin or after euglycemic-hyperinsulinemic clamps in vivo. Activation of IR with insulin induces protein kinase A (PKA) and G-protein receptor kinase 2 (GRK2) phosphorylation of the β(2)AR, which promotes β(2)AR coupling to the inhibitory G-protein, G(i). The insulin-induced phosphorylation of β(2)AR is dependent on IRS1 and IRS2. After insulin pretreatment, the activated β(2)AR-G(i) signaling effectively attenuates cAMP/PKA activity after β-adrenergic stimulation in cardiomyocytes and consequently inhibits PKA phosphorylation of phospholamban and contractile responses in myocytes in vitro and in Langendorff perfused hearts. These data indicate that increased IR signaling, as occurs in hyperinsulinemic states, may directly impair βAR-regulated cardiac contractility. This β(2)AR-dependent IR and βAR signaling cross-talk offers a molecular basis for the broad interaction between these signaling cascades in the heart and other tissues or organs that may contribute to the pathophysiology of metabolic and cardiovascular dysfunction in insulin-resistant states. American Diabetes Association 2014-08 2014-07-17 /pmc/articles/PMC4113065/ /pubmed/24677713 http://dx.doi.org/10.2337/db13-1763 Text en © 2014 by the American Diabetes Association. Readers may use this article as long as the work is properly cited, the use is educational and not for profit, and the work is not altered.
spellingShingle Signal Transduction
Fu, Qin
Xu, Bing
Liu, Yongming
Parikh, Dippal
Li, Jing
Li, Ying
Zhang, Yuan
Riehle, Christian
Zhu, Yi
Rawlings, Tenley
Shi, Qian
Clark, Richard B.
Chen, Xiongwen
Abel, E. Dale
Xiang, Yang K.
Insulin Inhibits Cardiac Contractility by Inducing a G(i)-Biased β(2)-Adrenergic Signaling in Hearts
title Insulin Inhibits Cardiac Contractility by Inducing a G(i)-Biased β(2)-Adrenergic Signaling in Hearts
title_full Insulin Inhibits Cardiac Contractility by Inducing a G(i)-Biased β(2)-Adrenergic Signaling in Hearts
title_fullStr Insulin Inhibits Cardiac Contractility by Inducing a G(i)-Biased β(2)-Adrenergic Signaling in Hearts
title_full_unstemmed Insulin Inhibits Cardiac Contractility by Inducing a G(i)-Biased β(2)-Adrenergic Signaling in Hearts
title_short Insulin Inhibits Cardiac Contractility by Inducing a G(i)-Biased β(2)-Adrenergic Signaling in Hearts
title_sort insulin inhibits cardiac contractility by inducing a g(i)-biased β(2)-adrenergic signaling in hearts
topic Signal Transduction
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4113065/
https://www.ncbi.nlm.nih.gov/pubmed/24677713
http://dx.doi.org/10.2337/db13-1763
work_keys_str_mv AT fuqin insulininhibitscardiaccontractilitybyinducingagibiasedb2adrenergicsignalinginhearts
AT xubing insulininhibitscardiaccontractilitybyinducingagibiasedb2adrenergicsignalinginhearts
AT liuyongming insulininhibitscardiaccontractilitybyinducingagibiasedb2adrenergicsignalinginhearts
AT parikhdippal insulininhibitscardiaccontractilitybyinducingagibiasedb2adrenergicsignalinginhearts
AT lijing insulininhibitscardiaccontractilitybyinducingagibiasedb2adrenergicsignalinginhearts
AT liying insulininhibitscardiaccontractilitybyinducingagibiasedb2adrenergicsignalinginhearts
AT zhangyuan insulininhibitscardiaccontractilitybyinducingagibiasedb2adrenergicsignalinginhearts
AT riehlechristian insulininhibitscardiaccontractilitybyinducingagibiasedb2adrenergicsignalinginhearts
AT zhuyi insulininhibitscardiaccontractilitybyinducingagibiasedb2adrenergicsignalinginhearts
AT rawlingstenley insulininhibitscardiaccontractilitybyinducingagibiasedb2adrenergicsignalinginhearts
AT shiqian insulininhibitscardiaccontractilitybyinducingagibiasedb2adrenergicsignalinginhearts
AT clarkrichardb insulininhibitscardiaccontractilitybyinducingagibiasedb2adrenergicsignalinginhearts
AT chenxiongwen insulininhibitscardiaccontractilitybyinducingagibiasedb2adrenergicsignalinginhearts
AT abeledale insulininhibitscardiaccontractilitybyinducingagibiasedb2adrenergicsignalinginhearts
AT xiangyangk insulininhibitscardiaccontractilitybyinducingagibiasedb2adrenergicsignalinginhearts

Ejemplares similares