The A2b Adenosine Receptor Modulates Glucose Homeostasis and Obesity

High fat diet and its induced changes in glucose homeostasis, inflammation and obesity continue to be an epidemic in developed countries. The A2b adenosine receptor (A2bAR) is known to regulate inflammation. We used a diet-induced obesity murine knockout model to investigate the role of this recepto...

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Published in	PloS one Vol. 7; no. 7; p. e40584
Main Authors	Johnston-Cox, Hillary, Koupenova, Milka, Yang, Dan, Corkey, Barbara, Gokce, Noyan, Farb, Melissa G., LeBrasseur, Nathan, Ravid, Katya
Format	Journal Article
Language	English
Published	United States Public Library of Science 25.07.2012 Public Library of Science (PLoS)
Subjects	Adenosine Adenosine A2 Receptor Agonists - pharmacology Adult AKT protein Aminopyridines - pharmacology Analysis Animal tissues Animals Biology Cholesterol Cholesterol - adverse effects Cholesterol - pharmacology Developed countries Development and progression Diabetes mellitus Diabetes Mellitus, Type 2 - drug therapy Diabetes Mellitus, Type 2 - genetics Diabetes Mellitus, Type 2 - metabolism Diabetes Mellitus, Type 2 - pathology Diet Dietary Fats - adverse effects Dietary Fats - pharmacokinetics Epidemics Female Gene Expression Regulation - drug effects Gene Expression Regulation - genetics Glucose Glucose - metabolism Health risk assessment High cholesterol diet High fat diet Homeostasis Humans Inflammation Inflammation - drug therapy Inflammation - genetics Inflammation - metabolism Inflammation - pathology Insulin Insulin - genetics Insulin - metabolism Insulin Receptor Substrate Proteins - biosynthesis Insulin Receptor Substrate Proteins - genetics Insulin resistance Kinases Male Mediation Medical research Medicine Mice Mice, Knockout Middle Aged Obesity Obesity - drug therapy Obesity - genetics Obesity - metabolism Obesity - pathology Pharmacology Phosphorylation Receptor, Adenosine A2B - genetics Receptor, Adenosine A2B - metabolism Rodents Signaling Sterol Regulatory Element Binding Protein 1 - biosynthesis Sterol Regulatory Element Binding Protein 1 - genetics Sterol regulatory element-binding protein Tumor necrosis factor-TNF Type 2 diabetes Western blotting United States > US Massachusetts
Online Access	Get full text
ISSN	1932-6203 1932-6203
DOI	10.1371/journal.pone.0040584

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Abstract	High fat diet and its induced changes in glucose homeostasis, inflammation and obesity continue to be an epidemic in developed countries. The A2b adenosine receptor (A2bAR) is known to regulate inflammation. We used a diet-induced obesity murine knockout model to investigate the role of this receptor in mediating metabolic homeostasis, and correlated our findings in obese patient samples. Administration of high fat, high cholesterol diet (HFD) for sixteen weeks vastly upregulated the expression of the A2bAR in control mice, while A2bAR knockout (KO) mice under this diet developed greater obesity and hallmarks of type 2 diabetes (T2D), assessed by delayed glucose clearance and augmented insulin levels compared to matching control mice. We identified a novel link between the expression of A2bAR, insulin receptor substrate 2 (IRS-2), and insulin signaling, determined by Western blotting for IRS-2 and tissue Akt phosphorylation. The latter is impaired in tissues of A2bAR KO mice, along with a greater inflammatory state. Additional mechanisms involved include A2bAR regulation of SREBP-1 expression, a repressor of IRS-2. Importantly, pharmacological activation of the A2bAR by injection of the A2bAR ligand BAY 60-6583 for four weeks post HFD restores IRS-2 levels, and ameliorates T2D. Finally, in obese human subjects A2bAR expression correlates strongly with IRS-2 expression. Our study identified the A2bAR as a significant regulator of HFD-induced hallmarks of T2D, thereby pointing to its therapeutic potential.
AbstractList	High fat diet and its induced changes in glucose homeostasis, inflammation and obesity continue to be an epidemic in developed countries. The A2b adenosine receptor (A2bAR) is known to regulate inflammation. We used a diet-induced obesity murine knockout model to investigate the role of this receptor in mediating metabolic homeostasis, and correlated our findings in obese patient samples. Administration of high fat, high cholesterol diet (HFD) for sixteen weeks vastly upregulated the expression of the A2bAR in control mice, while A2bAR knockout (KO) mice under this diet developed greater obesity and hallmarks of type 2 diabetes (T2D), assessed by delayed glucose clearance and augmented insulin levels compared to matching control mice. We identified a novel link between the expression of A2bAR, insulin receptor substrate 2 (IRS-2), and insulin signaling, determined by Western blotting for IRS-2 and tissue Akt phosphorylation. The latter is impaired in tissues of A2bAR KO mice, along with a greater inflammatory state. Additional mechanisms involved include A2bAR regulation of SREBP-1 expression, a repressor of IRS-2. Importantly, pharmacological activation of the A2bAR by injection of the A2bAR ligand BAY 60-6583 for four weeks post HFD restores IRS-2 levels, and ameliorates T2D. Finally, in obese human subjects A2bAR expression correlates strongly with IRS-2 expression. Our study identified the A2bAR as a significant regulator of HFD-induced hallmarks of T2D, thereby pointing to its therapeutic potential. High fat diet and its induced changes in glucose homeostasis, inflammation and obesity continue to be an epidemic in developed countries. The A2b adenosine receptor (A2bAR) is known to regulate inflammation. We used a diet-induced obesity murine knockout model to investigate the role of this receptor in mediating metabolic homeostasis, and correlated our findings in obese patient samples. Administration of high fat, high cholesterol diet (HFD) for sixteen weeks vastly upregulated the expression of the A2bAR in control mice, while A2bAR knockout (KO) mice under this diet developed greater obesity and hallmarks of type 2 diabetes (T2D), assessed by delayed glucose clearance and augmented insulin levels compared to matching control mice. We identified a novel link between the expression of A2bAR, insulin receptor substrate 2 (IRS-2), and insulin signaling, determined by Western blotting for IRS-2 and tissue Akt phosphorylation. The latter is impaired in tissues of A2bAR KO mice, along with a greater inflammatory state. Additional mechanisms involved include A2bAR regulation of SREBP-1 expression, a repressor of IRS-2. Importantly, pharmacological activation of the A2bAR by injection of the A2bAR ligand BAY 60-6583 for four weeks post HFD restores IRS-2 levels, and ameliorates T2D. Finally, in obese human subjects A2bAR expression correlates strongly with IRS-2 expression. Our study identified the A2bAR as a significant regulator of HFD-induced hallmarks of T2D, thereby pointing to its therapeutic potential. Background High fat diet and its induced changes in glucose homeostasis, inflammation and obesity continue to be an epidemic in developed countries. The A2b adenosine receptor (A2bAR) is known to regulate inflammation. We used a diet-induced obesity murine knockout model to investigate the role of this receptor in mediating metabolic homeostasis, and correlated our findings in obese patient samples. Methodology/Principal Findings Administration of high fat, high cholesterol diet (HFD) for sixteen weeks vastly upregulated the expression of the A2bAR in control mice, while A2bAR knockout (KO) mice under this diet developed greater obesity and hallmarks of type 2 diabetes (T2D), assessed by delayed glucose clearance and augmented insulin levels compared to matching control mice. We identified a novel link between the expression of A2bAR, insulin receptor substrate 2 (IRS-2), and insulin signaling, determined by Western blotting for IRS-2 and tissue Akt phosphorylation. The latter is impaired in tissues of A2bAR KO mice, along with a greater inflammatory state. Additional mechanisms involved include A2bAR regulation of SREBP-1 expression, a repressor of IRS-2. Importantly, pharmacological activation of the A2bAR by injection of the A2bAR ligand BAY 60-6583 for four weeks post HFD restores IRS-2 levels, and ameliorates T2D. Finally, in obese human subjects A2bAR expression correlates strongly with IRS-2 expression. Conclusions/Significance Our study identified the A2bAR as a significant regulator of HFD-induced hallmarks of T2D, thereby pointing to its therapeutic potential. Background High fat diet and its induced changes in glucose homeostasis, inflammation and obesity continue to be an epidemic in developed countries. The A2b adenosine receptor (A2bAR) is known to regulate inflammation. We used a diet-induced obesity murine knockout model to investigate the role of this receptor in mediating metabolic homeostasis, and correlated our findings in obese patient samples. Methodology/Principal Findings Administration of high fat, high cholesterol diet (HFD) for sixteen weeks vastly upregulated the expression of the A2bAR in control mice, while A2bAR knockout (KO) mice under this diet developed greater obesity and hallmarks of type 2 diabetes (T2D), assessed by delayed glucose clearance and augmented insulin levels compared to matching control mice. We identified a novel link between the expression of A2bAR, insulin receptor substrate 2 (IRS-2), and insulin signaling, determined by Western blotting for IRS-2 and tissue Akt phosphorylation. The latter is impaired in tissues of A2bAR KO mice, along with a greater inflammatory state. Additional mechanisms involved include A2bAR regulation of SREBP-1 expression, a repressor of IRS-2. Importantly, pharmacological activation of the A2bAR by injection of the A2bAR ligand BAY 60-6583 for four weeks post HFD restores IRS-2 levels, and ameliorates T2D. Finally, in obese human subjects A2bAR expression correlates strongly with IRS-2 expression. Conclusions/Significance Our study identified the A2bAR as a significant regulator of HFD-induced hallmarks of T2D, thereby pointing to its therapeutic potential. High fat diet and its induced changes in glucose homeostasis, inflammation and obesity continue to be an epidemic in developed countries. The A2b adenosine receptor (A2bAR) is known to regulate inflammation. We used a diet-induced obesity murine knockout model to investigate the role of this receptor in mediating metabolic homeostasis, and correlated our findings in obese patient samples.BACKGROUNDHigh fat diet and its induced changes in glucose homeostasis, inflammation and obesity continue to be an epidemic in developed countries. The A2b adenosine receptor (A2bAR) is known to regulate inflammation. We used a diet-induced obesity murine knockout model to investigate the role of this receptor in mediating metabolic homeostasis, and correlated our findings in obese patient samples.Administration of high fat, high cholesterol diet (HFD) for sixteen weeks vastly upregulated the expression of the A2bAR in control mice, while A2bAR knockout (KO) mice under this diet developed greater obesity and hallmarks of type 2 diabetes (T2D), assessed by delayed glucose clearance and augmented insulin levels compared to matching control mice. We identified a novel link between the expression of A2bAR, insulin receptor substrate 2 (IRS-2), and insulin signaling, determined by Western blotting for IRS-2 and tissue Akt phosphorylation. The latter is impaired in tissues of A2bAR KO mice, along with a greater inflammatory state. Additional mechanisms involved include A2bAR regulation of SREBP-1 expression, a repressor of IRS-2. Importantly, pharmacological activation of the A2bAR by injection of the A2bAR ligand BAY 60-6583 for four weeks post HFD restores IRS-2 levels, and ameliorates T2D. Finally, in obese human subjects A2bAR expression correlates strongly with IRS-2 expression.METHODOLOGY/PRINCIPAL FINDINGSAdministration of high fat, high cholesterol diet (HFD) for sixteen weeks vastly upregulated the expression of the A2bAR in control mice, while A2bAR knockout (KO) mice under this diet developed greater obesity and hallmarks of type 2 diabetes (T2D), assessed by delayed glucose clearance and augmented insulin levels compared to matching control mice. We identified a novel link between the expression of A2bAR, insulin receptor substrate 2 (IRS-2), and insulin signaling, determined by Western blotting for IRS-2 and tissue Akt phosphorylation. The latter is impaired in tissues of A2bAR KO mice, along with a greater inflammatory state. Additional mechanisms involved include A2bAR regulation of SREBP-1 expression, a repressor of IRS-2. Importantly, pharmacological activation of the A2bAR by injection of the A2bAR ligand BAY 60-6583 for four weeks post HFD restores IRS-2 levels, and ameliorates T2D. Finally, in obese human subjects A2bAR expression correlates strongly with IRS-2 expression.Our study identified the A2bAR as a significant regulator of HFD-induced hallmarks of T2D, thereby pointing to its therapeutic potential.CONCLUSIONS/SIGNIFICANCEOur study identified the A2bAR as a significant regulator of HFD-induced hallmarks of T2D, thereby pointing to its therapeutic potential.
Audience	Academic
Author	Johnston-Cox, Hillary Yang, Dan Gokce, Noyan Farb, Melissa G. Koupenova, Milka Corkey, Barbara Ravid, Katya LeBrasseur, Nathan
AuthorAffiliation	University of Colorado Denver, United States of America 4 Evans Center for Interdisciplinary Biomedical Research, Boston University School of Medicine, Boston, Massachusetts, United States of America 3 Whitaker Cardiovascular Institute, Boston University School of Medicine, Boston, Massachusetts, United States of America 1 Departments of Medicine, Boston University School of Medicine, Boston, Massachusetts, United States of America 2 Department Biochemistry, Boston University School of Medicine, Boston, Massachusetts, United States of America
AuthorAffiliation_xml	– name: 4 Evans Center for Interdisciplinary Biomedical Research, Boston University School of Medicine, Boston, Massachusetts, United States of America – name: University of Colorado Denver, United States of America – name: 2 Department Biochemistry, Boston University School of Medicine, Boston, Massachusetts, United States of America – name: 3 Whitaker Cardiovascular Institute, Boston University School of Medicine, Boston, Massachusetts, United States of America – name: 1 Departments of Medicine, Boston University School of Medicine, Boston, Massachusetts, United States of America
Author_xml	– sequence: 1 givenname: Hillary surname: Johnston-Cox fullname: Johnston-Cox, Hillary – sequence: 2 givenname: Milka surname: Koupenova fullname: Koupenova, Milka – sequence: 3 givenname: Dan surname: Yang fullname: Yang, Dan – sequence: 4 givenname: Barbara surname: Corkey fullname: Corkey, Barbara – sequence: 5 givenname: Noyan surname: Gokce fullname: Gokce, Noyan – sequence: 6 givenname: Melissa G. surname: Farb fullname: Farb, Melissa G. – sequence: 7 givenname: Nathan surname: LeBrasseur fullname: LeBrasseur, Nathan – sequence: 8 givenname: Katya surname: Ravid fullname: Ravid, Katya
BackLink	https://www.ncbi.nlm.nih.gov/pubmed/22848385$$D View this record in MEDLINE/PubMed
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Copyright	COPYRIGHT 2012 Public Library of Science 2012 Johnston-Cox et al. This is an open-access article distributed under the terms of the Creative Commons Attribution License: https://creativecommons.org/licenses/by/4.0/ (the “License”), which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited. Notwithstanding the ProQuest Terms and Conditions, you may use this content in accordance with the terms of the License. Johnston-Cox et al. 2012
Copyright_xml	– notice: COPYRIGHT 2012 Public Library of Science – notice: 2012 Johnston-Cox et al. This is an open-access article distributed under the terms of the Creative Commons Attribution License: https://creativecommons.org/licenses/by/4.0/ (the “License”), which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited. Notwithstanding the ProQuest Terms and Conditions, you may use this content in accordance with the terms of the License. – notice: Johnston-Cox et al. 2012
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Notes	ObjectType-Article-1 SourceType-Scholarly Journals-1 ObjectType-Feature-2 content type line 14 content type line 23 Conceived and designed the experiments: HJC MK KR. Performed the experiments: HJC MK DY MGF. Analyzed the data: HJC MK NG MGF NL KR. Contributed reagents/materials/analysis tools: HJC MK BC NG MGF NL KR. Wrote the paper: HJC MK KR.
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Snippet	High fat diet and its induced changes in glucose homeostasis, inflammation and obesity continue to be an epidemic in developed countries. The A2b adenosine... Background High fat diet and its induced changes in glucose homeostasis, inflammation and obesity continue to be an epidemic in developed countries. The A2b... Background High fat diet and its induced changes in glucose homeostasis, inflammation and obesity continue to be an epidemic in developed countries. The A2b...
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SubjectTerms	Adenosine Adenosine A2 Receptor Agonists - pharmacology Adult AKT protein Aminopyridines - pharmacology Analysis Animal tissues Animals Biology Cholesterol Cholesterol - adverse effects Cholesterol - pharmacology Developed countries Development and progression Diabetes mellitus Diabetes Mellitus, Type 2 - drug therapy Diabetes Mellitus, Type 2 - genetics Diabetes Mellitus, Type 2 - metabolism Diabetes Mellitus, Type 2 - pathology Diet Dietary Fats - adverse effects Dietary Fats - pharmacokinetics Epidemics Female Gene Expression Regulation - drug effects Gene Expression Regulation - genetics Glucose Glucose - metabolism Health risk assessment High cholesterol diet High fat diet Homeostasis Humans Inflammation Inflammation - drug therapy Inflammation - genetics Inflammation - metabolism Inflammation - pathology Insulin Insulin - genetics Insulin - metabolism Insulin Receptor Substrate Proteins - biosynthesis Insulin Receptor Substrate Proteins - genetics Insulin resistance Kinases Male Mediation Medical research Medicine Mice Mice, Knockout Middle Aged Obesity Obesity - drug therapy Obesity - genetics Obesity - metabolism Obesity - pathology Pharmacology Phosphorylation Receptor, Adenosine A2B - genetics Receptor, Adenosine A2B - metabolism Rodents Signaling Sterol Regulatory Element Binding Protein 1 - biosynthesis Sterol Regulatory Element Binding Protein 1 - genetics Sterol regulatory element-binding protein Tumor necrosis factor-TNF Type 2 diabetes Western blotting
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Title	The A2b Adenosine Receptor Modulates Glucose Homeostasis and Obesity
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