Critical role for adenosine receptor A2a in β-cell proliferation

Critical role for adenosine receptor A2a in β-cell proliferation

Objective: Pharmacological activation of adenosine signaling has been shown to increase β-cell proliferation and thereby β-cell regeneration in zebrafish and rodent models of diabetes. However, whether adenosine has an endogenous role in regulating β-cell proliferation is unknown. The objective of t...

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Main Authors: Nadja Schulz, Ka-Cheuk Liu, Jérémie Charbord, Charlotte L. Mattsson, Lingjie Tao, Dominika Tworus, Olov Andersson
Format: Article
Language:English
Published: Elsevier 2016-11-01
Series:Molecular Metabolism
Online Access:http://www.sciencedirect.com/science/article/pii/S2212877816301570
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spelling doaj-9534a2d0becc4097ab5b790f52b06eb42020-11-24T22:43:11ZengElsevierMolecular Metabolism2212-87782016-11-0151111381146Critical role for adenosine receptor A2a in β-cell proliferationNadja Schulz0Ka-Cheuk Liu1Jérémie Charbord2Charlotte L. Mattsson3Lingjie Tao4Dominika Tworus5Olov Andersson6Department of Cell and Molecular Biology, Karolinska Institutet, von Eulers väg 3, 17177 Stockholm, SwedenDepartment of Cell and Molecular Biology, Karolinska Institutet, von Eulers väg 3, 17177 Stockholm, SwedenDepartment of Cell and Molecular Biology, Karolinska Institutet, von Eulers väg 3, 17177 Stockholm, SwedenDepartment of Cell and Molecular Biology, Karolinska Institutet, von Eulers väg 3, 17177 Stockholm, SwedenDepartment of Cell and Molecular Biology, Karolinska Institutet, von Eulers väg 3, 17177 Stockholm, SwedenDepartment of Cell and Molecular Biology, Karolinska Institutet, von Eulers väg 3, 17177 Stockholm, SwedenCorresponding author.; Department of Cell and Molecular Biology, Karolinska Institutet, von Eulers väg 3, 17177 Stockholm, SwedenObjective: Pharmacological activation of adenosine signaling has been shown to increase β-cell proliferation and thereby β-cell regeneration in zebrafish and rodent models of diabetes. However, whether adenosine has an endogenous role in regulating β-cell proliferation is unknown. The objective of this study was to determine whether endogenous adenosine regulates β-cell proliferation—either in the basal state or states of increased demand for insulin—and to delineate the mechanisms involved. Methods: We analyzed the effect of pharmacological adenosine agonists on β-cell proliferation in in vitro cultures of mouse islets and in zebrafish models with β- or δ-cell ablation. In addition, we performed physiological and histological characterization of wild-type mice and mutant mice with pancreas- or β-cell-specific deficiency in Adora2a (the gene encoding adenosine receptor A2a). The mutant mice were used for in vivo studies on the role of adenosine in the basal state and during pregnancy (a state of increased demand for insulin), as well as for in vitro studies of cultured islets. Results: Pharmacological adenosine signaling in zebrafish had a stronger effect on β-cell proliferation during β-cell regeneration than in the basal state, an effect that was independent of the apoptotic microenvironment of the regeneration model. In mice, deficiency in Adora2a impaired glucose control and diminished compensatory β-cell proliferation during pregnancy but did not have any overt phenotype in the basal state. Islets isolated from Adora2a-deficient mice had a reduced baseline level of β-cell proliferation in vitro, consistent with our finding that UK432097, an A2a-specific agonist, promotes the proliferation of mouse β-cells in vitro. Conclusions: This is the first study linking endogenously produced adenosine to β-cell proliferation. Moreover, we show that adenosine signaling via the A2a receptor has an important role in compensatory β-cell proliferation, a feature that could be harnessed pharmacologically for β-cell expansion and future therapeutic development for diabetes. Keywords: β-cell proliferation, Adenosine, Islet biology, Gestational diabeteshttp://www.sciencedirect.com/science/article/pii/S2212877816301570
collection DOAJ
language English
format Article
sources DOAJ
author Nadja Schulz
Ka-Cheuk Liu
Jérémie Charbord
Charlotte L. Mattsson
Lingjie Tao
Dominika Tworus
Olov Andersson
spellingShingle Nadja Schulz
Ka-Cheuk Liu
Jérémie Charbord
Charlotte L. Mattsson
Lingjie Tao
Dominika Tworus
Olov Andersson
Critical role for adenosine receptor A2a in β-cell proliferation
Molecular Metabolism
author_facet Nadja Schulz
Ka-Cheuk Liu
Jérémie Charbord
Charlotte L. Mattsson
Lingjie Tao
Dominika Tworus
Olov Andersson
author_sort Nadja Schulz
title Critical role for adenosine receptor A2a in β-cell proliferation
title_short Critical role for adenosine receptor A2a in β-cell proliferation
title_full Critical role for adenosine receptor A2a in β-cell proliferation
title_fullStr Critical role for adenosine receptor A2a in β-cell proliferation
title_full_unstemmed Critical role for adenosine receptor A2a in β-cell proliferation
title_sort critical role for adenosine receptor a2a in β-cell proliferation
publisher Elsevier
series Molecular Metabolism
issn 2212-8778
publishDate 2016-11-01
description Objective: Pharmacological activation of adenosine signaling has been shown to increase β-cell proliferation and thereby β-cell regeneration in zebrafish and rodent models of diabetes. However, whether adenosine has an endogenous role in regulating β-cell proliferation is unknown. The objective of this study was to determine whether endogenous adenosine regulates β-cell proliferation—either in the basal state or states of increased demand for insulin—and to delineate the mechanisms involved. Methods: We analyzed the effect of pharmacological adenosine agonists on β-cell proliferation in in vitro cultures of mouse islets and in zebrafish models with β- or δ-cell ablation. In addition, we performed physiological and histological characterization of wild-type mice and mutant mice with pancreas- or β-cell-specific deficiency in Adora2a (the gene encoding adenosine receptor A2a). The mutant mice were used for in vivo studies on the role of adenosine in the basal state and during pregnancy (a state of increased demand for insulin), as well as for in vitro studies of cultured islets. Results: Pharmacological adenosine signaling in zebrafish had a stronger effect on β-cell proliferation during β-cell regeneration than in the basal state, an effect that was independent of the apoptotic microenvironment of the regeneration model. In mice, deficiency in Adora2a impaired glucose control and diminished compensatory β-cell proliferation during pregnancy but did not have any overt phenotype in the basal state. Islets isolated from Adora2a-deficient mice had a reduced baseline level of β-cell proliferation in vitro, consistent with our finding that UK432097, an A2a-specific agonist, promotes the proliferation of mouse β-cells in vitro. Conclusions: This is the first study linking endogenously produced adenosine to β-cell proliferation. Moreover, we show that adenosine signaling via the A2a receptor has an important role in compensatory β-cell proliferation, a feature that could be harnessed pharmacologically for β-cell expansion and future therapeutic development for diabetes. Keywords: β-cell proliferation, Adenosine, Islet biology, Gestational diabetes
url http://www.sciencedirect.com/science/article/pii/S2212877816301570
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