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Conditional Hypovascularization and Hypoxia in Islets Do Not Overtly Influence Adult β-Cell Mass or Function

It is generally accepted that vascularization and oxygenation of pancreatic islets are essential for the maintenance of an optimal β-cell mass and function and that signaling by vascular endothelial growth factor (VEGF) is crucial for pancreas development, insulin gene expression/secretion, and (com...

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Autores principales: D'Hoker, Joke, De Leu, Nico, Heremans, Yves, Baeyens, Luc, Minami, Kohtaro, Ying, Cai, Lavens, Astrid, Chintinne, Marie, Stangé, Geert, Magenheim, Judith, Swisa, Avital, Martens, Geert, Pipeleers, Daniel, van de Casteele, Mark, Seino, Susumo, Keshet, Eli, Dor, Yuval, Heimberg, Harry
Formato: Online Artículo Texto
Lenguaje:English
Publicado: American Diabetes Association 2013
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3837025/
https://www.ncbi.nlm.nih.gov/pubmed/23974922
http://dx.doi.org/10.2337/db12-1827
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author D'Hoker, Joke
De Leu, Nico
Heremans, Yves
Baeyens, Luc
Minami, Kohtaro
Ying, Cai
Lavens, Astrid
Chintinne, Marie
Stangé, Geert
Magenheim, Judith
Swisa, Avital
Martens, Geert
Pipeleers, Daniel
van de Casteele, Mark
Seino, Susumo
Keshet, Eli
Dor, Yuval
Heimberg, Harry
author_facet D'Hoker, Joke
De Leu, Nico
Heremans, Yves
Baeyens, Luc
Minami, Kohtaro
Ying, Cai
Lavens, Astrid
Chintinne, Marie
Stangé, Geert
Magenheim, Judith
Swisa, Avital
Martens, Geert
Pipeleers, Daniel
van de Casteele, Mark
Seino, Susumo
Keshet, Eli
Dor, Yuval
Heimberg, Harry
author_sort D'Hoker, Joke
collection PubMed
description It is generally accepted that vascularization and oxygenation of pancreatic islets are essential for the maintenance of an optimal β-cell mass and function and that signaling by vascular endothelial growth factor (VEGF) is crucial for pancreas development, insulin gene expression/secretion, and (compensatory) β-cell proliferation. A novel mouse model was designed to allow conditional production of human sFlt1 by β-cells in order to trap VEGF and study the effect of time-dependent inhibition of VEGF signaling on adult β-cell fate and metabolism. Secretion of sFlt1 by adult β-cells resulted in a rapid regression of blood vessels and hypoxia within the islets. Besides blunted insulin release, β-cells displayed a remarkable capacity for coping with these presumed unfavorable conditions: even after prolonged periods of blood vessel ablation, basal and stimulated blood glucose levels were only slightly increased, while β-cell proliferation and mass remained unaffected. Moreover, ablation of blood vessels did not prevent β-cell generation after severe pancreas injury by partial pancreatic duct ligation or partial pancreatectomy. Our data thus argue against a major role of blood vessels to preserve adult β-cell generation and function, restricting their importance to facilitating rapid and adequate insulin delivery.
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spelling pubmed-38370252014-12-01 Conditional Hypovascularization and Hypoxia in Islets Do Not Overtly Influence Adult β-Cell Mass or Function D'Hoker, Joke De Leu, Nico Heremans, Yves Baeyens, Luc Minami, Kohtaro Ying, Cai Lavens, Astrid Chintinne, Marie Stangé, Geert Magenheim, Judith Swisa, Avital Martens, Geert Pipeleers, Daniel van de Casteele, Mark Seino, Susumo Keshet, Eli Dor, Yuval Heimberg, Harry Diabetes Original Research It is generally accepted that vascularization and oxygenation of pancreatic islets are essential for the maintenance of an optimal β-cell mass and function and that signaling by vascular endothelial growth factor (VEGF) is crucial for pancreas development, insulin gene expression/secretion, and (compensatory) β-cell proliferation. A novel mouse model was designed to allow conditional production of human sFlt1 by β-cells in order to trap VEGF and study the effect of time-dependent inhibition of VEGF signaling on adult β-cell fate and metabolism. Secretion of sFlt1 by adult β-cells resulted in a rapid regression of blood vessels and hypoxia within the islets. Besides blunted insulin release, β-cells displayed a remarkable capacity for coping with these presumed unfavorable conditions: even after prolonged periods of blood vessel ablation, basal and stimulated blood glucose levels were only slightly increased, while β-cell proliferation and mass remained unaffected. Moreover, ablation of blood vessels did not prevent β-cell generation after severe pancreas injury by partial pancreatic duct ligation or partial pancreatectomy. Our data thus argue against a major role of blood vessels to preserve adult β-cell generation and function, restricting their importance to facilitating rapid and adequate insulin delivery. American Diabetes Association 2013-12 2013-11-16 /pmc/articles/PMC3837025/ /pubmed/23974922 http://dx.doi.org/10.2337/db12-1827 Text en © 2013 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. See http://creativecommons.org/licenses/by-nc-nd/3.0/ for details.
spellingShingle Original Research
D'Hoker, Joke
De Leu, Nico
Heremans, Yves
Baeyens, Luc
Minami, Kohtaro
Ying, Cai
Lavens, Astrid
Chintinne, Marie
Stangé, Geert
Magenheim, Judith
Swisa, Avital
Martens, Geert
Pipeleers, Daniel
van de Casteele, Mark
Seino, Susumo
Keshet, Eli
Dor, Yuval
Heimberg, Harry
Conditional Hypovascularization and Hypoxia in Islets Do Not Overtly Influence Adult β-Cell Mass or Function
title Conditional Hypovascularization and Hypoxia in Islets Do Not Overtly Influence Adult β-Cell Mass or Function
title_full Conditional Hypovascularization and Hypoxia in Islets Do Not Overtly Influence Adult β-Cell Mass or Function
title_fullStr Conditional Hypovascularization and Hypoxia in Islets Do Not Overtly Influence Adult β-Cell Mass or Function
title_full_unstemmed Conditional Hypovascularization and Hypoxia in Islets Do Not Overtly Influence Adult β-Cell Mass or Function
title_short Conditional Hypovascularization and Hypoxia in Islets Do Not Overtly Influence Adult β-Cell Mass or Function
title_sort conditional hypovascularization and hypoxia in islets do not overtly influence adult β-cell mass or function
topic Original Research
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3837025/
https://www.ncbi.nlm.nih.gov/pubmed/23974922
http://dx.doi.org/10.2337/db12-1827
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