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DOI: 10.1055/s-2008-1081486
© J. A. Barth Verlag in Georg Thieme Verlag KG Stuttgart · New York
Reduced Insulin Secretion and Content in VEGF-A Deficient Mouse Pancreatic Islets
Publication History
received 18.02.2008
accepted 20.03.2008
Publication Date:
05 September 2008 (online)
Abstract
Mice, deficient for vascular endothelial growth factor VEGF-A in pancreatic islets, have reduced insulin gene expression levels and an impaired glucose tolerance. Here, we investigated whether VEGF-A was required for physiological glucose-stimulated insulin secretion and insulin content. We performed in situ pancreas perfusions and islet perifusions on mice lacking VEGF-A in the pancreatic epithelium in order to study their ability to secrete insulin in response to glucose. We identified insulin secretion defects in the pancreata of VEGF-A deficient mice, including a delayed and blunted response to glucose. Islet perifusion experiments revealed a missing first phase and weaker second phase of insulin secretion, in two of three VEGF-A deficient mice. On average, insulin content in VEGF-A deficient islets was significantly reduced when compared with control islets. We conclude that VEGF-A is required in pancreatic islets for normal glucose-stimulated insulin secretion and physiological insulin content. Thus, VEGF-A is a key factor for pancreatic islet function.
Key words
vascular endothelial growth factor - capillary network - pancreatic islet - insulin secretion - pancreas perfusion - islet perifusion
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Correspondence
E. Lammert
Max Planck Institute of Molecular Cell Biology and Genetics
Pfotenhauerstr. 108
01307 Dresden
Germany
Phone: +49/351/210 27 77
Fax: +49/351/210 12 09
Email: lammert@mpi-cbg.de