Targeted Disruption of Pancreatic-Derived Factor (PANDER, FAM3B) Impairs Pancreatic β-Cell Function

OBJECTIVE: Pancreatic-derived factor (PANDER, FAM3B) is a pancreatic islet-specific cytokine-like protein that is secreted from β-cells upon glucose stimulation. The biological function of PANDER is unknown, and to address this we generated and characterized a PANDER knockout mouse. RESEARCH DESIGN...

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Autores principales: Robert-Cooperman, Claudia E., Carnegie, Jason R., Wilson, Camella G., Yang, Jichun, Cook, Joshua R., Wu, Jianmei, Young, Robert A., Wolf, Bryan A., Burkhardt, Brant R.
Formato: Texto
Lenguaje:English
Publicado: American Diabetes Association 2010
Materias:
Islet Studies
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2927943/
https://www.ncbi.nlm.nih.gov/pubmed/20566664
http://dx.doi.org/10.2337/db09-1552
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author Robert-Cooperman, Claudia E.
Carnegie, Jason R.
Wilson, Camella G.
Yang, Jichun
Cook, Joshua R.
Wu, Jianmei
Young, Robert A.
Wolf, Bryan A.
Burkhardt, Brant R.
author_facet Robert-Cooperman, Claudia E.
Carnegie, Jason R.
Wilson, Camella G.
Yang, Jichun
Cook, Joshua R.
Wu, Jianmei
Young, Robert A.
Wolf, Bryan A.
Burkhardt, Brant R.
author_sort Robert-Cooperman, Claudia E.
collection PubMed
description OBJECTIVE: Pancreatic-derived factor (PANDER, FAM3B) is a pancreatic islet-specific cytokine-like protein that is secreted from β-cells upon glucose stimulation. The biological function of PANDER is unknown, and to address this we generated and characterized a PANDER knockout mouse. RESEARCH DESIGN AND METHODS: To generate the PANDER knockout mouse, the PANDER gene was disrupted and its expression was inhibited by homologous recombination via replacement of the first two exons, secretion signal peptide and transcriptional start site, with the neomycin gene. PANDER(−/−) mice were then phenotyped by a number of in vitro and in vivo tests to evaluate potential effects on glucose regulation, insulin sensitivity, and β-cell morphology and function. RESULTS: Glucose tolerance tests demonstrated significantly higher blood glucose levels in PANDER(−/−) versus wild-type male mice. To identify the mechanism of the glucose intolerance, insulin sensitivity and pancreatic β-cell function were examined. Hyperinsulinemic-euglycemic clamps and insulin tolerance testing showed similar insulin sensitivity for both the PANDER(−/−) and wild-type mice. The in vivo insulin response following intraperitoneal glucose injection surprisingly produced significantly higher insulin levels in the PANDER(−/−) mice, whereas insulin release was blunted with arginine administration. Islet perifusion and calcium imaging studies showed abnormal responses of the PANDER(−/−) islets to glucose stimulation. In contrast, neither islet architecture nor insulin content was impacted by the loss of PANDER. Interestingly, the elevated insulin levels identified in vivo were attributed to decreased hepatic insulin clearance in the PANDER(−/−) islets. Taken together, these results demonstrated decreased pancreatic β-cell function in the PANDER(−/−) mouse. CONCLUSIONS: These results support a potential role of PANDER in the pancreatic β-cell for regulation or facilitation of insulin secretion.
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spelling pubmed-29279432011-09-01 Targeted Disruption of Pancreatic-Derived Factor (PANDER, FAM3B) Impairs Pancreatic β-Cell Function Robert-Cooperman, Claudia E. Carnegie, Jason R. Wilson, Camella G. Yang, Jichun Cook, Joshua R. Wu, Jianmei Young, Robert A. Wolf, Bryan A. Burkhardt, Brant R. Diabetes Islet Studies OBJECTIVE: Pancreatic-derived factor (PANDER, FAM3B) is a pancreatic islet-specific cytokine-like protein that is secreted from β-cells upon glucose stimulation. The biological function of PANDER is unknown, and to address this we generated and characterized a PANDER knockout mouse. RESEARCH DESIGN AND METHODS: To generate the PANDER knockout mouse, the PANDER gene was disrupted and its expression was inhibited by homologous recombination via replacement of the first two exons, secretion signal peptide and transcriptional start site, with the neomycin gene. PANDER(−/−) mice were then phenotyped by a number of in vitro and in vivo tests to evaluate potential effects on glucose regulation, insulin sensitivity, and β-cell morphology and function. RESULTS: Glucose tolerance tests demonstrated significantly higher blood glucose levels in PANDER(−/−) versus wild-type male mice. To identify the mechanism of the glucose intolerance, insulin sensitivity and pancreatic β-cell function were examined. Hyperinsulinemic-euglycemic clamps and insulin tolerance testing showed similar insulin sensitivity for both the PANDER(−/−) and wild-type mice. The in vivo insulin response following intraperitoneal glucose injection surprisingly produced significantly higher insulin levels in the PANDER(−/−) mice, whereas insulin release was blunted with arginine administration. Islet perifusion and calcium imaging studies showed abnormal responses of the PANDER(−/−) islets to glucose stimulation. In contrast, neither islet architecture nor insulin content was impacted by the loss of PANDER. Interestingly, the elevated insulin levels identified in vivo were attributed to decreased hepatic insulin clearance in the PANDER(−/−) islets. Taken together, these results demonstrated decreased pancreatic β-cell function in the PANDER(−/−) mouse. CONCLUSIONS: These results support a potential role of PANDER in the pancreatic β-cell for regulation or facilitation of insulin secretion. American Diabetes Association 2010-09 2010-06-21 /pmc/articles/PMC2927943/ /pubmed/20566664 http://dx.doi.org/10.2337/db09-1552 Text en © 2010 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 Islet Studies
Robert-Cooperman, Claudia E.
Carnegie, Jason R.
Wilson, Camella G.
Yang, Jichun
Cook, Joshua R.
Wu, Jianmei
Young, Robert A.
Wolf, Bryan A.
Burkhardt, Brant R.
Targeted Disruption of Pancreatic-Derived Factor (PANDER, FAM3B) Impairs Pancreatic β-Cell Function
title Targeted Disruption of Pancreatic-Derived Factor (PANDER, FAM3B) Impairs Pancreatic β-Cell Function
title_full Targeted Disruption of Pancreatic-Derived Factor (PANDER, FAM3B) Impairs Pancreatic β-Cell Function
title_fullStr Targeted Disruption of Pancreatic-Derived Factor (PANDER, FAM3B) Impairs Pancreatic β-Cell Function
title_full_unstemmed Targeted Disruption of Pancreatic-Derived Factor (PANDER, FAM3B) Impairs Pancreatic β-Cell Function
title_short Targeted Disruption of Pancreatic-Derived Factor (PANDER, FAM3B) Impairs Pancreatic β-Cell Function
title_sort targeted disruption of pancreatic-derived factor (pander, fam3b) impairs pancreatic β-cell function
topic Islet Studies
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2927943/
https://www.ncbi.nlm.nih.gov/pubmed/20566664
http://dx.doi.org/10.2337/db09-1552
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