Enhanced glucose tolerance in pancreatic-derived factor (PANDER) knockout C57BL/6 mice

Enhanced glucose tolerance in pancreatic-derived factor (PANDER) knockout C57BL/6 mice

Pancreatic-derived factor (PANDER; also known as FAM3B) is a uniquely structured protein strongly expressed within and secreted from the endocrine pancreas. PANDER has been hypothesized to regulate fasting and fed glucose homeostasis, hepatic lipogenesis and insulin signaling, and to serve a potenti...

Full description

Bibliographic Details
Main Authors: Shari L. Moak, Grace C. Dougan, Catherine B. MarElia, Whitney A. Danse, Amanda M. Fernandez, Melanie N. Kuehl, Mark G. Athanason, Brant R. Burkhardt
Format: Article
Language:English
Published: The Company of Biologists 2014-11-01
Series:Disease Models & Mechanisms
Subjects:
Pancreatic-derived factor
FAM3B
Knockout model
Glycemic regulation
Hepatic insulin signaling
Glucose tolerance
Online Access:http://dmm.biologists.org/content/7/11/1307
id doaj-5d48683149f1492aa6efbaa4439f360c
record_format Article
spelling doaj-5d48683149f1492aa6efbaa4439f360c2020-11-25T02:00:14ZengThe Company of BiologistsDisease Models & Mechanisms1754-84031754-84112014-11-017111307131510.1242/dmm.016402016402Enhanced glucose tolerance in pancreatic-derived factor (PANDER) knockout C57BL/6 miceShari L. MoakGrace C. DouganCatherine B. MarEliaWhitney A. DanseAmanda M. FernandezMelanie N. KuehlMark G. AthanasonBrant R. BurkhardtPancreatic-derived factor (PANDER; also known as FAM3B) is a uniquely structured protein strongly expressed within and secreted from the endocrine pancreas. PANDER has been hypothesized to regulate fasting and fed glucose homeostasis, hepatic lipogenesis and insulin signaling, and to serve a potential role in the onset or progression of type 2 diabetes (T2D). Despite having potentially pivotal pleiotropic roles in glycemic regulation and T2D, there has been limited generation of stable animal models for the investigation of PANDER function, and there are no models on well-established genetic murine backgrounds for T2D. Our aim was to generate an enhanced murine model to further elucidate the biological function of PANDER. Therefore, a pure-bred PANDER knockout C57BL/6 (PANKO-C57) model was created and phenotypically characterized with respect to glycemic regulation and hepatic insulin signaling. The PANKO-C57 model exhibited an enhanced metabolic phenotype, particularly with regard to enhanced glucose tolerance. Male PANKO-C57 mice displayed decreased fasting plasma insulin and C-peptide levels, whereas leptin levels were increased as compared with matched C57BL/6J wild-type mice. Despite similar peripheral insulin sensitivity between both groups, hepatic insulin signaling was significantly increased during fasting conditions, as demonstrated by increased phosphorylation of hepatic PKB/Akt and AMPK, along with mature SREBP-1 expression. Insulin stimulation of PANKO-C57 mice resulted in increased hepatic triglyceride and glycogen content as compared with wild-type C57BL/6 mice. In summary, the PANKO-C57 mouse represents a suitable model for the investigation of PANDER in multiple metabolic states and provides an additional tool to elucidate the biological function and potential role in T2D.http://dmm.biologists.org/content/7/11/1307Pancreatic-derived factorFAM3BKnockout modelGlycemic regulationHepatic insulin signalingGlucose tolerance
collection DOAJ
language English
format Article
sources DOAJ
author Shari L. Moak
Grace C. Dougan
Catherine B. MarElia
Whitney A. Danse
Amanda M. Fernandez
Melanie N. Kuehl
Mark G. Athanason
Brant R. Burkhardt
spellingShingle Shari L. Moak
Grace C. Dougan
Catherine B. MarElia
Whitney A. Danse
Amanda M. Fernandez
Melanie N. Kuehl
Mark G. Athanason
Brant R. Burkhardt
Enhanced glucose tolerance in pancreatic-derived factor (PANDER) knockout C57BL/6 mice
Disease Models & Mechanisms
Pancreatic-derived factor
FAM3B
Knockout model
Glycemic regulation
Hepatic insulin signaling
Glucose tolerance
author_facet Shari L. Moak
Grace C. Dougan
Catherine B. MarElia
Whitney A. Danse
Amanda M. Fernandez
Melanie N. Kuehl
Mark G. Athanason
Brant R. Burkhardt
author_sort Shari L. Moak
title Enhanced glucose tolerance in pancreatic-derived factor (PANDER) knockout C57BL/6 mice
title_short Enhanced glucose tolerance in pancreatic-derived factor (PANDER) knockout C57BL/6 mice
title_full Enhanced glucose tolerance in pancreatic-derived factor (PANDER) knockout C57BL/6 mice
title_fullStr Enhanced glucose tolerance in pancreatic-derived factor (PANDER) knockout C57BL/6 mice
title_full_unstemmed Enhanced glucose tolerance in pancreatic-derived factor (PANDER) knockout C57BL/6 mice
title_sort enhanced glucose tolerance in pancreatic-derived factor (pander) knockout c57bl/6 mice
publisher The Company of Biologists
series Disease Models & Mechanisms
issn 1754-8403
1754-8411
publishDate 2014-11-01
description Pancreatic-derived factor (PANDER; also known as FAM3B) is a uniquely structured protein strongly expressed within and secreted from the endocrine pancreas. PANDER has been hypothesized to regulate fasting and fed glucose homeostasis, hepatic lipogenesis and insulin signaling, and to serve a potential role in the onset or progression of type 2 diabetes (T2D). Despite having potentially pivotal pleiotropic roles in glycemic regulation and T2D, there has been limited generation of stable animal models for the investigation of PANDER function, and there are no models on well-established genetic murine backgrounds for T2D. Our aim was to generate an enhanced murine model to further elucidate the biological function of PANDER. Therefore, a pure-bred PANDER knockout C57BL/6 (PANKO-C57) model was created and phenotypically characterized with respect to glycemic regulation and hepatic insulin signaling. The PANKO-C57 model exhibited an enhanced metabolic phenotype, particularly with regard to enhanced glucose tolerance. Male PANKO-C57 mice displayed decreased fasting plasma insulin and C-peptide levels, whereas leptin levels were increased as compared with matched C57BL/6J wild-type mice. Despite similar peripheral insulin sensitivity between both groups, hepatic insulin signaling was significantly increased during fasting conditions, as demonstrated by increased phosphorylation of hepatic PKB/Akt and AMPK, along with mature SREBP-1 expression. Insulin stimulation of PANKO-C57 mice resulted in increased hepatic triglyceride and glycogen content as compared with wild-type C57BL/6 mice. In summary, the PANKO-C57 mouse represents a suitable model for the investigation of PANDER in multiple metabolic states and provides an additional tool to elucidate the biological function and potential role in T2D.
topic Pancreatic-derived factor
FAM3B
Knockout model
Glycemic regulation
Hepatic insulin signaling
Glucose tolerance
url http://dmm.biologists.org/content/7/11/1307
work_keys_str_mv AT sharilmoak enhancedglucosetoleranceinpancreaticderivedfactorpanderknockoutc57bl6mice
AT gracecdougan enhancedglucosetoleranceinpancreaticderivedfactorpanderknockoutc57bl6mice
AT catherinebmarelia enhancedglucosetoleranceinpancreaticderivedfactorpanderknockoutc57bl6mice
AT whitneyadanse enhancedglucosetoleranceinpancreaticderivedfactorpanderknockoutc57bl6mice
AT amandamfernandez enhancedglucosetoleranceinpancreaticderivedfactorpanderknockoutc57bl6mice
AT melanienkuehl enhancedglucosetoleranceinpancreaticderivedfactorpanderknockoutc57bl6mice
AT markgathanason enhancedglucosetoleranceinpancreaticderivedfactorpanderknockoutc57bl6mice
AT brantrburkhardt enhancedglucosetoleranceinpancreaticderivedfactorpanderknockoutc57bl6mice
_version_ 1724961998287929344

Similar Items