Abnormal endocrine pancreas function at birth in cystic fibrosis ferrets
Alicia K. Olivier, … , Andrew W. Norris, John F. Engelhardt
Alicia K. Olivier, … , Andrew W. Norris, John F. Engelhardt
Published September 17, 2012
Citation Information: J Clin Invest. 2012;122(10):3755-3768. https://doi.org/10.1172/JCI60610.
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Technical Advance Metabolism

Abnormal endocrine pancreas function at birth in cystic fibrosis ferrets

Abstract

Diabetes is a common comorbidity in cystic fibrosis (CF) that worsens prognosis. The lack of an animal model for CF-related diabetes (CFRD) has made it difficult to dissect how the onset of pancreatic pathology influences the emergence of CFRD. We evaluated the structure and function of the neonatal CF endocrine pancreas using a new CFTR-knockout ferret model. Although CF kits are born with only mild exocrine pancreas disease, progressive exocrine and endocrine pancreatic loss during the first months of life was associated with pancreatic inflammation, spontaneous hyperglycemia, and glucose intolerance. Interestingly, prior to major exocrine pancreas disease, CF kits demonstrated significant abnormalities in blood glucose and insulin regulation, including diminished first-phase and accentuated peak insulin secretion in response to glucose, elevated peak glucose levels following glucose challenge, and variably elevated insulin and C-peptide levels in the nonfasted state. Although there was no difference in lobular insulin and glucagon expression between genotypes at birth, significant alterations in the frequencies of small and large islets were observed. Newborn cultured CF islets demonstrated dysregulated glucose-dependent insulin secretion in comparison to controls, suggesting intrinsic abnormalities in CF islets. These findings demonstrate that early abnormalities exist in the regulation of insulin secretion by the CF endocrine pancreas.

Authors

Alicia K. Olivier, Yaling Yi, Xingshen Sun, Hongshu Sui, Bo Liang, Shanming Hu, Weiliang Xie, John T. Fisher, Nicholas W. Keiser, Diana Lei, Weihong Zhou, Ziying Yan, Guiying Li, Turan I.A. Evans, David K. Meyerholz, Kai Wang, Zoe A. Stewart, Andrew W. Norris, John F. Engelhardt

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Figure 2

Progressive pancreatic fibrosis and inflammation in the neonatal CF ferret pancreas.

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Progressive pancreatic fibrosis and inflammation in the neonatal CF ferr...
(A) Time-dependent fibrosis of CF pancreata within the first month of life. Fibrous tissue stains blue by Masson trichrome stain in the interstitium (arrows). Note that the intraluminal material within dilated acinoductular units is nonspecific staining. Scale bars: 100 μm. (B and C) Inflammation scores were determined using a 0–3 scoring system based on number of interstitial inflammatory cells (arrows) per high-power field (HPF): 0 (no inflammatory cells/HPF), 1+ (1–9 inflammatory cells/HPF), 2+ (10–30 inflammatory cells/HPF), 3+ (>30 inflammatory cells/HPF). Degenerative neutrophils in acinoductular lumens, which increased with age, were not included in the inflammation scoring. (B) Histologic examples and scores for CF animals of various ages. Scale bars: 25 μm. (C) Average score for each animal evaluated for the various age groups, with n total animals in each group. *P < 0.001, 9- to 32-day-old CF versus non-CF controls, Kruskal-Wallis non-parametric 1-way ANOVA with a Dunn’s post-test. Differences between genotypes in newborns or 2- to 5-day-old animals were not significant.