Permanent Neonatal Diabetes in INSC94Y Transgenic Pigs

Author:

Renner Simone1,Braun-Reichhart Christina1,Blutke Andreas2,Herbach Nadja2,Emrich Daniela2,Streckel Elisabeth1,Wünsch Annegret1,Kessler Barbara1,Kurome Mayuko13,Bähr Andrea1,Klymiuk Nikolai1,Krebs Stefan4,Puk Oliver5,Nagashima Hiroshi3,Graw Jochen5,Blum Helmut5,Wanke Ruediger2,Wolf Eckhard143

Affiliation:

1. Chair for Molecular Animal Breeding and Biotechnology, Ludwig Maximilian University Munich, Munich, Germany

2. Institute of Veterinary Pathology at the Centre for Clinical Veterinary Medicine, Ludwig Maximilian University Munich, Munich, Germany

3. Meiji University, International Institute for Bio-Resource Research, Kawasaki, Japan

4. Laboratory for Functional Genome Analysis, Gene Center, Ludwig Maximilian University Munich, Munich, Germany

5. Helmholtz Center Munich-German Research Center for Environmental Health, Institute of Developmental Genetics, Neuherberg, Germany

Abstract

Mutations in the insulin (INS) gene may cause permanent neonatal diabetes mellitus (PNDM). Ins2 mutant mouse models provided important insights into the disease mechanisms of PNDM but have limitations for translational research. To establish a large animal model of PNDM, we generated INSC94Y transgenic pigs. A line expressing high levels of INSC94Y mRNA (70–86% of wild-type INS transcripts) exhibited elevated blood glucose soon after birth but unaltered β-cell mass at the age of 8 days. At 4.5 months, INSC94Y transgenic pigs exhibited 41% reduced body weight, 72% decreased β-cell mass (−53% relative to body weight), and 60% lower fasting insulin levels compared with littermate controls. β-cells of INSC94Y transgenic pigs showed a marked reduction of insulin secretory granules and severe dilation of the endoplasmic reticulum. Cataract development was already visible in 8-day-old INSC94Y transgenic pigs and became more severe with increasing age. Diabetes-associated pathological alterations of kidney and nervous tissue were not detected during the observation period of 1 year. The stable diabetic phenotype and its rescue by insulin treatment make the INSC94Y transgenic pig an attractive model for insulin supplementation and islet transplantation trials, and for studying developmental consequences of maternal diabetes mellitus.

Publisher

American Diabetes Association

Subject

Endocrinology, Diabetes and Metabolism,Internal Medicine

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