A mouse model of gestational glucose intolerance through exposure to a low protein diet during fetal and neonatal development

Sandra K Szlapinski; Renee T King; Gabrielle Retta; Erica Yeo; Brenda J Strutt; David J Hill

doi:10.1113/JP277884

A mouse model of gestational glucose intolerance through exposure to a low protein diet during fetal and neonatal development

J Physiol. 2019 Aug;597(16):4237-4250. doi: 10.1113/JP277884. Epub 2019 Jul 11.

Authors

Sandra K Szlapinski^{1

2}, Renee T King², Gabrielle Retta², Erica Yeo², Brenda J Strutt^{1

2}, David J Hill^{1

2}

Affiliations

¹ Department of Physiology and Pharmacology, Western University, 1151 Richmond St., London, ON, Canada.
² Lawson Health Research Institute, St Joseph's Health Care, 268 Grosvenor St., F4-124, London, ON, Canada.

PMID: 31206692
DOI: 10.1113/JP277884

Abstract

Key points: Pancreatic β-cell dysfunction is hypothesized to be the significant determinant of gestational diabetes pathogenesis, however pancreatic samples from patients are scarce. This study reports a novel mouse model of gestational glucose intolerance in pregnancy, originating from previous nutrition restriction in utero, in which glucose intolerance was restricted to late gestation as is seen in human gestational diabetes. Glucose intolerance was attributed to reduced β-cell proliferation, leading to impaired gestational β-cell mass expansion in maternal endocrine pancreas, in addition to reduced glucose-stimulated insulin secretion. This model reproduces some of the features of gestational diabetes and is suitable for testing safe therapeutic interventions that increase β-cell mass during pregnancy and prevent or reverse gestational glucose intolerance.

Abstract: Gestational diabetes mellitus (GDM) is an increasingly prevalent form of diabetes that appears during pregnancy. Pathological studies link a failure to adaptively increase maternal pancreatic β-cell mass (BCM) in pregnancy to GDM. Due to the scarcity of pancreatic samples from GDM patients, we sought to develop a novel mouse model for impaired gestational glucose tolerance. Mature female C57Bl/6 mouse offspring (F1) born to dams fed either a control (C) or low-protein (LP) diet during gestation and lactation were randomly allocated into two subsequent study groups: pregnant (CP, LPP) or non-pregnant (CNP, LPNP). Glucose tolerance tests were performed at gestational day (GD) 9, 12 and 18. Subsequently, pancreata were removed for fluorescence immunohistochemistry to assess α-cell mass (ACM), BCM and β-cell proliferation. An additional group of animals was used to measure insulin secretion from isolated islets at GD18. LPP females displayed glucose intolerance compared to CP females at GD18 (P < 0.001). BCM increased threefold at GD18 in CP females. However, LPP females had reduced BCM expansion (P < 0.01) concurrent with reduced β-cell proliferation at GD12 (P < 0.05). LPP females also had reduced ACM expansion at GD18 (P < 0.01). LPP islets had impaired glucose-stimulated insulin secretion in vitro compared to CP islets (P < 0.01). Therefore, impaired glucose tolerance during pregnancy is associated with a failure to adequately adapt BCM, as a result of reduced β-cell proliferation, in addition to lower glucose-stimulated insulin secretion. This model could be used to evaluate novel interventions during pregnancy to increase BCM or function as a strategy to prevent/reverse GDM.

Keywords: glucose tolerance; insulin secretion; low protein diet; mouse; pregnancy; β-cell mass.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Animal Feed / analysis
Animals
Animals, Newborn
Diabetes, Gestational / chemically induced*
Diet / veterinary
Diet, Protein-Restricted / adverse effects*
Female
Fetal Development
Glucose Intolerance
Glucose Tolerance Test
Insulin-Secreting Cells / metabolism
Male
Maternal Nutritional Physiological Phenomena
Mice
Pregnancy
Prenatal Exposure Delayed Effects