Hyperglycaemia induces metabolic dysfunction and glycogen accumulation in pancreatic β-cells

Melissa F. Brereton(University of Oxford), Maria Rohm(University of Oxford), Kenju Shimomura(University of Oxford), Christian Holland(University of Oxford), Sharona Tornovsky-Babeay(Hadassah Medical Center), Daniela Dadon, Michaela Iberl(University of Oxford), Margarita V. Chibalina(Churchill Hospital), Sheena Lee(University of Oxford), Benjamin Gläser(Hadassah Medical Center), Yuval Dor, Patrik Rorsman(Churchill Hospital), Anne Clark(Churchill Hospital), Frances M. Ashcroft(University of Oxford)
Nature Communications
November 24, 2016
10.1038/ncomms13496
Cited by 120Open Access
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Abstract

Insulin secretion from pancreatic β-cells is impaired in all forms of diabetes. The resultant hyperglycaemia has deleterious effects on many tissues, including β-cells. Here we show that chronic hyperglycaemia impairs glucose metabolism and alters expression of metabolic genes in pancreatic islets. In a mouse model of human neonatal diabetes, hyperglycaemia results in marked glycogen accumulation, and increased apoptosis in β-cells. Sulphonylurea therapy rapidly normalizes blood glucose levels, dissipates glycogen stores, increases autophagy and restores β-cell metabolism. Insulin therapy has the same effect but with slower kinetics. Similar changes are observed in mice expressing an activating glucokinase mutation, in in vitro models of hyperglycaemia, and in islets from type-2 diabetic patients. Altered β-cell metabolism may underlie both the progressive impairment of insulin secretion and reduced β-cell mass in diabetes.

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