Glucose metabolism in the Belgrade rat, a model of iron-loading anemia.

Jia X, Kim J, Veuthey T, Lee CH, Wessling-Resnick M.
Journal   Am J Physiol Gastrointest Liver Physiol.
Species  
Analytes Measured   Insulin
Matrix Tested   Serum
Year   2013
Volume  
Page Numbers  
Application   Metabolic
Abstract
The iron-diabetes hypothesis proposes an association between iron overload and glucose metabolism that is supported by a number of epidemiological studies. The prevalence of type 2 diabetes in patients with hereditary hemochromatosis and iron-loading thalassemia support this hypothesis. The Belgrade rat carries a mutation in the iron transporter DMT1 resulting in iron-loading anemia. In this study, we characterized the glycometabolic status of the Belgrade rat. Belgrade rats displayed normal glycemic control. Insulin signaling and secretion were not impaired, and pancreatic tissue did not incur damage despite high levels of non-heme iron. These findings suggest that loss of DMT1 protects against oxidative damage to the pancreas and helps to maintain insulin sensitivity despite iron overload. Belgrade rats had lower body weight but increased food consumption compared to heterozygous littermates. The unexpected energy balance was associated with increased urinary glucose output. Increased urinary excretion of electrolytes, including iron, was also observed. Histopathological evidence suggests that altered renal function is secondary to changes in kidney morphology including glomerulosclerosis. Thus, loss of DMT1 appears to protect the pancreas from injury but damages the integrity of kidney structure and function.

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