Pioglitazone preserves pancreatic islet structure and insulin secretory function in three murine models of type 2 diabetes

Thiazolidinediones may slow the progression of type 2 diabetes by preserving pancreatic beta-cells. The effects of pioglitazone (PIO) on structure and function of beta-cells in KKA(y), C57BL/6J ob/ob, and C57BL/KsJ db/db mice ( genetic models of type 2 diabetes) were examined. ob/ob (n = 7) and db/db ( n = 9) mice were randomly assigned to 50 - 125 mg . kg body wt(-1) . day(-1) of PIO in chow beginning at 6 - 10 wk of age. Control ob/ob ( n = 7) and db/db mice ( n = 9) were fed chow without PIO. KKA( y) mice ( n = 15) were fed PIO daily at doses of 62 - 144 mg . kg body wt(-1) . day(-1). Control KKA(y) mice ( n = 10) received chow without PIO. Treatment continued until euthanasia at 14 - 26 wk of age. Blood was collected at baseline ( before treatment) and just before euthanasia and was analyzed for glucose, glycosylated hemoglobin, and plasma insulin. Some of the splenic pancreas of each animal was resected and partially sectioned for light or electron microscopy. The remainder of the pancreas was assayed for insulin content. Compared with baseline and control groups, PIO treatment significantly reduced blood glucose and glycosylated hemoglobin levels. Plasma insulin levels decreased significantly in ob/ob mice treated with PIO. All groups treated with PIO exhibited significantly greater beta-cell granulation, evidence of reduced beta-cell stress, and 1.5- to 15-fold higher levels of pancreatic insulin. The data from these studies suggest that comparable effects would be expected to slow the progression of type 2 diabetes, either delaying or possibly preventing progression to an insulin-dependent state.