| Literature DB >> 26406478 |
Jose F López-Acosta1,2, Pablo Villa-Pérez1,2, Cristina M Fernández-Díaz1, Daniel de Luis Román3, Ana R Díaz-Marrero4, Mercedes Cueto5, Germán Perdomo6, Irene Cózar-Castellano1.
Abstract
Diabetes is a consequence of a decrease on functional β-cell mass. We have recently demonstrated that epoxypukalide (Epoxy) is a natural compound with beneficial effects on primary cultures of rat islets. In this study, we extend our previous investigations to test the hypothesis that Epoxy protects β-cells and improves glucose metabolism in STZ-induced diabetic mice. We used 3-months old male mice that were treated with Epoxy at 200 μg/kg body weight. Glucose intolerance was induced by multiple intraperitoneal low-doses of streptozotocin (STZ) on 5 consecutive days. Glucose homeostasis was evaluated measuring plasma insulin levels and glucose tolerance. Histomorphometry was used to quantify the number of pancreatic β-cells per islet. β-cell proliferation was assessed by BrdU incorporation, and apoptosis by TUNEL staining. Epoxy treatment significantly improved glucose tolerance and plasma insulin levels. These metabolic changes were associated with increased β-cell numbers, as a result of a two-fold increase in β-cell proliferation and a 50% decrease in β-cell death. Our results demonstrate that Epoxy improves whole-body glucose homeostasis by preventing pancreatic β-cell death due to STZ-induced toxicity in STZ-treated mice.Entities:
Keywords: diabetes; epoxypukalide; hypoglycaemic agent; pancreatic β-cells
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Year: 2015 PMID: 26406478 PMCID: PMC4878260 DOI: 10.1080/19382014.2015.1078053
Source DB: PubMed Journal: Islets ISSN: 1938-2014 Impact factor: 2.694