RESUMEN
Uric acid is an antioxidant in the extracellular environment, while it has prooxidative effects inside the cell. It is thought that antioxidative effects of uric acid may be protective, particularly in neurological diseases. While prooxidative effects of uric acid has a leading role in the development and progress of chronic kidney disease, metabolic syndrome and cardiovascular diseases. Uric acid is more than a product of purine metabolism. The uric acid paradox indicates that uric acid may play a central role in many diseases. This article was tried to review the researches and clinic studies of hyperuricemia from the viewpoint of the inflammation in recent years.
RESUMEN
Objective To evaluate the effects of elevated circulating free fatty acids (FFA) level on basal and glucose stimulated insulin secretion (GSIS) of islet β-cell and to explore the pathophysiological link between FFA and impaired β-cell dysfunction. Methods Male SD rats underwent infusions with normal saline (C group), intralipid+heparin (FFA group) and N-acetylcysteine+FFA (NAC group) for 2-4 days. Insulin secretion from pancreatic tissues was evaluated during intravenous glucose tolerance test and isolated pancreas perfasion test at the end of 2 and 4 days infusion. Results After 2 days infusion, the basal insulin secretion from isolated perfused pancreas was increased in FFA group [(55.5±19.4 vs 27.4±6.7) mU/L, P<0.01], but the response to 16.7 mmol/L glucose in isolated perfased pancreas was similar in FFA and C groups. The peak value during GSIS was inhibited by 4 days FFA infusion [(46.8±33.0 vs 214.7±27.4)mIU/L,P<0.05]. GSIS was also decreased in FFA group compared with C group in IVGTr. After interfered with NAC, GSIS was partly recovered [(165.4± 14.8)mIU/L, P<0.01]. Conclusion Elevated circulating FFA levels may contribute to the abnormality of pancreatic islet β-cell through oxidative stress.