-The onset of diabetic nephropathy (DN) is associated with both systemic and renal changes. Fibroblast growth factor (FGF)-21 prevents diabetic complications mainly by improving systemic metabolism. In addition, low-dose radiation (LDR) protects mice from DN directly by preventing renal oxidative stress and inflammation. In the present study, we tried to define whether the combination of FGF21 and LDR could further prevent DN by blocking its systemic and renal pathogeneses. To this end, type 2 diabetes was induced by feeding a high-fat diet for 12 wk followed by a single dose injection of streptozotocin. Diabetic mice were exposed to 50 mGy LDR every other day for 4 wk with and without 1.5 mg/kg FGF21 daily for 8 wk. The changes in systemic parameters, including blood glucose levels, lipid profiles, and insulin resistance, as well as renal pathology, were examined. Diabetic mice exhibited renal dysfunction and pathological abnormalities, all of which were prevented significantly by LDR and/or FGF21; the best effects were observed in the group that received the combination treatment. Our studies revealed that the additive renal protection conferred by the combined treatment against diabetes-induced renal fibrosis, inflammation, and oxidative damage was associated with the systemic improvement of hyperglycemia, hyperlipidemia, and insulin resistance. These results suggest that the combination treatment with LDR and FGF21 prevented DN more efficiently than did either treatment alone. The mechanism behind these protective effects could be attributed to the suppression of both systemic and renal pathways. low-dose radiation; fibroblast growth factor-21; insulin resistance; inflammation; oxidative stress DIABETIC NEPHROPATHY (DN) is a severe complication of diabetes and the leading cause of end-stage renal disease (38). DN initiates with the thickening of the glomerular basement membrane, which is followed by mild and moderate mesangial expansion, capillary collapse in the renal tubule, epithelial cell degeneration, and a gradual increase in proteinuria, and finally leads to renal fibrosis and kidney failure (43, 56). Hyperglycemia, hyperlipidemia, and subsequent insulin resistance are the initial and systemic pathogeneses of DN, which is also associated with renal pathogeneses, such as oxidative stress, inflammation, and fibrosis. There are currently multiple therapies to treat patients with DN, including reducing blood sugar levels, lowering lipid levels, enhancing insulin sensitivity, and reducing oxidative stress, inflammation, or fibrosis (1, 19, 50). However, most of these treatments just slow rather than arrest the progression toward DN, since blocking any single pathway is not sufficient to prevent the development of DN (8,19). Therefore, identifying a treatment that inhibits both the systemic and renal pathogeneses will prevent the development of DN efficiently.Fibroblast growth factor (FGF)-21 is a novel member of the FGF family that functions as an endocrine hormone rather than regulating cellular prolifera...
