In renal failure, hyperphosphatemia occurs despite a marked elevation in serum fibroblast growth factor (FGF)-23. Abnormal regulation of the FGFR1-Klotho receptor complex may cause a resistance to the phosphaturic action of FGF23. The purpose of the present study was to investigate the regulation of renal Klotho and FGF receptor (FEFR)-1 in healthy and uremic rats induced by 5/6 nephrectomy. In normal rats, the infusion of rat recombinant FGF23 enhanced phosphaturia and increased renal FGFR1 expression; however, Klotho expression was reduced. Uremic rats on a highphosphate (HP) diet presented hyperphosphatemia with marked elevation of FGF23 and an increased fractional excretion of phosphate (P) that was associated with a marked reduction of Klotho expression and an increase in FGFR1. After neutralization of FGF23 by anti-FGF23 administration, phosphaturia was still abundant, Klotho expression remained low, and the FGFR1 level was reduced. These results suggest that the expression of renal Klotho is modulated by phosphaturia, whereas the FGFR1 expression is regulated by FGF23. Calcitriol (CTR) administration prevented a decrease in renal Klotho expression. In HEK293 cells HP produced nuclear translocation of b-catenin, together with a reduction in Klotho. Wnt/b-catenin inhibition with Dkk-1 prevented the P-induced down-regulation of Klotho. The addition of CTR to HP medium was able to recover Klotho expression. In summary, high FGF23 levels increase FGFR1, whereas phosphaturia decreases Klotho expression through the activation of Wnt/b-catenin pathway.-Muñoz-Castañeda, J. R., Herencia, C., Pendón-Ruiz de Mier, M. V., Rodriguez-Ortiz, M. E., Diaz-Tocados, J. M., Vergara, N., Martínez-Moreno, J. M., Salmerón, M. D., Richards, W. G., Felsenfeld, A., Kuro-O, M., Almadén, Y., Rodríguez, M. Differential regulation of renal Klotho and FGFR1 in normal and uremic rats. FASEB J. 31, 3858-3867 (2017). www.fasebj.orgFibroblast growth factor (FGF)-23 is produced by osteocytes and acts on a kidney-specific receptor, fibroblast growth factor receptor (FGFR)-1-Klotho, to decrease both tubular reabsorption of phosphate (P) and synthesis of 1,25(OH) 2 D 3 (calcitriol, or CTR) (1). Lack of FGF23 causes hyperphosphatemia, increased production of CTR, and vascular calcification (2). FGF23 also inhibits parathyroid hormone (PTH) secretion by acting on its specific receptor, which is also expressed on parathyroid cells (3, 4). The serum level of FGF23 increases during the early development of renal failure and contributes to the control of P by enhancing phosphaturia, but it also causes a reduction in CTR production that is commonly observed even at early stages of renal failure (5). It is widely accepted that FGF23 plays an essential role in the development of chronic kidney disease (CKD) and mineral and bone disorders. A high concentration of FGF23 is also associated with mortality (6), left ventricular hypertrophy (7), and progressive deterioration of renal function (8).
