Publication | Open Access
Initial FGF23-Mediated Signaling Occurs in the Distal Convoluted Tubule
233
Citations
26
References
2009
Year
Distal Convoluted TubuleFgf23 InjectionRenal InflammationFgf23 BioactivityCellular PhysiologyRenal FunctionSignaling PathwayDct CellsFibroblast Growth FactorKidney Tubule RemodelingChronic Kidney DiseaseCell SignalingMolecular PhysiologyMorphogenesisCell BiologyUrologySignal TransductionDiabetic Kidney DiseaseMedicineNephrologyKidney ResearchExtracellular Matrix
Fibroblast growth factor-23 (FGF23), a hormone central to phosphate and vitamin D metabolism, reduces renal absorption of phosphate by downregulating the sodium-phosphate cotransporter Npt2a. However, the mechanisms of FGF23 action in the kidney are unclear, as Npt2a localizes to the proximal tubule (PT) and the FGF23 coreceptor alpha-Klotho (KL) localizes to the distal convoluted tubule (DCT). Immunofluorescent analyses following FGF23 injection in mice showed robust staining for phospho-ERK1/2, a marker of FGF23 bioactivity, only within the DCT in a subset of KL-positive cells. This activity colocalized with the FGF23 receptor FGFR1 and was present in DCT cells that were adjacent to Npt2a-expressing PT segments. Although KL is expressed as both secreted and membrane-bound isoforms, only the membrane-bound isoform was capable of mediating FGF23 bioactivity. These findings provide novel insight into the mechanisms of hormone-regulated phosphate metabolism by identifying an intrarenal signaling axis for FGF23.
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