Regulation of Fibroblast Growth Factor-23 Signaling by Klotho

Kurosu, Hiroshi; Ogawa, Yasushi; Miyoshi, Masayoshi; Yamamoto, Masaya; Nandi, Animesh; Rosenblatt, Kevin P.; Baum, Michel; Schiavi, Susan C.; Hu, Ming‐Chang; Moe, Orson W.; Kuro‐o, Makoto

doi:10.1074/jbc.c500457200

Cited by 1,215 publications

(1,174 citation statements)

References 27 publications

Supporting

Mentioning

1,105

Contrasting

Unclassified

Order By: Relevance

“…The wide-ranging activity of klotho raises the possibility that regulation of Ca and phosphate metabolism is an Urinary P ↑ Urinary Ca ↓ essential feature of many systems of the body, not just those connected with the skeleton. Further information on this area of discussion is available (1,20,(32)(33)(34)(35)(36)(37)(38)(39)(40)(41)(42)(43)(44)(45)(46)(47)(48) .…”

Section: Low Serum Calciummentioning

confidence: 99%

Elsie Widdowson Lecture 2006 Mining the depths: metabolic insights into mineral nutrition

Prentice

2007

Proc. Nutr. Soc.

View full text Add to dashboard Cite

2006 marked the centenary of the birth of Dr Elsie Widdowson, a pioneer of nutrition science. One of the hallmarks of Elsie Widdowson's research was an integrative approach that recognised the importance of investigating the mechanisms underpinning a public health or clinical issue at all levels, looking into the physiology, comparative biology, intermediate metabolism and basic science. The theme of the present lecture, given in celebration of the work of Dr Widdowson, is mineral nutrition, with a particular focus on Ca, P and vitamin D. The contributions of Dr Widdowson to the early understanding of mineral nutrition are reviewed and the latest scientific findings in this rapidly-expanding field of research are presented.

show abstract

Section: Low Serum Calciummentioning

confidence: 99%

Elsie Widdowson Lecture 2006 Mining the depths: metabolic insights into mineral nutrition

Prentice

2007

Proc. Nutr. Soc.

View full text Add to dashboard Cite

show abstract

“…These mutations replace the arginine (R) residues at positions 176 or 179 with glutamine (Q) or tryptophan (W) within a 176 RXXR 179 / S 180 subtilisin-like proprotein convertase (SPC) site that separates the conserved FGF-like N-terminal domain from the variable Cterminal tail (2)(3)(4). Acting through the coreceptor α-Klotho (5) and a fibroblast growth factor receptor (FGFR) (5,6), FGF23 reduces renal phosphate reabsorption through down-regulation of the sodium phosphate cotransporters NPT2a and NPT2c and suppresses kidney 1,25(OH) 2 vitamin D production by inhibiting and increasing vitamin D 1α-hydroxylase (Cyp27b1) and 24-hydroxylase expression (Cyp24), respectively (7). Compared with WT Fgf23 protein, ADHR-mutant FGF23 shows increased but not complete resistance to SPC proteolytic cleavage (3,4).…”

mentioning

confidence: 99%

Iron deficiency drives an autosomal dominant hypophosphatemic rickets (ADHR) phenotype in fibroblast growth factor-23 (Fgf23) knock-in mice

Farrow

Summers

et al. 2011

Proc. Natl. Acad. Sci. U.S.A.

327

324

View full text Add to dashboard Cite

Autosomal dominant hypophosphatemic rickets (ADHR) is unique among the disorders involving Fibroblast growth factor 23 (FGF23) because individuals with R176Q/W and R179Q/W mutations in the FGF23 176 RXXR 179 /S 180 proteolytic cleavage motif can cycle from unaffected status to delayed onset of disease. This onset may occur in physiological states associated with iron deficiency, including puberty and pregnancy. To test the role of iron status in development of the ADHR phenotype, WT and R176Q-Fgf23 knock-in (ADHR) mice were placed on control or low-iron diets. Both the WT and ADHR mice receiving low-iron diet had significantly elevated bone Fgf23 mRNA. WT mice on a low-iron diet maintained normal serum intact Fgf23 and phosphate metabolism, with elevated serum C-terminal Fgf23 fragments. In contrast, the ADHR mice on the low-iron diet had elevated intact and C-terminal Fgf23 with hypophosphatemic osteomalacia. We used in vitro iron chelation to isolate the effects of iron deficiency on Fgf23 expression. We found that iron chelation in vitro resulted in a significant increase in Fgf23 mRNA that was dependent upon Mapk. Thus, unlike other syndromes of elevated FGF23, our findings support the concept that late-onset ADHR is the product of gene-environment interactions whereby the combined presence of an Fgf23-stabilizing mutation and iron deficiency can lead to ADHR.Online Mendelian Inheritance in Man no. 193100) is characterized by low serum phosphate concentrations due to isolated renal phosphate wasting, inappropriately normal or low serum 1,25(OH) 2 vitamin D (1,25D) concentrations, and rickets/osteomalacia and fracture (1). Heterozygous missense mutations in the fibroblast growth factor-23 (FGF23) gene cause ADHR (2). These mutations replace the arginine (R) residues at positions 176 or 179 with glutamine (Q) or tryptophan (W) within a 176 RXXR 179 / S 180 subtilisin-like proprotein convertase (SPC) site that separates the conserved FGF-like N-terminal domain from the variable Cterminal tail (2-4). Acting through the coreceptor α-Klotho (5) and a fibroblast growth factor receptor (FGFR) (5, 6), FGF23 reduces renal phosphate reabsorption through down-regulation of the sodium phosphate cotransporters NPT2a and NPT2c and suppresses kidney 1,25(OH) 2 vitamin D production by inhibiting and increasing vitamin D 1α-hydroxylase (Cyp27b1) and 24-hydroxylase expression (Cyp24), respectively (7). Compared with WT Fgf23 protein, ADHR-mutant FGF23 shows increased but not complete resistance to SPC proteolytic cleavage (3, 4). When expressed in mammalian cells, the R176Q-, R179Q-, and R179W-FGF23 proteins are secreted primarily as the full-length (32-kDa) polypeptide, in contrast to the full-length and cleavage products (20 and 12 kDa) typically observed for WT FGF23 (3). This proteolytic event inactivates the mature FGF23 polypeptide, as full-length FGF23, but not N-terminal fragments (residues 25-179) or C-terminal fragments (residues 180-251), reduces serum phosphate concentrations when injected into rodents (4).The ADHR...

show abstract

“…FGF23 contains a consensus binding domain for FGFRs and several studies have suggested that FGF23 may bind and activate signaling through one or more FGFRs [31][32][33]. Recent in vivo genetic manipulation studies suggest that both FGF23 and KLOTHO act through a common signaling pathway [30] and that KLOTHO facilitates FGF23 binding to an FGFR [34]. Of relevance is the absence of the canonical FGFR binding domain on the bioactive FGF23 180-251 fragment.…”

Section: Discussionmentioning

confidence: 99%

Biological activity of FGF-23 fragments

Berndt

Craig

McCormick

et al. 2007

Pflugers Arch - Eur J Physiol

View full text Add to dashboard Cite

SUMMARYThe phosphaturic activity of intact, full-length, fibroblast growth factor-23 (FGF-23) is well documented. FGF-23 circulates as the intact protein, and as fragments generated as the result of proteolysis of the full-length protein. To assess whether short fragments of FGF-23 are phosphaturic, we compared the effect of acute, equimolar infusions of full-length FGF-23 and various FGF-23 fragments carboxyl-terminal to amino acid 176. In rats, intravenous infusions of full-length FGF-23, and FGF-23 176-251, significantly and equivalently increased fractional phosphate excretion (FE Pi)) from 14±3 to 32±5% and 15±2 to 33±2% (p <0.001), respectively. reduced Na + -dependent Pi uptake and enhanced internalization of the Na + -Pi IIa co-transporter. We conclude that carboxyl terminal fragments of FGF-23 are phosphaturic, and that a short, 26 amino acid fragment of FGF-23 retains significant phosphaturic activity.

show abstract

Regulation of Fibroblast Growth Factor-23 Signaling by Klotho

Cited by 1,215 publications

References 27 publications

Elsie Widdowson Lecture 2006 Mining the depths: metabolic insights into mineral nutrition

Elsie Widdowson Lecture 2006 Mining the depths: metabolic insights into mineral nutrition

Iron deficiency drives an autosomal dominant hypophosphatemic rickets (ADHR) phenotype in fibroblast growth factor-23 (Fgf23) knock-in mice

Biological activity of FGF-23 fragments

Contact Info

Product

Resources

About