Bacchetta J, Cochat P, Salusky I B
Centre de référence des maladies rénales rares, hôpital Femme-Mère-Enfant, boulevard Pinel, 69677 Bron cedex, France.
Arch Pediatr. 2011 Jun;18(6):686-95. doi: 10.1016/j.arcped.2011.03.004. Epub 2011 Apr 16.
Since its first description as a phosphaturic agent in the early 2000’s, the Fibroblast Growth Factor 23 (FGF23) has rapidly become the third key player of phosphate/calcium metabolism with the two ‘old’ PTH and vitamin D. FGF23 is a protein synthesized by osteocytes that acts mainly as a phosphaturic factor and a suppressor of 1α hydroxylase activity in the kidney. It inhibits the expression of type IIa and IIc sodium-phosphate cotransporters on the apical membrane of proximal tubular cells, thus leading to an inhibition of phosphate reabsorption. Moreover, it also inhibits the 1α hydroxylase activity. These two renal pathways account together for the hypophosphatemic effect of FGF23, but FGF23 has also been recently described as an inhibiting factor for PTH synthesis. Its exact role in bone remains to be defined. A transmembrane protein, Klotho, is an essential cofactor for FGF23 biological activity, but it can also act by itself for calcium and PTH regulation. This paper gives an overview of these recent data of phosphate/calcium physiology, as well as a description of clinical conditions associated with FGF23 deregulation (genetic diseases and chronic kidney disease). As a conclusion, future therapeutic consequences of the FGF23/Klotho axis are discussed.
自21世纪初首次被描述为一种排磷因子以来,成纤维细胞生长因子23(FGF23)迅速成为磷酸盐/钙代谢的第三个关键调节因子,与另外两个“老牌”调节因子甲状旁腺激素(PTH)和维生素D并列。FGF23是一种由骨细胞合成的蛋白质,主要作为一种排磷因子和肾脏中1α羟化酶活性的抑制剂发挥作用。它抑制近端肾小管细胞顶端膜上IIa型和IIc型钠-磷酸盐共转运蛋白的表达,从而导致磷酸盐重吸收受到抑制。此外,它还抑制1α羟化酶的活性。这两条肾脏途径共同构成了FGF23的降磷作用,但FGF23最近也被描述为PTH合成的抑制因子。它在骨骼中的具体作用仍有待确定。一种跨膜蛋白,即klotho蛋白,是FGF23生物学活性的必需辅助因子,但它也可以独立发挥调节钙和PTH的作用。本文概述了这些关于磷酸盐/钙生理学的最新数据,并描述了与FGF23失调相关的临床情况(遗传性疾病和慢性肾脏病)。最后,讨论了FGF23/klotho轴未来的治疗意义。