The Roles of Specific Genes Implicated as Circulating Factors Involved in Normal and Disordered Phosphate Homeostasis: Frizzled Related Protein-4, Matrix Extracellular Phosphoglycoprotein, and Fibroblast Growth Factor 23
Kenneth E. White,
Tobias E. Larsson and
Michael J. Econs
Department of Medical and Molecular Genetics (K.E.W., T.E.L., M.J.E.) and Department of Medicine (M.J.E.), Indiana University School of Medicine, Indianapolis, Indiana 46202
Correspondence: Address all correspondence and requests for reprints to: Michael J. Econs, Department of Medicine, Indiana University School of Medicine, Indianapolis, Indiana 46202. E-mail: mecons{at}iupui.edu
Normal serum phosphate (Pi) concentrations are relatively tightlycontrolled by endocrine mediators of Pi balance. Recent datainvolving several disorders of Pi homeostasis have shed newlight on the regulation of serum Pi balance. It has been hypothesizedthat circulating phosphaturic factors, or phosphatonins, existthat, when present at high serum concentrations, directly acton the kidney to induce renal Pi wasting. This review will focusupon recently discovered factors that are overexpressed in tumorsassociated with tumor-induced osteomalacia and have reportedactivity consistent with effecting Pi balance in vivo. Currently,the best-characterized group of phosphatonin-like polypeptidesincludes secreted frizzled related protein-4, matrix extracellularphosphoglycoprotein, and fibroblast growth factor-23. Our understandingof these factors will, in the short term, aid us in understandingnormal Pi balance and, in the future, help to design novel therapeuticstrategies for disorders of Pi handling.
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