Evidence for a signaling axis by which intestinal phosphate rapidly modulates renal phosphate reabsorption

  1. Theresa Berndt*,
  2. Leslie F. Thomas*,
  3. Theodore A. Craig*,
  4. Stacy Sommer*,
  5. Xujian Li,
  6. Eric J. Bergstralh, and
  7. Rajiv Kumar*,,§
  1. *Division of Nephrology and Hypertension, Department of Internal Medicine,
  2. Division of Biostatistics, Department of Health Sciences Research, and
  3. Department of Biochemistry and Molecular Biology, Mayo Clinic, 200 First Street Southwest, Rochester, MN 55905

  1. Communicated by Hector F. DeLuca, University of Wisconsin, Madison, WI, May 14, 2007 (received for review February 28, 2007)

Abstract

The mechanisms by which phosphorus homeostasis is preserved in mammals are not completely understood. We demonstrate the presence of a mechanism by which the intestine detects the presence of increased dietary phosphate and rapidly increases renal phosphate excretion. The mechanism is of physiological relevance because it maintains plasma phosphate concentrations in the normal range after ingestion of a phosphate-containing meal. When inorganic phosphate is infused into the duodenum, there is a rapid increase in the renal fractional excretion of phosphate (FE Pi). The phosphaturic effect of intestinal phosphate is specific for phosphate because administration of sodium chloride does not elicit a similar response. Phosphaturia after intestinal phosphate administration occurs in thyro-parathyroidectomized rats, demonstrating that parathyroid hormone is not essential for this effect. The increase in renal FE Pi in response to the intestinal administration of phosphate occurs without changes in plasma concentrations of phosphate (filtered load), parathyroid hormone, FGF-23, or secreted frizzled related protein-4. Denervation of the kidney does not attenuate phosphaturia elicited after intestinal phosphate administration. Phosphaturia is not elicited when phosphate is instilled in other parts of the gastrointestinal tract such as the stomach. Infusion of homogenates of the duodenal mucosa increases FE Pi, which demonstrates the presence of one or more substances within the intestinal mucosa that directly modulate renal phosphate reabsorption. Our experiments demonstrate the presence of a previously unrecognized phosphate gut–renal axis that rapidly modulates renal phosphate excretion after the intestinal administration of phosphate.

Footnotes

  • §To whom correspondence should be addressed. E-mail: rkumar{at}mayo.edu

  • Author contributions: R.K. designed research; T.B., L.F.T., T.A.C., S.S., and R.K. performed research; X.L., E.J.B., and R.K. analyzed data; and R.K. wrote the paper.

  • The authors declare no conflict of interest.

  • Abbreviations:
    FE Pi,
    fractional excretion of phosphate;
    FE Na,
    fractional excretion of sodium;
    sFRP-4,
    secreted frizzled related protein-4;
    1α,
    25(OH)2D, 1α, 25-dihydroxyvitamin D;
    PTH,
    parathyroid hormone;
    TPTX,
    thyro-parathyroidectomized.

  • Freely available online through the PNAS open access option.

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  1. Published online before print June 12, 2007, doi: 10.1073/pnas.0704446104 PNAS June 26, 2007 vol. 104 no. 26 11085-11090
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