Literature DB >> 2250617

Mechanism and regulation of intestinal phosphate absorption.

H S Cross1, H Debiec, M Peterlik.   

Abstract

Proper absorption of inorganic phosphate (Pi) from the lumen of the small intestine is of great importance for the achievement of Pi homeostasis. Although due to intralumenal H+ and Pi concentrations, Pi probably can be absorbed as H2PO4- by passive means in the duodenum, transepithelial transport of HPO4(2)- requires uptake from the lumen by an active transport system. The latter has been identified in many species as a Na(+)-Pi cotransport system at the brush-border membrane of the enterocyte. Although it is still a matter of debate whether the intestinal Na+ gradient-driven Pi transport system is electrogenic or electroneutral, there is agreement that the transporter accepts H2PO4- and HPO4(2)- alike. Recently, two laboratories independently isolated a Na(+)-Pi-binding protein which has been tentatively identified as part of the Na(+)-Pi cotransport system. Movement of Pi from the cytosol across the basolateral membrane into the interstitial space has only been preliminarily characterized as transfer by facilitated diffusion. Na(+)-Pi cotransport across the brush-border membrane is under control by the active vitamin D metabolite, 1,25-dihydroxyvitamin D3 (1,25-(OH)2D3). The sterol increases the intrinsic activity, i.e. the number and/or mobility of Na(+)-Pi carriers through genomic and probably also nongenomic actions. In addition, the rate of Na(+)-gradient-driven Pi transport can be enhanced by the hormone also through reduction of transmembrane Na+ fluxes so that more energy for translocation becomes available from the transmembrane Na+ gradient. Evidence is accumulating that thyroid hormones as well as glucocorticoids, apart from stimulating vitamin D-independent Pi uptake, potentiate the effect of 1,25-(OH)2D3 on Na(+)-Pi cotransport across the brush-border membrane.

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Year:  1990        PMID: 2250617

Source DB:  PubMed          Journal:  Miner Electrolyte Metab        ISSN: 0378-0392


  19 in total

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Review 2.  Arterial calcification in chronic kidney disease: key roles for calcium and phosphate.

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3.  Targeted inactivation of Npt2 in mice leads to severe renal phosphate wasting, hypercalciuria, and skeletal abnormalities.

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4.  Amino acids involved in sodium interaction of murine type II Na(+)-P(i) cotransporters expressed in Xenopus oocytes.

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5.  Characterizing and evaluating the expression of the type IIb sodium-dependent phosphate cotransporter (slc34a2) gene and its potential influence on phosphorus utilization efficiency in yellow catfish (Pelteobagrus fulvidraco).

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6.  Mechanisms of phosphate uptake into brush-border membrane vesicles from goat jejunum.

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7.  Developmental Changes in Phosphate Homeostasis.

Authors:  Tate MacDonald; Matthew Saurette; Megan R Beggs; R Todd Alexander
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8.  Characterization of a murine type II sodium-phosphate cotransporter expressed in mammalian small intestine.

Authors:  H Hilfiker; O Hattenhauer; M Traebert; I Forster; H Murer; J Biber
Journal:  Proc Natl Acad Sci U S A       Date:  1998-11-24       Impact factor: 11.205

Review 9.  The sodium phosphate cotransporter family SLC34.

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10.  The calcium-sensing receptor promotes urinary acidification to prevent nephrolithiasis.

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