Human sodium phosphate transporter 4 (hNPT4/SLC17A3) as a common renal secretory pathway for drugs and urate

J Biol Chem. 2010 Nov 5;285(45):35123-32. doi: 10.1074/jbc.M110.121301. Epub 2010 Sep 1.

Abstract

The evolutionary loss of hepatic urate oxidase (uricase) has resulted in humans with elevated serum uric acid (urate). Uricase loss may have been beneficial to early primate survival. However, an elevated serum urate has predisposed man to hyperuricemia, a metabolic disturbance leading to gout, hypertension, and various cardiovascular diseases. Human serum urate levels are largely determined by urate reabsorption and secretion in the kidney. Renal urate reabsorption is controlled via two proximal tubular urate transporters: apical URAT1 (SLC22A12) and basolateral URATv1/GLUT9 (SLC2A9). In contrast, the molecular mechanism(s) for renal urate secretion remain unknown. In this report, we demonstrate that an orphan transporter hNPT4 (human sodium phosphate transporter 4; SLC17A3) was a multispecific organic anion efflux transporter expressed in the kidneys and liver. hNPT4 was localized at the apical side of renal tubules and functioned as a voltage-driven urate transporter. Furthermore, loop diuretics, such as furosemide and bumetanide, substantially interacted with hNPT4. Thus, this protein is likely to act as a common secretion route for both drugs and may play an important role in diuretics-induced hyperuricemia. The in vivo role of hNPT4 was suggested by two hyperuricemia patients with missense mutations in SLC17A3. These mutated versions of hNPT4 exhibited reduced urate efflux when they were expressed in Xenopus oocytes. Our findings will complete a model of urate secretion in the renal tubular cell, where intracellular urate taken up via OAT1 and/or OAT3 from the blood exits from the cell into the lumen via hNPT4.

Publication types

  • Research Support, Non-U.S. Gov't

MeSH terms

  • Animals
  • Bumetanide / adverse effects
  • Bumetanide / pharmacokinetics*
  • Bumetanide / pharmacology
  • Diuretics / adverse effects
  • Diuretics / pharmacokinetics*
  • Diuretics / pharmacology
  • Furosemide / adverse effects
  • Furosemide / pharmacokinetics*
  • Furosemide / pharmacology
  • Genetic Predisposition to Disease
  • Glucose Transport Proteins, Facilitative / genetics
  • Glucose Transport Proteins, Facilitative / metabolism
  • Gout / genetics
  • Gout / metabolism
  • Humans
  • Hyperuricemia / chemically induced
  • Hyperuricemia / genetics
  • Hyperuricemia / metabolism
  • Ion Transport / drug effects
  • Ion Transport / genetics
  • Kidney Tubules, Proximal / metabolism*
  • Liver / metabolism
  • Models, Biological*
  • Mutation, Missense
  • Organic Anion Transport Protein 1 / genetics
  • Organic Anion Transport Protein 1 / metabolism
  • Organic Anion Transporters / genetics
  • Organic Anion Transporters / metabolism
  • Organic Anion Transporters, Sodium-Independent / genetics
  • Organic Anion Transporters, Sodium-Independent / metabolism
  • Organic Cation Transport Proteins / genetics
  • Organic Cation Transport Proteins / metabolism
  • Sodium-Phosphate Cotransporter Proteins, Type I / genetics
  • Sodium-Phosphate Cotransporter Proteins, Type I / metabolism*
  • Urate Oxidase / genetics
  • Urate Oxidase / metabolism
  • Uric Acid / metabolism*
  • Xenopus laevis

Substances

  • Diuretics
  • Glucose Transport Proteins, Facilitative
  • Organic Anion Transport Protein 1
  • Organic Anion Transporters
  • Organic Anion Transporters, Sodium-Independent
  • Organic Cation Transport Proteins
  • SLC17A3 protein, human
  • SLC22A12 protein, human
  • SLC2A9 protein, human
  • Sodium-Phosphate Cotransporter Proteins, Type I
  • organic anion transport protein 3
  • Bumetanide
  • Uric Acid
  • Furosemide
  • Urate Oxidase