Sodium-glucose cotransporters display sodium- and phlorizin-dependent water permeability.

J. D. Loike , S. Hickman , K. Kuang , M. Xu , L. Cao , J. C. Vera , S. C. Silverstein , J. Fischbarg

Abstract

Expression of Na(+)-glucose cotransporters of the SGLT-1 type by Xenopus laevis oocytes increased the osmotic water permeability (Pf) of oocytes by a factor of 1.9-2.8, in the presence and in the absence of 5 mM extracellular glucose. The Pf increase was correlated with the amount of SGLT-1 cRNA injected. In oocytes expressing SGLT-1, either addition of phlorizin to the medium or the replacement of Na+ by choline inhibited the uptake of methyl-alpha-D-glucopyranoside, a specific substrate for SGLT-1, and returned oocyte Pf to its level in uninjected oocytes. Phlorizin inhibited the SGLT-1-attributable increase in Pf with an inhibition constant (Ki) of 6.1 microM, a value analogous to the Ki for phlorizin inhibition of sugar uptake. However, neither the presence of phlorizin nor the absence of extracellular Na+ significantly affected the increase in Pf elicited in oocytes expressing GLUT-1, a facilitative glucose transporter. These findings suggest that SGLT-1 forms a pore that allows the transmembrane passage of water and that water and glucose traverse the protein through this pore. The finding that removal of extracellular Na+ abolishes the increase in Pf attributable to SGLT-1 suggests that extracellular Na+ is required to maintain patency of this transporter's water-permeable transmembrane pore.

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Título de la Revista: AMERICAN JOURNAL OF PHYSIOLOGY-CELL PHYSIOLOGY
Volumen: 271
Número: 5 Pt1
Editorial: AMER PHYSIOLOGICAL SOC
Fecha de publicación: 1996
Página de inicio: C1774
Página final: C1779
Idioma: English
Notas: ISI