Literature DB >> 1294062

Electrogenic properties of the cloned Na+/glucose cotransporter: II. A transport model under nonrapid equilibrium conditions.

L Parent1, S Supplisson, D D Loo, E M Wright.   

Abstract

The results of the accompanying electrophysiological study of the cloned Na+/glucose cotransporter from small intestine (Parent, L., Supplisson, S., Loo, D.D.F., Wright, E.M. (1992) J. Mémbrane Biol. 125:49-62) were evaluated in terms of a kinetic model. The steady-state and presteady-state cotransporter properties are described by a 6-state ordered kinetic model ("mirror" symmetry) with a Na+:alpha MDG stoichiometry of 2. Carrier translocation in the membrane as well as Na+ and sugar binding and dissociation are treated as a function of their individual rate constants. Empty carrier translocation and Na+ binding/dissociation are the only steps considered to be voltage dependent. Currents were associated with the translocation of the negatively charged carrier in the membrane. Negative membrane potential facilitates sugar transport. One numerical solution was found for the 14 rate constants that account quantitatively for our experiment observations: i.e., (i) sigmoidal shape of the sugar-specific current-voltage curves (absence of outward currents and inward current saturation at high negative potentials), (ii) Na+ and voltage dependence of Ksugar0.5 and isugarmax, (iii) sugar and voltage dependence of KNa0.5 and iNamax, (iv) presteady-state currents and their dependence on external Na+, alpha MDG and membrane potential, and (v) and carrier Na+ leak current. We conclude that the main voltage effect is on carrier translocation. Na+ ions that migrate from the extracellular medium to their binding sites sense 25 to 35% of the transmembrane voltage, whereas charges associated with the carrier translocation experiences 60 to 75% of the membrane electrical field. Internal Na+ ion binding is not voltage dependent. In our nonrapid equilibrium model, the rate-limiting step for sugar transport is a function of the membrane potential, [Na]o and [alpha MDG]o. At 0 mV and at saturating [Na]o and [alpha MDG]o, the rate-limiting step for sugar transport is the empty carrier translocation (5 sec-1). As the membrane potential is made more negative, the empty carrier translocation gets faster and the internal Na+ dissociation becomes increasingly rate limiting. However, as [Na]o is decreased to less than 10 mM, the rate-limiting step is the external Na+ ions binding in the 0 to -150 mV potential range. At 0 mV, the external Na+ dissociation constant KNa' is 80 mM and decreases to 24 mM at -150 mV. The external sugar dissociation constant KNaS' is estimated to be 200 microM and voltage independent. Finally, the internal leak pathway (CNa2 translocation) is insignificant.(ABSTRACT TRUNCATED AT 400 WORDS)

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Year:  1992        PMID: 1294062     DOI: 10.1007/bf00235798

Source DB:  PubMed          Journal:  J Membr Biol        ISSN: 0022-2631            Impact factor:   1.843


  28 in total

1.  Presteady-state kinetics and carrier-mediated transport: a theoretical analysis.

Authors:  W Wierzbicki; A Berteloot; G Roy
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2.  Electrogenic properties of the sodium-alanine cotransporter in pancreatic acinar cells: II. Comparison with transport models.

Authors:  P Jauch; P Läuger
Journal:  J Membr Biol       Date:  1986       Impact factor: 1.843

3.  Generalized kinetic analysis of ion-driven cotransport systems: a unified interpretation of selective ionic effects on Michaelis parameters.

Authors:  D Sanders; U P Hansen; D Gradmann; C L Slayman
Journal:  J Membr Biol       Date:  1984       Impact factor: 1.843

Review 4.  Relaxation studies of ion transport systems in lipid bilayer membranes.

Authors:  P Läuger; R Benz; G Stark; E Bamberg; P C Jordan; A Fahr; W Brock
Journal:  Q Rev Biophys       Date:  1981-11       Impact factor: 5.318

5.  Co-transport of anions and neutral solutes with cations across charged biological membranes. Effects of surface potential on uptake kinetics.

Authors:  G M Roomans; G W Borst-Pauwels
Journal:  J Theor Biol       Date:  1978-08-08       Impact factor: 2.691

6.  Intestinal Na+/glucose cotransporter expressed in Xenopus oocytes is electrogenic.

Authors:  J A Umbach; M J Coady; E M Wright
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7.  Na+-coupled sugar transport: membrane potential-dependent Km and Ki for Na+.

Authors:  G A Kimmich; J Randles
Journal:  Am J Physiol       Date:  1988-10

8.  Sodium and sugar fluxes across the mucosal border of rabbit ileum.

Authors:  A M Goldner; S G Schultz; P F Curran
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9.  Phlorizin as a probe of the small-intestinal Na+,D-glucose cotransporter. A model.

Authors:  G Toggenburger; M Kessler; G Semenza
Journal:  Biochim Biophys Acta       Date:  1982-06-14

10.  The mechanistic nature of the membrane potential dependence of sodium-sugar cotransport in small intestine.

Authors:  D Restrepo; G A Kimmich
Journal:  J Membr Biol       Date:  1985       Impact factor: 1.843

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  92 in total

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6.  Effects of pH on kinetic parameters of the Na-HCO3 cotransporter in renal proximal tubule.

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7.  The relation between charge movement and transport-associated currents in the rat GABA cotransporter rGAT1.

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8.  Electrogenic properties of the cloned Na+/glucose cotransporter: I. Voltage-clamp studies.

Authors:  L Parent; S Supplisson; D D Loo; E M Wright
Journal:  J Membr Biol       Date:  1992-01       Impact factor: 1.843

9.  A tool for multi-scale modelling of the renal nephron.

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10.  The actual ionic nature of the leak current through the Na+/glucose cotransporter SGLT1.

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