Beside the ongoing efforts to determine structural information, detailed functional studies on transporters are essential to entirely understand the underlying transport mechanisms. We recently found that solid supported membrane-based electrophysiology (SSME) enables the measurement of both sugar binding and transport in the Na/sugar cotransporter SGLT1 (Bazzone et al, 2022a). Here, we continued with a detailed kinetic characterization of SGLT1 using SSME, determining K and K for different sugars, k values for sugar-induced conformational transitions and the effects of Na, Li, H and Cl on sugar binding and transport. We found that the sugar-induced pre-steady-state (PSS) charge translocation varies with the bound ion (Na, Li, H or Cl), but not with the sugar species, indicating that the conformational state upon sugar binding depends on the ion. Rate constants for the sugar-induced conformational transitions upon binding to the Na-bound carrier range from 208 s for D-glucose to 95 s for 3-OMG. In the absence of Na, rate constants are decreased, but all sugars bind to the empty carrier. From the steady-state transport current, we found a sequence for sugar specificity (V/K): D-glucose > MDG > D-galactose > 3-OMG > D-xylose. While K differs 160-fold across tested substrates and plays a major role in substrate specificity, V only varies by a factor of 1.9. Interestingly, D-glucose has the lowest V across all tested substrates, indicating a rate limiting step in the sugar translocation pathway following the fast sugar-induced electrogenic conformational transition. SGLT1 specificity for D-glucose is achieved by optimizing two ratios: the sugar affinity of the empty carrier for D-glucose is similarly low as for all tested sugars (K = 210 mM). Affinity for D-glucose increases 14-fold (K = 15 mM) in the presence of sodium as a result of cooperativity. Apparent affinity for D-glucose during transport increases 8-fold (K = 1.9 mM) compared to K due to optimized kinetics. In contrast, K and K values for 3-OMG and D-xylose are of similar magnitude. Based on our findings we propose an 11-state kinetic model, introducing a random binding order and intermediate states corresponding to the electrogenic transitions detected SSME upon substrate binding.
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| http://dx.doi.org/10.3389/fphys.2023.1058583 | DOI Listing |
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