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Interaction among anion,cation and glucose transport proteins in the human red cell
Authors:Janoshazi  Agnes  Solomon  A. K.
Affiliation:(1) Biophysical Laboratory, Harvard Medical School, 02115 Boston, Massachusetts
Abstract:Summary The time course of binding of the fluorescent stilbene anion exchange inhibitor, DBDS (4,4prime-dibenzamido-2,2prime-stilbene disulfonate), to band 3 can be measured by the stopped-flow method. We have previously used the reaction time constant, tauDBDS, to obtain the kinetic constants for binding and, thus, to report on the conformational state of the band 3 binding site. To validate the method, we have now shown that the ID50 (0.3±0.1 mgrm) for H2-DIDS (4,4prime-diisothiocyano-2,2prime-dihydrostilbene disulfonate) inhibition of tauDBDS is virtually the same as the ID50 (0.47±0.04 mgrm) for H2-DIDS inhibition of red cell Cl flux, thus relating tauDBDS directly to band 3 anion exchange. The specific glucose transport inhibitor, cytochalasin B, causes significant changes in tauDBDS, which can be reversed with intracellular, but not extracellular,d-glucose. ID50 for cytochalasin B modulation of tauDBDS is 0.1±0.2 mgrm in good agreement withKD=0.06±0.005 mgrm for cytochalasin B binding to the glucose transport protein. These experiments suggest that the glucose transport protein is either adjacent to band 3, or linked to it through a mechanism, which can transmit conformational information. Ouabain (0.1 mgrm), the specific inhibitor of red cell Na+,K+-ATPase, increases red cell Cl exchange flux in red cells by a factor of about two. This interaction indicates that the Na+,K+-ATPase, like the glucose transport protein, is either in contact with, or closely linked to, band 3. These results would be consistent with a transport proteincomplex, centered on band 3, and responsible for the entire transport process, not only the provision of metabolic energy, but also the actual carriage of the cations and anions themselves.
Keywords:red cell  Na+,K+-ATPase  band 3  anion exchange protein  glucose transport protein  stilbene anion exchange inhibitors  DBDS
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