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Literature DB >> 8833347

Effects of external pH on binding of external sulfate, 4.4-dinitro-stilbene-2,2'-disulfonate (DNDS), and chloride to the band 3 anion exchange protein.

Abstract

A model in which two positively-charged titratable sites enhance the affinity for anionic substrates can explain the increase in external iodide dissociation constant (K(O)(I)) with increasing pH(O) (Liu, S. J., F.-Y. Law, and P.A. Knauf. 1996.f Gen.Physiol. 107:271-291). If sulfate binds to the same external site as I-, this model predicts that the SO(4)= dissociation constant (K(O)(S)) should also increase. The data at pH 0 8.5 to 10 fit this prediction, and the pK for the titration is not significantly different from that (pKc) for the low-pK group that affects K(O)(1). The dissociation constant for the apparently competitive inhibitor, DNDS (4,4-dinitrostilbene-2,2'-disulfonate), also increases greatly as pH(O) increases. Particularly at high pH(O), a noncompetitive inhibition by DNDS is also evident. Increasing pH(O) from 7.2 to 11.2 increases the competitive dissociation constant by 700-fold, but the noncompetitive is only increased 20-fold. The pK values for these effects are similar to pKc for K(O)(1), as expected if DNDS binds near the external transport site, but it seems likely that additional titratable groups also affect DNDS binding. The apparent affinity for external Cl- is also affected by pH(O), in a manner similar to that observed for I-. Pretreatment with the amino-selective reagent, bis-sulfosuccinimidyl suberate (BSSS), decreases the apparent Cl- affinity at pH 8.5, but two titrations are still evident, the first (lower) of which decreases the apparent C- affinity, and the second of which surprisingly increases it. Thus, the BSSS-reactive amino groups (probably Lys-539 and Lys-851) do not seem to be involved in the titrations that affect Cl- affinity. In general, the data support the concept that a positively charged amino group (or groups), together with a guanidino group, plays an important role in the binding of substrates and inhibitors at or near the external transport site.

Entities: Chemical Disease Gene

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Year: 1996 PMID： 8833347 PMCID： PMC2219265 DOI： 10.1085/jgp.107.2.293

Source DB: PubMed Journal: J Gen Physiol ISSN： 0022-1295 Impact factor: 4.086

29 in total

1. Cross-linking and chymotryptic digestion of the extracytoplasmic domain of the anion exchange channel in intact human erythrocytes.

Authors: J V Staros; B P Kakkad
Journal: J Membr Biol Date: 1983 Impact factor: 1.843

2. A comparison of the inhibitory potency of reversibly acting inhibitors of anion transport on chloride and sulfate movements across the human red cell membrane.

Authors: C P Ku; M L Jennings; H Passow
Journal: Biochim Biophys Acta Date: 1979-05-03

3. 35Cl nuclear magnetic resonance line broadening shows that eosin-5-maleimide does not block the external anion access channel of band 3.

Authors: D Liu; S D Kennedy; P A Knauf
Journal: Biophys J Date: 1995-08 Impact factor: 4.033

4. Asymmetry of the red cell anion exchange system. Different mechanisms of reversible inhibition by N-(4-azido-2-nitrophenyl)-2-aminoethylsulfonate (NAP-taurine) at the inside and outside of the membrane.

Authors: P A Knauf; S Ship; W Breuer; L McCulloch; A Rothstein
Journal: J Gen Physiol Date: 1978-11 Impact factor: 4.086

5. Identification of the Cl- transport site of human red blood cells by a kinetic analysis of the inhibitory effects of a chemical probe.

Authors: Y Shami; A Rothstein; P A Knauf
Journal: Biochim Biophys Acta Date: 1978-04-04

6. Effects of external pH on substrate binding and on the inward chloride translocation rate constant of band 3.

Authors: S Q Liu; F Y Law; P A Knauf
Journal: J Gen Physiol Date: 1996-02 Impact factor: 4.086

7. Chloride net efflux from intact erythrocytes under slippage conditions. Evidence for a positive charge on the anion binding/transport site.

Authors: O Fröhlich; C Leibson; R B Gunn
Journal: J Gen Physiol Date: 1983-01 Impact factor: 4.086

8. Proton-sulfate co-transport: mechanism of H+ and sulfate addition to the chloride transporter of human red blood cells.

Authors: M A Milanick; R B Gunn
Journal: J Gen Physiol Date: 1982-01 Impact factor: 4.086

9. Asymmetry in the mechanism for anion exchange in human red blood cell membranes. Evidence for reciprocating sites that react with one transported anion at a time.

Authors: R B Gunn; O Fröhlich
Journal: J Gen Physiol Date: 1979-09 Impact factor: 4.086

10. Titration of transport and modifier sites in the red cell anion transport system.

Authors: J O Wieth; P J Bjerrum
Journal: J Gen Physiol Date: 1982-02 Impact factor: 4.086

2 in total

1. Identification and characterization of a second 4,4'-dibenzamido-2,2'-stilbenedisulphonate (DBDS)-binding site on band 3 and its relationship with the anion/proton co-transport function.

Authors: James M Salhany; Karen S Cordes; Renee L Sloan
Journal: Biochem J Date: 2005-05-15 Impact factor: 3.857

2. Effects of external pH on substrate binding and on the inward chloride translocation rate constant of band 3.

Authors: S Q Liu; F Y Law; P A Knauf
Journal: J Gen Physiol Date: 1996-02 Impact factor: 4.086

2 in total