Literature DB >> 12149479

Substrate-dependent reversal of anion transport site orientation in the human red blood cell anion-exchange protein, AE1.

Philip A Knauf1, Foon-Yee Law, Tze-Wah Vivian Leung, Austin U Gehret, Martha L Perez.   

Abstract

The tightly coupled, one-for-one exchange of anions mediated by the human red blood cell AE1 anion-exchange protein involves a ping-pong mechanism, in which AE1 alternates between a state with the anion-binding site facing inward toward the cytoplasm (Ei) and a state with the site facing outward toward the external medium (Eo). The conformational shift (Ei <--> Eo) is only permitted when a suitable substrate such as Cl(-) or HCO(3)(-) (B(-)) is bound. With no anions bound, or with Cl(-) bound, far more AE1 molecules are in the inward-facing than the outward-facing forms (Ei Eo, ECli EClo). We have constructed a model for CI(-)-B(-) exchange based on Cl(-)-Cl(-) and B(-)-B(-) exchange data, and have used it to predict the heteroexchange flux under extremely asymmetric conditions, with either all Cl(-) inside and all B(-) outside (Cli-Bo) or vice versa (Bi-Clo). The experimental values of the ratio of the exchange rate for Bi-Clo to that for Cli-Bo are only compatible with the model if the asymmetry of bicarbonate-loaded sites (A(B) = EBo/EBi) > 10, the opposite of the asymmetry for unloaded or Cl-loaded sites. Furthermore, the Eo form has a higher affinity for HCO(3)(-) than for Cl(-), whereas the Ei form has a higher affinity for Cl(-). The fact that this "passive" system exhibits changes in substrate selectivity with site orientation ("sidedness"), a characteristic usually associated with energy-coupled "active" pumps, suggests that changes in affinity with changes in sidedness are a more general property of transport proteins than previously thought.

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Year:  2002        PMID: 12149479      PMCID: PMC125063          DOI: 10.1073/pnas.162402399

Source DB:  PubMed          Journal:  Proc Natl Acad Sci U S A        ISSN: 0027-8424            Impact factor:   11.205


  13 in total

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Authors:  O Fröhlich; R B Gunn
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6.  Source of transport site asymmetry in the band 3 anion exchange protein determined by NMR measurements of external Cl- affinity.

Authors:  D Liu; S D Kennedy; P A Knauf
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7.  The kinetic equation for the chloride transport cycle of band 3. A 35Cl and 37Cl NMR study.

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8.  Stoichiometry of a half-turnover of band 3, the chloride transport protein of human erythrocytes.

Authors:  M L Jennings
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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
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10.  Kinetics of bicarbonate and chloride transport in human red cell membranes.

Authors:  P K Gasbjerg; J Brahm
Journal:  J Gen Physiol       Date:  1991-02       Impact factor: 4.086

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  10 in total

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2.  A provisional transport mechanism for a chloride channel-type Cl-/H+ exchanger.

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7.  Hydrogen ion dynamics in human red blood cells.

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8.  Identification of multiple substrate binding sites in SLC4 transporters in the outward-facing conformation: insights into the transport mechanism.

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9.  Separate ion pathways in a Cl-/H+ exchanger.

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Review 10.  Cell physiology and molecular mechanism of anion transport by erythrocyte band 3/AE1.

Authors:  Michael L Jennings
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  10 in total

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