Structure–Function Relations of the First and Fourth Extracellular Linkers of the Type IIa Na(+)/P(i) Cotransporter: II. Substrate Interaction and Voltage Dependency of Two Functionally Important Sites

Functionally important sites in the predicted first and fourth extracellular linkers of the type IIa Na(+)/P(i) cotransporter (NaPi-IIa) were identified by cysteine scanning mutagenesis (Ehnes et al., 2004). Cysteine substitution or modification with impermeant and permeant methanethiosulfonate (MTS...

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Autores principales: Ehnes, Colin, Forster, Ian C., Bacconi, Andrea, Kohler, Katja, Biber, Jürg, Murer, Heini
Formato: Texto
Lenguaje:English
Publicado: The Rockefeller University Press 2004
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Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2234003/
https://www.ncbi.nlm.nih.gov/pubmed/15504899
http://dx.doi.org/10.1085/jgp.200409061
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author Ehnes, Colin
Forster, Ian C.
Bacconi, Andrea
Kohler, Katja
Biber, Jürg
Murer, Heini
author_facet Ehnes, Colin
Forster, Ian C.
Bacconi, Andrea
Kohler, Katja
Biber, Jürg
Murer, Heini
author_sort Ehnes, Colin
collection PubMed
description Functionally important sites in the predicted first and fourth extracellular linkers of the type IIa Na(+)/P(i) cotransporter (NaPi-IIa) were identified by cysteine scanning mutagenesis (Ehnes et al., 2004). Cysteine substitution or modification with impermeant and permeant methanethiosulfonate (MTS) reagents at certain sites resulted in changes to the steady-state voltage dependency of the cotransport mode (1 mM P(i), 100 mM Na(+) at pH 7.4) of the mutants. At Gly-134 (ECL-1) and Met-533 (ECL-4), complementary behavior of the voltage dependency was documented with respect to the effect of cys-substitution and modification. G134C had a weak voltage dependency that became even stronger than that of the wild type (WT) after MTS incubation. M533C showed a WT-like voltage dependency that became markedly weaker after MTS incubation. To elucidate the underlying mechanism, the steady-state and presteady-state kinetics of these mutants were studied in detail. The apparent affinity constants for P(i) and Na(+) did not show large changes after MTS exposure. However, the dependency on external protons was changed in a complementary manner for each mutant. This suggested that cys substitution at Gly-134 or modification of Cys-533 had induced similar conformational changes to alter the proton modulation of transport kinetics. The changes in steady-state voltage dependency correlated with changes in the kinetics of presteady-state charge movements determined in the absence of P(i), which suggested that voltage-dependent transitions in the transport cycle were altered. The steady-state and presteady-state behavior was simulated using an eight-state kinetic model in which the transition rate constants of the empty carrier and translocation of the fully loaded carrier were found to be critical determinants of the transport kinetics. The simulations predict that cys substitution at Gly-134 or cys modification of Cys-533 alters the preferred orientation of the empty carrier from an inward to outward-facing conformation for hyperpolarizing voltages.
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spelling pubmed-22340032008-03-21 Structure–Function Relations of the First and Fourth Extracellular Linkers of the Type IIa Na(+)/P(i) Cotransporter: II. Substrate Interaction and Voltage Dependency of Two Functionally Important Sites Ehnes, Colin Forster, Ian C. Bacconi, Andrea Kohler, Katja Biber, Jürg Murer, Heini J Gen Physiol Article Functionally important sites in the predicted first and fourth extracellular linkers of the type IIa Na(+)/P(i) cotransporter (NaPi-IIa) were identified by cysteine scanning mutagenesis (Ehnes et al., 2004). Cysteine substitution or modification with impermeant and permeant methanethiosulfonate (MTS) reagents at certain sites resulted in changes to the steady-state voltage dependency of the cotransport mode (1 mM P(i), 100 mM Na(+) at pH 7.4) of the mutants. At Gly-134 (ECL-1) and Met-533 (ECL-4), complementary behavior of the voltage dependency was documented with respect to the effect of cys-substitution and modification. G134C had a weak voltage dependency that became even stronger than that of the wild type (WT) after MTS incubation. M533C showed a WT-like voltage dependency that became markedly weaker after MTS incubation. To elucidate the underlying mechanism, the steady-state and presteady-state kinetics of these mutants were studied in detail. The apparent affinity constants for P(i) and Na(+) did not show large changes after MTS exposure. However, the dependency on external protons was changed in a complementary manner for each mutant. This suggested that cys substitution at Gly-134 or modification of Cys-533 had induced similar conformational changes to alter the proton modulation of transport kinetics. The changes in steady-state voltage dependency correlated with changes in the kinetics of presteady-state charge movements determined in the absence of P(i), which suggested that voltage-dependent transitions in the transport cycle were altered. The steady-state and presteady-state behavior was simulated using an eight-state kinetic model in which the transition rate constants of the empty carrier and translocation of the fully loaded carrier were found to be critical determinants of the transport kinetics. The simulations predict that cys substitution at Gly-134 or cys modification of Cys-533 alters the preferred orientation of the empty carrier from an inward to outward-facing conformation for hyperpolarizing voltages. The Rockefeller University Press 2004-11 /pmc/articles/PMC2234003/ /pubmed/15504899 http://dx.doi.org/10.1085/jgp.200409061 Text en Copyright © 2004, The Rockefeller University Press This article is distributed under the terms of an Attribution–Noncommercial–Share Alike–No Mirror Sites license for the first six months after the publication date (see http://www.rupress.org/terms). After six months it is available under a Creative Commons License (Attribution–Noncommercial–Share Alike 4.0 Unported license, as described at http://creativecommons.org/licenses/by-nc-sa/4.0/).
spellingShingle Article
Ehnes, Colin
Forster, Ian C.
Bacconi, Andrea
Kohler, Katja
Biber, Jürg
Murer, Heini
Structure–Function Relations of the First and Fourth Extracellular Linkers of the Type IIa Na(+)/P(i) Cotransporter: II. Substrate Interaction and Voltage Dependency of Two Functionally Important Sites
title Structure–Function Relations of the First and Fourth Extracellular Linkers of the Type IIa Na(+)/P(i) Cotransporter: II. Substrate Interaction and Voltage Dependency of Two Functionally Important Sites
title_full Structure–Function Relations of the First and Fourth Extracellular Linkers of the Type IIa Na(+)/P(i) Cotransporter: II. Substrate Interaction and Voltage Dependency of Two Functionally Important Sites
title_fullStr Structure–Function Relations of the First and Fourth Extracellular Linkers of the Type IIa Na(+)/P(i) Cotransporter: II. Substrate Interaction and Voltage Dependency of Two Functionally Important Sites
title_full_unstemmed Structure–Function Relations of the First and Fourth Extracellular Linkers of the Type IIa Na(+)/P(i) Cotransporter: II. Substrate Interaction and Voltage Dependency of Two Functionally Important Sites
title_short Structure–Function Relations of the First and Fourth Extracellular Linkers of the Type IIa Na(+)/P(i) Cotransporter: II. Substrate Interaction and Voltage Dependency of Two Functionally Important Sites
title_sort structure–function relations of the first and fourth extracellular linkers of the type iia na(+)/p(i) cotransporter: ii. substrate interaction and voltage dependency of two functionally important sites
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2234003/
https://www.ncbi.nlm.nih.gov/pubmed/15504899
http://dx.doi.org/10.1085/jgp.200409061
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