The Voltage Dependence of a Cloned Mammalian Renal Type II Na(+)/P(i) Cotransporter (NaP(i)-2)

The voltage dependence of the rat renal type II Na(+)/P(i) cotransporter (NaP(i)-2) was investigated by expressing NaP(i)-2 in Xenopus laevis oocytes and applying the two-electrode voltage clamp. In the steady state, superfusion with inorganic phosphate (P(i)) induced inward currents (I(p)) in the p...

Descripción completa

Detalles Bibliográficos
Autores principales: Forster, Ian, Hernando, Nati, Biber, Jürg, Murer, Heini
Formato: Texto
Lenguaje:English
Publicado: The Rockefeller University Press 1998
Materias:
Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2229411/
https://www.ncbi.nlm.nih.gov/pubmed/9649580
_version_ 1782150122121986048
author Forster, Ian
Hernando, Nati
Biber, Jürg
Murer, Heini
author_facet Forster, Ian
Hernando, Nati
Biber, Jürg
Murer, Heini
author_sort Forster, Ian
collection PubMed
description The voltage dependence of the rat renal type II Na(+)/P(i) cotransporter (NaP(i)-2) was investigated by expressing NaP(i)-2 in Xenopus laevis oocytes and applying the two-electrode voltage clamp. In the steady state, superfusion with inorganic phosphate (P(i)) induced inward currents (I(p)) in the presence of 96 mM Na(+) over the potential range −140 ≤ V ≤ +40 mV. With P(i) as the variable substrate, the apparent affinity constant (K (m) (Pi)) was strongly dependent on Na(+), increasing sixfold for a twofold reduction in external Na(+). K (m) (Pi) increased with depolarizing voltage and was more sensitive to voltage at reduced Na(+). The Hill coefficient was close to unity and the predicted maximum I(p) (I(pmax)) was 40% smaller at 50 mM Na(+). With Na(+) as the variable substrate, K (m) (Na) was weakly dependent on both P(i) and voltage, the Hill coefficient was close to 3 and I(pmax) was independent of P(i) at −50 mV. The competitive inhibitor phosphonoformic acid suppressed the steady state holding current in a Na(+)-dependent manner, indicating the existence of uncoupled Na(+) slippage. Voltage steps induced pre–steady state relaxations typical for Na(+)-coupled cotransporters. NaP(i)-2-dependent relaxations were quantitated by a single, voltage-dependent exponential. At 96 mM Na(+), a Boltzmann function was fit to the steady state charge distribution (Q-V) to give a midpoint voltage (V(0.5)) in the range −20 to −50 mV and an apparent valency of ∼0.5 e(−). V(0.5) became more negative as Na(+) was reduced. P(i) suppressed relaxations in a dose-dependent manner, but had little effect on their voltage dependence. Reducing external pH shifted V(0.5) to depolarizing potentials and suppressed relaxations in the absence of Na(+), suggesting that protons interact with the unloaded carrier. These findings were incorporated into an ordered kinetic model whereby Na(+) is the first and last substrate to bind, and the observed voltage dependence arises from the unloaded carrier and first Na(+) binding step.
format Text
id pubmed-2229411
institution National Center for Biotechnology Information
language English
publishDate 1998
publisher The Rockefeller University Press
record_format MEDLINE/PubMed
spelling pubmed-22294112008-04-22 The Voltage Dependence of a Cloned Mammalian Renal Type II Na(+)/P(i) Cotransporter (NaP(i)-2) Forster, Ian Hernando, Nati Biber, Jürg Murer, Heini J Gen Physiol Article The voltage dependence of the rat renal type II Na(+)/P(i) cotransporter (NaP(i)-2) was investigated by expressing NaP(i)-2 in Xenopus laevis oocytes and applying the two-electrode voltage clamp. In the steady state, superfusion with inorganic phosphate (P(i)) induced inward currents (I(p)) in the presence of 96 mM Na(+) over the potential range −140 ≤ V ≤ +40 mV. With P(i) as the variable substrate, the apparent affinity constant (K (m) (Pi)) was strongly dependent on Na(+), increasing sixfold for a twofold reduction in external Na(+). K (m) (Pi) increased with depolarizing voltage and was more sensitive to voltage at reduced Na(+). The Hill coefficient was close to unity and the predicted maximum I(p) (I(pmax)) was 40% smaller at 50 mM Na(+). With Na(+) as the variable substrate, K (m) (Na) was weakly dependent on both P(i) and voltage, the Hill coefficient was close to 3 and I(pmax) was independent of P(i) at −50 mV. The competitive inhibitor phosphonoformic acid suppressed the steady state holding current in a Na(+)-dependent manner, indicating the existence of uncoupled Na(+) slippage. Voltage steps induced pre–steady state relaxations typical for Na(+)-coupled cotransporters. NaP(i)-2-dependent relaxations were quantitated by a single, voltage-dependent exponential. At 96 mM Na(+), a Boltzmann function was fit to the steady state charge distribution (Q-V) to give a midpoint voltage (V(0.5)) in the range −20 to −50 mV and an apparent valency of ∼0.5 e(−). V(0.5) became more negative as Na(+) was reduced. P(i) suppressed relaxations in a dose-dependent manner, but had little effect on their voltage dependence. Reducing external pH shifted V(0.5) to depolarizing potentials and suppressed relaxations in the absence of Na(+), suggesting that protons interact with the unloaded carrier. These findings were incorporated into an ordered kinetic model whereby Na(+) is the first and last substrate to bind, and the observed voltage dependence arises from the unloaded carrier and first Na(+) binding step. The Rockefeller University Press 1998-07-01 /pmc/articles/PMC2229411/ /pubmed/9649580 Text en 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
Forster, Ian
Hernando, Nati
Biber, Jürg
Murer, Heini
The Voltage Dependence of a Cloned Mammalian Renal Type II Na(+)/P(i) Cotransporter (NaP(i)-2)
title The Voltage Dependence of a Cloned Mammalian Renal Type II Na(+)/P(i) Cotransporter (NaP(i)-2)
title_full The Voltage Dependence of a Cloned Mammalian Renal Type II Na(+)/P(i) Cotransporter (NaP(i)-2)
title_fullStr The Voltage Dependence of a Cloned Mammalian Renal Type II Na(+)/P(i) Cotransporter (NaP(i)-2)
title_full_unstemmed The Voltage Dependence of a Cloned Mammalian Renal Type II Na(+)/P(i) Cotransporter (NaP(i)-2)
title_short The Voltage Dependence of a Cloned Mammalian Renal Type II Na(+)/P(i) Cotransporter (NaP(i)-2)
title_sort voltage dependence of a cloned mammalian renal type ii na(+)/p(i) cotransporter (nap(i)-2)
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2229411/
https://www.ncbi.nlm.nih.gov/pubmed/9649580
work_keys_str_mv AT forsterian thevoltagedependenceofaclonedmammalianrenaltypeiinapicotransporternapi2
AT hernandonati thevoltagedependenceofaclonedmammalianrenaltypeiinapicotransporternapi2
AT biberjurg thevoltagedependenceofaclonedmammalianrenaltypeiinapicotransporternapi2
AT murerheini thevoltagedependenceofaclonedmammalianrenaltypeiinapicotransporternapi2
AT forsterian voltagedependenceofaclonedmammalianrenaltypeiinapicotransporternapi2
AT hernandonati voltagedependenceofaclonedmammalianrenaltypeiinapicotransporternapi2
AT biberjurg voltagedependenceofaclonedmammalianrenaltypeiinapicotransporternapi2
AT murerheini voltagedependenceofaclonedmammalianrenaltypeiinapicotransporternapi2

Ejemplares similares