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Literature DB >> 26536262

Importance of the Voltage Dependence of Cardiac Na/K ATPase Isozymes.

Christopher M Stanley¹, Dominique G Gagnon², Adam Bernal¹, Dylan J Meyer¹, Joshua J Rosenthal³, Pablo Artigas⁴.

Abstract

Cardiac cells express more than one isoform of the Na, K-ATPase (NKA), the heteromeric enzyme that creates the Na(+) and K(+) gradients across the plasmalemma. Cardiac isozymes contain one catalytic α-subunit isoform (α1, α2, or α3) associated with an auxiliary β-subunit isoform (β1 or β2). Past studies using biochemical approaches have revealed minor kinetic differences between isozymes formed by different α-β isoform combinations; these results make it difficult to understand the physiological requirement for multiple isoforms. In intact cells, however, NKA enzymes operate in a more complex environment, which includes a substantial transmembrane potential. We evaluated the voltage dependence of human cardiac NKA isozymes expressed in Xenopus oocytes, and of native NKA isozymes in rat ventricular myocytes, using normal mammalian physiological concentrations of Na(+)o and K(+)o. We demonstrate that although α1 and α3 pumps are functional at all physiologically relevant voltages, α2β1 pumps and α2β2 pumps are inhibited by ∼75% and ∼95%, respectively, at resting membrane potentials, and only activate appreciably upon depolarization. Furthermore, phospholemman (FXYD1) inhibits pump function without significantly altering the pump's voltage dependence. Our observations provide a simple explanation for the physiological relevance of the α2 subunit (∼20% of total α subunits in rat ventricle): they act as a reserve and are recruited into action for extra pumping during the long-lasting cardiac action potential, where most of the Na(+) entry occurs. This strong voltage dependence of α2 pumps also helps explain how cardiotonic steroids, which block NKA pumps, can be a beneficial treatment for heart failure: by only inhibiting the α2 pumps, they selectively reduce NKA activity during the cardiac action potential, leading to an increase in systolic Ca(2+), due to reduced extrusion through the Na/Ca exchanger, without affecting resting Na(+) and Ca(2+) concentrations.

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Year: 2015 PMID： 26536262 PMCID： PMC4643266 DOI： 10.1016/j.bpj.2015.09.015

Source DB: PubMed Journal: Biophys J ISSN： 0006-3495 Impact factor: 4.033

73 in total

1. The Na,K-ATPase alpha 2 isoform is expressed in neurons, and its absence disrupts neuronal activity in newborn mice.

Authors: Amy E Moseley; Steve P Lieske; Randall K Wetzel; Paul F James; Suiwen He; Daniel A Shelly; Richard J Paul; Gregory P Boivin; David P Witte; Jan Marino Ramirez; Kathleen J Sweadner; Jerry B Lingrel
Journal: J Biol Chem Date: 2002-11-27 Impact factor: 5.157

2. Electrogenic K+ transport by the Na(+)-K+ pump in rat cardiac ventricular myocytes.

Authors: R D Peluffo; J R Berlin
Journal: J Physiol Date: 1997-05-15 Impact factor: 5.182

3. The influence of calcium on sodium efflux in squid axons.

Authors: P F Baker; M P Blaustein; A L Hodgkin; R A Steinhardt
Journal: J Physiol Date: 1969-02 Impact factor: 5.182

4. Molecular cloning of three distinct forms of the Na+,K+-ATPase alpha-subunit from rat brain.

Authors: G E Shull; J Greeb; J B Lingrel
Journal: Biochemistry Date: 1986-12-16 Impact factor: 3.162

5. Regulation of Ca2+ signaling by Na+ pump alpha-2 subunit expression.

Authors: Vera Golovina; Hong Song; Paul James; Jerry Lingrel; Mordecai Blaustein
Journal: Ann N Y Acad Sci Date: 2003-04 Impact factor: 5.691

6. Electrophysiological analysis of the mutated Na,K-ATPase cation binding pocket.

Authors: Jan B Koenderink; Sven Geibel; Eva Grabsch; Jan Joep H H M De Pont; Ernst Bamberg; Thomas Friedrich
Journal: J Biol Chem Date: 2003-10-07 Impact factor: 5.157

7. Electrophysiologic properties of intercostal muscle fibers in human neuromuscular diseases.

Authors: R Gruener; L Z Stern; D Markovitz; C Gerdes
Journal: Muscle Nerve Date: 1979 May-Jun Impact factor: 3.217

8. Quaternary organic amines inhibit Na,K pump current in a voltage-dependent manner: direct evidence of an extracellular access channel in the Na,K-ATPase.

Authors: R Daniel Peluffo; Yukio Hara; Joshua R Berlin
Journal: J Gen Physiol Date: 2004-03 Impact factor: 4.086

9. Excitation-contraction coupling in cardiac Purkinje fibers. Effects of cardiotonic steroids on the intracellular [Ca2+] transient, membrane potential, and contraction.

Authors: W G Wier; P Hess
Journal: J Gen Physiol Date: 1984-03 Impact factor: 4.086

10. Block of squid axon K channels by internally and externally applied barium ions.

Authors: C M Armstrong; R P Swenson; S R Taylor
Journal: J Gen Physiol Date: 1982-11 Impact factor: 4.086

23 in total

1. Na/K Pump Mutations Associated with Primary Hyperaldosteronism Cause Loss of Function.

Authors: Dylan J Meyer; Craig Gatto; Pablo Artigas
Journal: Biochemistry Date: 2019-03-14 Impact factor: 3.162

2. Selective Assembly of Na,K-ATPase α2β2 Heterodimers in the Heart: DISTINCT FUNCTIONAL PROPERTIES AND ISOFORM-SELECTIVE INHIBITORS.

Authors: Michael Habeck; Elmira Tokhtaeva; Yotam Nadav; Efrat Ben Zeev; Sean P Ferris; Randal J Kaufman; Elizabeta Bab-Dinitz; Jack H Kaplan; Laura A Dada; Zvi Farfel; Daniel M Tal; Adriana Katz; George Sachs; Olga Vagin; Steven J D Karlish
Journal: J Biol Chem Date: 2016-09-13 Impact factor: 5.157

Importance of the Voltage Dependence of Cardiac Na/K ATPase Isozymes.

1. The Na,K-ATPase alpha 2 isoform is expressed in neurons, and its absence disrupts neuronal activity in newborn mice.

2. Electrogenic K+ transport by the Na(+)-K+ pump in rat cardiac ventricular myocytes.

3. The influence of calcium on sodium efflux in squid axons.

4. Molecular cloning of three distinct forms of the Na+,K+-ATPase alpha-subunit from rat brain.

5. Regulation of Ca2+ signaling by Na+ pump alpha-2 subunit expression.

6. Electrophysiological analysis of the mutated Na,K-ATPase cation binding pocket.

7. Electrophysiologic properties of intercostal muscle fibers in human neuromuscular diseases.

8. Quaternary organic amines inhibit Na,K pump current in a voltage-dependent manner: direct evidence of an extracellular access channel in the Na,K-ATPase.

9. Excitation-contraction coupling in cardiac Purkinje fibers. Effects of cardiotonic steroids on the intracellular [Ca2+] transient, membrane potential, and contraction.

10. Block of squid axon K channels by internally and externally applied barium ions.

1. Na/K Pump Mutations Associated with Primary Hyperaldosteronism Cause Loss of Function.

2. Selective Assembly of Na,K-ATPase α2β2 Heterodimers in the Heart: DISTINCT FUNCTIONAL PROPERTIES AND ISOFORM-SELECTIVE INHIBITORS.

3. External Ion Access in the Na/K Pump: Kinetics of Na⁺, K⁺, and Quaternary Amine Interaction.

4. Subcellular localization of Na/K-ATPase isoforms in ventricular myocytes.

Review 5. Role of Na⁺/K⁺-ATPase in ischemic stroke: in-depth perspectives from physiology to pharmacology.

6. Role of a conserved ion-binding site tyrosine in ion selectivity of the Na+/K+ pump.

Review 7. Regulation of Cardiac Contractility by the Alpha 2 Subunit of the Na⁺/K⁺-ATPase.

8. Maturation of the Na,K-ATPase in the Endoplasmic Reticulum in Health and Disease.

Review 9. Roles of Key Ion Channels and Transport Proteins in Age-Related Hearing Loss.

Review 10. Diseases caused by mutations in the Na⁺/K⁺ pump α1 gene ATP1A1.

Review 5. Role of Na+/K+-ATPase in ischemic stroke: in-depth perspectives from physiology to pharmacology.

Review 7. Regulation of Cardiac Contractility by the Alpha 2 Subunit of the Na+/K+-ATPase.

Review 9. Roles of Key Ion Channels and Transport Proteins in Age-Related Hearing Loss.

Review 10. Diseases caused by mutations in the Na+/K+ pump α1 gene ATP1A1.

Review 5. Role of Na⁺/K⁺-ATPase in ischemic stroke: in-depth perspectives from physiology to pharmacology.

Review 7. Regulation of Cardiac Contractility by the Alpha 2 Subunit of the Na⁺/K⁺-ATPase.

Review 10. Diseases caused by mutations in the Na⁺/K⁺ pump α1 gene ATP1A1.