The Electrogenic Sodium Pump in Guinea-pig Ventricular Muscle: Inhibition of Pump Current by Cardiac Glycosides

Overview

Journal J Physiol

Specialty Physiology

Date 1982 Sep 1

PMID 6294287

Citations 25

Authors

J Daut

R Rudel

Affiliations

Soon will be listed here.

Abstract

1. The inhibition of the electrogenic sodium pump in guinea-pig ventricular muscle by cardiac glycosides was studied with a voltage-clamp technique.2. Superfusion of the preparation with dihydro-ouabain (DHO) produced a reversible depolarization of up to 7 mV. When the membrane potential was clamped to a constant value near the resting potential application of DHO produced a corresponding current change in the inward direction which reached a steady state in less than 1 min.3. The drug-induced current change (I(D)) was found to be the result of a parallel shift of the current-voltage relation. The contributions of a change in extracellular K or intracellular Na to the measured I(D) were shown to be very small. From these findings and the results summarized below it was concluded that I(D) represents the blockage of the electrogenic pump current by DHO and that it is proportional to the number of drug molecules bound to the Na-K-ATPase in the intact cell.4. The dependence of I(D) on the concentration of DHO applied (5 x 10(-6)-8 x 10(-4) M) was found to be consistent with the predictions of the law of mass action for reversible one-to-one binding of the drug to the Na-K pump under equilibrium conditions. From a Scatchard-type plot the equilibrium dissociation constant (K(D)) of DHO was determined to be 4.6 (+/-2.3) x 10(-5) M.5. The steady-state pump current in the resting preparation was calculated to be 0.81+/-0.26 muA/cm(2). It contributed 6.4+/-0.9 mV to the resting potential in Tyrode solution containing 3 mM-K.6. In the smallest preparations used the measured time course of the onset and decay of I(D) agreed with the chemical kinetics of binding and unbinding calculated for various DHO concentrations. The rate constant of unbinding (k(2)) was found to be 3.4 (+/-0.7) x 10(-2) S(-1) and the average rate constant of binding (k(1)) was 7.4 x 10(2) M(-1) S(-1).7. By comparing the effects of ouabain and DHO in the same preparation the following estimates of the chemical constants of ouabain binding to the Na-K pump were obtained: K(D) approximately 1.5 x 10(-6) M; k(1) approximately 4 x 10(3) M(-1) S(-1); k(2) approximately 6 x 10(-3) S(-1).8. An analysis of the transmembrane movements of Na and K in the steady state showed that the measured pump current density is consistent with a counter-transport of 3 Na and 2 K ions.

Citing Articles

The potassium current carried by TREK-1 channels in rat cardiac ventricular muscle.

Bodnar M, Schlichthorl G, Daut J Pflugers Arch. 2014; 467(5):1069-79.

PMID: 25539776 DOI: 10.1007/s00424-014-1678-9.

Oxidative phosphorylation in myocardial mitochondria 'in situ': a calorimetric study on permeabilized cardiac muscle preparations.

Kohnke D, Schramm M, Daut J Mol Cell Biochem. 1997; 174(1-2):101-13.

PMID: 9309673

Effects of acetylcholine on the Na(+)-K+ pump current in guinea-pig ventricular myocytes.

Gao J, Mathias R, Cohen I, Baldo G J Physiol. 1997; 501 ( Pt 3):527-35.

PMID: 9218213 PMC: 1159454. DOI: 10.1111/j.1469-7793.1997.527bm.x.

Cholinergic stimulation of the Na+/K+ adenosine triphosphatase as revealed by microphysiometry.

Miller D, Olson J, Parce J, Owicki J Biophys J. 1993; 64(3):813-23.

PMID: 8386019 PMC: 1262395. DOI: 10.1016/S0006-3495(93)81442-5.

Ionic mechanisms of action potential prolongation at low temperature in guinea-pig ventricular myocytes.

Kiyosue T, Arita M, Muramatsu H, Spindler A, Noble D J Physiol. 1993; 468:85-106.

PMID: 8254536 PMC: 1143816. DOI: 10.1113/jphysiol.1993.sp019761.

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