Electrical Restitution and Its Modifications by Antiarrhythmic Drugs in Undiseased Human Ventricular Muscle

INTRODUCTION: Re-entry is a basic mechanism of ventricular fibrillation, which can be elicited by extrasystolic activity, but the timing of an extrasystole can be critical. The action potential duration (APD) of an extrasystole depends on the proximity of the preceding beat, and the relation between...

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Autores principales: Árpádffy-Lovas, Tamás, Baczkó, István, Baláti, Beáta, Bitay, Miklós, Jost, Norbert, Lengyel, Csaba, Nagy, Norbert, Takács, János, Varró, András, Virág, László
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2020
Materias:
Pharmacology
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7203420/
https://www.ncbi.nlm.nih.gov/pubmed/32425771
http://dx.doi.org/10.3389/fphar.2020.00479
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author Árpádffy-Lovas, Tamás
Baczkó, István
Baláti, Beáta
Bitay, Miklós
Jost, Norbert
Lengyel, Csaba
Nagy, Norbert
Takács, János
Varró, András
Virág, László
author_facet Árpádffy-Lovas, Tamás
Baczkó, István
Baláti, Beáta
Bitay, Miklós
Jost, Norbert
Lengyel, Csaba
Nagy, Norbert
Takács, János
Varró, András
Virág, László
author_sort Árpádffy-Lovas, Tamás
collection PubMed
description INTRODUCTION: Re-entry is a basic mechanism of ventricular fibrillation, which can be elicited by extrasystolic activity, but the timing of an extrasystole can be critical. The action potential duration (APD) of an extrasystole depends on the proximity of the preceding beat, and the relation between its timing and its APD is called electrical restitution. The aim of the present work was to study and compare the effect of several antiarrhythmic drugs on restitution in preparations from undiseased human ventricular muscle, and other mammalian species. METHODS: Action potentials were recorded in preparations obtained from rat, guinea pig, rabbit, and dog hearts; and from undiseased human donor hearts using the conventional microelectrode technique. Preparations were stimulated with different basic cycle lengths (BCLs) ranging from 300 to 5,000 ms. To study restitution, single test pulses were applied at every 20th beat while the preparation was driven at 1,000 ms BCL. RESULTS: Marked differences were found between the animal and human preparations regarding restitution and steady-state frequency dependent curves. In human ventricular muscle, restitution kinetics were slower in preparations with large phase 1 repolarization with shorter APDs at 1000 ms BCL compared to preparations with small phase 1. Preparations having APD longer than 300 ms at 1000 ms BCL had slower restitution kinetics than those having APD shorter than 250 ms. The selective I(Kr) inhibitors E-4031 and sotalol increased overall APD and slowed the restitution kinetics, while I(Ks) inhibition did not influence APD and electrical restitution. Mexiletine and nisoldipine shortened APD, but only mexiletine slowed restitution kinetics. DISCUSSION: Frequency dependent APD changes, including electrical restitution, were partly determined by the APD at the BCL. Small phase 1 associated with slower restitution suggests a role of I(to) in restitution. APD prolonging drugs slowed restitution, while mexiletine, a known inhibitor of I(Na), shortened basic APD but also slowed restitution. These results indicate that although basic APD has an important role in restitution, other transmembrane currents, such as I(Na) or I(to), can also affect restitution kinetics. This raises the possibility that ion channel modifier drugs slowing restitution kinetics may have antiarrhythmic properties by altering restitution.
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spelling pubmed-72034202020-05-18 Electrical Restitution and Its Modifications by Antiarrhythmic Drugs in Undiseased Human Ventricular Muscle Árpádffy-Lovas, Tamás Baczkó, István Baláti, Beáta Bitay, Miklós Jost, Norbert Lengyel, Csaba Nagy, Norbert Takács, János Varró, András Virág, László Front Pharmacol Pharmacology INTRODUCTION: Re-entry is a basic mechanism of ventricular fibrillation, which can be elicited by extrasystolic activity, but the timing of an extrasystole can be critical. The action potential duration (APD) of an extrasystole depends on the proximity of the preceding beat, and the relation between its timing and its APD is called electrical restitution. The aim of the present work was to study and compare the effect of several antiarrhythmic drugs on restitution in preparations from undiseased human ventricular muscle, and other mammalian species. METHODS: Action potentials were recorded in preparations obtained from rat, guinea pig, rabbit, and dog hearts; and from undiseased human donor hearts using the conventional microelectrode technique. Preparations were stimulated with different basic cycle lengths (BCLs) ranging from 300 to 5,000 ms. To study restitution, single test pulses were applied at every 20th beat while the preparation was driven at 1,000 ms BCL. RESULTS: Marked differences were found between the animal and human preparations regarding restitution and steady-state frequency dependent curves. In human ventricular muscle, restitution kinetics were slower in preparations with large phase 1 repolarization with shorter APDs at 1000 ms BCL compared to preparations with small phase 1. Preparations having APD longer than 300 ms at 1000 ms BCL had slower restitution kinetics than those having APD shorter than 250 ms. The selective I(Kr) inhibitors E-4031 and sotalol increased overall APD and slowed the restitution kinetics, while I(Ks) inhibition did not influence APD and electrical restitution. Mexiletine and nisoldipine shortened APD, but only mexiletine slowed restitution kinetics. DISCUSSION: Frequency dependent APD changes, including electrical restitution, were partly determined by the APD at the BCL. Small phase 1 associated with slower restitution suggests a role of I(to) in restitution. APD prolonging drugs slowed restitution, while mexiletine, a known inhibitor of I(Na), shortened basic APD but also slowed restitution. These results indicate that although basic APD has an important role in restitution, other transmembrane currents, such as I(Na) or I(to), can also affect restitution kinetics. This raises the possibility that ion channel modifier drugs slowing restitution kinetics may have antiarrhythmic properties by altering restitution. Frontiers Media S.A. 2020-04-30 /pmc/articles/PMC7203420/ /pubmed/32425771 http://dx.doi.org/10.3389/fphar.2020.00479 Text en Copyright © 2020 Árpádffy-Lovas, Baczkó, Baláti, Bitay, Jost, Lengyel, Nagy, Takács, Varró and Virág http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) and the copyright owner(s) are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.
spellingShingle Pharmacology
Árpádffy-Lovas, Tamás
Baczkó, István
Baláti, Beáta
Bitay, Miklós
Jost, Norbert
Lengyel, Csaba
Nagy, Norbert
Takács, János
Varró, András
Virág, László
Electrical Restitution and Its Modifications by Antiarrhythmic Drugs in Undiseased Human Ventricular Muscle
title Electrical Restitution and Its Modifications by Antiarrhythmic Drugs in Undiseased Human Ventricular Muscle
title_full Electrical Restitution and Its Modifications by Antiarrhythmic Drugs in Undiseased Human Ventricular Muscle
title_fullStr Electrical Restitution and Its Modifications by Antiarrhythmic Drugs in Undiseased Human Ventricular Muscle
title_full_unstemmed Electrical Restitution and Its Modifications by Antiarrhythmic Drugs in Undiseased Human Ventricular Muscle
title_short Electrical Restitution and Its Modifications by Antiarrhythmic Drugs in Undiseased Human Ventricular Muscle
title_sort electrical restitution and its modifications by antiarrhythmic drugs in undiseased human ventricular muscle
topic Pharmacology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7203420/
https://www.ncbi.nlm.nih.gov/pubmed/32425771
http://dx.doi.org/10.3389/fphar.2020.00479
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