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Effects of early afterdepolarizations on excitation patterns in an accurate model of the human ventricles

Early Afterdepolarizations, EADs, are defined as the reversal of the action potential before completion of the repolarization phase, which can result in ectopic beats. However, the series of mechanisms of EADs leading to these ectopic beats and related cardiac arrhythmias are not well understood. Th...

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Autores principales: Van Nieuwenhuyse, Enid, Seemann, Gunnar, Panfilov, Alexander V., Vandersickel, Nele
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2017
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5720514/
https://www.ncbi.nlm.nih.gov/pubmed/29216239
http://dx.doi.org/10.1371/journal.pone.0188867
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author Van Nieuwenhuyse, Enid
Seemann, Gunnar
Panfilov, Alexander V.
Vandersickel, Nele
author_facet Van Nieuwenhuyse, Enid
Seemann, Gunnar
Panfilov, Alexander V.
Vandersickel, Nele
author_sort Van Nieuwenhuyse, Enid
collection PubMed
description Early Afterdepolarizations, EADs, are defined as the reversal of the action potential before completion of the repolarization phase, which can result in ectopic beats. However, the series of mechanisms of EADs leading to these ectopic beats and related cardiac arrhythmias are not well understood. Therefore, we aimed to investigate the influence of this single cell behavior on the whole heart level. For this study we used a modified version of the Ten Tusscher-Panfilov model of human ventricular cells (TP06) which we implemented in a 3D ventricle model including realistic fiber orientations. To increase the likelihood of EAD formation at the single cell level, we reduced the repolarization reserve (RR) by reducing the rapid delayed rectifier Potassium current and raising the L-type Calcium current. Varying these parameters defined a 2D parametric space where different excitation patterns could be classified. Depending on the initial conditions, by either exciting the ventricles with a spiral formation or burst pacing protocol, we found multiple different spatio-temporal excitation patterns. The spiral formation protocol resulted in the categorization of a stable spiral (S), a meandering spiral (MS), a spiral break-up regime (SB), spiral fibrillation type B (B), spiral fibrillation type A (A) and an oscillatory excitation type (O). The last three patterns are a 3D generalization of previously found patterns in 2D. First, the spiral fibrillation type B showed waves determined by a chaotic bi-excitable regime, i.e. mediated by both Sodium and Calcium waves at the same time and in same tissue settings. In the parameter region governed by the B pattern, single cells were able to repolarize completely and different (spiral) waves chaotically burst into each other without finishing a 360 degree rotation. Second, spiral fibrillation type A patterns consisted of multiple small rotating spirals. Single cells failed to repolarize to the resting membrane potential hence prohibiting the Sodium channel gates to recover. Accordingly, we found that Calcium waves mediated these patterns. Third, a further reduction of the RR resulted in a more exotic parameter regime whereby the individual cells behaved independently as oscillators. The patterns arose due to a phase-shift of different oscillators as disconnection of the cells resulted in continuation of the patterns. For all patterns, we computed realistic 9 lead ECGs by including a torso model. The B and A type pattern exposed the behavior of Ventricular Tachycardia (VT). We conclude that EADs at the single cell level can result in different types of cardiac fibrillation at the tissue and 3D ventricle level.
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spelling pubmed-57205142017-12-15 Effects of early afterdepolarizations on excitation patterns in an accurate model of the human ventricles Van Nieuwenhuyse, Enid Seemann, Gunnar Panfilov, Alexander V. Vandersickel, Nele PLoS One Research Article Early Afterdepolarizations, EADs, are defined as the reversal of the action potential before completion of the repolarization phase, which can result in ectopic beats. However, the series of mechanisms of EADs leading to these ectopic beats and related cardiac arrhythmias are not well understood. Therefore, we aimed to investigate the influence of this single cell behavior on the whole heart level. For this study we used a modified version of the Ten Tusscher-Panfilov model of human ventricular cells (TP06) which we implemented in a 3D ventricle model including realistic fiber orientations. To increase the likelihood of EAD formation at the single cell level, we reduced the repolarization reserve (RR) by reducing the rapid delayed rectifier Potassium current and raising the L-type Calcium current. Varying these parameters defined a 2D parametric space where different excitation patterns could be classified. Depending on the initial conditions, by either exciting the ventricles with a spiral formation or burst pacing protocol, we found multiple different spatio-temporal excitation patterns. The spiral formation protocol resulted in the categorization of a stable spiral (S), a meandering spiral (MS), a spiral break-up regime (SB), spiral fibrillation type B (B), spiral fibrillation type A (A) and an oscillatory excitation type (O). The last three patterns are a 3D generalization of previously found patterns in 2D. First, the spiral fibrillation type B showed waves determined by a chaotic bi-excitable regime, i.e. mediated by both Sodium and Calcium waves at the same time and in same tissue settings. In the parameter region governed by the B pattern, single cells were able to repolarize completely and different (spiral) waves chaotically burst into each other without finishing a 360 degree rotation. Second, spiral fibrillation type A patterns consisted of multiple small rotating spirals. Single cells failed to repolarize to the resting membrane potential hence prohibiting the Sodium channel gates to recover. Accordingly, we found that Calcium waves mediated these patterns. Third, a further reduction of the RR resulted in a more exotic parameter regime whereby the individual cells behaved independently as oscillators. The patterns arose due to a phase-shift of different oscillators as disconnection of the cells resulted in continuation of the patterns. For all patterns, we computed realistic 9 lead ECGs by including a torso model. The B and A type pattern exposed the behavior of Ventricular Tachycardia (VT). We conclude that EADs at the single cell level can result in different types of cardiac fibrillation at the tissue and 3D ventricle level. Public Library of Science 2017-12-07 /pmc/articles/PMC5720514/ /pubmed/29216239 http://dx.doi.org/10.1371/journal.pone.0188867 Text en © 2017 Van Nieuwenhuyse et al http://creativecommons.org/licenses/by/4.0/ This is an open access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/4.0/) , which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
spellingShingle Research Article
Van Nieuwenhuyse, Enid
Seemann, Gunnar
Panfilov, Alexander V.
Vandersickel, Nele
Effects of early afterdepolarizations on excitation patterns in an accurate model of the human ventricles
title Effects of early afterdepolarizations on excitation patterns in an accurate model of the human ventricles
title_full Effects of early afterdepolarizations on excitation patterns in an accurate model of the human ventricles
title_fullStr Effects of early afterdepolarizations on excitation patterns in an accurate model of the human ventricles
title_full_unstemmed Effects of early afterdepolarizations on excitation patterns in an accurate model of the human ventricles
title_short Effects of early afterdepolarizations on excitation patterns in an accurate model of the human ventricles
title_sort effects of early afterdepolarizations on excitation patterns in an accurate model of the human ventricles
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5720514/
https://www.ncbi.nlm.nih.gov/pubmed/29216239
http://dx.doi.org/10.1371/journal.pone.0188867
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