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Efficient computation of electrograms and ECGs in human whole heart simulations using a reaction-eikonal model☆

Anatomically accurate and biophysically detailed bidomain models of the human heart have proven a powerful tool for gaining quantitative insight into the links between electrical sources in the myocardium and the concomitant current flow in the surrounding medium as they represent their relationship...

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Detalles Bibliográficos
Autores principales: Neic, Aurel, Campos, Fernando O., Prassl, Anton J., Niederer, Steven A., Bishop, Martin J., Vigmond, Edward J., Plank, Gernot
Formato: Online Artículo Texto
Lenguaje:English
Publicado: 2017
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5555399/
https://www.ncbi.nlm.nih.gov/pubmed/28819329
http://dx.doi.org/10.1016/j.jcp.2017.06.020
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author Neic, Aurel
Campos, Fernando O.
Prassl, Anton J.
Niederer, Steven A.
Bishop, Martin J.
Vigmond, Edward J.
Plank, Gernot
author_facet Neic, Aurel
Campos, Fernando O.
Prassl, Anton J.
Niederer, Steven A.
Bishop, Martin J.
Vigmond, Edward J.
Plank, Gernot
author_sort Neic, Aurel
collection PubMed
description Anatomically accurate and biophysically detailed bidomain models of the human heart have proven a powerful tool for gaining quantitative insight into the links between electrical sources in the myocardium and the concomitant current flow in the surrounding medium as they represent their relationship mechanistically based on first principles. Such models are increasingly considered as a clinical research tool with the perspective of being used, ultimately, as a complementary diagnostic modality. An important prerequisite in many clinical modeling applications is the ability of models to faithfully replicate potential maps and electrograms recorded from a given patient. However, while the personalization of electrophysiology models based on the gold standard bidomain formulation is in principle feasible, the associated computational expenses are significant, rendering their use incompatible with clinical time frames. In this study we report on the development of a novel computationally efficient reaction-eikonal (R-E) model for modeling extracellular potential maps and electrograms. Using a biventricular human electrophysiology model, which incorporates a topologically realistic His–Purkinje system (HPS), we demonstrate by comparing against a high-resolution reaction–diffusion (R–D) bidomain model that the R-E model predicts extracellular potential fields, electrograms as well as ECGs at the body surface with high fidelity and offers vast computational savings greater than three orders of magnitude. Due to their efficiency R-E models are ideally suitable for forward simulations in clinical modeling studies which attempt to personalize electrophysiological model features.
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spelling pubmed-55553992017-10-01 Efficient computation of electrograms and ECGs in human whole heart simulations using a reaction-eikonal model☆ Neic, Aurel Campos, Fernando O. Prassl, Anton J. Niederer, Steven A. Bishop, Martin J. Vigmond, Edward J. Plank, Gernot J Comput Phys Article Anatomically accurate and biophysically detailed bidomain models of the human heart have proven a powerful tool for gaining quantitative insight into the links between electrical sources in the myocardium and the concomitant current flow in the surrounding medium as they represent their relationship mechanistically based on first principles. Such models are increasingly considered as a clinical research tool with the perspective of being used, ultimately, as a complementary diagnostic modality. An important prerequisite in many clinical modeling applications is the ability of models to faithfully replicate potential maps and electrograms recorded from a given patient. However, while the personalization of electrophysiology models based on the gold standard bidomain formulation is in principle feasible, the associated computational expenses are significant, rendering their use incompatible with clinical time frames. In this study we report on the development of a novel computationally efficient reaction-eikonal (R-E) model for modeling extracellular potential maps and electrograms. Using a biventricular human electrophysiology model, which incorporates a topologically realistic His–Purkinje system (HPS), we demonstrate by comparing against a high-resolution reaction–diffusion (R–D) bidomain model that the R-E model predicts extracellular potential fields, electrograms as well as ECGs at the body surface with high fidelity and offers vast computational savings greater than three orders of magnitude. Due to their efficiency R-E models are ideally suitable for forward simulations in clinical modeling studies which attempt to personalize electrophysiological model features. 2017-10-01 /pmc/articles/PMC5555399/ /pubmed/28819329 http://dx.doi.org/10.1016/j.jcp.2017.06.020 Text en http://creativecommons.org/licenses/by-nc-nd/4.0/ This is an open access article under the CC BY-NC-ND license (http://creativecommons.org/licenses/by-nc-nd/4.0/).
spellingShingle Article
Neic, Aurel
Campos, Fernando O.
Prassl, Anton J.
Niederer, Steven A.
Bishop, Martin J.
Vigmond, Edward J.
Plank, Gernot
Efficient computation of electrograms and ECGs in human whole heart simulations using a reaction-eikonal model☆
title Efficient computation of electrograms and ECGs in human whole heart simulations using a reaction-eikonal model☆
title_full Efficient computation of electrograms and ECGs in human whole heart simulations using a reaction-eikonal model☆
title_fullStr Efficient computation of electrograms and ECGs in human whole heart simulations using a reaction-eikonal model☆
title_full_unstemmed Efficient computation of electrograms and ECGs in human whole heart simulations using a reaction-eikonal model☆
title_short Efficient computation of electrograms and ECGs in human whole heart simulations using a reaction-eikonal model☆
title_sort efficient computation of electrograms and ecgs in human whole heart simulations using a reaction-eikonal model☆
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5555399/
https://www.ncbi.nlm.nih.gov/pubmed/28819329
http://dx.doi.org/10.1016/j.jcp.2017.06.020
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