Normal interventricular differences in tissue architecture underlie right ventricular susceptibility to conduction abnormalities in a mouse model of Brugada syndrome

AIMS: Loss-of-function of the cardiac sodium channel Na(V)1.5 is a common feature of Brugada syndrome. Arrhythmias arise preferentially from the right ventricle (RV) despite equivalent Na(V)1.5 downregulation in the left ventricle (LV). The reasons for increased RV sensitivity to Na(V)1.5 loss-of-fu...

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Autores principales: Kelly, Allen, Salerno, Simona, Connolly, Adam, Bishop, Martin, Charpentier, Flavien, Stølen, Tomas, Smith, Godfrey L
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Oxford University Press 2018
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Original Articles
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5915948/
https://www.ncbi.nlm.nih.gov/pubmed/29267949
http://dx.doi.org/10.1093/cvr/cvx244
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author Kelly, Allen
Salerno, Simona
Connolly, Adam
Bishop, Martin
Charpentier, Flavien
Stølen, Tomas
Smith, Godfrey L
author_facet Kelly, Allen
Salerno, Simona
Connolly, Adam
Bishop, Martin
Charpentier, Flavien
Stølen, Tomas
Smith, Godfrey L
author_sort Kelly, Allen
collection PubMed
description AIMS: Loss-of-function of the cardiac sodium channel Na(V)1.5 is a common feature of Brugada syndrome. Arrhythmias arise preferentially from the right ventricle (RV) despite equivalent Na(V)1.5 downregulation in the left ventricle (LV). The reasons for increased RV sensitivity to Na(V)1.5 loss-of-function mutations remain unclear. Because ventricular electrical activation occurs predominantly in the transmural axis, we compare RV and LV transmural electrophysiology to determine the underlying cause of the asymmetrical conduction abnormalities in Scn5a haploinsufficient mice (Scn5a(+/−)). METHODS AND RESULTS: Optical mapping and two-photon microscopy in isolated-perfused mouse hearts demonstrated equivalent depression of transmural conduction velocity (CV) in the LV and RV of Scn5a(+/−) vs. wild-type littermates. Only RV transmural conduction was further impaired when challenged with increased pacing frequencies. Epicardial dispersion of activation and beat-to-beat variation in activation time were increased only in the RV of Scn5a(+/−) hearts. Analysis of confocal and histological images revealed larger intramural clefts between cardiomyocyte layers in the RV vs. LV, independent of genotype. Acute sodium current inhibition in wild type hearts using tetrodotoxin reproduced beat-to-beat activation variability and frequency-dependent CV slowing in the RV only, with the LV unaffected. The influence of clefts on conduction was examined using a two-dimensional monodomain computational model. When peak sodium channel conductance was reduced to 50% of normal the presence of clefts between cardiomyocyte layers reproduced the activation variability and conduction phenotype observed experimentally. CONCLUSIONS: Normal structural heterogeneities present in the RV are responsible for increased vulnerability to conduction slowing in the presence of reduced sodium channel function. Heterogeneous conduction slowing seen in the RV will predispose to functional block and the initiation of re-entrant ventricular arrhythmias.
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spelling pubmed-59159482018-04-30 Normal interventricular differences in tissue architecture underlie right ventricular susceptibility to conduction abnormalities in a mouse model of Brugada syndrome Kelly, Allen Salerno, Simona Connolly, Adam Bishop, Martin Charpentier, Flavien Stølen, Tomas Smith, Godfrey L Cardiovasc Res Original Articles AIMS: Loss-of-function of the cardiac sodium channel Na(V)1.5 is a common feature of Brugada syndrome. Arrhythmias arise preferentially from the right ventricle (RV) despite equivalent Na(V)1.5 downregulation in the left ventricle (LV). The reasons for increased RV sensitivity to Na(V)1.5 loss-of-function mutations remain unclear. Because ventricular electrical activation occurs predominantly in the transmural axis, we compare RV and LV transmural electrophysiology to determine the underlying cause of the asymmetrical conduction abnormalities in Scn5a haploinsufficient mice (Scn5a(+/−)). METHODS AND RESULTS: Optical mapping and two-photon microscopy in isolated-perfused mouse hearts demonstrated equivalent depression of transmural conduction velocity (CV) in the LV and RV of Scn5a(+/−) vs. wild-type littermates. Only RV transmural conduction was further impaired when challenged with increased pacing frequencies. Epicardial dispersion of activation and beat-to-beat variation in activation time were increased only in the RV of Scn5a(+/−) hearts. Analysis of confocal and histological images revealed larger intramural clefts between cardiomyocyte layers in the RV vs. LV, independent of genotype. Acute sodium current inhibition in wild type hearts using tetrodotoxin reproduced beat-to-beat activation variability and frequency-dependent CV slowing in the RV only, with the LV unaffected. The influence of clefts on conduction was examined using a two-dimensional monodomain computational model. When peak sodium channel conductance was reduced to 50% of normal the presence of clefts between cardiomyocyte layers reproduced the activation variability and conduction phenotype observed experimentally. CONCLUSIONS: Normal structural heterogeneities present in the RV are responsible for increased vulnerability to conduction slowing in the presence of reduced sodium channel function. Heterogeneous conduction slowing seen in the RV will predispose to functional block and the initiation of re-entrant ventricular arrhythmias. Oxford University Press 2018-04-01 2017-12-18 /pmc/articles/PMC5915948/ /pubmed/29267949 http://dx.doi.org/10.1093/cvr/cvx244 Text en © The Author(s) 2017. Published by Oxford University Press on behalf of the European Society of Cardiology 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 reuse, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Original Articles
Kelly, Allen
Salerno, Simona
Connolly, Adam
Bishop, Martin
Charpentier, Flavien
Stølen, Tomas
Smith, Godfrey L
Normal interventricular differences in tissue architecture underlie right ventricular susceptibility to conduction abnormalities in a mouse model of Brugada syndrome
title Normal interventricular differences in tissue architecture underlie right ventricular susceptibility to conduction abnormalities in a mouse model of Brugada syndrome
title_full Normal interventricular differences in tissue architecture underlie right ventricular susceptibility to conduction abnormalities in a mouse model of Brugada syndrome
title_fullStr Normal interventricular differences in tissue architecture underlie right ventricular susceptibility to conduction abnormalities in a mouse model of Brugada syndrome
title_full_unstemmed Normal interventricular differences in tissue architecture underlie right ventricular susceptibility to conduction abnormalities in a mouse model of Brugada syndrome
title_short Normal interventricular differences in tissue architecture underlie right ventricular susceptibility to conduction abnormalities in a mouse model of Brugada syndrome
title_sort normal interventricular differences in tissue architecture underlie right ventricular susceptibility to conduction abnormalities in a mouse model of brugada syndrome
topic Original Articles
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5915948/
https://www.ncbi.nlm.nih.gov/pubmed/29267949
http://dx.doi.org/10.1093/cvr/cvx244
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