Isogenic Sets of hiPSC-CMs Harboring Distinct KCNH2 Mutations Differ Functionally and in Susceptibility to Drug-Induced Arrhythmias

Mutations in KCNH2 can lead to long QT syndrome type 2. Variable disease manifestation observed with this channelopathy is associated with the location and type of mutation within the protein, complicating efforts to predict patient risk. Here, we demonstrated phenotypic differences in cardiomyocyte...

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Autores principales: Brandão, Karina O., van den Brink, Lettine, Miller, Duncan C., Grandela, Catarina, van Meer, Berend J., Mol, Mervyn P.H., de Korte, Tessa, Tertoolen, Leon G.J., Mummery, Christine L., Sala, Luca, Verkerk, Arie O., Davis, Richard P.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Elsevier 2020
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Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7664051/
https://www.ncbi.nlm.nih.gov/pubmed/33176122
http://dx.doi.org/10.1016/j.stemcr.2020.10.005
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author Brandão, Karina O.
van den Brink, Lettine
Miller, Duncan C.
Grandela, Catarina
van Meer, Berend J.
Mol, Mervyn P.H.
de Korte, Tessa
Tertoolen, Leon G.J.
Mummery, Christine L.
Sala, Luca
Verkerk, Arie O.
Davis, Richard P.
author_facet Brandão, Karina O.
van den Brink, Lettine
Miller, Duncan C.
Grandela, Catarina
van Meer, Berend J.
Mol, Mervyn P.H.
de Korte, Tessa
Tertoolen, Leon G.J.
Mummery, Christine L.
Sala, Luca
Verkerk, Arie O.
Davis, Richard P.
author_sort Brandão, Karina O.
collection PubMed
description Mutations in KCNH2 can lead to long QT syndrome type 2. Variable disease manifestation observed with this channelopathy is associated with the location and type of mutation within the protein, complicating efforts to predict patient risk. Here, we demonstrated phenotypic differences in cardiomyocytes derived from isogenic human induced pluripotent stem cells (hiPSC-CMs) genetically edited to harbor mutations either within the pore or tail region of the ion channel. Electrophysiological analysis confirmed that the mutations prolonged repolarization of the hiPSC-CMs, with differences between the mutations evident in monolayer cultures. Blocking the hERG channel revealed that the pore-loop mutation conferred greater susceptibility to arrhythmic events. These findings showed that subtle phenotypic differences related to KCNH2 mutations could be captured by hiPSC-CMs under genetically matched conditions. Moreover, the results support hiPSC-CMs as strong candidates for evaluating the underlying severity of individual KCNH2 mutations in humans, which could facilitate patient risk stratification.
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spelling pubmed-76640512020-11-20 Isogenic Sets of hiPSC-CMs Harboring Distinct KCNH2 Mutations Differ Functionally and in Susceptibility to Drug-Induced Arrhythmias Brandão, Karina O. van den Brink, Lettine Miller, Duncan C. Grandela, Catarina van Meer, Berend J. Mol, Mervyn P.H. de Korte, Tessa Tertoolen, Leon G.J. Mummery, Christine L. Sala, Luca Verkerk, Arie O. Davis, Richard P. Stem Cell Reports Article Mutations in KCNH2 can lead to long QT syndrome type 2. Variable disease manifestation observed with this channelopathy is associated with the location and type of mutation within the protein, complicating efforts to predict patient risk. Here, we demonstrated phenotypic differences in cardiomyocytes derived from isogenic human induced pluripotent stem cells (hiPSC-CMs) genetically edited to harbor mutations either within the pore or tail region of the ion channel. Electrophysiological analysis confirmed that the mutations prolonged repolarization of the hiPSC-CMs, with differences between the mutations evident in monolayer cultures. Blocking the hERG channel revealed that the pore-loop mutation conferred greater susceptibility to arrhythmic events. These findings showed that subtle phenotypic differences related to KCNH2 mutations could be captured by hiPSC-CMs under genetically matched conditions. Moreover, the results support hiPSC-CMs as strong candidates for evaluating the underlying severity of individual KCNH2 mutations in humans, which could facilitate patient risk stratification. Elsevier 2020-11-10 /pmc/articles/PMC7664051/ /pubmed/33176122 http://dx.doi.org/10.1016/j.stemcr.2020.10.005 Text en © 2020 The Authors http://creativecommons.org/licenses/by/4.0/ This is an open access article under the CC BY license (http://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Brandão, Karina O.
van den Brink, Lettine
Miller, Duncan C.
Grandela, Catarina
van Meer, Berend J.
Mol, Mervyn P.H.
de Korte, Tessa
Tertoolen, Leon G.J.
Mummery, Christine L.
Sala, Luca
Verkerk, Arie O.
Davis, Richard P.
Isogenic Sets of hiPSC-CMs Harboring Distinct KCNH2 Mutations Differ Functionally and in Susceptibility to Drug-Induced Arrhythmias
title Isogenic Sets of hiPSC-CMs Harboring Distinct KCNH2 Mutations Differ Functionally and in Susceptibility to Drug-Induced Arrhythmias
title_full Isogenic Sets of hiPSC-CMs Harboring Distinct KCNH2 Mutations Differ Functionally and in Susceptibility to Drug-Induced Arrhythmias
title_fullStr Isogenic Sets of hiPSC-CMs Harboring Distinct KCNH2 Mutations Differ Functionally and in Susceptibility to Drug-Induced Arrhythmias
title_full_unstemmed Isogenic Sets of hiPSC-CMs Harboring Distinct KCNH2 Mutations Differ Functionally and in Susceptibility to Drug-Induced Arrhythmias
title_short Isogenic Sets of hiPSC-CMs Harboring Distinct KCNH2 Mutations Differ Functionally and in Susceptibility to Drug-Induced Arrhythmias
title_sort isogenic sets of hipsc-cms harboring distinct kcnh2 mutations differ functionally and in susceptibility to drug-induced arrhythmias
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7664051/
https://www.ncbi.nlm.nih.gov/pubmed/33176122
http://dx.doi.org/10.1016/j.stemcr.2020.10.005
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