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

Karina O Brandão; Lettine van den Brink; Duncan C Miller; Catarina Grandela; Berend J van Meer; Mervyn P H Mol; Tessa de Korte; Leon G J Tertoolen; Christine L Mummery; Luca Sala; Arie O Verkerk; Richard P Davis

doi:10.1016/j.stemcr.2020.10.005

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

Stem Cell Reports. 2020 Nov 10;15(5):1127-1139. doi: 10.1016/j.stemcr.2020.10.005.

Affiliations

¹ Department of Anatomy and Embryology, Leiden University Medical Center, 2300RC Leiden, The Netherlands.
² Istituto Auxologico Italiano, IRCCS, Laboratory of Cardiovascular Genetics, 20095 Milan, Italy.
³ Department of Medical Biology, Amsterdam UMC, University of Amsterdam, 1105AZ Amsterdam, The Netherlands; Department of Experimental Cardiology, Amsterdam UMC, University of Amsterdam, 1105AZ Amsterdam, The Netherlands.
⁴ Department of Anatomy and Embryology, Leiden University Medical Center, 2300RC Leiden, The Netherlands. Electronic address: r.p.davis@lumc.nl.

Abstract

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.

Keywords: arrhythmia; disease modeling; electrophysiology; genome editing; induced pluripotent stem cells; isogenic; long QT syndrome 2; risk stratification.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Arrhythmias, Cardiac / chemically induced
Cell Line
ERG1 Potassium Channel / genetics
ERG1 Potassium Channel / metabolism*
Electrophysiology
Gene Editing
Genetic Predisposition to Disease
Humans
Induced Pluripotent Stem Cells / drug effects
Induced Pluripotent Stem Cells / physiology*
Long QT Syndrome / genetics
Long QT Syndrome / metabolism*
Models, Biological
Mutation
Myocytes, Cardiac / drug effects
Myocytes, Cardiac / physiology*
Patch-Clamp Techniques
Piperidines / adverse effects
Pyridines / adverse effects

Substances

ERG1 Potassium Channel
KCNH2 protein, human
Piperidines
Pyridines
E 4031

Supplementary concepts

Long Qt Syndrome 2