Long QT Syndrome KCNH2 Variant Induces hERG1a/1b Subunit Imbalance in Patient-Specific Induced Pluripotent Stem Cell–Derived Cardiomyocytes-Reference-Cited by-同舟云学术

Long QT Syndrome KCNH2 Variant Induces hERG1a/1b Subunit Imbalance in Patient-Specific Induced Pluripotent Stem Cell–Derived Cardiomyocytes

Published:2021-04 Issue:4 Volume:14 Page:
ISSN:1941-3149
Container-title:Circulation: Arrhythmia and Electrophysiology
language:en
Short-container-title:Circ: Arrhythmia and Electrophysiology

Author:

Feng Li¹²^ORCID,Zhang Jianhua¹,Lee ChangHwan³,Kim Gina¹,Liu Fang⁴,Petersen Andrew J.⁵^ORCID,Lim Evi¹^ORCID,Anderson Corey L.¹^ORCID,Orland Kate M.¹,Robertson Gail A.⁴^ORCID,Eckhardt Lee L.¹^ORCID,January Craig T.¹,Kamp Timothy J.¹⁶^ORCID

Affiliation:

1. Cellular and Molecular Arrhythmia Research Program, Division of Cardiovascular Medicine, Department of Medicine (L.F., J.Z., G.K., E.L., C.L.A., K.M.O., L.L.E., C.T.J., T.J.K.), University of Wisconsin-Madison.

2. Department of Cardiology, Beijing Anzhen Hospital, Capital Medical University, National Clinical Research Center for Cardiovascular Diseases, China (L.F.).

3. Department of Biological Sciences, University at Albany, State University of New York (C.L.).

4. Department of Neuroscience, Wisconsin Institutes for Medical Research (F.L., G.A.R.), University of Wisconsin-Madison.

5. Waisman Center (A.J.P.), University of Wisconsin-Madison.

6. Department of Cell and Regenerative Biology (T.J.K.), University of Wisconsin-Madison.

Abstract

Background: Inherited long QT syndrome type 2 results from variants in the KCNH2 gene encoding the human Ether-à-go-go related gene 1 (hERG1) potassium channel. Two main isoforms, hERG1a and hERG1b, assemble to form tetrameric channel. The N-terminal PAS (Per/Arnt/Sim) domain, present only on hERG1a subunits, is a hotspot for pathogenic variants, but it is unknown whether PAS domain variants impact hERG1b expression to contribute to the long QT syndrome type 2 phenotype. We aimed to use patient-specific induced pluripotent stem cell-derived cardiomyocytes (iPSC-CMs) to investigate the pathogenesis of the hERG1a PAS domain variant hERG1-H70R. Methods: Human iPSCs were derived from a patient with long QT syndrome type 2 carrying the PAS domain variant hERG1-H70R. CRISPR/Cas9 gene editing produced isogenic control iPSC lines. Differentiated iPSC-CMs were evaluated for their electrophysiology, hERG1a/1b mRNA expression, and hERG1a/1b protein expression. Results: Action potentials from single hERG1-H70R iPSC-CMs were prolonged relative to controls, and voltage clamp studies showed an underlying decrease in I Kr with accelerated deactivation. In hERG1-H70R iPSC-CMs, transcription of hERG1a and hERG1b mRNA was unchanged compared with controls based on nascent nuclear transcript analysis, but hERG1b mRNA was significantly increased as was the ratio of hERG1b / hERG1a in mRNA complexes, suggesting posttranscriptional changes. Expression of complex glycosylated hERG1a in hERG1-H70R iPSC-CMs was reduced due to impaired protein trafficking, whereas the expression of the complex glycosylated form of hERG1b was unchanged. Conclusions: Patient-specific hERG1-H70R iPSC-CMs reveal a newly appreciated mechanism of pathogenesis of the long QT syndrome type 2 phenotype due to both impaired trafficking of hERG1a and maintained expression of hERG1b that produces subunit imbalance and reduced I Kr with accelerated deactivation. Graphic Abstract: A graphic abstract is available for this article.

Publisher

Ovid Technologies (Wolters Kluwer Health)

Subject

Physiology (medical),Cardiology and Cardiovascular Medicine

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