Genetic Ablation of TASK-1 (Tandem of P Domains in a Weak Inward Rectifying K+ Channel-Related Acid-Sensitive K+ Channel-1) (K2P3.1) K+ Channels Suppresses Atrial Fibrillation and Prevents Electrical Remodeling

Constanze Schmidt; Felix Wiedmann; Christoph Beyersdorf; Zhihan Zhao; Ibrahim El-Battrawy; Huan Lan; Gabor Szabo; Xin Li; Siegfried Lang; Sevil Korkmaz-Icöz; Kleopatra Rapti; Andreas Jungmann; Antonius Ratte; Oliver J Müller; Matthias Karck; Gunnar Seemann; Ibrahim Akin; Martin Borggrefe; Xiao-Bo Zhou; Hugo A Katus; Dierk Thomas

doi:10.1161/CIRCEP.119.007465

Genetic Ablation of TASK-1 (Tandem of P Domains in a Weak Inward Rectifying K⁺ Channel-Related Acid-Sensitive K⁺ Channel-1) (K_2P3.1) K⁺ Channels Suppresses Atrial Fibrillation and Prevents Electrical Remodeling

Circ Arrhythm Electrophysiol. 2019 Sep;12(9):e007465. doi: 10.1161/CIRCEP.119.007465. Epub 2019 Sep 13.

Authors

Constanze Schmidt^{1

2

3}, Felix Wiedmann^{1

2

3}, Christoph Beyersdorf^{1

2

3}, Zhihan Zhao^{2

4}, Ibrahim El-Battrawy^{2

4}, Huan Lan^{2

4}, Gabor Szabo⁵, Xin Li⁴, Siegfried Lang^{2

4}, Sevil Korkmaz-Icöz⁵, Kleopatra Rapti^{1

2}, Andreas Jungmann^{1

2}, Antonius Ratte^{1

2

3}, Oliver J Müller^{6

7}, Matthias Karck⁵, Gunnar Seemann^{8

9}, Ibrahim Akin^{2

4}, Martin Borggrefe^{2

4}, Xiao-Bo Zhou^{2

4}, Hugo A Katus^{1

2

3}, Dierk Thomas^{1

2}

Affiliations

¹ Department of Cardiology (C.S., F.W., C.B., K.R., A.J., A.R., H.A.K., D.T.), University of Heidelberg.
² DZHK (German Centre for Cardiovascular Research), partner site Heidelberg/Mannheim (C.S., F.W., C.B., Z.Z., I.E.-B., H.L., S.L., K.R., A.J., A.R., I.A., M.B., X.-B.Z., H.A.K., D.T.), University of Heidelberg.
³ HCR (Heidelberg Center for Heart Rhythm Disorders) (C.S., F.W., C.B., A.R., H.A.K., D.T.), University Hospital Heidelberg.
⁴ First Department of Medicine, University Medical Center Mannheim (Z.Z., I.E.-B., H.L., X.L., S.L., I.A., M.B., X.-B.Z.).
⁵ Department of Cardiac Surgery (G. Szabo, S.K.-I., M.K.), University Hospital Heidelberg.
⁶ Department of Internal Medicine III (O.J.M.), University of Kiel.
⁷ DZHK, partner site Hamburg/Kiel/Lübeck (O.J.M.), University of Kiel.
⁸ Institute for Experimental Cardiovascular Medicine, University Heart Centre Freiburg/Bad Krozingen (G. Seemann).
⁹ Faculty of Medicine, Albert-Ludwigs University of Freiburg, Germany (G. Seemann).

PMID: 31514528
DOI: 10.1161/CIRCEP.119.007465

Abstract

Background: Despite an increasing understanding of atrial fibrillation (AF) pathophysiology, translation into mechanism-based treatment options is lacking. In atrial cardiomyocytes of patients with chronic AF, expression, and function of tandem of P domains in a weak inward rectifying TASK-1 (K⁺ channel-related acid-sensitive K⁺ channel-1) (K_2P3.1) atrial-specific 2-pore domain potassium channels is enhanced, resulting in action potential duration shortening. TASK-1 channel inhibition prevents action potential duration shortening to maintain values observed among sinus rhythm subjects. The present preclinical study used a porcine AF model to evaluate the antiarrhythmic efficacy of TASK-1 inhibition by adeno-associated viral anti-TASK-1-siRNA (small interfering RNA) gene transfer.

Methods: AF was induced in domestic pigs by atrial burst stimulation via implanted pacemakers. Adeno-associated viral vectors carrying anti-TASK-1-siRNA were injected into both atria to suppress TASK-1 channel expression. After the 14-day follow-up period, porcine cardiomyocytes were isolated from right and left atrium, followed by electrophysiological and molecular characterization.

Results: AF was associated with increased TASK-1 transcript, protein and ion current levels leading to shortened action potential duration in atrial cardiomyocytes compared to sinus rhythm controls, similar to previous findings in humans. Anti-TASK-1 adeno-associated viral application significantly reduced AF burden in comparison to untreated AF pigs. Antiarrhythmic effects of anti-TASK-1-siRNA were associated with reduction of TASK-1 currents and prolongation of action potential durations in atrial cardiomyocytes to sinus rhythm values. Conclusions Adeno-associated viral-based anti-TASK-1 gene therapy suppressed AF and corrected cellular electrophysiological remodeling in a porcine model of AF. Suppression of AF through selective reduction of TASK-1 currents represents a new option for antiarrhythmic therapy.

Keywords: action potential; atrial fibrillation; catheter ablation; potassium; risk factor.

Publication types

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

MeSH terms

Action Potentials / physiology
Animals
Anti-Arrhythmia Agents / therapeutic use*
Atrial Fibrillation / genetics*
Atrial Fibrillation / metabolism
Atrial Fibrillation / therapy
Atrial Remodeling / physiology*
Disease Models, Animal
Electrocardiography
Gene Expression Regulation*
Genetic Therapy / methods*
Heart Atria / physiopathology*
Myocytes, Cardiac / metabolism
Nerve Tissue Proteins / antagonists & inhibitors
Nerve Tissue Proteins / biosynthesis
Nerve Tissue Proteins / genetics*
Potassium Channels, Tandem Pore Domain / antagonists & inhibitors
Potassium Channels, Tandem Pore Domain / biosynthesis
Potassium Channels, Tandem Pore Domain / genetics*
RNA / genetics
Rats
Swine

Substances

Anti-Arrhythmia Agents
Nerve Tissue Proteins
Potassium Channels, Tandem Pore Domain
potassium channel subfamily K member 3
RNA