Gene- and variant-specific efficacy of serum/glucocorticoid-regulated kinase 1 inhibition in long QT syndrome types 1 and 2-Reference-Cited by-同舟云学术

Gene- and variant-specific efficacy of serum/glucocorticoid-regulated kinase 1 inhibition in long QT syndrome types 1 and 2

Published:2023-04-26 Issue:5 Volume:25 Page:
ISSN:1099-5129
Container-title:Europace
language:en
Short-container-title:

Author:

Giannetti Federica¹,Barbieri Miriam²,Shiti Assad³,Casini Simona⁴,Sager Philip T⁵⁶,Das Saumya⁵⁷,Pradhananga Sabindra⁵,Srinivasan Dinesh⁵,Nimani Saranda²,Alerni Nicolò²,Louradour Julien²,Mura Manuela⁸,Gnecchi Massimiliano⁸⁹,Brink Paul¹⁰,Zehender Manfred¹¹,Koren Gideon¹²,Zaza Antonio¹³,Crotti Lia¹¹⁴,Wilde Arthur A M⁴,Schwartz Peter J¹,Remme Carol Ann⁴,Gepstein Lior³¹⁵,Sala Luca¹¹³,Odening Katja E²

Affiliation:

1. Istituto Auxologico Italiano IRCCS, Center for Cardiac Arrhythmias of Genetic Origin and Laboratory of Cardiovascular Genetics , Milan , Italy

2. Translational Cardiology, Department of Cardiology and Department of Physiology, University Hospital Bern, University of Bern , Bühlplatz 5, 3012 Bern , Switzerland

3. Rappaport Faculty of Medicine and Research Institute, Technion–Israel Institute of Technology , Haifa , Israel

4. Amsterdam UMC Location AMC Department of Clinical and Experimental Cardiology, Heart Centre , Amsterdam , The Netherlands

5. Thryv Therapeutics Inc. , Montreal , Canada

6. Cardiovascular Research Institute, Stanford University , Palo Alto, CA , USA

7. Massachusetts General Hospital, Harvard Medical School , Boston, MA , USA

8. Department of Cardiothoracic and Vascular Sciences–Translational Cardiology Center, Fondazione IRCCS Policlinico San Matteo , Pavia , Italy

9. Department of Molecular Medicine, Unit of Cardiology, University of Pavia , Pavia , Italy

10. Department of Medicine, University of Stellenbosch , Tygerberg , South Africa

11. Department of Cardiology and Angiology I, University Heart Center Freiburg, University Medical Center Freiburg , Freiburg , Germany

12. Cardiovascular Research Center, Brown University , Providence, RI , USA

13. Department of Biotechnology and Biosciences, University of Milano-Bicocca , Milan , Italy

14. Department of Medicine and Surgery, University of Milano-Bicocca , Milan , Italy

15. Cardiology Department, Rambam Health Care Campus , Haifa , Israel

Abstract

Abstract Aims Current long QT syndrome (LQTS) therapy, largely based on beta-blockade, does not prevent arrhythmias in all patients; therefore, novel therapies are warranted. Pharmacological inhibition of the serum/glucocorticoid-regulated kinase 1 (SGK1-Inh) has been shown to shorten action potential duration (APD) in LQTS type 3. We aimed to investigate whether SGK1-Inh could similarly shorten APD in LQTS types 1 and 2. Methods and results Human-induced pluripotent stem cell-derived cardiomyocytes (hiPSC-CMs) and hiPSC-cardiac cell sheets (CCS) were obtained from LQT1 and LQT2 patients; CMs were isolated from transgenic LQT1, LQT2, and wild-type (WT) rabbits. Serum/glucocorticoid-regulated kinase 1 inhibition effects (300 nM–10 µM) on field potential durations (FPD) were investigated in hiPSC-CMs with multielectrode arrays; optical mapping was performed in LQT2 CCS. Whole-cell and perforated patch clamp recordings were performed in isolated LQT1, LQT2, and WT rabbit CMs to investigate SGK1-Inh (3 µM) effects on APD. In all LQT2 models across different species (hiPSC-CMs, hiPSC-CCS, and rabbit CMs) and independent of the disease-causing variant (KCNH2-p.A561V/p.A614V/p.G628S/IVS9-28A/G), SGK1-Inh dose-dependently shortened FPD/APD at 0.3–10 µM (by 20–32%/25–30%/44–45%). Importantly, in LQT2 rabbit CMs, 3 µM SGK1-Inh normalized APD to its WT value. A significant FPD shortening was observed in KCNQ1-p.R594Q hiPSC-CMs at 1/3/10 µM (by 19/26/35%) and in KCNQ1-p.A341V hiPSC-CMs at 10 µM (by 29%). No SGK1-Inh-induced FPD/APD shortening effect was observed in LQT1 KCNQ1-p.A341V hiPSC-CMs or KCNQ1-p.Y315S rabbit CMs at 0.3–3 µM. Conclusion A robust SGK1-Inh-induced APD shortening was observed across different LQT2 models, species, and genetic variants but less consistently in LQT1 models. This suggests a genotype- and variant-specific beneficial effect of this novel therapeutic approach in LQTS.

Funder

European Joint Research Program on Rare Diseases

Biomedical Research

Leducq Foundation for Cardiovascular Research

European Research Council

Publisher

Oxford University Press (OUP)

Subject

Physiology (medical),Cardiology and Cardiovascular Medicine

Link

https://academic.oup.com/europace/article-pdf/25/5/euad094/50487443/euad094.pdf

Reference69 articles.