Nocturnal Atrial Fibrillation Caused by Mutation in KCND2, Encoding Pore-Forming (α) Subunit of the Cardiac Kv4.2 Potassium Channel

Max Drabkin; Noam Zilberberg; Sasson Menahem; Wesam Mulla; Daniel Halperin; Yuval Yogev; Ohad Wormser; Yonatan Perez; Rotem Kadir; Yoram Etzion; Amos Katz; Ohad S Birk

doi:10.1161/CIRCGEN.118.002293

Nocturnal Atrial Fibrillation Caused by Mutation in KCND2, Encoding Pore-Forming (α) Subunit of the Cardiac Kv4.2 Potassium Channel

Circ Genom Precis Med. 2018 Nov;11(11):e002293. doi: 10.1161/CIRCGEN.118.002293.

Authors

Max Drabkin¹, Noam Zilberberg², Sasson Menahem³, Wesam Mulla^{1

4}, Daniel Halperin¹, Yuval Yogev¹, Ohad Wormser¹, Yonatan Perez¹, Rotem Kadir¹, Yoram Etzion⁴, Amos Katz^{5

6}, Ohad S Birk^{1

7

6}

Affiliations

¹ The Morris Kahn Laboratory of Human Genetics, National Institute for Biotechnology in the Negev and Department of Microbiology, Immunology and Genetics, Faculty of Health Sciences, Ben-Gurion University of the Negev, Beer-Sheva, Israel. (M.D., W.M., D.H., Y.Y., O.W., Y.P., R.K., O.S.B.).
² Department of Life Sciences and Zlotowski Center for Neuroscience, Ben-Gurion University, Beer-Sheva, Israel (N.Z.).
³ Department of Family Medicine, Faculty of Health Sciences, Ben-Gurion University of the Negev, Beer-Sheva, Israel. (S.M.).
⁴ Regenerative Medicine and Stem Cell Research Center and Department of Physiology and Cell Biology, Faculty of Health Sciences, Ben-Gurion University of the Negev, Beer-Sheva, Israel. (W.M., Y.E.).
⁵ Department of Cardiology, Barzilai University Medical Center, Ashkelon, Israel (A.K.).
⁶ affiliated to the Faculty of Health Sciences, Ben-Gurion University of the Negev, Beer-Sheva, Israel. (A.K., O.S.B.).
⁷ The Genetics Institute, Soroka University Medical Center, Beer-Sheva, Israel (O.S.B.).

PMID: 30571183
DOI: 10.1161/CIRCGEN.118.002293

Abstract

Background: Paroxysmal atrial fibrillation (AF) can be caused by gain-of-function mutations in genes, encoding the cardiac potassium channel subunits KCNJ2, KCNE1, and KCNH2 that mediate the repolarizing potassium currents I_k1, I_ks, and I_kr, respectively.

Methods: Linkage analysis, whole-exome sequencing, and Xenopus oocyte electrophysiology studies were used in this study.

Results: Through genetic studies, we showed that autosomal dominant early-onset nocturnal paroxysmal AF is caused by p.S447R mutation in KCND2, encoding the pore-forming (α) subunit of the Kv4.2 cardiac potassium channel. Kv4.2, along with Kv4.3, contributes to the cardiac fast transient outward K⁺ current, I_to. I_to underlies the early phase of repolarization in the cardiac action potential, thereby setting the initial potential of the plateau phase and governing its duration and amplitude. In Xenopus oocytes, the mutation increased the channel's inactivation time constant and affected its regulation: p.S447 resides in a protein kinase C (PKC) phosphorylation site, which normally allows attenuation of Kv4.2 membrane expression. The mutant Kv4.2 exhibited impaired response to PKC; hence, Kv4.2 membrane expression was augmented, enhancing potassium currents. Coexpression of mutant and wild-type channels (recapitulating heterozygosity in affected individuals) showed results similar to the mutant channel alone. Finally, in a hybrid channel composed of Kv4.3 and Kv4.2, simulating the mature endogenous heterotetrameric channel underlying I_to, the p.S447R Kv4.2 mutation exerted a gain-of-function effect on Kv4.3.

Conclusions: The mutation alters Kv4.2's kinetic properties, impairs its inhibitory regulation, and exerts gain-of-function effect on both Kv4.2 homotetramers and Kv4.2-Kv4.3 heterotetramers. These effects presumably increase the repolarizing potassium current I_to, thereby abbreviating action potential duration, creating arrhythmogenic substrate for nocturnal AF. Interestingly, Kv4.2 expression was previously shown to demonstrate circadian variation, with peak expression at daytime in murine hearts (human nighttime), with possible relevance to the nocturnal onset of paroxysmal AF symptoms in our patients. The atrial-specific phenotype suggests that targeting Kv4.2 might be effective in the treatment of nocturnal paroxysmal AF, avoiding adverse ventricular effects.

Keywords: atrial fibrillation; flecainide; genetics; mutation; potassium channels; propafenone.

Publication types

Clinical Trial

MeSH terms

Action Potentials / genetics*
Animals
Atrial Fibrillation* / genetics
Atrial Fibrillation* / metabolism
Atrial Fibrillation* / pathology
Atrial Fibrillation* / physiopathology
Female
Humans
Male
Mice
Middle Aged
Mutation*
Shal Potassium Channels* / genetics
Shal Potassium Channels* / metabolism

Substances

KCND2 protein, human
Kcnd2 protein, mouse
Shal Potassium Channels

Supplementary concepts

Atrial fibrillation, familial 1