The Role of <i>RYR2</i> in Atrial Fibrillation

Boehm, Bernhard M.; Gaa, Jochen; Hoppmann, Petra; Martens, Eimo; Westphal, Dominik S.

doi:https://doi.org/10.1155/2023/6555998

Case Reports in Cardiology

On this page

Abstract Introduction Case Presentation Discussion Data Availability Consent Conflicts of Interest Authors’ Contributions Acknowledgments References Copyright Related Articles

Case Report | Open Access

Volume 2023 | Article ID 6555998 | https://doi.org/10.1155/2023/6555998

The Role of RYR2 in Atrial Fibrillation

Bernhard M. Boehm,¹Jochen Gaa,²Petra Hoppmann,³Eimo Martens,³and Dominik S. Westphal^1,3

Academic Editor: Luigi Sciarra

Received06 Feb 2023

Revised20 Feb 2023

Accepted04 Mar 2023

Published15 Mar 2023

Abstract

Background. Atrial fibrillation (AF) is a common arrhythmia in elderly patients and is associated with increased risk of mortality. The pathogenesis of AF is complex and based on multiple genetic and environmental factors. Genome-wide association studies identified several loci in AF patients, indicating the complex genetic architecture of this disease. In rare cases, familial forms of AF have been described. Today, pathogenic variants in at least 11 different genes are associated with monogenic AF. Case presentation. The 37-year-old male patient presented to our emergency department with AF. At the age of 35, he had already been diagnosed with paroxysmal AF. Additionally, his 34-year-old brother had also been diagnosed with AF as well as nonobstructive hypertrophic cardiomyopathy. Moreover, the patient’s father was diagnosed with AF in his twenties. Transthoracic echocardiography and cardiac MRI revealed a reduced systolic left ventricular ejection without any signs of hypertrophic cardiomyopathy. Genetic testing identified the heterozygous missense variants c.3371C > T, p.(Pro1124Leu) in RYR2 (NM_001035.3) and c.2524C > A, p.(Pro842Thr) in HCN4 (NM_005477.3) in the patient’s and his brother’s DNA. Discussion. This case of familial AF helps to strengthen the role of RYR2 as a disease gene in the context of AF. Although the variant in RYR2 needs to be classified formally as variant of unknown significance, we regard it as probably disease-causing due to the previously published data. As RYR2 has already been identified as a possible target for prevention and therapy of AF, the knowledge of variants in RYR2 might become even more crucial for individual molecular therapies in the future.

1. Introduction

Atrial fibrillation (AF) is a common arrhythmic disease, affecting an estimate of approximately 33 million patients globally [1]. It is characterized by irregular and often increased heart rate. Arterial hypertension, diabetes mellitus, advancing age, adiposity, and cardiovascular disease are reported amongst predisposing factors for developing AF. Complications of AF include thromboembolic stroke, heart failure, dementia, and increased risk of death [2, 3].

The pathogenesis of AF is influenced by genetic and environmental factors. A previous study has shown familial clustering of patients with lone AF [4], while a study on monozygotic twins suggested a heritability of AF as high as about 60% [5]. Therefore, a strong genetic component could be early assumed. This assumption was confirmed by modern genome-wide association studies (GWAS) which are based on the analysis of single-nucleotide polymorphisms in large patient and control cohorts. One of these studies estimated the heritability of AF in patients of European descent at about 22% [6]. Additionally, following GWAS identified almost 140 different AF loci in participants of predominantly European ancestry [7, 8], emphasizing the complex underlying genetic architecture of this common disease.

While most cases of AF are based on interaction of multiple genetic and environmental factors, familial forms of AF have also been described in rare cases. Today, the Online Mendelian Inheritance in Man (OMIM) database lists 11 different genes in which pathogenic variants have a distinct association with familial AF (https://www.omim.org/, last accessed: 02/23). Most of these genes are coding for ion channels and their associated forms of AF are inherited in an autosomal-dominant manner. Some of these genes are associated with other inborn arrhythmias, like the well-known long QT syndrome (LQTS). The first described variant of familial AF, for example, was caused by variants in KCNQ1. The loss-of-function of KCNQ1 leads to LQTS type 1, while the gain function causes shortening of the atrial refractory period, which in turn increases the risk of developing AF [9]. In this case study, we report two brothers, in which a missense variant in RYR2 might explain early-onset AF combined with hypertrophic cardiomyopathy (HCM) in one of the siblings.

2. Case Presentation

A 37-year-old male patient presented to our emergency department with dyspnea, palpitations, and AF (Figure 1). Paroxysmal AF had already been diagnosed 2 years prior. The patient’s family history was positive for AF. The 34-year-old brother had also been diagnosed with persistent AF as well as HCM (Figure 2). His father was affected by AF with onset in his twenties. There were no further affected family members reported. Transthoracic echocardiography (TTE) of the patient revealed a reduced systolic left ventricular ejection fraction (LVEF) of 40%. Medication for heart rate control and heart failure consisting of bisoprolol, ramipril, spironolactone, and torasemide was started while already taken oral anticoagulation with apixaban was continued. Coronary artery disease was excluded via cardiac catheter examination. Additionally, performed cardiac MRI confirmed the reduced LVEF, however, without any signs of HCM (end-diastolic interventricular septum thickness: 11 mm) despite repolarization abnormalities in the initial resting electrocardiogram (ECG, Figure 1). Eventually, pulmonary vein isolation (PVI) was done, but there was an early relapse after a few days. Since treatment with amiodarone failed to restore sinus rhythm, electrical cardioversion was performed. Asymptomatic AF recurred again, shortly after the executed intervention, and the patient was discharged from our clinic with a long-term amiodarone therapy. A week later, the patient presented to our hospital again because of increasing palpitations and fatigue. The heart rhythm was converted to sinus rhythm by external electrical cardioversion. At 6-month follow-up, the patient reported a reduction of symptoms under amiodarone and heart failure medication. Long-term ECG showed sinus rhythm without any signs of AF. TTE revealed an increase of LVEF to 50%. Diuretic medication (spironolactone, torasemide) and amiodarone were discontinued. At 1.5-year follow-up, the patient was asymptomatic without any signs of AF in resting (Figure 3) and long-term ECG. Oral anticoagulation as well as heart failure medication consisting of bisoprolol and ramipril have been continued until today.

(a)

(b)

Additionally performed DNA analysis by duo exome sequencing identified the heterozygous missense variants c.3371C > T, p.(Pro1124Leu) in RYR2 (NM_001035.3) and c.2524C > A, p.(Pro842Thr) in HCN4 (NM_005477.3) in the patient’s and his brother’s DNA. Testing of the parents for the variants was recommended but declined until today. There are no further siblings for segregation analysis. Since catecholaminergic polymorphic ventricular tachycardia (CPVT) was reported in patients with pathogenic variants in RYR2, an exercise ECG examination was done in the patient and his brother but did not reveal any signs of exercise-triggered arrhythmia.

3. Discussion

RYR2 encodes the cardiac ryanodine receptor 2 (RYR2), an ion channel protein located in the membrane of the sarcoplasmic reticulum (SR). The receptor is fundamental for cardiac muscle contraction by releasing calcium ions from SR to the cytosol and is activated by inward flow of calcium ions via L-type calcium channels in close proximity [10]. Pathogenic variants in RYR2 variants have been associated with different cardiac diseases in the OMIM database, namely the arrhythmogenic right ventricular cardiomyopathy type 2 (ARVC2, OMIM #600996), the catecholaminergic polymorphic ventricular tachycardia type 1 (CPVT1, OMIM #604772), and ventricular arrhythmias due to cardiac ryanodine receptor calcium release deficiency syndrome (VACRDS, OMIM #115000) (last accessed: 02/23). Moreover, variants in RYR2 have been identified in patients with HCM [11] as well as AF [12, 13].

The hereby reported heterozygous missense variant p.(Pro1124Leu) in RYR2 has also already been identified in a patient with HCM. Following functional cell studies of the variant showed that it leads to a cytosolic loss-of-function and a luminal gain-of-function of the RYR2. Knock-in mice carrying the variant demonstrated a mild HCM phenotype with homozygous carriers being more affected than the heterozygous ones. Additionally, an increased susceptibility for cardiac arrhythmia could be detected in these mice. The authors suggested that the observed phenotype was caused by increased expression of calmodulin [14]. The z-score of RYR2 in the Genome Aggregated Database (gnomAD) is 5.78 indicating a high intolerance for missense variants, although it is not an ultra-rare variant since the variant’s minor allele frequency is 0.003% (7 heterozygous carriers, https://gnomad.broadinstitute.org/, last accessed: 02/23). However, the in silico prediction score “Combined Annotation Dependent Depletion” (CADD) for the reported variant is 32 emphasizing its possible disease-causing effect. Furthermore, three other missense variants in RYR2 that were associated with CPVT in humans (p.(Arg2474Ser), p.(Arg2386Ile), p.(Leu433Pro)) have been associated with increased susceptibility for AF in mouse models [15].

Exome sequencing also identified the rare heterozygous missense variant c.2524C > A, p.(Pro824Thr) in HCN4 (NM_005477.3) in both brothers. HCN4 encodes a hyperpolarization-activated cyclic nucleotide-gated ion channel that is expressed in the heart and the brain [16]. HCN4 variants have been associated with sick sinus syndrome type 2 (OMIM #163800) in which AF could be observed [17]. HCN4 has also been identified as a susceptibility locus for AF in a GWAS [18]. Nevertheless, the HCN4 variant found in our patient was not reported before. The variant was therefore classified as variant of unknown significance (VUS).

We cannot exclude a contribution of the variant in HCN4 to the AF, and the variant in RYR2 needs to be classified formally as VUS. Nevertheless, we regard the missense variant c.3371C > T, p.(Pro1124Leu) in RYR2 (NM_001035.3) as most likely disease-causing due to the previously published data. This reported case helps to strengthen the role of RYR2 as a disease gene in context of AF. The knowledge of RYR2 variants in patients with AF might become even more crucial for individual molecular therapies, as the RYR2 has already been identified as possible target of prevention and treatment of AF [19, 20].

Data Availability

The data that support the findings of this study are available from the corresponding author upon reasonable request.

Written informed consent to publish the data and the pictures was obtained from the patient.

Conflicts of Interest

The authors declare that they have no conflicts of interest.

Authors’ Contributions

Drafting the manuscript: BMB, DSW. Obtaining clinical data: all. Critical reviewing the manuscript and final approval: all.

Acknowledgments

We would like to thank the patient for participating in this study.

References

S. S. Chugh, R. Havmoeller, K. Narayanan et al., “Worldwide epidemiology of atrial fibrillation: a Global Burden of Disease 2010 Study,” Circulation, vol. 129, no. 8, pp. 837–847, 2014.
View at: Publisher Site | Google Scholar
R. R. Huxley, F. L. Lopez, A. R. Folsom et al., “Absolute and attributable risks of atrial fibrillation in relation to optimal and borderline risk factors: the Atherosclerosis Risk in Communities (ARIC) study,” Circulation, vol. 123, no. 14, pp. 1501–1508, 2011.
View at: Publisher Site | Google Scholar
C. Magnussen, T. J. Niiranen, F. M. Ojeda et al., “Sex differences and similarities in atrial fibrillation epidemiology, risk factors, and mortality in community cohorts: results from the BiomarCaRE consortium (Biomarker for Cardiovascular Risk Assessment in Europe),” Circulation, vol. 136, no. 17, pp. 1588–1597, 2017.
View at: Publisher Site | Google Scholar
P. T. Ellinor, D. M. Yoerger, J. N. Ruskin, and C. A. MacRae, “Familial aggregation in lone atrial fibrillation,” Human Genetics, vol. 118, no. 2, pp. 179–184, 2005.
View at: Publisher Site | Google Scholar
I. E. Christophersen, L. S. Ravn, E. Budtz-Joergensen et al., “Familial aggregation of atrial fibrillation: a study in Danish twins,” Circulation: Arrhythmia and Electrophysiology, vol. 2, no. 4, pp. 378–383, 2009.
View at: Publisher Site | Google Scholar
L. C. Weng, S. H. Choi, D. Klarin et al., “Heritability of atrial fibrillation,” Circulation: Cardiovascular Genetics, vol. 10, no. 6, p. 3, 2017.
View at: Publisher Site | Google Scholar
J. B. Nielsen, R. B. Thorolfsdottir, L. G. Fritsche et al., “Biobank-driven genomic discovery yields new insight into atrial fibrillation biology,” Nature Genetics, vol. 50, no. 9, pp. 1234–1239, 2018.
View at: Publisher Site | Google Scholar
C. Roselli, M. D. Chaffin, L. C. Weng et al., “Multi-ethnic genome-wide association study for atrial fibrillation,” Nature Genetics, vol. 50, no. 9, pp. 1225–1233, 2018.
View at: Publisher Site | Google Scholar
Y. H. Chen, S. J. Xu, S. Bendahhou et al., “KCNQ1 gain-of-function mutation in familial atrial fibrillation,” Science, vol. 299, no. 5604, pp. 251–254, 2003.
View at: Publisher Site | Google Scholar
R. P. Polonen, K. Penttinen, H. Swan, and K. Aalto-Setala, “Antiarrhythmic effects of carvedilol and flecainide in cardiomyocytes derived from catecholaminergic polymorphic ventricular tachycardia patients,” Stem Cells International, vol. 2018, 2018.
View at: Google Scholar
A. P. Landstrom and M. J. Ackerman, “Beyond the cardiac myofilament: hypertrophic cardiomyopathy-associated mutations in genes that encode calcium-handling proteins,” Current Molecular Medicine, vol. 12, no. 5, pp. 507–518, 2012.
View at: Publisher Site | Google Scholar
A. Di Pino, E. Caruso, L. Costanzo, and P. Guccione, “A novel RyR2 mutation in a 2-year-old baby presenting with atrial fibrillation, atrial flutter, and atrial ectopic tachycardia,” Heart Rhythm, vol. 11, no. 8, pp. 1480–1483, 2014.
View at: Publisher Site | Google Scholar
Y. Zhou, C. Jiang, J. Wang, W. Huang, Y. Zhang, and R. Zhou, “Generation of one human induced pluripotent stem cell line (XACHi004-A) with heterozygous mutation of RYR2 gene from an atrial fibrillation patient,” Stem Cell Research, vol. 65, p. 102955, 2022.
View at: Publisher Site | Google Scholar
F. J. Alvarado, J. M. Bos, Z. Yuchi et al., “Cardiac hypertrophy and arrhythmia in mice induced by a mutation in ryanodine receptor 2,” JCI Insight, vol. 5, no. 7, pp. 2–10, 2019.
View at: Google Scholar
J. Shan, W. Xie, M. Betzenhauser et al., “Calcium leak through ryanodine receptors leads to atrial fibrillation in 3 mouse models of catecholaminergic polymorphic ventricular tachycardia,” Circulation Research, vol. 111, no. 6, pp. 708–717, 2012.
View at: Publisher Site | Google Scholar
G. Campostrini, J. C. DiFrancesco, B. Castellotti et al., “A loss-of-function HCN4 mutation associated with familial benign myoclonic epilepsy in infancy causes increased neuronal excitability,” Frontiers in Molecular Neuroscience, vol. 11, p. 269, 2018.
View at: Publisher Site | Google Scholar
A. Milano, A. M. Vermeer, E. M. Lodder et al., “HCN4 mutations in multiple families with bradycardia and left ventricular noncompaction cardiomyopathy,” Journal of the American College of Cardiology, vol. 64, no. 8, pp. 745–756, 2014.
View at: Publisher Site | Google Scholar
P. T. Ellinor, K. L. Lunetta, C. M. Albert et al., “Meta-analysis identifies six new susceptibility loci for atrial fibrillation,” Nature Genetics, vol. 44, no. 6, pp. 670–675, 2012.
View at: Publisher Site | Google Scholar
M. B. Shoemaker, Z. T. Yoneda, D. M. Crawford et al., “A mechanistic clinical trial using (R)- versus (S)-propafenone to test RyR2 (ryanodine receptor) inhibition for the prevention of atrial fibrillation induction,” Circulation: Arrhythmia and Electrophysiology, vol. 15, no. 10, p. e010713, 2022.
View at: Publisher Site | Google Scholar
A. M. Gillis and D. Dobrev, “Targeting the RyR2 to prevent atrial fibrillation,” Circulation: Arrhythmia and Electrophysiology, vol. 15, no. 10, p. e011514, 2022.
View at: Google Scholar

Copyright

Copyright © 2023 Bernhard M. Boehm et al. This is an open access article distributed under the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.

PDF Download Citation

Download other formats

Order printed copies

Views

936

Downloads

494

Citations