Clinical characterization of the first Belgian SCN5A founder mutation cohort

Aims We identified the first Belgian SCN5A founder mutation, c.4813 + 3_4813 + 6dupGGGT. To describe the clinical spectrum and disease severity associated with this mutation, clinical data of 101 SCN5A founder mutation carriers and 46 non-mutation carrying family members from 25 Belgian families were collected. Methods and results The SCN5A founder mutation was confirmed by haplotype analysis. The clinical history and electrocardiographic parameters of the mutation carriers and their family members were gathered and compared. A cardiac electrical abnormality was observed in the majority (82%) of the mutation carriers. Cardiac conduction defects, defined as PR or QRS prolongation on electrocardiogram (ECG), were most frequent, occurring in 65% of the mutation carriers. Brugada syndrome (BrS) was the second most prevalent phenotype identified in 52%, followed by atrial dysrythmia in 11%. Overall, 33% of tested mutation carriers had a normal sodium channel blocker test. Negative tests were more common in family members distantly related to the proband. Overall, 23% of the mutation carriers were symptomatic, with 8% displaying major adverse events. As many as 13% of the patients tested with a sodium blocker developed ventricular arrhythmia. One family member who did not carry the founder mutation was diagnosed with BrS. Conclusion The high prevalence of symptoms and sensitivity to sodium channel blockers in our founder population highlights the adverse effect of the founder mutation on cardiac conduction. The large phenotypical heterogeneity, variable penetrance, and even non-segregation suggest that other genetic (and environmental) factors modify the disease expression, severity, and outcome in these families.

Language

English

Source (journal)

Europace. - Oxford

Publication

Oxford : 2021

ISSN

1099-5129

DOI

10.1093/EUROPACE/EUAA305

Volume/pages

23 :6 (2021) , p. 918-927

Article Reference

euaa305

ISI

000693738700014

Pubmed ID

33221854

Medium

E-only publicatie

Full text (Publisher's DOI)

https://doi.org/10.1093/EUROPACE/EUAA305

Full text (open access)

https://repository.uantwerpen.be/docstore/d:irua:4773

Full text (publisher's version - intranet only)

https://repository.uantwerpen.be/docstore/d:iruaintra:2937

Faculty/Department				Faculty of Medicine and Health Sciences Faculty of Pharmaceutical, Biomedical and Veterinary Sciences . Biomedical Sciences

Research group				Cardiovascular diseases (CARDIOVASC) Experimental Neurobiology Unit (ENU)
Project info				Towards a better understanding of the molecular mechanisms underlying thoracic aortic aneurysms and dissections. Development of a functional assay to determine the pathogenicity of genetic variants with unknown significance identified in patients with cardiac arrhythmia. Genomic Modifiers of Inherited Aortapathy (Genomia). Infla-Med: Fundamental and translational research into targets for the treatment of inflammatory diseases. Inherited cardiac arrhythmias: identification of novel genes and development of a new diagnostic tool for translating genetic diagnosis into precision medicine.
Publication type				A1 Journal article

Subject				Biology Human medicine

Affiliation				Publications with a UAntwerp address

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Identifier

Creation

16.02.2021

Last edited

10.11.2024

To cite this reference

https://hdl.handle.net/10067/1754240151162165141