Spectrum of genetic variants and yield of genetic testing in Slovenian probands with suspected cardiomyopathies surviving sudden cardiac arrest

Spectrum of genetic variants and yield of genetic testing in Slovenian probands with suspected cardiomyopathies surviving sudden cardiac arrest

Abstract Background Cardiomyopathies (CMs) present phenotypically on a spectrum and in a proportion of patients the initial presentation is sudden cardiac arrest (SCA). Studies performing genetic screening of SCA survivors have identified (likely) pathogenic (LP/P) variants in 2–50% of probands, wit...

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Bibliographic Details
Main Authors: Nina Vodnjov, Aleš Maver, Borut Petelin, Karin Writzl
Format: Article
Language:English
Published: SpringerOpen 2025-06-01
Series:Egyptian Journal of Forensic Sciences
Subjects:
Sudden cardiac arrest
Genetic testing
Molecular pathology
(likely) pathogenic variants
Hereditary cardiomyopathy
Online Access:https://doi.org/10.1186/s41935-025-00461-1
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Summary:Abstract Background Cardiomyopathies (CMs) present phenotypically on a spectrum and in a proportion of patients the initial presentation is sudden cardiac arrest (SCA). Studies performing genetic screening of SCA survivors have identified (likely) pathogenic (LP/P) variants in 2–50% of probands, with mean cohort ages ranging from 28 to 64 years. Due to inconsistent data in the literature, our study aimed to genetically characterise Slovenian SCA survivors with clinically confirmed/suspected cardiomyopathy (CM). The present study included 29 probands (17 women, 59%) with clinically confirmed/suspected CM who survived SCA and were referred to the Clinical Institute of Genomic Medicine for genetic testing between January 2010 and July 2024. The majority of probands (23; 79%) underwent whole exome sequencing, and the remainder either clinical exome (5; 17%) or panel sequencing (1; 4%). Genetic data were analysed following ACMG/AMP guidelines and ACGS recommendations. Results Probands survived SCA at a mean age of 49 ± 17 years (range 15–71), and 12 (41%) were < 50 years old. The majority had clinically confirmed/suspected arrhythmogenic (10; 34.5%) or dilated (9; 31.0%) CM, while the remainder had clinically undefined (5; 17.2%), hypertrophic (4; 13.8%), or non-compaction (1; 3.4%) CM. Seven LP/P variants in CM-related genes were identified in eight (28.6%) probands. In addition, 16 variants of uncertain significance (VUS) were identified in 12 (41.3%) probands. Probands’ age at SCA did not significantly affect the yield, as LP/P variants were identified in four probands < 50 years at SCA and in four > 50 years (p = 0.56), nor did the positive family history of heart disease (p = 0.55) or sudden cardiac death (p = 0.43). There were also no significant differences in probands' age and test outcome, as the mean age of patients with LP/P variants was 46 ± 21 years, those with the VUS(s) were 45 ± 15 years, and those without candidate variant(s) were 55 ± 12 years (p = 0.41). Conclusions LP/P variants were identified in almost one-third of Slovenian SCA survivors with clinically confirmed/suspected CM. Genetic testing of SCA survivors with structural clinical findings provides additional confirmation of the clinical diagnosis and a basis for identifying relatives at risk of heart disease, allowing for better management.
ISSN:2090-5939

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