Molecular-genetic profile in patients with cardiomyopathy in Bulgaria

P. Angelova; N. Stoyanov; V. Velchev; S. Atemin; M. Sleptsova; T. Todorov; D. Gencheva; M. Gospodinova; D. Pechilkov; A Dasheva; T. Tchamova; A. Taneva; I. Tournev; V. Mitev; A. Todorova

doi:10.3897/bgcardio.30.e127156

Българска кардиология (Sep 2024)

Molecular-genetic profile in patients with cardiomyopathy in Bulgaria

P. Angelova,
N. Stoyanov,
V. Velchev,
S. Atemin,
M. Sleptsova,
T. Todorov,
D. Gencheva,
M. Gospodinova,
D. Pechilkov,
A Dasheva,
T. Tchamova,
A. Taneva,
I. Tournev,
V. Mitev,
A. Todorova

Affiliations

P. Angelova: Medical University of Sofia
N. Stoyanov: UMHAT "Sveta Anna"
V. Velchev: UMHAT "Sveta Anna"
S. Atemin: Genetic laboratory "Genika"
M. Sleptsova: Genetic laboratory "Genika"
T. Todorov: Genetic laboratory "Genika"
D. Gencheva: UMHAT Sv. Georgi
M. Gospodinova: UMHAT Sv. Ivan Rilski
D. Pechilkov: National Heart Hospital
A Dasheva: Specialised Hospital for Active Treatment of Children's Diseases “Prof. Ivan Mitev”
T. Tchamova: UMHAT “Alexandrovska”
A. Taneva: UMHAT “Alexandrovska”
I. Tournev: Medical University of Sofia
V. Mitev: Medical University of Sofia
A. Todorova: Medical University of Sofia

DOI: https://doi.org/10.3897/bgcardio.30.e127156
Journal volume & issue: Vol. 30, no. 2
pp. 83 – 105

Abstract

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Introduction: Cardiomyopathies are a clinically and genetically heterogeneous group of diseases, that are associated with significant morbidity and mortality. The aim of the present study is to clarify the molecular-genetic characteristics of cardiomyopathies in patients in Bulgaria. Material and methods: In the present study, targeted analysis of an expanded panel of 242 genes, associated with cardiomyopathy, and an additional panel of 20 genes, associated with hereditary amyloidosis, was performed in a total of 20 Bulgarian patients, diagnosed with cardiomyopathy, as follows: 12 patients with hypertrophic cardiomyopathy (HCM), including 1 pediatric patient, 6 patients with dilated cardiomyopathy (DCM), of whom 2 pediatric patients, and 2 patients with restrictive cardiomyopathy (RCM). Family segregation analyses were performed by direct Sanger sequencing. Results: Genetic findings were present in 90% of the patients. Pathogenic/likely pathogenic variants were found in 12 of the patients (60%), while genetic findings related to the clinical symptoms were not detected in the RCM patients (10%). Approximately 1/3 of the patients had a family history of sudden cardiac death or cardiomyopathy. Pathogenic/likely pathogenic variants were found in 55% of HCM patients with no family history, in ~67% of HCM patients with family history or with sporadic DCM, and in 100% of DCM patients with a positive family history. A respectively 2,5 and 4-fold higher frequency of truncating variants was found in the study group compared to the reports of around 10% in the literature, both in patients with HCM, and in patients with DCM. Pathogenic/likely pathogenic variants in the MYBPC3 gene (71%) were found with the highest frequency in HCM, while DCM is characterized by a diverse genetic profile, and genetic findings in the NDUFB11 and TAZ genes were associated with severe clinical presentation in pediatric patients in the first postnatal days. Results of segregation analyses were reported in 6 of the affected families. Conclusion: The data from the present study supports the importance of conducted genetic testing and medical-genetic counseling in patients and affected families with cardiomyopathy in Bulgaria

Published in Българска кардиология

ISSN: 1310-7488 (Print); 2683-1015 (Online)
Publisher: Pensoft Publishers
Country of publisher: Bulgaria
LCC subjects: Medicine: Internal medicine: Specialties of internal medicine: Diseases of the circulatory (Cardiovascular) system
Website: https://journal.bgcardio.org/

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