Brugada Syndrome--an Under-recognized Electrical Disease in Patients with Sudden Cardiac Death

Overview

Journal Cardiology

Specialty Cardiology & Vascular Diseases

Date 2004 Feb 18

PMID 14967959

Citations 17

Authors

Jyh-Ming Juang

Shoei K Stephen Huang

Affiliations

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Abstract

In 1992, Brugada and Brugada described 8 patients with a history of aborted sudden death and a distinct ECG pattern of right bundle-branch block with ST segment elevation in leads V1-V3 and normal QT interval in the absence of any structural heart disease. It is called Brugada syndrome now and is believed to be responsible for 4-12% of all sudden deaths and around 20% of deaths in patients with structurally normal hearts. Although this syndrome is observed worldwide and the exact prevalence is unknown, it is more common in the Southeast Asian countries. Repeated syncope, ventricular fibrillation, and sudden cardiac death have been reported in patients with Brugada syndrome. The clinical presentation of Brugada syndrome is distinguished by a male predominance and the appearance of arrhythmic events at an average age of 40 years. The Brugada syndrome is inherited in an autosomal dominant manner with incomplete penetrance and an incidence ranging between 5 and 66 per 10,000. The surface ECG manifestations of the syndrome can transiently disappear, but can be unmasked by potent sodium channel blockers in some cases. Mutations of the cardiac sodium channel SCN5A have been detectable in <20% of patients with Brugada syndrome. Recent genetic studies have confirmed the genetic heterogeneity of the disorder. Antiarrhythmic drugs appear to be of little use in prolonging survival and in preventing recurrences of ventricular arrhythmias. To date, implantable cardioverter defibrillator remains the best therapy to prevent sudden death in these patients.

Citing Articles

Brugada syndrome update.

Xu T, Wang S, Wang J, Xing J Front Physiol. 2025; 15:1520008.

PMID: 39896197 PMC: 11782167. DOI: 10.3389/fphys.2024.1520008.

Sudden Cardiac Death and Channelopathies: What Lies behind the Clinical Significance of Rare Splice-Site Alterations in the Genes Involved?.

Pesaresi M, Bernini Di Michele A, Melchionda F, Onofri V, Alessandrini F, Turchi C Genes (Basel). 2024; 15(10).

PMID: 39457396 PMC: 11507433. DOI: 10.3390/genes15101272.

Brugada Syndrome: From Molecular Mechanisms and Genetics to Risk Stratification.

Popa I, Serban D, Maranduca M, Serban I, Tamba B, Tudorancea I Int J Mol Sci. 2023; 24(4).

PMID: 36834739 PMC: 9967917. DOI: 10.3390/ijms24043328.

The SCN5A Gene Is a Predictor of Phenotype Severity in Brugada Syndrome: A Comprehensive Literature Review.

Deica A, Paduraru L, Paduraru D, Andronic O Med Princ Pract. 2022; 32(1):1-8.

PMID: 36446338 PMC: 10267483. DOI: 10.1159/000528375.

Diagnostic yield and variant reassessment in the genes encoding Nav1.5 channel in Russian patients with Brugada syndrome.

Zaklyazminskaya E, Shestak A, Podolyak D, Komoliatova V, Makarov L, Novitskaya A Front Pharmacol. 2022; 13:984299.

PMID: 36091819 PMC: 9449364. DOI: 10.3389/fphar.2022.984299.