Abstract
Brugada syndrome (BrS) is a hereditary clinical-electrocardiographic arrhythmic entity with low worldwide prevalence. The syndrome is caused by changes in the structure and function of certain cardiac ion channels and reduced expression of Connexin 43 (Cx43) in the Right Ventricle (RV), predominantly in the Right Ventricular Outflow Tract (VSVD), causing electromechanical abnormalities. The diagnosis is based on the presence of spontaneous or medicated ST elevation, characterized by boost of the J point and the ST segment ≥2 mm, of superior convexity "hollow type" (subtype 1A) or descending rectilinear model (subtype 1B). BrS is associated with an increased risk of syncope, palpitations, chest pain, convulsions, difficulty in breathing (nocturnal agonal breathing) and/or Sudden Cardiac Death (SCD) secondary to PVT/VF, unexplained cardiac arrest or documented PVT/VF or Paroxysmal atrial fibrillation (AF) in the absence of apparent macroscopic or structural heart disease, electrolyte disturbance, use of certain medications or coronary heart disease and fever. In less than three decades since the discovery of Brugada syndrome, the concept of Mendelian heredity has come undone. The enormous variants and mutations found mean that we are still far from being able to concretely clarify a genotype-phenotype relationship. There is no doubt that the entity is oligogenetic, associated with environmental factors, and that there are variants of uncertain significance, especially the rare variants of the SCN5A mutation, with European or Japanese ancestors, as well as a spontaneous type 1 or induced pattern, thanks to gnomAD (coalition) researchers who seek to aggregate and harmonize exome and genome sequencing data from a variety of large scale sequencing projects and make summary data available to the scientific community at large). Thus, we believe that this in depth analytical study of the countless mutations attributed to BrS may constitute a real cornerstone that will help to better understand this intriguing syndrome.
Highlights
The Brugada Syndrome (BrS) is a hereditary clinical-electrocardiographic arrhythmic entity with a low prevalence worldwide (0.5 per 1,000 or 5 to 20 per 10,000 individuals), endemic in Southeast Asia
There is no doubt that the entity is oligogenetic associated with environmental factors
What did the researchers do and find? Recent research by the American College of Medical Genetics and Genomics / Association for Molecular Pathology (ACMG/AMP) has shown us that variants of uncertain significance, especially the rare variants of the SCN5A mutation, with European or Japanese ancestors, as well as spontaneous type 1 pattern or induced, thanks to Genome Aggregation Database. What do these findings mean? The enormous variants and mutations found mean that we are still far from being able to concretely clarify a genotype-phenotype relationship. We believe that this in-depth analytical study of the numerous mutations attributed to BrS can constitute a truly cornerstone that will help to better understand this intriguing syndrome
Summary
Andrés Ricardo Pérez-Rieraa , Joseane Elza Tonussi Mendesa, Fabiola Ferreira da Silvaa, Frank Yanowitzb, Luiz Carlos de Abreua, f, g, José Luiz Figueiredoh , Rodrigo Daminello Raimundoa , Raimundo Barbosa-Barrosc , Kjell Nikusd , Pedro Brugadae. Centro Universitário FMABC, Santo André, São Paulo, Brazil. BIntermountain Medical Center, Intermountain Heart Institute, Salt Lake City, UT, United States; The University of Utah, Department of Internal Medicine, Salt Lake City, UT, United States. CCoronary Center of the Hospital de Messejana Dr Carlos Alberto Studart Gomes, Fortaleza, Ceará, Brazil. Federal University of Espírito Santo, ES, Brazil. HDepartment of Surgery, Experimental Surgery Unit, Federal University of Pernambuco, Recife, Pernambuco, Brazil. Manuscript received: December 2020 Manuscript accepted: February 2021 Version of record online: March 2021
Sign-in/Register to view highlights & summary 
Published Version (
Free)
Talk to us
Join us for a 30 min session where you can share your feedback and ask us any queries you have
Schedule a call