Cardiac channelopathies: The role of sodium channel mutations

Abstract

Abstract Introduction and objectives The importance of sodium channels for the normal electrical activity of the heart is emphasized by the fact that mutations (inherited or de novo) in genes that encode for these channels or their associated proteins cause arrhythmogenic syndromes such as the Brugada syndrome and the long QT syndrome (LQTS). The aim of this study is to conduct a review of the literature on the mutations in the sodium channel complex responsible for heart disease and the implications of a close relationship between genetics and the clinical aspects of the main cardiac channelopathies, namely at the level of diagnosis, risk stratification, prognosis, screening of family members and treatment. Methods The online Pubmed® database was used to search for articles published in this field in indexed journals. The MeSH database was used to define the following query: “Mutation [Mesh] AND Sodium Channels [Mesh] AND Heart Diseases [Mesh]”, and articles published in the last 15 years, written in English or Portuguese and referring to research in human beings were included. Conclusions In the past few years, significant advances have been made to clarify the genetic and molecular basis of these syndromes. A greater understanding of the underlying pathophysiological mechanisms showed the importance of the relationship between genotype and phenotype and led to progress in the clinical approach to these patients. However, it is still necessary to improve diagnostic capacity, optimize risk stratification, and develop new specific treatments according to the genotype-phenotype binomial.