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HERO ID
514274
Reference Type
Journal Article
Title
Cardiac sodium channel overlap syndromes: Different faces of SCN5A mutations
Author(s)
Remme, CA; Wilde, AAM; Bezzina, CR
Year
2008
Is Peer Reviewed?
1
Journal
Trends in Cardiovascular Medicine
ISSN:
1050-1738
EISSN:
1873-2615
Volume
18
Issue
3
Page Numbers
78-87
Language
English
Abstract
Cardiac sodium channel dysfunction caused by mutations in the SCN5A gene is associated with a number of relatively uncommon arrhythmia syndromes, including long-QT syndrome type 3 (LQT3), Brugada syndrome, conduction disease, sinus node dysfunction, and atrial standstill, which potentially lead to fatal arrhythmias in relatively young individuals. Although these various arrhythmia syndromes were originally considered separate entities, recent evidence indicates more overlap in clinical presentation and biophysical defects of associated mutant channels than previously appreciated. Various SCN5A mutations are now known to present with mixed phenotypes, a presentation that has become known as overlap syndrome of cardiac sodium channelopathy.(a) over cap In many cases, multiple biophysical defects of single SCN5A mutations are suspected to underlie the overlapping clinical manifestations. Here, we provide an overview of current knowledge on SCN5A mutations associated with sodium channel overlap syndromes and discuss a possible role for modifiers in determining disease expressivity the individual patient.
Keywords
long-qt syndrome; conduction system disease; st-segment elevation; sick; sinus syndrome; brugada-syndrome; na+ channel; molecular-mechanism; risk stratification; atrial standstill; missense mutation
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