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A common polymorphism of the human cardiac sodium channel alpha subunit (SCN5A) gene is associated with sudden cardiac death in chronic ischemic heart disease
Authors
A Carè
AF Baas
+47 more
AJ Aarnoudse
AM Kulminski
AV Treuer
BB Kelly
Boglárka Marcsa
CM Albert
CR Bezzina
CW Israel
D Miller
Dan E. Arking
E Kotyuk
EC Klaver
Gergely Keszler
Gergely Rácz
GI Fishman
H Morita
J Arakawa
JK Park
K Lakatos
K Maekawa
Klára Törő
Krisztina Vörös
LM Blayney
M Petersen
MC Gavin
MJ Cutler
MK Son
ML Becker
Mária Sasvári-Székely
N Earle
P Flevari
P Francia
P Han
P Yang
Réka Dénes
S Nakajima
T Boehringer
T Schwark
TM Kolettis
Y Imamichi
Y Jamshidi
Y Ran
Y Zhang
YM Choi
Z Zeng
ZH Tseng
Zsolt Rónai
Publication date
1 January 2015
Publisher
'Public Library of Science (PLoS)'
Doi
View
on
PubMed
Abstract
Cardiac death remains one of the leading causes of mortality worldwide. Recent research has shed light on pathophysiological mechanisms underlying cardiac death, and several genetic variants in novel candidate genes have been identified as risk factors. However, the vast majority of studies performed so far investigated genetic associations with specific forms of cardiac death only (sudden, arrhythmogenic, ischemic etc.). The aim of the present investigation was to find a genetic marker that can be used as a general, powerful predictor of cardiac death risk. To this end, a case-control association study was performed on a heterogeneous cohort of cardiac death victims (n=360) and age-matched controls (n=300). Five single nucleotide polymorphisms (SNPs) from five candidate genes (beta2 adrenergic receptor, nitric oxide synthase 1 adaptor protein, ryanodine receptor 2, sodium channel type V alpha subunit and transforming growth factor-beta receptor 2) that had previously been shown to associate with certain forms of cardiac death were genotyped using sequence-specific real-time PCR probes. Logistic regression analysis revealed that the CC genotype of the rs11720524 polymorphism in the SCN5A gene encoding a subunit of the cardiac voltage-gated sodium channel occurred more frequently in the highly heterogeneous cardiac death cohort compared to the control population (p=0.019, odds ratio: 1.351). A detailed subgroup analysis uncovered that this effect was due to an association of this variant with cardiac death in chronic ischemic heart disease (p=0.012, odds ratio =1.455). None of the other investigated polymorphisms showed association with cardiac death in this context. In conclusion, our results shed light on the role of this non-coding polymorphism in cardiac death in ischemic cardiomyopathy. Functional studies are needed to explore the pathophysiological background of this association. © 2015 Marcsa et al. This is an open access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited
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