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(Circulation Research. 2005;96:693.)
© 2005 American Heart Association, Inc.

Clinical Research

Common Variants in Myocardial Ion Channel Genes Modify the QT Interval in the General Population

Results From the KORA Study

Arne Pfeufer, Shapour Jalilzadeh, Siegfried Perz, Jakob C. Mueller, Martin Hinterseer, Thomas Illig, Mahmut Akyol, Cornelia Huth, Andreas Schöpfer-Wendels, Bernhard Kuch, Gerhard Steinbeck, Rolf Holle, Michael Näbauer, H. -Erich Wichmann, Thomas Meitinger, Stefan Kääb

From the Institute of Human Genetics (A.P., S.J., M.A., T.M.), Technical University Munich, Munich; Institutes of Human Genetics (A.P., S.J., J.C.M., M.A., T.M.), Medical Informatics (S.P.), Epidemiology (T.I., C.H., A.S.-W., H.-E.W.), and Health Economics and Health Care Management (R.H.), GSF National Research Center, Neuherberg; Department of Medicine I, Klinikum Grosshadern (M.H., G.S., M.N., S.K.), and Institute of Epidemiology (C.H., H.-E.W.), University of Munich, Munich; Zentralklinikum Augsburg (B.K.), Department of Medicine I, Augsburg, Germany.

Correspondence to Stefan Kääb, MD, LMU-University, Klinikum Grosshadern, Department of Medicine I, Marchioninistr. 15, D-81366 Munich, Germany. E-mail stefan.kaab{at}med.uni-muenchen.de

Altered myocardial repolarization is one of the important substrates of ventricular tachycardia and fibrillation. The influence of rare gene variants on repolarization is evident in familial long QT syndrome. To investigate the influence of common gene variants on the QT interval we performed a linkage disequilibrium based SNP association study of four candidate genes. Using a two-step design we analyzed 174 SNPs from the KCNQ1, KCNH2, KCNE1, and KCNE2 genes in 689 individuals from the population-based KORA study and 14 SNPs with results suggestive of association in a confirmatory sample of 3277 individuals from the same survey. We detected association to a gene variant in intron 1 of the KCNQ1 gene (rs757092, +1.7 ms/allele, P=0.0002) and observed weaker association to a variant upstream of the KCNE1 gene (rs727957, +1.2 ms/allele, P=0.0051). In addition we detected association to two SNPs in the KCNH2 gene, the previously described K897T variant (rs1805123, –1.9 ms/allele, P=0.0006) and a gene variant that tags a different haplotype in the same block (rs3815459, +1.7 ms/allele, P=0.0004). The analysis of additive effects by an allelic score explained a 10.5 ms difference in corrected QT interval length between extreme score groups and 0.95% of trait variance (P<0.00005). These results confirm previous heritability studies indicating that repolarization is a complex trait with a significant heritable component and demonstrate that high-resolution SNP-mapping in large population samples can detect and fine map quantitative trait loci even if locus specific heritabilities are small.

Key Words: arrhythmia • cardiovascular genomics • ECG • quantitative trait locus • multiple locus association study

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