Novel genes for QTc interval. How much heritability is explained, and how much is left to find?

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作者
Yalda Jamshidi
Ilja M Nolte
Timothy D Spector
Harold Snieder
机构
[1] St George's University of London,Division of Clinical Developmental Sciences
[2] King's College London,Department of Twin Research and Genetic Epidemiology Unit, St Thomas' Campus
[3] St Thomas' Hospital,Unit of Genetic Epidemiology and Bioinformatics, Department of Epidemiology, University Medical Center Groningen
[4] University of Groningen,undefined
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Celiac Disease; Risk Allele; Genetic Risk Score; Modest Effect Size; Congenital LQTS;
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摘要
The corrected QT (QTc) interval is a complex quantitative trait, believed to be influenced by several genetic and environmental factors. It is a strong prognostic indicator of cardiovascular mortality in patients with and without cardiac disease. More than 700 mutations have been described in 12 genes (LQT1-LQT12) involved in congenital long QT syndrome. However, the heritability (genetic contribution) of QTc interval in the general population cannot be adequately explained by these long QT syndrome genes. In order to further investigate the genetic architecture underlying QTc interval in the general population, genome-wide association studies, in which up to one million single nucleotide polymorphisms are assayed in thousands of individuals, are now being employed and have already led to the discovery of variants in seven novel loci and five loci that are known to cause congenital long or short QT syndrome. Here we show that a combined risk score using 11 of these loci explains about 10% of the heritability of QTc. Additional discovery of both common and rare variants will yield further etiological insight and accelerate clinical applications.
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