Genetic association study of QT interval highlights role for calcium signaling pathways in myocardial repolarization.
Arking DE., Pulit SL., Crotti L., van der Harst P., Munroe PB., Koopmann TT., Sotoodehnia N., Rossin EJ., Morley M., Wang X., Johnson AD., Lundby A., Gudbjartsson DF., Noseworthy PA., Eijgelsheim M., Bradford Y., Tarasov KV., Dörr M., Müller-Nurasyid M., Lahtinen AM., Nolte IM., Smith AV., Bis JC., Isaacs A., Newhouse SJ., Evans DS., Post WS., Waggott D., Lyytikäinen L-P., Hicks AA., Eisele L., Ellinghaus D., Hayward C., Navarro P., Ulivi S., Tanaka T., Tester DJ., Chatel S., Gustafsson S., Kumari M., Morris RW., Naluai ÅT., Padmanabhan S., Kluttig A., Strohmer B., Panayiotou AG., Torres M., Knoflach M., Hubacek JA., Slowikowski K., Raychaudhuri S., Kumar RD., Harris TB., Launer LJ., Shuldiner AR., Alonso A., Bader JS., Ehret G., Huang H., Kao WHL., Strait JB., Macfarlane PW., Brown M., Caulfield MJ., Samani NJ., Kronenberg F., Willeit J., CARe Consortium None., COGENT Consortium None., Smith JG., Greiser KH., Meyer Zu Schwabedissen H., Werdan K., Carella M., Zelante L., Heckbert SR., Psaty BM., Rotter JI., Kolcic I., Polašek O., Wright AF., Griffin M., Daly MJ., DCCT/EDIC None., Arnar DO., Hólm H., Thorsteinsdottir U., eMERGE Consortium None., Denny JC., Roden DM., Zuvich RL., Emilsson V., Plump AS., Larson MG., O'Donnell CJ., Yin X., Bobbo M., D'Adamo AP., Iorio A., Sinagra G., Carracedo A., Cummings SR., Nalls MA., Jula A., Kontula KK., Marjamaa A., Oikarinen L., Perola M., Porthan K., Erbel R., Hoffmann P., Jöckel K-H., Kälsch H., Nöthen MM., HRGEN Consortium None., den Hoed M., Loos RJF., Thelle DS., Gieger C., Meitinger T., Perz S., Peters A., Prucha H., Sinner MF., Waldenberger M., de Boer RA., Franke L., van der Vleuten PA., Beckmann BM., Martens E., Bardai A., Hofman N., Wilde AAM., Behr ER., Dalageorgou C., Giudicessi JR., Medeiros-Domingo A., Barc J., Kyndt F., Probst V., Ghidoni A., Insolia R., Hamilton RM., Scherer SW., Brandimarto J., Margulies K., Moravec CE., del Greco M F., Fuchsberger C., O'Connell JR., Lee WK., Watt GCM., Campbell H., Wild SH., El Mokhtari NE., Frey N., Asselbergs FW., Mateo Leach I., Navis G., van den Berg MP., van Veldhuisen DJ., Kellis M., Krijthe BP., Franco OH., Hofman A., Kors JA., Uitterlinden AG., Witteman JCM., Kedenko L., Lamina C., Oostra BA., Abecasis GR., Lakatta EG., Mulas A., Orrú M., Schlessinger D., Uda M., Markus MRP., Völker U., Snieder H., Spector TD., Ärnlöv J., Lind L., Sundström J., Syvänen A-C., Kivimaki M., Kähönen M., Mononen N., Raitakari OT., Viikari JS., Adamkova V., Kiechl S., Brion M., Nicolaides AN., Paulweber B., Haerting J., Dominiczak AF., Nyberg F., Whincup PH., Hingorani AD., Schott J-J., Bezzina CR., Ingelsson E., Ferrucci L., Gasparini P., Wilson JF., Rudan I., Franke A., Mühleisen TW., Pramstaller PP., Lehtimäki TJ., Paterson AD., Parsa A., Liu Y., van Duijn CM., Siscovick DS., Gudnason V., Jamshidi Y., Salomaa V., Felix SB., Sanna S., Ritchie MD., Stricker BH., Stefansson K., Boyer LA., Cappola TP., Olsen JV., Lage K., Schwartz PJ., Kääb S., Chakravarti A., Ackerman MJ., Pfeufer A., de Bakker PIW., Newton-Cheh C.
The QT interval, an electrocardiographic measure reflecting myocardial repolarization, is a heritable trait. QT prolongation is a risk factor for ventricular arrhythmias and sudden cardiac death (SCD) and could indicate the presence of the potentially lethal mendelian long-QT syndrome (LQTS). Using a genome-wide association and replication study in up to 100,000 individuals, we identified 35 common variant loci associated with QT interval that collectively explain ∼8-10% of QT-interval variation and highlight the importance of calcium regulation in myocardial repolarization. Rare variant analysis of 6 new QT interval-associated loci in 298 unrelated probands with LQTS identified coding variants not found in controls but of uncertain causality and therefore requiring validation. Several newly identified loci encode proteins that physically interact with other recognized repolarization proteins. Our integration of common variant association, expression and orthogonal protein-protein interaction screens provides new insights into cardiac electrophysiology and identifies new candidate genes for ventricular arrhythmias, LQTS and SCD.