Genome-wide association study of PR interval

Pfeufer, A.; Noord, C. van; Marciante, K.; Arking, D.E.; Larson, M.G.; Smith, A.V.; Tarasov, K.V.; Müller, M.; Sotoodehnia, N.; Sinner, M.F.; Verwoert, G.C.; Li, M.; Kao, W.H.L.; Köttgen, A.; Coresh, J.; Bis, J.C.; Psaty, B.M.; Rice, K.; Rotter, J.I.; Rivadeneira Ramirez, F.; Hofman, A.; Kors, J.A.; Stricker, B.H.Ch.; Uitterlinden, A.G.; Tikka-Kleemola, P.; Beckmann, B.M.; Sauter, W.; Gieger, C.; Lubitz, S.A.; Newton-Cheh, C.; Wang, T.J.; Magnani, J.W.; Schnabel, R.; Chung, M.K.; Barnard, J.; Wagoner, D.R. van; Vasan, R.S.; Aspelund, T.; Eiriksdottir, G.; Harris, T.B.; Launer, L.J.; Najjar, S.S.; Lakatta, E.; Schlessinger, D.; Uda, M.; Abecasis, G.R.; Artto, V.; Ehret, G.B.; Boerwinkle, E.; Chakravarti, A.; Soliman, E.Z.; Lunetta, K.L.; Perz, S.; Wichmann, H.E.; Meitinger, T.; Levy, D.; Gudnason, V.; Ellinor, P.T.; Sanna, S.; Kääb, S.; Witteman, J.C.M.; Alonso, A.; Benjamin, E.J.; Heckbert, S.R.

doi:http://dx.doi.org/10.1038/ng.517

http://hdl.handle.net/1765/28298
http://dx.doi.org/10.1038/ng.517
pubmed: 20062060
scopus: 75749097235

Genome-wide association study of PR interval

Pfeufer, A.

Noord, C. van

Marciante, K.

Arking, D.E.

Larson, M.G.

Smith, A.V.

Tarasov, K.V.

Müller, M.

Sotoodehnia, N.

Sinner, M.F.

Verwoert, G.C.

Li, M.

Kao, W.H.L.

Köttgen, A.

Coresh, J.

Bis, J.C.

Psaty, B.M.

Rice, K.

Rotter, J.I.

Rivadeneira Ramirez, F.

Hofman, A.

Kors, J.A.

Stricker, B.H.Ch.

Uitterlinden, A.G.

Tikka-Kleemola, P.

Beckmann, B.M.

Sauter, W.

Gieger, C.

Lubitz, S.A.

Newton-Cheh, C.

Wang, T.J.

Magnani, J.W.

Schnabel, R.

Chung, M.K.

Barnard, J.

Wagoner, D.R. van

Vasan, R.S.

Aspelund, T.

Eiriksdottir, G.

Harris, T.B.

Launer, L.J.

Najjar, S.S.

Lakatta, E.

Schlessinger, D.

Uda, M.

Abecasis, G.R.

Artto, V.

Ehret, G.B.

Boerwinkle, E.

Chakravarti, A.

Soliman, E.Z.

Lunetta, K.L.

Perz, S.

Wichmann, H.E.

Meitinger, T.

Levy, D.

Gudnason, V.

Ellinor, P.T.

Sanna, S.

Kääb, S.

Witteman, J.C.M.

Alonso, A.

Benjamin, E.J.

Heckbert, S.R.

, et al.

February 2010
Article

Nature Genetics

volume 42, issue 2 pp 153-159.

(Free full text at PubMed)

Internal Medicine

Repository contains one file which is not publicly available

The electrocardiographic PR interval (or PQ interval) reflects atrial and atrioventricular nodal conduction, disturbances of which increase risk of atrial fibrillation. We report a meta-analysis of genome-wide association studies for PR interval from seven population-based European studies in the CHARGE Consortium: AGES, ARIC, CHS, FHS, KORA, Rotterdam Study, and SardiNIA (N = 28,517). We identified nine loci associated with PR interval at P 5 × 10 8. At the 3p22.2 locus, we observed two independent associations in voltage-gated sodium channel genes, SCN10A and SCN5A. Six of the loci were near cardiac developmental genes, including CAV1-CAV2, NKX2-5 (CSX1), SOX5, WNT11, MEIS1, and TBX5-TBX3, providing pathophysiologically interesting candidate genes. Five of the loci, SCN5A, SCN10A, NKX2-5, CAV1-CAV2, and SOX5, were also associated with atrial fibrillation (N = 5,741 cases, P 0.0056). This suggests a role for common variation in ion channel and developmental genes in atrial and atrioventricular conduction as well as in susceptibility to atrial fibrillation.

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