Note to users. If you're seeing this message, it means that your browser cannot find this page's style/presentation instructions -- or possibly that you are using a browser that does not support current Web standards. Find out more about why this message is appearing, and what you can do to make your experience of our site the best it can be.
A Common Variant on Chromosome 9p21 Affects the Risk of Myocardial Infarction
Anna Helgadottir,1*Gudmar Thorleifsson,1*Andrei Manolescu,1*Solveig Gretarsdottir,1Thorarinn Blondal,1Aslaug Jonasdottir,1Adalbjorg Jonasdottir,1Asgeir Sigurdsson,1Adam Baker,1Arnar Palsson,1Gisli Masson,1Daniel F. Gudbjartsson,1Kristinn P. Magnusson,1Karl Andersen,2Allan I. Levey,3Valgerdur M. Backman,1Sigurborg Matthiasdottir,1Thorbjorg Jonsdottir,1Stefan Palsson,1Helga Einarsdottir,1Steinunn Gunnarsdottir,1Arnaldur Gylfason,1Viola Vaccarino,3W. Craig Hooper,3Muredach P. Reilly,4Christopher B. Granger,5Harland Austin,3Daniel J. Rader,4Svati H. Shah,5Arshed A. Quyyumi,3Jeffrey R. Gulcher,1Gudmundur Thorgeirsson,2Unnur Thorsteinsdottir,1Augustine Kong,1Kari Stefansson1
The global endemic of cardiovascular diseases calls for improvedrisk assessment and treatment. Here, we describe an associationbetween myocardial infarction (MI) and a common sequence varianton chromosome 9p21. This study included a total of 4587 casesand 12,767 controls. The identified variant, adjacent to thetumor suppressor genes CDKN2A and CDKN2B, was associated withthe disease with high significance. Approximately 21% of individualsin the population are homozygous for this variant, and theirestimated risk of suffering myocardial infarction is 1.64 timesas great as that of noncarriers. The corresponding risk is 2.02times as great for early-onset cases. The population attributablerisk is 21% for MI in general and 31% for early-onset cases.
1 deCODE genetics, Sturlugata 8, IS-101 Reykjavik, Iceland. 2 Landspitali University Hospital, Reykjavik, Iceland. 3 Emory University School of Medicine, Atlanta, GA 30322, USA. 4 University of Pennsylvania School of Medicine, Philadelphia, PA 19104, USA. 5 Duke University School of Medicine, Durham, NC 27710, USA.
* These authors contributed equally to this work.
To whom correspondence should be addressed. E-mail: augustine.kong{at}decode.is (A.K.); kstefans{at}decode.is (K.S.)
The editors suggest the following Related Resources on Science sites:
In Science Magazine
LETTERS
Erik Rifkin, Edward Bouwer;, Kari Stefansson, and Augustine Kong (7 September 2007) Science317 (5843), 1322b.
[DOI: 10.1126/science.317.5843.1322b] |Full Text »|PDF »
THIS ARTICLE HAS BEEN CITED BY OTHER ARTICLES:
Susceptibility locus for clinical and subclinical coronary artery disease at chromosome 9p21 in the multi-ethnic ADVANCE study.
T. L. Assimes, J. W. Knowles, A. Basu, C. Iribarren, A. Southwick, H. Tang, D. Absher, J. Li, J. M. Fair, G. D. Rubin, et al. (2008)
Hum. Mol. Genet.
17, 2320-2328
|Abstract »|Full Text »|PDF »
Association of Genetic Variation on Chromosome 9p21 With Susceptibility and Progression of Atherosclerosis: A Population-Based, Prospective Study.
S. Ye, J. Willeit, F. Kronenberg, Q. Xu, and S. Kiechl (2008)
J. Am. Coll. Cardiol.
52, 378-384
|Abstract »|Full Text »|PDF »
Gaining Insights in Coronary Disease Genomics.
S. S. Murray and E. J. Topol (2008)
J. Am. Coll. Cardiol.
52, 385-386
|Full Text »|PDF »
Genomics in cardiac metabolism.
J.-L. Samuel, M. C. Schaub, M. Zaugg, M. Mamas, W. B. Dunn, and B. Swynghedauw (2008)
Cardiovasc Res
79, 218-227
|Abstract »|Full Text »|PDF »
Application of Metabolomics to Cardiovascular Biomarker and Pathway Discovery.
G. D. Lewis, A. Asnani, and R. E. Gerszten (2008)
J. Am. Coll. Cardiol.
52, 117-123
|Abstract »|Full Text »|PDF »
Replication study of 10 genetic polymorphisms associated with coronary heart disease in a specific high-risk population with familial hypercholesterolemia.
J. B. van der Net, D. M. Oosterveer, J. Versmissen, J. C. Defesche, M. Yazdanpanah, B. E. Aouizerat, E. W. Steyerberg, M. J. Malloy, C. R. Pullinger, J. J.P. Kastelein, et al. (2008)
Eur. Heart J.
|Abstract »|Full Text »|PDF »
Approaches for Unraveling the Joint Genetic Determinants of Schizophrenia and Bipolar Disorder.
Comprehensive genetic analysis of the platelet activating factor acetylhydrolase (PLA2G7) gene and cardiovascular disease in case-control and family datasets.
B. S. Sutton, D. R. Crosslin, S. H. Shah, S. C. Nelson, A. Bassil, A. B. Hale, C. Haynes, P. J. Goldschmidt-Clermont, J. M. Vance, D. Seo, et al. (2008)
Hum. Mol. Genet.
17, 1318-1328
|Abstract »|Full Text »|PDF »
Whole Genome Analyses Suggest Ischemic Stroke and Heart Disease Share an Association With Polymorphisms on Chromosome 9p21.
M. Matarin, W. M. Brown, A. Singleton, J. A. Hardy, J. F. Meschia, and for the ISGS investigators (2008)
Stroke
39, 1586-1589
|Abstract »|Full Text »|PDF »
Angiotensin II Type 1 Receptor 1166C Polymorphism Is Associated With Abdominal Aortic Aneurysm in Three Independent Cohorts.
G. T. Jones, A. R. Thompson, F. M. van Bockxmeer, H. Hafez, J. A. Cooper, J. Golledge, S. E. Humphries, P. E. Norman, and A. M. van Rij (2008)
Arterioscler. Thromb. Vasc. Biol.
28, 764-770
|Abstract »|Full Text »|PDF »
Where Do We Go for Atherothrombotic Disease Genetics?.
S.-M. Brand-Herrmann (2008)
Stroke
39, 1070-1075
|Full Text »|PDF »
Repeated Replication and a Prospective Meta-Analysis of the Association Between Chromosome 9p21.3 and Coronary Artery Disease.
H. Schunkert, A. Gotz, P. Braund, R. McGinnis, D.-A. Tregouet, M. Mangino, P. Linsel-Nitschke, F. Cambien, C. Hengstenberg, K. Stark, et al. (2008)
Circulation
117, 1675-1684
|Abstract »|Full Text »|PDF »
Polymorphisms Associated with Cholesterol and Risk of Cardiovascular Events.
S. Kathiresan, O. Melander, D. Anevski, C. Guiducci, N. P. Burtt, C. Roos, J. N. Hirschhorn, G. Berglund, B. Hedblad, L. Groop, et al. (2008)
N. Engl. J. Med.
358, 1240-1249
|Abstract »|Full Text »|PDF »
Susceptibility to coronary artery disease and diabetes is encoded by distinct, tightly linked SNPs in the ANRIL locus on chromosome 9p.
H. M. Broadbent, J. F. Peden, S. Lorkowski, A. Goel, H. Ongen, F. Green, R. Clarke, R. Collins, M. G. Franzosi, G. Tognoni, et al. (2008)
Hum. Mol. Genet.
17, 806-814
|Abstract »|Full Text »|PDF »
Can Fishing for New Genes Catch Patients at Risk of Coronary Artery Disease?.
J. Emmerich and P. M Ridker (2008)
Clin. Chem.
54, 453-455
|Full Text »|PDF »
Chromosome 9p21.3 Coronary Heart Disease Locus Genotype and Prospective Risk of CHD in Healthy Middle-Aged Men.
P. J. Talmud, J. A. Cooper, J. Palmen, R. Lovering, F. Drenos, A. D. Hingorani, and S. E. Humphries (2008)
Clin. Chem.
54, 467-474
|Abstract »|Full Text »|PDF »
New cardiovascular risk determinants do exist and are clinically useful.
Y. M. Smulders, A. Thijs, and J. W. Twisk (2008)
Eur. Heart J.
29, 436-440
|Abstract »|Full Text »|PDF »
Four SNPs on Chromosome 9p21 in a South Korean Population Implicate a Genetic Locus That Confers High Cross-Race Risk for Development of Coronary Artery Disease.
G.-Q. Shen, L. Li, S. Rao, K. G. Abdullah, J. M. Ban, B.-S. Lee, J. E. Park, and Q. K. Wang (2008)
Arterioscler. Thromb. Vasc. Biol.
28, 360-365
|Abstract »|Full Text »|PDF »
Commentary: Genetic association studies see light at the end of the tunnel.
T. M Frayling (2008)
Int. J. Epidemiol.
37, 133-135
|Full Text »|PDF »
Rationale, Design, and Methodology of the Women's Genome Health Study: A Genome-Wide Association Study of More Than 25 000 Initially Healthy American Women.
P. M Ridker, D. I. Chasman, R. Y.L. Zee, A. Parker, L. Rose, N. R. Cook, J. E Buring, and for the Women's Genome Health Study Working Group (2008)
Clin. Chem.
54, 249-255
|Abstract »|Full Text »|PDF »
Update on the Genetics of Stroke and Cerebrovascular Disease 2007.
R. A. Hegele and M. Dichgans (2008)
Stroke
39, 252-254
|Full Text »|PDF »
Surprises of the genome and "personalized" medicine..
A. J. Marian (2008)
J. Am. Coll. Cardiol.
51, 456-458
|Full Text »|PDF »
Required sample size and nonreplicability thresholds for heterogeneous genetic associations.
R. Moonesinghe, M. J. Khoury, T. Liu, and J. P. A. Ioannidis (2008)
PNAS
105, 617-622
|Abstract »|Full Text »|PDF »
Genome-Wide Association: Which Do You Want First: the Good News, the Bad News, or the Good News?.
K. D. Taylor, J. M. Norris, and J. I. Rotter (2007)
Diabetes
56, 2844-2848
|Full Text »|PDF »
Future Use of Genomics in Coronary Artery Disease.
Validity of Reported Genetic Risk Factors for Acute Coronary Syndrome Reply.
T. M. Morgan, H. M. Krumholz, R. P. Lifton, and J. A. Spertus (2007)
JAMA
298, 1759
|Full Text »|PDF »
Genetics of sporadic amyotrophic lateral sclerosis.
J.C. Schymick, K. Talbot, and B.J. Traynor (2007)
Hum. Mol. Genet.
16, R233-R242
|Abstract »|Full Text »|PDF »
Interpreting P Values in Pharmacogenetic Studies: A Call for Process and Perspective.
M. L. Maitland, M. J. Ratain, and N. J. Cox (2007)
J. Clin. Oncol.
25, 4513-4515
|Full Text »|PDF »
Genetics of Cardiovascular Diseases: From Single Mutations to the Whole Genome.
F. Cambien and L. Tiret (2007)
Circulation
116, 1714-1724
|Full Text »|PDF »
Genetic Susceptibility to Peripheral Arterial Disease: A Dark Corner in Vascular Biology.
J. W. Knowles, T. L. Assimes, J. Li, T. Quertermous, and J. P. Cooke (2007)
Arterioscler. Thromb. Vasc. Biol.
27, 2068-2078
|Abstract »|Full Text »|PDF »
Scanning the Genome for Coronary Risk.
A. Rosenzweig (2007)
N. Engl. J. Med.
357, 497-499
|Full Text »|PDF »
Genomewide Association Analysis of Coronary Artery Disease.
N. J. Samani, J. Erdmann, A. S. Hall, C. Hengstenberg, M. Mangino, B. Mayer, R. J. Dixon, T. Meitinger, P. Braund, H.-E. Wichmann, et al. (2007)
N. Engl. J. Med.
357, 443-453
|Abstract »|Full Text »|PDF »
The Genomics Gold Rush.
E. J. Topol, S. S. Murray, and K. A. Frazer (2007)
JAMA
298, 218-221
|Full Text »|PDF »
Allele on Chromosome 9 Affects Heart Disease Risk.
(2007)
Journal Watch (General)
2007, 6
|Full Text »
To whom correspondence should be addressed. E-mail: 
