Abstract

Myocardial infarction (MI) continues to be the number one cause of morbidity and mortality in the developed world with over a million MIs per year in the US alone, despite enormous progress in the diagnosis and aggressive treatment of conventional risk factors such as hypercholesterolemia, hypertension, and diabetes. The genetic contribution to MI is well established and development of diagnostic/prognostic tools and novel therapies based on unraveling these mechanisms should add substantially to the efforts of reducing conventional cardiovascular risk factors. The main objective of our study is to identify genetic variants that contribute to the risk of MI. To attain this goal we propose to conduct a broad-based and highly-powered strategy in a genome-wide association study using a high-yield and accurate tag-SNP array genotyping a total of 4500 MI patients and 7500 controls from US (Caucasians) and Iceland. Additionally, for cross-ethnic group testing of signals found in Caucasians, the study will include 600 MI patients and 600 controls of African-American ethnicity. The genome-wide association study will be carried out with a two-stage design which will lower the cost of genotyping while maintaining most of the power, thus allowing us to genotype more individuals resulting in a substantial increase in power to detect significant association. In the first stage approximately 35% of the total discovery group available is genotyped (1000 patients and 5000 controls) with the entire set of markers using 317K markers (Phase I genotyping). The most promising SNPs from the first stage will then be tested on the remaining 65% of the discovery group (2000 patients and 1000 controls), taking forward ~1% of the original SNPs (Phase II genotyping). The data from Phase I and Phase II will then be jointly analyzed to define markers that show significant association even after correcting for multiple testing. Significant SNPs from the joint analysis of the Phase I and II data will then be confirmed in an independent group of patients and controls (1500 patients and 1500 controls). Follow up genotyping of additional markers within the genes/regions showing association to MI will be done on the discovery cohort and also on the African-American case/control group. With the follow up genotyping we intend to identify additional Mi-associated markers that might correlate with the original signal and possibly show stronger association to the disease. The different populations will be analyzed (a) jointly, in order to identify risk variants common across the populations, and (2) separately to identify population specific risk variants and to explore ethnic effects. The project will use a high-yield and accurate array-based system from Illumina, Inc to genotype genome-wide tag-SNPs and a case/control single-point association analysis will be performed. Given that MI is a heterogeneous disorder that may depend on the impact of many genetic and environ- mental risk factors our study will also involve the analysis of interactions between genes (gene-gene) and between genetic and environmental factors (gene-environment) in both the discovery and confirmation groups.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Heart, Lung, and Blood Institute (NHLBI)
Type
Research Project (R01)
Project #
5R01HL089650-03
Application #
7626320
Study Section
Cardiovascular and Sleep Epidemiology (CASE)
Program Officer
Jaquish, Cashell E
Project Start
2007-09-01
Project End
2011-06-30
Budget Start
2009-07-01
Budget End
2010-06-30
Support Year
3
Fiscal Year
2009
Total Cost
$646,072
Indirect Cost

  Institution

Name
Decode Genetics, Inc.
Department
Type
DUNS #
132219176
City
Reykjavik
State
Country
Iceland
Zip Code
IS101

  Publications

Schultz, William M; Kelli, Heval M; Lisko, John C et al. (2018) Socioeconomic Status and Cardiovascular Outcomes: Challenges and Interventions. Circulation 137:2166-2178
Samman Tahhan, Ayman; Hammadah, Muhammad; Raad, Mohamad et al. (2018) Progenitor Cells and Clinical Outcomes in Patients With Acute Coronary Syndromes. Circ Res 122:1565-1575
Hajjar, Ihab; Hayek, Salim S; Goldstein, Felicia C et al. (2018) Oxidative stress predicts cognitive decline with aging in healthy adults: an observational study. J Neuroinflammation 15:17
Samman Tahhan, Ayman; Hammadah, Muhammad; Kelli, Heval Mohamed et al. (2018) Circulating Progenitor Cells and Racial Differences. Circ Res 123:467-476
Topel, Matthew L; Shen, Jia; Morris, Alanna A et al. (2018) Comparisons of the Framingham and Pooled Cohort Equation Risk Scores for Detecting Subclinical Vascular Disease in Blacks Versus Whites. Am J Cardiol 121:564-569
Ghasemzedah, Nima; Hayek, Salim S; Ko, Yi-An et al. (2017) Pathway-Specific Aggregate Biomarker Risk Score Is Associated With Burden of Coronary Artery Disease and Predicts Near-Term Risk of Myocardial Infarction and Death. Circ Cardiovasc Qual Outcomes 10:
Hayek, Salim S; Ko, Yi-An; Awad, Mosaab et al. (2017) Cardiovascular Disease Biomarkers and suPAR in Predicting Decline in Renal Function: A Prospective Cohort Study. Kidney Int Rep 2:425-432
Samman Tahhan, Ayman; Hayek, Salim S; Sandesara, Pratik et al. (2017) Circulating soluble urokinase plasminogen activator receptor levels and peripheral arterial disease outcomes. Atherosclerosis 264:108-114
Samman Tahhan, Ayman; Sandesara, Pratik B; Hayek, Salim S et al. (2017) Association between oxidative stress and atrial fibrillation. Heart Rhythm 14:1849-1855
Samman Tahhan, Ayman; Hammadah, Muhammad; Sandesara, Pratik B et al. (2017) Progenitor Cells and Clinical Outcomes in Patients With Heart Failure. Circ Heart Fail 10:

Showing the most recent 10 out of 45 publications