Cardiovascular Diseases Clinical Trial
To investigate genetic markers of coronary heart disease in type 2 diabetes.
BACKGROUND:
Coronary heart disease (CHD), as the leading cause of death in the United States, is of
significant public health concern. Despite the knowledge that atherosclerosis is the
underlying cause of CHD, the recognition that both genetic and environmental factors
contribute to the occurrence of disease, and the identification of a large number of genetic
and environmental factors that have been found to be associated with disease risk, the
etiology of atherosclerosis with the later development CHD continues to be not very well
understood.
DESIGN NARRATIVE:
The nested case-control study will determine whether variability in 20 genes belonging to
endothelial and inflammatory dysfunction pathways is related to the risk of coronary heart
disease (CHD) among men and women diagnosed with type 2 diabetes in two large ongoing
prospective studies, the Nurses' Health Study (NHS) and Health Professionals' Follow-up
Study (HPFS). This will be accomplished by combining two complementary approaches that are
made possible by the recent advances in knowledge of the human genome and high-throughput
genotyping technologies. The investigators will directly target functional variants in the
coding regions of the candidate genes and also investigate the association between CHD and
ancestral haplotypes at each locus. The specific aims are: 1. To identify novel variants in
10 candidate genes of the inflammatory, and endothelial dysfunction pathways that have not
been systematically screened for polymorphisms by targeted resequencing; 2. To assess the
relationship between functional variants in 20 candidate genes in the inflammatory and
endothelial dysfunction pathways and risk of CHD among subjects with diabetes of the NHS and
HPFS cohorts; 3. To identify the subset of polymorphisms that best capture the overall
genetic variability at each locus (haplotype tagging single nucleotide polymorphisms (SNPs)
or htSNPs) and investigate the association between CHD risk and the haplotypes defined by
these htSNPs; 4. To examine individual SNPs as well as haplotypes in relation to biochemical
markers of inflammation and endothelial activation such as CRP, ICAM-1, VCAM-1, E-selectin,
and TNF-a in diabetic individuals; and 5. To examine gene-environment interactions in
relation to CHD risk in diabetic subjects. By 2006, an estimated 820 cases of CHD will have
been confirmed among diabetic men and women in the blood cohorts. The large size,
prospective design, high follow-up rates, detailed and reliable long-term lifestyle and
outcome information, and the availability of blood specimens make these cohorts a valuable
and unique resource for studying genetic determinants of accelerated atherosclerosis in
diabetic patients.
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