Cardiovascular Diseases Clinical Trial
To locate and identify genes contributing to the genetic component of subclinical cardiovascular disease (CVD) in Type 2 diabetes and to evaluate the impact of lifestyle and environment on the expression of these genetic components of subclinical CVD.
BACKGROUND:
Atherosclerosis is the most important complication of diabetes and the reason for its
accelerated course in patients with this condition is poorly understood. Diabetes is
increasing in prevalence and will exact a heavy disease burden on the United States
population over the coming years. Secondary prevention of atherosclerotic complications
would be of great value. The rationale underlying genetic studies is that new pathways could
be identified through functional genomics.
DESIGN NARRATIVE:
The following hypotheses are tested: 1) The risk of developing Type 2 diabetes-associated
cardiovascular disease (CVD) has a significant heritable component that can be measured, and
2) The chromosomal locations of genes contributing to CVD in Type 2 diabetes can be
determined and the genes identified using modern molecular genetic approaches. The
investigators predict that these genetic factors can be detected in studies of sibling pairs
with Type 2 diabetes through genetic epidemiology methods and linkage analysis. Type 2
diabetes-affected sibling pairs, unaffected siblings, and parents, if available, will be
recruited and multiple clinical and subclinical measures of subclinical CVD risk will be
assessed, including coronary artery calcification (CAC), carotid arterial wall thickness
(IMT), ECG variables, and prevalent CVD. Data on the patients are collected in one visit to
the General Clinical Research Center (GCRC) which includes an interview and physical
examination, a resting 12-lead electrocardiogram (ECG), B-mode ultrasound of the carotid
arteries, retrospectively gated helical CT (RGHCT), and a spectrum of clinical laboratory
measures. Genetic and epidemiological methods will be used to evaluate the familial
aggregation of subclinical CVD taking into consideration the effects of shared environmental
exposures (e.g. smoking, diet, alcohol intake and physical activity) and clinical measures
(e.g., body mass index, blood pressure, lipids, age, sex, etc.). Initial estimates of
heritability suggest a significant heritable component to subclinical CVD. Clinical
evaluation will be followed by a comprehensive molecular genetic analysis of the sib
pairs/families including a genome wide screen, which will be followed by a focused effort to
create a high quality dataset by regenotyping or replacing problem markers. Evidence for
linkage to quantitative trait loci (QTLs) influencing CAC and IMT will be pursued in those
chromosomal regions showing suggestive evidence for linkage and then performing further
analyses to detect associations with these "saturation" markers.
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