Cardiovascular Diseases Clinical Trial
To determine the relative risk in a defined population of angiographically demonstrated coronary artery disease due to genetic polymorphisms at the four apolipoprotein genomic regions.
BACKGROUND:
Numerous epidemiological studies have shown that the risk of coronary heart disease is
strongly influenced by plasma lipid levels, especially HDL and LDL cholesterol, and their
specific apolipoprotein constituents. Genetic studies have established significant
heritability of these lipid components, and have also identified relatively rare major genes
that result in extreme lipid values and increased risk of coronary heart disease.
Geneticists have identified a number of segregating polymorphisms at the four major
apolipoprotein genomic regions, using a combination of protein and DNA assays. However, in
1988 when the study was initiated, the relationship between these polymorphisms and risk of
coronary heart disease had not yet been properly defined.
DESIGN NARRATIVE:
The study had a case-control design. Cases were consecutively selected from the pool of
eligible Latter Day Saints Hospital patients referred for coronary angiogram. Eligibility
criteria included residing in the Wasatch County or Southern Idaho counties, being healthy
at the time of angiogram and having greater than 60 percent occlusion. Approximately 80-100
controls were retrospectively selected from the clinic records of the past four years.
Fasting lipid profiles were defined for cases and controls in terms of total cholesterol,
total triglycerides, HDL levels, LDL levels, VLDL levels, density gradient distribution of
HDL-LDL subfractions, and levels of apo A-1, apo B, and apo E. The distribution of genetic
polymorphisms at the four major apolipoprotein genomic regions was determined by typing all
cases and controls for isoforms of apo E and apo AIV and a wide variety of DNA
polymorphisms. Approximately 800 first degree relatives of cases and controls were also
typed for DNA polymorphisms. Data were collected on risk factors including smoking, alcohol
use, obesity, physical activity, and diet. Clinical data included medical and family history
of cardiovascular disease and medication status. Multivariate statistical analysis was used
to define the relative risk of coronary disease associated with segregating polymorphisms,
and DNA haplotypes at these loci in conjunction with lipid profiles and risk factors.
Analyses were also conducted on the extent to which the genetic segregation at these
apolipoprotein genomic regions influenced the distribution of lipid profiles and whether the
distribution of risk factors was influenced by the interaction of environmental risk factors
such as smoking and genotypes at these regions.
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