Cardiovascular Diseases Clinical Trial
To perform genetic studies of low density lipoprotein (LDL) subclasses in 160 families in whom the probands had metabolically defined hypercholesterolemia.
BACKGROUND:
Low density lipoprotein cholesterol has been convincingly established as a major coronary
heart disease risk factor by many epidemiologic studies, clinical trials, and experimental
studies. A strong inverse association exists between high density lipoprotein cholesterol
and coronary heart disease. However, the status of very low density lipoprotein (VLDL)
cholesterol and plasma triglyceride levels as independent risk factors for cardiovascular
disease is less clear. Case control studies have shown a positive association between
coronary heart disease and plasma levels of apoprotein B, the major protein on LDL
particles, and an inverse relationship with apoprotein AI, the primary protein constituent
of HDL particles. In fact, it has been proposed that plasma levels of the apoproteins may be
stronger risk factors than lipid levels. Thus, understanding the mechanisms underlying
variations in both lipoprotein and apoprotein levels among individuals is essential to
elucidating the etiology of coronary heart disease in the general population.
Cardiovascular disease is also known to cluster in families, and this may be related to the
clustering of lipid and lipoprotein levels among family members. A review suggested that the
familial aggregation of heart disease may be primarily a reflection of the familial
aggregation of known risk factors, including cholesterol levels. The work of Goldstein and
Brown on familial hypercholesterolemia demonstrated that genetic control of lipoprotein
metabolism can play a causative role in the development of atherosclerosis. However,
familial hypercholesterolemia is a relatively rare disorder: the prevalence of heterozygotes
is estimated to be 1 in 500, homozygotes 1 in a million. In 1987, little was understood
about more common genetic contributions to lipid and lipoprotein abnormalities leading to
the familial aggregation of coronary heart disease.
DESIGN NARRATIVE:
The design was that of a cross-sectional family study. The recruitment and screening of
probands were conducted over a four-year period at the University of Texas at Dallas under
separate funding. The recruitment and screening of first-degree relatives were carried out
at Berkeley. Blood samples were obtained from relatives for LDL subclass analysis and for
lipid and apoprotein determination. An interview was conducted to obtain demographic
information and information on behavioral and environmental risk factors such as smoking,
exercise, and diet. The data were used to determine whether LDL subclasses were genetically
controlled in families with hypercholesterolemia due to overproduction of LDL or defective
clearance of LDL particles. Segregation analysis of LDL subclasses in these two types of
families was performed to search for a single major genetic locus and to simultaneously test
for the influence of polygenes and environmental effects. The relationships between the LDL
subclass phenotype characterized by a predominance of small, dense LDL and overproduction of
apoprotein B and LDL clearance defects were investigated in family members. A determination
was made as to whether an age-of-onset effect existed for the expression of LDL subclass
phenotypes. Genetic-environmental interactions were also studied.
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