Cardiovascular Diseases Clinical Trial
To relate observations at the DNA level to the distribution of coronary heart disease in the population at large.
BACKGROUND:
The Rochester Family Heart Study was initiated in 1983 to study the genetic basis for
familial aggregation of apolipoprotein A-I and hypertension in Rochester, Minnesota.
Recruitment began in 1985 and resulted in data on 2,259 individuals in 300 three generation
pedigrees. The study was supported by R01HL24489.
Lipid levels play a central role in determining the predisposition to coronary heart
disease. In Western industrialized societies diseases of the heart rank as the number one
cause of morbidity and mortality in the adult population. Thirty percent of all deaths in
the United States in 1982 were attributable to coronary heart disease. Epidemiological
studies of total communities including Framingham, Massachusetts and Tecumseh, Michigan have
established a long list of factors that predict increased risk to coronary heart disease.
Those that have been implicated include male gender, aging, positive family history,
sedentary life style, diabetes, high blood pressure, cigarette smoking, overweight and
abnormal plasma levels of lipids and lipoproteins. Although there is great variation among
individuals in the risk factors associated with the development of coronary heart disease,
the disease typically involves the infiltration of cholesterol into the intimal wall of the
arteries beginning early in life. It has been hypothesized that each individual inherits or
experiences an array of risk factors that determine susceptibility to the disease process
that progresses through the phases of injury to the vascular wall, infiltration of lipids,
accumulation of cholesterol esters, a proliferation of cells, stenosis and finally occlusion
that leads to the coronary heart disease outcome. Lipid metabolism plays a central role in
determining the progression of this process. A role for elevated lipids in the etiology of
coronary heart disease is supported by the Lipid Research Clinics trial of cholestyramine
which established that a 20 percent reduction of plasma low density lipoprotein (LDL) in
particular, results in a 19 percent reduction of coronary heart disease after seven years in
high risk males. Most studies to date have focused on environmental factors associated with
variability in risk factors. Biometrical studies have estimated the role of genes in
determining interindividual variability in lipid and lipoprotein phenotypes by comparing and
contrasting the levels in related and unrelated individuals living together and apart. With
the advent of new techniques to measure variability in gene products and at the DNA level,
it is now possible to expand our studies of the role of genes in both lipid metabolism and
coronary heart disease. Knowledge about the genetic epidemiology of coronary heart disease
will provide valuable tools for clinical screening and diagnosis and will make it possible
to develop a rational strategy to intervene. Not all individuals respond in the same way to
lipid-lowering strategies. By knowing the genes involved in regulating the metabolic factors
that are altered in coronary heart disease we will be able to sort out those individuals who
will respond to specific treatments.
DESIGN NARRATIVE:
Beginning in 1987 and using blood samples and data from the RFHS, variation at the DNA level
was determined using restriction fragment length polymorphisms and at the protein level by
isoelectric focusing. The relationships were defined in the population among the
apolipoproteins, cholesterol, triglycerides, high density lipoprotein cholesterol phenotypes
and estimates were done on the effects of age, sex, smoking, drug use, and obesity on these
relationships. Estimates were determined for the fraction of interindividual variation in
the apos attributable to gene loci coding for these molecules. Estimates were also
determined for the fraction of interindividual variation in cholesterol, triglycerides, and
high density lipoprotein cholesterol attributable to gene loci coding for the apos and the
LDL receptor. A determination was also made as to whether genotypic variation for the gene
loci coding for the apo and LDL-receptor contributed to the prediction of coronary heart
disease beyond that provided by the effects of these gene loci on the interindividual
variation in the apos, cholesterol, triglycerides, and high density lipoprotein cholesterol.
Radioimmunoassay and medical information collection took place at the Mayo Clinic. DNA
probes, DNA studies of special families, and definition of new restriction fragment length
polymorphism took place at Charing Cross Hospital in London, England. RFLP typing of genes
coding for the apolipoproteins and the LDL receptor and electrophoretic typing of the known
apo E and AIV protein polymorphisms took place at the University of Pittsburgh. The genetic
architecture responsible for phenotypic variability in the population at large was defined
at the University of Michigan and Washington University, St. Louis.
The study was renewed in 1992 to carry out six aims that 1) provided new information about
four polymorphic genes involved in reverse cholesterol transport; 2) completed the
investigators' studies to evaluate the utility of genetic variation in 12 candidate genes
for prediction of coronary artery disease; 3) identified individuals who carry mutations
that have an impact on coronary artery disease; and 4) began molecular studies of these
individuals to define the DNA changes that are responsible. New noninvasive measures of
coronary artery disease in asymptomatic individuals using ultrafast cardiac computed
tomography complemented efforts to evaluate the role of measured genetic variation in
predicting coronary artery disease.
The study was renewed again in 1997 with five specific aims. Aims 1 and 2 identified genomic
regions containing new coronary artery disease susceptibility genes, using 234 tandem repeat
marker loci at a 10 centimorgan (cM) density and the variance component method of linkage in
274 multigeneration pedigrees, both globally and in particular contexts defined by gender,
age, body mass index and smoking. For those regions that showed linkage, confirmatory
linkage analysis was conducted in a second independent sample of 301 multigeneration
pedigrees. In regions where linkage was replicated, fine structure linkage analyses was
conducted, using additional marker loci, located approximately every 1 cM. Specific aims 3
and 4 identified functional DNA variations in the new candidate coronary artery disease
susceptibility genes. Direct DNA sequencing and cladistic analyses were used to estimate the
average, context dependent, dominant, and epistatic effects associated with these functional
DNA variations. Specific aim 5 estimated the association between the risk of coronary artery
disease and functional genotypes identified by the cladistic analyses carried out in
specific aims 3 and 4 before and after considering the intermediate biological risk factors
that link the effects of genetic and environmental variation to variation in risk of
disease.
The study was renewed in 2001 through July 2006 to continue to investigate innovative
analytic and molecular aspects of risk of coronary artery disease, in particular, the
contribution of polymorphic variation at the ApoE locus and two other candidate regions of
the genome on variation in plasma ApoE level.
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