Hypertension Clinical Trial
Official title:
Family Blood Pressure Program - GENOA (Genetic Epidemiology Network of Atherosclerosis)
GENOA, the Genetic Epidemiology Network of Arteriopathy, consists of a network of three field centers and biochemical and genetic core labs to study the common polymorphic genetic variations to determine individual differences in blood pressure and essential hypertension in 1,500 sibling pairs in three racial groups. Linkage analyses are performed using an extensive array of candidate genes and anonymous markers throughout the genome.
Each collaborating investigator is responsible for an essential element of the network: Eric
Boerwinkle for genotyping and linkage analyses, Robert Ferrell for genotyping, Craig Hanis
for recruiting Mexican-Americans, Richard Hutchinson for recruiting African-Americans,
Sharon Kardia for cladistic and prediction analyses and data management, and Stephen Turner
for recruiting Non-Hispanic whites and measuring physiologic variables. Between 1995 and
2000, the network carried out five specific aims to localize and characterize the genetic
determinants of high blood pressure. Aim 1 used robust sibling pair linkage methods in 500
hypertensive sibling pairs in each racial group (a total of 1,500 sibling pairs) to localize
genes influencing interindividual differences in the occurrence of essential hypertension.
Aims 2 and 3 took advantage of previously collected blood pressure and intermediate
predictor trait data from 1,488 normotensive sibling pairs from the Rochester Family Heart
Study to localize genes contributing to essential hypertension. The linkage analyses (Aims
1-3) used both an extensive array of candidate genes and a large number of anonymous markers
throughout the genome. Aim 4 used multiple diallelic sequence polymorphisms and cladistic
analyses within a linked gene to identify haplotypes for further DNA sequencing in order to
identify candidate functional DNA sequence variation contributing to interindividual
differences in BP levels and essential hypertension status. Aim 5 evaluated the ability of
candidate functional DNA sequence variation to predict essential hypertension status in the
three racial groups.
The study was renewed in September 2000 to pursue two lines of investigation. The first is
to identify and characterize genes contributing to atherosclerotic coronary heart disease
using electron beam computed tomography (EBCT) to quantify coronary artery calcification as
a measure of preclinical disease. Robust sibling-pair linkage methods will be used to
determine whether any of the more than 375 highly polymorphic tandem repeat marker loci
spanning the genome are linked to genes influencing EBCT measures of coronary artery
calcification in at least 500 GENOA sibships from Rochester, Minnesota. Association analysis
will be used to determine whether biallelic markers of DNA sequence variation in candidate
genes identified by GENOA or others to influence blood pressure level or diagnostic category
also influence EBCT measures of coronary artery calcification in at least 500 GENOA
participants from Rochester, Minnesota. The second line of investigation extends analytical
methods (linkage disequilibrium regression and combinatorial partitioning) to more finely
localize positional candidate genes and loci, and to identify gene-gene and gene-environment
interaction effects influencing the measured Family Blood Pressure Program and GENOA
phenotypes.
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Time Perspective: Prospective
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