Cardiovascular Diseases Clinical Trial
Official title:
Coronary Disease Detection by Thallium SPECT and Fast CT
The purpose of this study is to compare two methods of diagnosing coronary artery disease (CAD), thallium single photon emission computed tomography (SPECT) and ultrafast computed tomography (CT).
BACKGROUND:
The ability to noninvasively detect CAD at a subclinical stage is fundamental to
understanding the biology of the transition of occult CAD to clinical CAD in asymptomatic
people at the highest risk for future CAD.
DESIGN NARRATIVE:
The cross-sectional study is designed to identify the factors explaining why some individuals
have exercise ischemia without significant coronary artery calcium (CAC) while others have
extensive CAC without exercise ischemia. The investigators will compare the
pathophysiological features of a functional test for subclinical CAD detection (exercise
radionuclide perfusion SPECT) and an anatomical test to detect coronary calcification
(ultrafast CT) in a high-risk asymptomatic population of 30 to 59 year old siblings of people
with premature CAD. Siblings will undergo screening for occult CAD using both detection
methods. Individuals who are abnormal on either test (exercise-induced ischemia or calcium
score greater than 75th percentile for age and sex) will be offered cardiac catheterization,
which will include quantitative coronary angiography, assessment of endothelial function by
intracoronary acetylcholine, and measurement of plaque volume and composition in a selected
coronary artery by intravascular ultrasound (IVUS). The study will focus on the
pathophysiology of occult CAD among individuals who have exercise ischemia with low calcium
scores and other individuals who have high calcium scores without ischemia. Discrepancies
between these two tests measure potentially different biological pathways and such
discrepancies are observed frequently in high-risk asymptomatic siblings (40% in our recent
pilot study). Analyses will be done to determine which biological risk factors can account
for variation in plaque calcification that results in discordances between these two measures
of occult disease (including lipid levels and subclasses, Lp(a), diabetes, thrombotic
factors, pro-inflammatory cytokines, and importantly, those factors involved in calcium
regulation, and bone regulatory proteins). In those siblings undergoing cardiac
catheterization, analyses will be done to determine whether the severity or extent of
coronary luminal narrowing, the presence of epicardial or microvascular endothelial
dysfunction, or the volume or calcium content of plaque by IVUS can account for discordances
between the two screening tests. Polymorphisms in several candidate genes that may affect
tissue calcification will be examined as a possible explanation for variations in plaque
calcification as reflected in test discordance. Plasma and DNA will also be collected for
novel studies of factors that may account for variability in coronary plaque calcification in
this unique well characterized asymptomatic high risk population. This will be the first
comprehensive study to define the unique biological and genetic factors related to occult
CAD, as detected by both perfusion imaging and ultrafast CT.
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