Cardiovascular Diseases Clinical Trial
To evaluate innovative diagnostic methods that will improve the diagnostic reliability of cardiovascular testing in evaluation of ischemic heart disease in women. Innovative approaches proposed include physiologic or functional measurements such as impaired metabolism, perfusion, or endothelial function as well as assessment of epicardial coronary arteries by angiography. Other objectives include developing safe, accurate, and cost effective diagnostic approaches for evaluating women with suspected ischemic heart disease, and determining the frequency of myocardial ischemia in the absence of significant epicardial coronary stenosis, as well as the frequency of non-ischemic or non-cardiac chest pain. A key aspect of the WISE study is to determine whether evidence of myocardial ischemia occurs in the absence of obstructive coronary disease.
BACKGROUND:
Cardiovascular disease exacts a heavy burden on the health of women. Ischemic heart disease
claims the lives of nearly 250,000 women in the United States each year. Recognition of
ischemic heart disease in women is a major challenge to the primary care physician.
Diagnosis of ischemic heart disease requires recognition of clinical symptoms such as chest
pain, or events such as a myocardial infarction, which are evaluated by a physician who will
confirm the diagnosis with objective tests. Unfortunately, both symptom recognition and
diagnostic tests confuse rather than confirm a diagnosis of myocardial ischemia in women.
Chest pain syndromes suspicious for myocardial ischemia are common in women. Noninvasive
diagnostic methods which often confirm the diagnosis and assess disease severity in men are
less reliable in women. This lack of objective data to support the diagnosis of chronic or
acute myocardial ischemia may influence the physician's decision to further evaluate women
at risk. With precision in diagnosis, efforts to optimize therapies are hampered.
The detection of epicardial coronary atherosclerosis is a major objective in clinical
cardiology. The utility of this approach is well established. However, although the presence
of atherosclerosis is sufficient to cause myocardial ischemia, whether significant ischemia
or risk of ischemia exists in the absence of angiographic epicardial stenosis, is not known
and may be important for women.
Recent progress in understanding the pathophysiology of myocardial ischemia provides a more
complex causal pathway than the heretofore notion of fixed atherosclerotic obstructions in
passive conduits. Diseased arteries which may appear angiographically normal as well as
arteries with fixed obstructions can respond to vasomotor influences with a detrimental
amount of vasoconstriction. The endothelium generates vasoactive and anticoagulant factors
that are important mediators of thrombosis. Cycling hormones may further influence these
complex interactions. Methods which do not rely solely on fixed obstruction of epicardial
arteries are not only possible but may be useful to recognize early atherosclerosis or, for
example, endothelial dysfunction which places the patient at risk for untoward coronary
events.
The concept for the study was developed by the Cardiology Advisory Committee in
collaboration with staff and was approved by the May 1993 National Heart, Lung, and Blood
Advisory Council. The Request for Proposals was released in April 1994.
DESIGN NARRATIVE:
The Women's Ischemia Syndrome Evaluation (WISE) was a four center study designed to evaluate
ischemic heart disease and its pathophysiology in women. WISE testing focused on three
areas: 1) optimizing symptom evaluation and diagnostic testing for ischemic heart disease;
2) exploring mechanisms for symptoms and evidence of myocardial ischemia in the absence of
epicardial coronary artery disease; 3) evaluating the influence of reproductive hormones on
symptoms and diagnostic test response. The WISE core data base included demographic and
clinical data, symptom and psychosocial variables, coronary angiography and ventriculography
data, blood lipoprotein/homocysteine/lipid peroxidation/genetic/hormone/ phytoestrogen
analysis, brachial artery reactivity testing, and resting/ambulatory electrocardiographic
(ECG) monitoring. Site specific complementary methods included physiologic and functional
cardiovascular assessments of myocardial perfusion and metabolism, ventriculography,
endothelial vascular function and coronary angiography. Women were followed for at least one
year to assess clinical events and symptom status. In the Phase I (1996-7), a pilot phase,
256 women were studied. Phase II has completed enrolling 1008 women in the study. The WISE
study defined contemporary and comprehensive state-of-the-art diagnostic testing to evaluate
women with suspected ischemic heart disease, and explore sex specific ischemic heart disease
pathophysiology.
The study has been renewed through April, 2005 to extend patient follow-up for a minimum of
five years. Dr. Kelsey (U01HL64829) of the Data Coordinating Center at the University of
Pittsburgh will continue the follow-up, develop sex-specific incremental outcome models to
evaluate the prognostic value of female reproductive variables, assess cost effectiveness of
the WISE testing techniques, and continue data analyses. Dr. Reis (U01HL64914) will study
the immunologic basis of coronary disease in women, focusing on the role of inflammation and
cytokine production. He will measure several cytokines and cytokine-related proteins and
genotypes in approximately 900 stored samples from WISE participants. Dr. Pepine
(U01HL64924) will study the renin angiotensin system in coronary microvascular dysfunction,
focusing on whether polymorphisms of the renin-angiotensin/kallikrein-kinin systems and
beta-adrenergic receptors polymorphisms are associated with abnormal coronary microvascular
function determined by coronary flow reserve measurements.
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Primary Purpose: Diagnostic
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