Coronary Artery Disease Clinical Trial
Official title:
Discovery of New Circulating Biomarkers of Coronary Atherosclerosis Using Differential Proteomics: the BIOmarkers of CORonary Events (BIOCORE) Study
The study hypothesis is that differential proteomic techniques can be used to discover new circulating biomarkers of coronary atherosclerosis in the blood of patients suffering from coronary artery disease (either stable or unstable) who will be compared to a group of patients without coronary artery disease
Hypothesis: Our hypothesis is that coronary atherosclerosis induces both quantitative and
qualitative modifications of circulating proteins, which can be captured by a differential
proteomic approach applied to serum or plasma samples. Identification of such modifications
in the circulating blood of patients with coronary artery disease (versus patients without
coronary artery disease) and/or of patients with acute coronary syndromes (versus stable
coronary artery disease) may lead to discovery of new biomarkers of coronary atherosclerosis
and of atherosclerotic plaque vulnerability.
Objectives:
Primary objective: Identification of new circulating biomarkers of stable and unstable
coronary artery disease using a new approach of differential proteomics.
Secondary objectives:
- Evaluation of the diagnostic value of these new biomarkers for the diagnosis of stable
and unstable coronary artery disease.
- Comparison of the diagnostic value of these new biomarkers to the diagnostic value of
1) other validated biomarkers of atherosclerosis (eg, CRP, IL-6, CD40L, markers of
leukocyte activation, …); and 2) of non-invasive measures of arterial function (eg,
carotid artery intima-media thickness, pulse wave velocity, ankle/brachial index, …)
- Description of the relationship between these new biomarkers and major adverse coronary
events (death, myocardial infarction, revascularization) during a 12-month follow-up.
Methods:
Uniq center, prospective study. Three groups of patients will be studied. Group 1:
Non-ST-elevation acute myocardial infarction; Group 2: Stable coronary artery disease; Group
3: normal coronary arteries and absence of other detectable atherosclerotic lesions.
A new proteomic approach will be applied to serum and plasma samples obtained 1 month after
the index hospitalisation. This approach includes 3 steps: 1) equalisation of circulating
proteins (expose low-concentration proteins belonging to the "deep-proteome"); 2) Retention
chromatography; and 3) protein separation using 2D-electrophoresis and Surface-Enhanced
Laser Desorption/Ionisation Time-of-Flight (SELDI-TOF).
Biomarkers with the highest diagnostic value will be subsequently identified using
Matrix-Assisted Laser Desorbtion/Ionisation Time-of-Flight (MALDI-TOF) and tandem mass
spectrometry (MS/MS).
Perspectives:
Validation of the diagnostic and prognostic values of the new biomarkers discovered and
identified using the proteomic approach described above will require development of more
straightforward measurement techniques (eg, ELISA), which will be used prospectively or
retrospectively in other cohorts of patients with coronary artery disease. Basic studies
will be performed in parallel, so as to better understand the role of these new biomarkers
in the pathophysiology of atherosclerosis.
;
Time Perspective: Prospective
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