Unstable Angina Clinical Trial
Official title:
Matrix Metalloproteinase Genetic Polymorphisms and Outcome of Non-ST Elevated Acute Coronary Syndromes
Some Matrix Metalloproteases, proteases degrading the extracellular matrix, play a relevant
role in structure and stability of atherosclerotic plaques. Atherosclerotic plaques
triggering acute coronary syndromes show increased expression of MMP-1, MMP-3 and MMP-9.
Regulation of these MMPs is plaid by genetic polymorphisms, G+/G- at –1563 for MMP-1, 4A/5A-
at –1612 for MMP-3, and a microsatellite (13-27 CA repeats around –90) for MMP-9.
It is conceivable that these polymorphisms correlate with the clinical outcome of acute
coronary syndromes, particularly with those without ST segment Elevation (NSTEACS).
Non-ST elevation acute coronary syndrome (NSTEACS) is a syndrome encompassing a spectrum of
clinical manifestations between ischemic heart disease and acute myocardial infarction. It
represents an important cause of morbidity and hospitalization in western countries: its
incidence is estimated around 2/1000 subjects/year and about 10% of patients with acute
coronary syndrome develop an acute myocardial infarction within 6 months. Another reason of
concern is that patients require an invasive treatment, usually PTCA or CABG. ACS
encompasses features of both an inflammatory and thrombotic disease; their abnormalities
could be critical for evolution and complication of acute coronary syndrome.
Many inflammatory and coagulation indicators have been investigated, although the critical
factors responsible for complications in NSTEACS remain elusive.
Matrix remodeling and consequent erosion or fissuration of the unstable plaque is supposed
to be a key step of the development of acute coronary syndromes.
Neutral matrix metalloproteinases 1, 3 and 9 have been demonstrated to be actively produced
in atherosclerotic tissue, compared to unaffected arteries. Mechanisms responsible for such
increased expression might be related to inflammation, but also genetic regulation could
account for an increased expression leading to a different clinical outcome of the syndrome.
Genetic polymorphisms are described for all three MMPs involved in ACS. MMP-1 insertion of a
G in position creates an ets binding site that induces an eight times increase of the
synthesis rate. For MMP-3 (stromelysin) polymorphism, a deletion of an A (adenosine) in
position -1171 doubles the transcription activity and has been recently associated with
acute myocardial infarction and progression of coronary stenosis. In MMP-9 a more complex
polymorphism involves a microsatellite (AC) repeat in position –90 to –131. The mechanism
leading to increased MMP-9 expression is probably related to the transition to Z-DNA within
the microsatellite, which eases transcription. In vitro studies show that the longer the
tandem repeats sequence, the higher the transcription.
No studies on metalloproteinase polymorphism in NSTEACS have been carried out, so far.
This study has been planned to assess if patients admitted to the hospital for NSTEACS could
be associated to a different in hospital clinical outcome according to the genetic
polymorphism of these proteases.
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