Acute Coronary Syndromes Clinical Trial
Official title:
Pharmacogenetics of Clopidogrel in Acute Coronary Syndromes
The antiplatelet agent clopidogrel is an effective drug for the prevention of thrombotic events in patients with acute coronary syndromes, and is therefore one of the most frequently prescribed drugs worldwide. Accumulating data suggest that the response to clopidogrel is characterised by significant inter-patient variability in the degree of platelet inhibition and the risk of cardiovascular events. Recent research findings have highlighted the role of genetic variations in determining antiplatelet response variability, and this has aroused interest in genotyping all thienopyridine-eligible patients in order to identify those who would be at increased risk of harm if treated with clopidogrel. This is a prospective, multicentre, randomised study enrolling consecutive patients hospitalised because of an ACS with or without ST-segment elevation. The patients are randomised to undergo or not tests for CYP2C19*2, CYP2C19*17 and ABCB1 3435 genetic variants immediately after diagnosis. The genotyping is done using a Q3 System (a compact platform that enables the classic laboratory analysis of DNA by means of real-time PCR). The Q3 has been designed as a low entry-cost, portable, point-of-care instrument for foolproof use by unskilled personnel. The patients randomised to the pharmacogenomic arm receive one of the ADP receptor antagonists (clopidogrel/prasugrel/ticagrelor) on the basis of an algorithm that consider genetic and clinical variables. The patients randomised to the standard treatment arm receive clopidogrel or prasugrel or ticagrelor on the basis of the standard of care (clinical algorithm alone). For each patient, a record is made of the occurrence of cardiovascular death, non-fatal MI, stroke, BARC-defined bleeding, and definite or probable stent thrombosis. The primary endpoint is the composite of death due to cardiovascular causes, non-fatal MI and stroke. The secondary endpoints is the occurrence of definite or probable stent thrombosis, and BARC-defined major bleeding events (types 3-5).
Antiplatelet therapy is the cornerstone of medical treatment of patients experiencing an
acute coronary syndrome (ACS). As a synergistic antiplatelet effect can be obtained by
simultaneously inhibiting thromboxane-A2 and adenosine diphosphate P2Y12 platelet receptors,
the current standard of care for all patients with ACS includes dual anti-platelet therapy
with aspirin (the first choice treatment for blocking thromboxane-A2 receptors) and one of
the three currently available ADP P2Y12 inhibitors: clopidogrel, prasugrel and ticagrelor.
Over the last few years, the clinical availability of the new potent P2Y12 inhibitors
prasugrel and ticagrelor has changed the ACS treatment paradigm. The revised European
guidelines downgrade clopidogrel to patients who cannot receive prasugrel and ticagrelor, and
clearly recommend the latter for patients with ACS (Recommendation Class I, Evidence Level B
for both). However, the choice of the optimal drug for each individual patient is still left
to clinicians, thus continuing the uncertainty as to how these new potent drugs should be
incorporated into everyday clinical practice.
The appropriate selection of antiplatelet agents has so far been guided only by the patients'
phenotypic characteristics, but taken together, the evidence does not support a wide use of
prasugrel and ticagrelor in clinical practice and considering subgroups with less clinical
benefit and limitations of TRITON TIMI-38 and PLATO study design, not all 100% of patients
with ACS appears eligible for treatment with new ADP receptors antagonists.
Recent research has highlighted the role of CYP enzyme and ABCB1 genetic variations in
determining the variability of the patients' antiplatelet response to clopidogrel, and shown
a clear relationship between lower levels of clopidogrel's active metabolite, reduced
platelet inhibition, and a higher rate of major adverse cardiovascular events. Specifically,
post-hoc analysis concerning association of CYP2C19 and ABCB1 genetic variants to clinical
outcomes showed an absolute 7.3% reduction in the risk of death from cardiovascular causes,
myocardial infarction or stroke among the study population who were not carriers of a CYP2C19
reduced-function allele, ABCB1 3435 TT homozygotes, or both, compared with individuals who
did carry either.
The impact of CYP2C19 alleles and ABCB1 genotype seems to be restricted to patients taking
clopidogrel as they do not significantly affect pharmacological or clinical outcomes in
patients treated with prasugrel and ticagrelor.
The aim of this project is to test the impact on clinical outcomes of strategy of conducting
dual antiplatelet therapy considering both genotype data and clinical variables in comparison
with a strategy based on clinical variables alone.
Methodology:
This is a prospective, multicentre, randomised study enrolling 3,612 consecutive patients
hospitalised because of an ACS with or without ST-segment elevation. The patients are
randomised to undergo or not tests for CYP2C19*2, CYP2C19*17 and ABCB1 3435 genetic variants
immediately after diagnosis. The genotyping is done using a Q3 System (a compact platform
that enables the classic laboratory analysis of DNA by means of real-time PCR). The Q3 has
been designed as a low entry-cost, portable, point-of-care instrument for foolproof use by
unskilled personnel.
The patients randomised to the pharmacogenomic arm receive one of the ADP receptor
antagonists (clopidogrel/prasugrel/ticagrelor) on the basis of an algorithm that consider
genetic and clinical variables. The patients randomised to the standard treatment arm receive
clopidogrel or prasugrel or ticagrelor on the basis of the standard of care (clinical
algorithm alone).
Patient enrolment is to be completed in 24 months. Each patient will be followed up for 12
months by means of outpatient visits after one, six and 12 months.
For each patient, a record is made of the occurrence of cardiovascular death, non-fatal MI,
stroke, BARC-defined bleeding, and definite or probable stent thrombosis.
The primary endpoint is the composite of death due to cardiovascular causes, non-fatal MI and
stroke.
The secondary endpoints is the occurrence of definite or probable stent thrombosis, and
BARC-defined major bleeding events (types 3-5).
The expected rate reduction of ischemic and bleeding events is 25% for a median of 12 months
of follow-up (data derived from PLATO trial) and the target relative risk reduction for
genotype-guided therapy versus standard therapy is 20%. It has been defined a 95% power, a
type alpha error of 5% and two-tail test. Therefore approximately 1806 patients for each arm
should be enrolled.
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