Coronary Artery Disease Clinical Trial
Official title:
Intensified Antiplatelet Therapy in Post-PCI Patients With High On-treatment Platelet Reactivity: the OPTIMA-2 Trial
High on-treatment platelet reactivity (HOPR) is associated with increased risk of cardiovascular events in patients undergoing percutaneous coronary intervention (PCI). We sought to investigate the efficacy and safety of 1-month intensified antiplatelet therapies in post-PCI patients with HOPR.
OPTImal Management of Antithrombotic agents: OPTIMA-2 trial
Dual antiplatelet therapy (DAPT) with aspirin and a P2Y12 receptor inhibitor is the
foundation antiplatelet therapy in patients undergoing percutaneous coronary intervention
(PCI). Clopidogrel is the most commonly used P2Y12 receptor inhibitor worldwide because it is
effective and inexpensive1. High on-treatment platelet reactivity (HOPR) occurs in as many as
one-third of patients treated with standard dose clopidogrel (75mg once daily), and is
associated with an increased risk of major adverse cardiovascular events (MACE).
Various approaches have been tested to overcome HOPR in patients treated with aspirin and
clopidogrel, including higher doses of clopidogrel; the addition of cilostazol; and
replacement of clopidogrel with prasugrel; however, the results of these intensified
treatments were controversial, and a more potent P2Y12 receptor inhibitor, ticagrelor has
never been studied in this scenario.
TOPIC study showed that short-term (i.e. 1-month) intensification of antiplatelet treatment
might be sufficient to achieve optimal outcomes. Similarly, TROPICAL ACS showed that guided
de-escalation of antiplatelet treatment with clopidogrel was non-inferior to the treatment
with prasugrel at 1 year after PCI in terms of net clinical benefit, which suggests that
routinely long-term intensification of antiplatelet treatment is not required for all PCI
patients.
Accordingly we performed a randomized trial to test the hypothesis that in patients with HOPR
intensification of antiplatelet therapy with double dose clopidogrel, the addition of
cilostazol, or replacement of clopidogrel with ticagrelor for 1 month followed by resumption
of conventional DAPT with aspirin and clopidogrel for 11 months would be superior to
conventional DAPT for 12 months in reducing the prevalence of HOPR and MACE without
increasing bleeding.
Inclusion criteria:
1. Successively recruit all patients who receive stent implantation;
2. Intended use of conventional DAPT with the combination of aspirin 100mg once daily and
clopidogrel 75mg once daily for at least 12 months;
3. Patient aged over 18 years;
4. Signed inform consent.
Exclusion criteria:
1. Allergy or intolerance to study drugs;
2. History of gastrointestinal or intracranial bleeding;
3. Need for anticoagulant therapy;
4. High risk of bleeding (e.g., myelodysplasia, baseline platelet count < 80 × 109/L);
5. Hemoglobin < 90g/L;
6. Active malignancy or life expectancy < 1 year;
7. Patients with other conditions made them unsuitable to be recruited at the discretion of
the investigators.
Study procedures:
Following treatment for at least 5 days with the combination of aspirin 100mg once daily and
clopidogrel 75mg once daily irrespective of a loading dose we measured platelet aggregation
in response to adenosine diphosphate (ADP) (PLADP) using light transmittance aggregometry
(LTA). HOPR was defined as PLADP > 40%. Patients with HOPR were continued on aspirin 100mg
once daily and were randomly assigned to one of the following 4 groups:
1. clopidogrel 150mg once daily (CLOP-150);
2. clopidogrel 75mg once daily plus cilostazol 100mg twice daily (CLOP+CILOST);
3. ticagrelor 90mg twice daily (TICAG);
4. clopidogrel 75mg once daily (conventional DAPT, CON). At 1 month, platelet aggregation
testing was repeated after which all patients were switched back to conventional DAPT
for a further 11 months.
All patients without HOPR were treated with conventional DAPT and followed to 12 months
(Non-HOPR).
Sample size calculation:
Based on the published literature, we assumed a 38% rate of persistent HOPR in patients
randomized to intensified treatment and 60% in those randomized to CON therapy. With a sample
size of 81 per group, we calculated that we would have 80% power to detect this difference
with a 2-sided P value of 0.05. After allowing for 20% study drug discontinuation rate at 1
month, we planned a sample size of 405 patients with HOPR.
Platelet Reactivity Assay
1. ADP-induced platelet aggregation: Light transmittancy aggregation (LTA) in response to
5μM ADP.
2. Blood sample collection time: baseline (more than 5 days after taking clopidogrel 75mg
daily and aspirin 100mg daily), 1month after randomization.
Clinical follow-up:
Time points: 1month, 6month, and 1year after randomization.
The study endpoints:
The primary outcome was the proportion of patients with persistent HOPR at 1 month.
The secondary outcomes included a composite of MACE including cardiovascular death, nonfatal
myocardial infarction (MI), ischemic stroke, target vessel revascularization (TVR), stent
thrombosis (ST) and cardiac readmission during 12-month follow-up, and any bleeding defined
by the Thrombolysis in Myocardial Infarction (TIMI) criteria.
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