Acute Myocardial Infarction Clinical Trial
Official title:
CYCLosporinE A in Reperfused Acute Myocardial Infarction Prospective, Controlled, Randomized, Multicentre Trial to Examine Whether a Single i.v. Bolus of Cyclosporine A Before PCI Can Reduce Myocardial Reperfusion Injury in Patients With STEMI.
Infarct size is a major determinant of prognosis after myocardial infarction (MI). It has
been reported that Cyclosporine A (CsA) administered immediately prior to percutaneous
coronary intervention (PCI) significantly could reduce reperfusion injury and consequently
infarct size in ST elevation MI (STEMI) patients.
CYCLE trial is a multicenter, controlled, randomized open label study, with blind assessment
of endpoint measures. The objective is to determine whether a single i.v. dose of CsA within
6 hour onset of symptoms of STEMI in 444 patients, improves outcomes after successful
primary PCI, by reducing myocardial injury associated to reperfusion.
The possibility of optimizing the results of an early and effective reopening of the
occluded artery by reducing/avoiding the impact of the so-called reperfusion injury has been
for many years one of the most elusive objectives of pharmacological research, with evolving
hypothesis and targets.
A recently published trial has provided support to a line of investigation focused on the
role of mitochondrial dysfunction, the so-called permeability transition, as cause of
irreversible myocardial injury associated to reperfusion. In fact, a single dose of the
widely used immunosuppressant agent, CsA, a potent inhibitor of mitochondrial permeability
transition pore opening, was reported to limit ischemia−reperfusion injury in 50 patients
with anterior MI who underwent primary PCI.
Since infarct size and left ventricular function are the main determinants of long-term
morbidity and mortality, a single measure to limit infarct size is of potential clinical
benefit. Therefore the results of the previously mentioned trial should be replicated in a
larger sample size, before going on to a trial with clinical endpoints.
- Sample size
Assuming an incidence of the primary endpoint of 55% in the control group, we calculated
that 444 patients (222 patients per group) will be required for the study to have 80% power
to detect a 25% relative improvement (resulting in an endpoint frequency of 68.7% in the CsA
group) with a 5% drop-out rate and a two-sided alpha level of 5%. The size of the trial will
allow to investigate treatment benefit for the secondary endpoint hsTnT: assuming a
concentration of 2.7 ng/mL on day 4 (common SD=2.1) in the control group, the study will
have a 90% power to show a 25% reduction with CsA at a two-sided alpha level of 5%.
- Safety
Adverse events with intravenous CsA (i.e. anaphylactoid reactions/anaphylactic shock, acute
renal failure, or hypertensive crisis) are reported to be very rare. In this trial, patients
will receive only one iv dose of CsA, therefore we expect a low probability of adverse
effects related to repeated administrations, i.e. acute renal failure or hypertensive
crisis. Nonetheless a close monitoring of the safety of the single dose of CsA is foreseen
with monthly examination of data of safety by the Steering Committee.
;
Allocation: Randomized, Endpoint Classification: Efficacy Study, Intervention Model: Parallel Assignment, Masking: Open Label, Primary Purpose: Treatment
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