STEMI Clinical Trial
Official title:
Cangrelor Administration Following Ticagrelor Loading vs Ticagrelor Loading Alone in ST Segment Elevation Myocardial Infarction Patients: A Randomized, Pharmacodynamic Study
Platelets and thrombus formation play a key role in the pathogenesis of acute coronary artery occlusion and subsequent myocardial infarction. Apart from mechanically opening the occluded artery with angioplasty, adjunctive antiplatelet treatment is of utmost importance. However, orally administered antiplatelet agents exhibit a delay in their onset of action in the setting of acute myocardial infarction and angioplasty is mostly performed without adequate platelet inhibition. Cangrelor is an intravenous antiplatelet agent which can provide almost immediate strong platelet inhibition. The investigators aim to compare a strategy of cangrelor administered on top of ticagrelor-an oral antiplatelet agent- vs ticagrelor alone, on their efficacy to inhibit platelet function in the early hours of an acute myocardial infarction.
A rapid and consistent platelet inhibition represents the cornerstone of pharmacological
treatment in the early hours of ST-segment elevation myocardial infarction (STEMI) with
expected improvement in outcome. Current practice guidelines recommend administration of a
loading dose (LD) of an oral P2Y12 receptor antagonist as early as possible or at the time of
percutaneous coronary intervention (PCI) or at first medical contact.
Pharmacodynamic data have clearly shown a delay in the onset of action when prasugrel or
ticagrelor are administered in patients with STEMI - compared to what is obtained in stable
or acute coronary syndrome (ACS) patients-, which is most likely caused by an impaired
absorption. Peri-interventional platelet inhibition is therefore suboptimal in most cases of
timely performed primary PCI, even when novel oral antiplatelet agents with faster than
clopidogrel action are used. Modifications of the loading dose or antiplatelet pre-hospital
administration may only partially 'bridge the gap" in platelet inhibition.
On the other hand, cangrelor is a parenteral P2Y12 antagonist, with a rapid -within minutes-
onset of action, able to provide very strong and consistent platelet inhibition and with
rapid offset of action- within 60 min of infusion discontinuation. In the CHAMPION PHOENIX
(Cangrelor Versus Standard Therapy to Achieve Optimal Management of Platelet Inhibition)
trial cangrelor reduced the incidence of ischemic events, without increasing the incidence of
severe bleeding. Ticagrelor is an oral antiplatelet agent which has been reported that can be
given before or during infusion of cangrelor without attenuation of cangrelor's
pharmacodynamic effects, while the pharmacodynamic effects of ticagrelor are preserved when
ticagrelor is given during infusion of cangrelor. It seems therefore, that ticagrelor has
favorable characteristics for patients intended to receive cangrelor.
In the present study, in STEMI patients undergoing primary PCI the investigators aim to
compare platelet inhibition achieved in patients loaded with ticagrelor followed by cangrelor
(bolus plus infusion) vs ticagrelor alone loaded patients.
This will be a prospective, randomized, 3-center, single-blind, investigator-initiated study
of parallel design to compare platelet inhibition provided by ticagrelor LD plus cangrelor
(bolus and infusion) vs ticagrelor LD alone. Participants will be consecutive P2Y12
inhibitor-naive STEMI patients with pain onset<12 hours admitted for primary PCI will be
considered.
Participants in both arms will receive ticagrelor 180 mg LD as early as possible (e.g. in the
spoke hospital in case of transfer or at the emergency department in cases of hub hospital
presentation), as per local practice. The exact time of ticagrelor administration will be
recorded. Randomization followed by immediate initiation of cangrelor administration will be
performed after angiography and immediately prior to PCI. Patients will be randomized (Hour
0) in a 1:1 ratio by an independent investigator to cangrelor 30 mcg/kg bolus + 4 mcg/kg/min
for 2 hours, or no IV antiplatelet .
Other treatment will be as per local standard of care in all participants. Investigators who
will perform platelet function testing will be blind to the actual treatment assignment,
whereas an independent investigator will monitor bleeding and adverse event data.
Platelet reactivity will be measured at randomization (Hour 0) and at 15 min, 1, 2 and 4
hours post randomization. Platelet function testing will be performed with the VerifyNow
(Accumetrics Inc, San Diego, CA) point-of-care P2Y12 function assay within 30 min from blood
sample collection. Platelet reactivity results will be reported in P2Y12 reaction units (PRU)
and % inhibition. The % inhibition is calculated as: ([BASE−PRU]/BASE)×100. High platelet
reactivity (HPR) will be defined as ≥208 PRU.
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