Cardiovascular Diseases Clinical Trial
Official title:
Hunting for the Off-Target Properties of Ticagrelor on Endothelial Function and Other Circulating Biomarkers in Humans
The purpose of this randomized, cross-over study, is to ascertain if ticagrelor, but not prasugrel or clopidogrel, is associated to an improved endothelial function as assessed with peripheral arterial tonometry and markers of endothelial function measurement in post-ACS patients.
Extensive literature documents that endothelial dysfunction is associated with almost every
condition predisposing to atherosclerosis and cardiovascular disease. Hence, endothelial
dysfunction is significantly associated with the burden of cardiovascular risk and can be
considered a barometer of the total risk burden. Importantly, microvascular dysfunction has
been shown to increase risk of future cardiovascular events.
This study aims to clarify if ticagrelor, but not prasugrel or clopidogrel is associated to
an improved reactive hyperemia index (RHI) and circulating levels of specific biomarkers of
endothelial function, at treatment steady state. Ticagrelor has previously been demonstrated
to increase adenosine levels by inhibiting adenosine reuptake in red blood cells, by
inhibiting the equilibrative nucleoside transporter (ENT)-1. Furthermore, ticagrelor can
induce adenosine triphosphate (ATP) release from human red blood cells. Interestingly,
ticagrelor, but not clopidogrel or prasugrel have been recently shown to be associated to an
improved endothelial function as evaluated with peripheral arterial tonometry after forearm
ischemia.
Post-ACS patients (who experienced an acute coronary syndrome and thereby started therapy
with an oral P2Y12 inhibitor at least 30 days before) will be consecutively screened for
possible inclusion. Patients will then be randomised to receive in a sequential manner the
three oral P2Y12 blockers (i.e.) ticagrelor, prasugrel or clopidogrel for at least 30 days
each, according to a balanced cross-over study design including the sequences below:
Seq\ Per P.I P.II P.III S.I T P C S.II T C P S.III P T C S.IV P C T S.V C T P S.VI C P T
During the three months study period the therapy with the P2Y12 inhibitor will be switched
as for randomization sequence scheme.
When started, each drug will be given with the corresponding loading dose of 600 mg for
clopidogrel and then continued at 75 mg/day, 180 mg for ticagrelor and then continued at 90
mg b.i.d. and 60 mg for prasugrel and then continued at 10 mg/day (5 mg/day for patients ≥75
years or weighing ≤ 60 kg).
The main measurements, including reactive hypermedia index, PRU, aspirin reaction units, and
circulating markers of endothelial function will be performed at baseline, after
P2Y12-inhibitor loading dose, before and after P2Y12-inhibitor maintenance dose.
During the visit, blood pressure will be measured in the contralateral arm before
examination. The EndoPAT probes will be placed on the index fingers. If the index finger
will be missing or deformed, another finger will be used, using the same finger on both
hands. Baseline registration will be conducted for 5 min. The test arm will be then occluded
for 5 min, using a standard blood pressure cuff placed on the upper arm. Subsequently, the
cuff was deflated and the registration continued for 5 more minutes. After EndoPAT, blood
will be drawn to collect serum and plasma for biomarkers assessment [Asymmetrical
dimethylarginine (ADMA), adenosine plasma concentration, von willebrand factor antigen,
endothelin-1, C-reactive protein, soluble fms-like tyrosine kinase-1 (sFLT-1), intercellular
cell adhesion molecule-1 (ICAM-1), vascular cell adhesion molecule-1 (VCAM-1), prothrombin
fragment 1+2, fibrinopeptide A, and thrombin-antithrombin complex (TAT)]. To assess the
relationship between residual platelet reactivity or percent inhibition and effect of P2Y12
oral blocker on endothelial function, platelet function testing will be also carried out
acutely and at treatment steady state by means of the Verifynow system using both P2Y12 and
aspirin assays.
Based on previous findings, we set mean RHI at 1.8 with a within subjects SD of 0.31. Hence,
36 patients completing all sequences (i.e. 6 pt/sequence) will provide 90% power to detect a
10% RHI relative change in the ticagrelor group with a two-sided alpha level at 5%. To
account for drop outs as well as incomplete data assessment at all time points, a final
sample size of 50 patients will be recruited.
Patients will be provided with a regular drug prescription (standard of care medication). At
each follow-up the investigator will collect information about adherence to the study drug
and register the charge number of the prescribed P2Y12.
Allocation of study treatment will be performed via a web-based interactive randomization
system, based on a computer-generated random sequence with a random block size stratified
according to the type of P2Y12 inhibitor (ticagrelor vs prasugrel vs clopidogrel) as well as
for the presence of diabetes mellitus.
Adverse events are defined as any undesirable experience occurring to a subject during the
study, whether or not considered related to study. All adverse events reported spontaneously
by the subject or observed by the investigator or his staff will be recorded. Serious
adverse events in this study are considered to be extremely rare.
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