Coronary Stenting Clinical Trial
Official title:
Randomized Comparison of PPI Versus no PPI on Top of Standard Dose Clopidogrel Therapy in Patients Stratified Based on CYC2C19 Activity Via a Genetic Point of Care System.
This study aims to prospectively assess whether there is an interaction between genetic status in terms of 2C19 activity and residual platelet reactivity after clopidogrel intake in patients who underwent coronary stenting for elective, urgent or emergent intervention.
In managing patients who undergo percutaneous coronary intervention (PCI), rapid and
predictable platelet inhibition for all patients is an important therapeutic goal.
Determining the optimal dose of antiplatelet therapy to achieve this goal has been hampered
by considerable interpatient variability in response to clopidogrel, which largely reflects
gene polymorphism. Most of the evidence is centred around cytochrome 450 2C19.
A substudy of TRITON TIMI 38 has recently shown that among persons treated with clopidogrel,
carriers of a reduced-function CYP2C19 allele had significantly lower levels of the active
metabolite of clopidogrel, diminished platelet inhibition, and a higher rate of major
adverse cardiovascular events, including stent thrombosis, than did noncarriers (N Engl J
Med 2009;360:354-62). As a contrary, common functional CYP genetic variants do not affect
active drug metabolite levels, inhibition of platelet aggregation, or clinical
cardiovascular event rates in persons treated with prasugrel (Circulation. 2009 May
19;119(19):2553-60).
More recently, it has been shown that CYP2C19*17 carrier status is significantly associated
with enhanced response to clopidogrel and an increased risk of bleeding. (Circulation.
2010;121:512-518). Whether CYP2C19*17 carrier status enhances response to prasugrel is
unknown.
Attention has also been placed on a potential interaction observed between clopidogrel and
the widely used proton pump inhibitors (PPIs).
The CYP2C19 isoform is the key enzyme in the metabolism of many of the PPIs, which are also
inhibitors of the CYP2C19 isoenzyme in varying degrees. This is important because the
antiplatelet effects of clopidogrel rely, to a degree, upon CYP2C19 activity. However, the
recent COGENT study and sub-analysis of the TRITON-TIMI 38 have both apparently mitigated
this concern. Nevertheless, it is unknown whether PPI can father blunt response to
clopidogrel especially in patients carrying the loss of function 2C19 allele.
A recent review paper (Aliment Pharmacol Ther 31, 810-823) included 23 studies covering
93,278 patients. There was substantial heterogeneity in the meta-analyses of major
cardiovascular events (19 studies, I2 = 79%) or myocardial infarction (12 studies, I2 =
77%). Analysis of propensity-matched or randomized trial participants showed no associated
cardiovascular risk with PPIs, whereas other observational studies generally showed a
significant association.
Thus, still today there is an emerging need for more studies, especially prospective
randomized studies, to investigate the effect of individual PPI agents on clopidogrel's
effectiveness. Such studies should also include a genetic component to stratify response
based on the presence of reduced-function alleles of the CYP2C19 enzyme
;
Allocation: Randomized, Endpoint Classification: Pharmacodynamics Study, Intervention Model: Parallel Assignment, Masking: Single Blind (Outcomes Assessor), Primary Purpose: Treatment
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