Ischemic Stroke Clinical Trial
Official title:
Clopidogrel Response and CYP2C19 Genotype in Ischemic Stroke Patients
Personalized therapy as prophylaxis in ischemic stroke patients is not yet an option. From patients with ischemic heart disease, we know that patients with in vitro high on treatment platelet reactivity (HTPR) have an increased risk of stent thrombosis following per-cutaneous coronary intervention. Other studies have shown association of CYP2C19 genotypes with different responses to the anti platelet drug Clopidogrel. We measure HTPR in ischemic stroke patients on increasing doses of clopidogrel and investigate the CYP2C19 genotype for each patient.
Background: Clopidogrel (CLO) is a pro-drug metabolized in the liver by the Cytochrom-P450
system to its active component. Studies in acute ischemic stroke (IS) patients have proven
that genetic differences in coding of an enzyme responsible for the metabolism of CLO
(CYP2C19) results in different response to CLO when tested in the blood. An American study in
cardiac patients have shown an association between the genotype and the CLO-response to
different dosages of CLO, meaning that patients who are non-responders to low dosages of CLO
may be responders to higher CLO dosages. Furthermore, the study showed that patients with a
distinct genotype does not gain CLO response even at high CLO dosages (300 mg/day).
Perspective: The study will have an impact on the patient, the relatives and the social
economy. The project answers if it is possible to give personalized therapy to IS patients
securing the best possible prophylactic treatment for each single patient. Hereby reducing
the risk of early death, disability and dependency. The project determines the genetic
distribution of CYP2C19 alleles in the Danish IS population and determine the association
between genotype and CLO-response in clinically relevant dosages in a Caucasian population of
IS patients.
Objective: To determine the correlation between genotype and Clopidogrel response to
different CLO dosage and to determine the distribution of different alleles of CYP2C19
genotypes in a Danish IS population.
Hypothesis: CLO response is determined by CYP2C19 genotype, and there is a correlation
between drug-response and CYP2C19 genotype.
Method: Systematic recording of data on 103 IS patients receiving prophylactic treatment with
CLO 75 mg/day.
Genotype is determined in collaboration with Division of Clinical Biochemistry, Dept. of
Diagnostics, Glostrup Hospital determining the CYP2C19 genotype *1(wild-type), *2(Loss Of
Function=LOF) and *17(Gain Of Function=GOF). CLO responder status is determined using the
VerifyNow P2Y12 assays.
Patients receiving CLO 75 mg/day who are non-responders when testing with VerifyNow P2Y12
assays have a blood sample for genetic testing. Patients carrying the *2 genotype on one or
both alleles are CLO responder status tested on increasing doses of CLO, rising 75 mg/day
every 14 days (150/225/300 mg) until maximum CLO 300 mg/day. Responder status is tested at
the end of every second week, before increasing dosage. If the patient is CLO responder on
the tested dose (150/225/300 mg) or non-responder on CLO 300 mg/day, the patient is ended in
the study and switched to treatment with ASA in combination with Dipyramidole.
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