Myocardial Infarction Clinical Trial
Official title:
Evaluation of Ticagrelor Pharmacokinetics in Patients With Non-ST Elevation Myocardial Infarction After a 180 mg Ticagrelor Loading Dose
Patients with myocardial infarction, which does not include all layers of the heart's muscle
wall are common and they often receive pharmacological treatment with the platelet
inhibiting drug ticagrelor. However, the drug uptake after an oral dose of 180mg ticagrelor
has not been thoroughly studied in these patients.
The present study will evaluate ticagrelor uptake and platelet aggregation after a 180 mg
loading dose ticagrelor in these patients.
This study is to be considered as an observational prospective case-controlled study,
according to the Swedish Medical Product Agency (MPA), in response to our enquiry. This is
due to lack of intervention in routine medical treatment.
Patients with non-ST elevation myocardial infarction (NSTEMI) are common, but the
pharmacokinetic properties of ticagrelor in the acute phase have, to the best of our
knowledge, not been thoroughly studied in these patients.
The present study will evaluate ticagrelor uptake and platelet aggregation after a 180 mg
loading dose ticagrelor in NSTEMI patients and compare results with a control group of
patients with stable coronary artery disease.
Hypotheses/questions The stress reaction from suffering an NSTEMI causes delayed absorption
and possibly delayed and lowered maximal plasma concentrations after a loading dose
ticagrelor and thus a delayed and possibly impaired inhibition of platelet aggregation.
Method Study population Subjects eligible for the study will be ticagrelor naïve patients
with NSTEMI presenting at the emergency room at Södersjukhuset. Upon arrival to the
emergency room written informed consent will be obtained before the patients receive their
180 mg loading dose of ticagrelor if the responsible physician choses this therapy.
Inclusion criteria: 1) a diagnosis of NSTEMI (i.e relevant symptoms associated with ischemic
ECG changes (not categorized as STEMI) and/or relevantly increased cardiac markers); 2) an
indication for a 180 mg ticagrelor loading dose.
Control group Patients with stable coronary artery disease presenting at the cardiology
clinic at Södersjukhuset. A single 180 mg loading dose of ticagrelor will be administrated
if the responsible physician choses this therapy. Inclusion criteria. The inclusion
criterion for the control group will be documented stable coronary artery disease. Exclusion
criteria: 1) ACS within the last 3 months; 2) Age <18 years; 3)Administration of ticagrelor
during the week before inclusion; 4) Treatment with glycoprotein IIb/IIIa antagonists within
48 hours before inclusion; 5) Ongoing morphine treatment.
Study procedures and methods Samples of venous blood will be collected into lithium-heparin
tubes, centrifuged at 1500 g at 4ºC for 10 min within 30 min of blood sampling at the
following time points: pre-dose, 1, 2, 3, 4, 5, and 6 hours post-dose, as shown in the table
below. For P2Y12-antagonist naïve patients and controls, sampling of venous blood into
Hirudin tubes for pharmacodynamics evaluation will be performed for analysis using an
ADP-induced platelet aggregation assay (Multiplate®, Roche Diagnostics International Ltd,
Rotkreuz, Switzerland).
The resulting plasma samples will then be stored below minus 20ºC until analyzed. Plasma
concentrations of ticagrelor and its active metabolite AR-C124910XX will be determined by
validated methods (high-performance liquid chromatography and tandem mass spectrometry
detection; LC-MS/MS) at a certified laboratory (Covance Laboratories Inc.).
Statistical analysis The median Tmax in the control group with stable coronary artery
disease can be expected at approximately 2 hours after a 180 mg loading dose. The range of
the Tmax in patients with stable coronary artery disease receiving a 180mg loading dose was
between 1 and 8 hours. A rough standard deviation estimate of 1.25 hours was obtained from
this range using the formula (ln (maxTmax) - ln (minTmax))/k from a statistical textbook by
Dixon et al. A statistician estimated k to 9.5 from a natural distribution table. The
estimated standard deviation of 0.22 on the logarithm scale was then calculated using the
calculation above. For the study group with NSTEMI, a larger standard deviation can be
expected and was estimated with the following formula provided by the statistician:
sqrt((0.22^2 )× 2)) =0.31.
To make a sample size calculation possible, the above calculated standard deviations were
anti-logged using the exponential function and found to be 1.25 hours and 1.36 hours,
respectively.
For the power calculation, a 50% delay in median ticagrelor Tmax (1 hour delay) was
considered, as this can be regarded as a clinical significant difference. A power
calculation with the above described time to Tmax and estimated standard deviations, showed
that a study with 80% power would require 40 patients in the study group and 20 patients in
the control group.
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Observational Model: Case Control, Time Perspective: Prospective
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