Diabetes Mellitus Clinical Trial
Official title:
Effect of Modifying Anti-platelet Treatment to Ticagrelor in Patients With Diabetes and Low Response to Clopidogrel
In recent years numerous studies have shown that the response of patients to the
anti-platelet drug clopidogrel is widely variable. Furthermore, patients who do not respond
well to the drug ("resistant") have been shown to be at increased risk to develop cardiac
events, including myocardial infarction and mortality. It thus seems reasonable to test the
efficacy of the drug (by platelet function tests) and modify treatment accordingly. However,
a large study that examined a strategy of routine testing of clopidogrel response in
thousands of patients (GRAVITAS study) did not show any clinical benefit. This study was
limited, however, by a very low event rate (2.3%), and by the strategy employed to treat
patients with low response (increasing the clopidogrel dose), which is currently known to be
ineffective in many patients with low response. To overcome these limitations the
investigators plan to examine a high risk population - patients with diabetes planned to
undergo coronary angiography - and to treat clopidogrel low responders by switching their
treatment to the potent anti-platelet drug ticagrelor, which has been shown to overcome
clopidogrel low response.
The investigators hypothesize that patients with diabetes and low response to clopidogrel
will benefit clinically from switching therapy to ticagrelor. The main endpoint of the study
will be the risk of myocardial enzyme elevation following percutaneous coronary intervention
(PCI); a marker which has been strongly associated with poor clinical outcome.
The aim of the study is, therefore, to assess whether a strategy of monitoring platelet
function during clopidogrel treatment in patients with diabetes undergoing PCI, and
modifying treatment to ticagrelor in patients with low response, will be associated with
reduced risk of myocardial enzyme release.
The investigators plan to enroll patients with treated diabetes, planned to undergo coronary
angiography. Patients with acute or recent myocardial infarction will be excluded. They will
be tested for response to clopidogrel by the VerifyNow P2Y12 assay (either on chronic
clopidogrel treatment or 12-24 hours after receiving 300 mg clopidogrel). Patients with low
response to clopidogrel (≥ 208 PRU) will be randomized to either continued treatment with
clopidogrel (75 mg/day), or switching of treatment to ticagrelor (90 mg twice a day) for 30
days (followed by continued clopidogrel therapy). The primary endpoint will be the rate of
troponin of CK-MB (cardiac enzymes) measured 20-24 hours after the PCI. Secondary endpoints
will be the occurrence of adverse clinical endpoints - myocardial infarction, need for
urgent revascularization or mortality at 30 days. The investigators aim to enroll 100
patients in each study group (ticagrelor vs. continued clopidogrel). Assuming a clopidogrel
low response rate of 40% among patients with diabetes, about 500 patients would have to be
screened to identify 200 patients with low response.
BACKGOUND The concept of monitoring platelet reactivity in patients treated with clopidogrel
and tailoring treatment according to the results has been under intense debate in recent
years. There is clear and consistent evidence that there is wide variability in the
anti-platelet response to clopidogrel, and that patients with low response (more accurately
termed - high on treatment platelet reactivity) are at increased risk of adverse cardiac
events - mainly stent thrombosis and myocardial infarction. However, the only large
randomized trial that examined a strategy of routing monitoring of platelet reactivity and
response to clopidogrel and tailoring treatment accordingly (by increasing the clopidogrel
maintenance dose) - the GRAVITAS study - was negative. Thus, although from a physiological
perspective it seems reasonable to monitor the effects of a drug with such wide variability
(and poor prognosis associated with low response), clinical evidence in support of routine
monitoring is lacking. When analyzing the negative results of the GRAVITAS study, two main
factors should be discussed: a very low clinical adverse event rate (2.3% in each of study
the groups) probably reflecting a low risk patient population, and the strategy chosen to
overcome high on treatment platelet reactivity (HTPR) - increasing the maintenance
clopidogrel dose from 75 mg daily to 150 mg daily, which is currently known to be
ineffective in overcoming clopidogrel HTPR in many of the patients.
In light of these potential limitations of the GRAVITAS study the investigators propose a
study based on the following aspects:
1. A potent strategy to overcome clopidogrel HTPR - treatment with ticagrelor, which has
been clearly shown to overcome low response to clopidogrel.
2. Higher risk population - only patients with treated diabetes (shown in the BARI-2D
study to have a 10-12% rate of major cardiovascular events at 1 year).
3. Rather than a composite clinical endpoint, the primary endpoint will be the rate of
CK-MB or troponin elevation following percutaneous coronary intervention (PCI), which
has been consistently associated with a higher risk of cardiovascular adverse events,
and occurs at a rate of about 35% in patients with low response to clopidogrel.
The aim of the study is to assess whether a strategy of monitoring platelet reactivity
during clopidogrel treatment in patients with diabetes undergoing PCI, and modifying the
treatment to ticagrelor in patients with HTPR, is associated with a lower rate of myocardial
enzyme elevation following PCI.
METHODS
See inclusion and exclusion criteria in the following sections.
Patients treated chronically with clopidogrel 75 mg per day will undergo platelet function
testing under this treatment regimen. Patients who are clopidogrel naïve will be given 300
mg loading of clopidogrel and be tested about 12-24 hours after this loading dose. For all
patients, platelet function testing will be performed before the coronary angiography.
Platelet function testing will be performed with the VerifyNow P2Y12 assay (Accumetrics
Inc.), using a cutoff value of ≥ 208 reaction units to define HTPR.
Patients with HTPR will be randomized 1:1 to receive either ticagrelor or additional
clopidogrel.
Ticagrelor regimen: 180 mg given 1-2 hours before the coronary angiography, followed by 90
mg twice a day for 30 days in case PCI was performed. After 30 days the patient will be
invited to a special research clinic in the hospital and his treatment will be switched to
clopidogrel (with 300 mg loading, and 75 mg a day thereafter for 11 additional months - for
a total period of 1 year). The 30 day ticagrelor period was chosen because prior studies
have shown that platelet hyper-reactivity and low response to clopidogrel are prominent in
the first days after PCI, and subside significantly within 30 days after the procedure. In
addition, most cases of stent thrombosis occur in the first month following PCI.
Clopidogrel regimen: 300 mg given 1-2 hours before coronary angiography (in addition to the
previous 300 mg load or chronic clopidogrel therapy the patient received), followed by 75 mg
a day for 1 year case PCI was performed.
The investigators aim to enroll a total of 200 patients with HTPR who will undergo PCI - 100
patients in each group (ticagrelor vs. continued clopidogrel). Patients who will not undergo
PCI will be withdrawn from the study.
Choice of stent during PCI will be left to the operator's discretion, but given the diabetes
status of all patients, use of drug eluting stents will be encouraged. PCI will be performed
according to standard practice and operator preferences (regarding to access, pre- and post
dilatation etc.). Use of glycoprotein IIb/IIIa inhibitors will be discouraged, unless in
bailout situations. Patients who will receive glycoprotein IIb/IIIa inhibitors will be
excluded from the analysis.
An additional VerifyNow P2Y12 test will be performed in the 200 patients with initial HTPR,
20-24 hours following the PCI; at this time point troponin and CK-MB levels will also be
evaluated.
Primary endpoint: rate of elevation of troponin or CK-MB (above the upper limit of normal,
and above 3 times the upper limit of normal) measured 20-24 hours after the PCI.
Secondary endpoint: rate of major adverse cardiovascular endpoints including death,
myocardial infarction or urgent target vessel revascularization at 30 days.
Sample size calculation: assuming a rate of CK-MB or troponin elevation post-PCI of 35%
among patients with low response to clopidogrel, 100 patients in each group would allow
detection of a 50% difference in the primary endpoint between the groups (50% reduction in
myocardial enzyme elevation rate with ticagrelor), with an alpha of 0.05 and power of 0.80.
Assuming a HTPR rate of 40% using the 208 VerifyNow cutoff value, 500 patients would have to
be screened in order to identify 200 patients with HTPR (not taking into consideration the
patients that would not require PCI and be withdrawn from the study).
;
Allocation: Randomized, Endpoint Classification: Efficacy Study, Intervention Model: Parallel Assignment, Masking: Open Label, Primary Purpose: Treatment
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