Transient Ischemic Attack Clinical Trial
Official title:
Dabigatran Treatment Following Transient Ischemic Attack and Minor Stroke
Objective: Demonstrate the safety of early use of dabigatran following TIA/minor stroke.
Background: Although aggressive antithrombotic therapy has been shown to reduce the number
of new ischemic events following stroke/TIA, this has always been offset by an increase in
the risk of hemorrhagic transformation. Dabigatran is much safer than previously tested
antithrombotic agents, with respect to intracranial bleeding and therefore offers a unique
treatment opportunity in these high-risk patients. TIA/minor stroke represent the largest
group of cerebrovascular disease patients. A short-term intervention such as 30 days of
dabigatran treatment has the potential for a very large impact from the population health
perspective, given the number of patients who may be treated if a benefit can be
demonstrated.
Study design:
This is an open label, single arm study. Patients with TIA/minor stroke (National Institutes
of Health Stroke Scale (NIHSS) score </=3) who can be treated within 24 hours of symptom
onset will be eligible. All patients will be treated with dabigatran for 30 days. The dose
of dabigatran will be determined by age and renal function (patients >80 years old and/or
with GFR 30-50 ml/min will received 110 mg bid, and all other patients will receive 150 mg
BID).The primary endpoint is symptomatic hemorrhagic transformation. Patients (n=50) with
TIA/minor stroke, defined as having a National Institutes of Health Stroke Scale Score of
</=3, will undergo an MRI, including diffusion-weighted imaging (DWI), as well as gradient
recall echo (GRE) sequences, which will be used to assess for hemorrhagic transformation.
Patients will have a repeat MRI examination at 7 and 30 days to assess for hemorrhagic
transformation and new lesion development. The primary endpoint of of phase I is symptomatic
hemorrhagic transformation, defined as a parenchymal hematoma on the day 7 MRI scan (GRE
sequence), associated with clinical worsening (>/=4 point increase in National Institutes of
Health Stroke Scale (NIHSS) score).
If dabigatran can be used safely in this population, a second phase aimed at demonstrating
the rate of new ischemic lesion development following TIA can be reduced with aggressive
antithrombotic therapy. A randomized open-label, blinded endpoint evaluation design will be
employed. The investigators hypothesize that dabigatran therapy administered within 24 hours
of symptom onset will reduce the rate of new ischemic lesions, relative to standard care,
one week and 30 days after onset.
Background: A transient ischemic attack (TIA) has traditionally been defined as a focal
neurologic deficit lasting less than 24 hours, but alternative definitions based on tissue
injury have been more recently proposed.1 This clinical definition has been based on the
assumption that TIAs are associated with complete resolution of brain ischemia occurring
rapidly enough to cause only transient symptoms and no permanent brain injury, i.e. stroke.
A recently completed MRI research study at the University of Alberta indicates that TIA and
minor stroke actually represent a continuum of symptoms secondary to brain ischemia.2 There
is also substantial evidence that the period shortly after a TIA or minor stroke is one of
elevated recurrent stroke risk; as high as 17% at 3 months.3, 4 We have previously reported
that MRI markers of new infarction are actually present within 7 days of the index event in
18% of patients.2 TIA and minor stroke can therefore be seen as a sentinel warning for
impending major stroke, which offers a potential window for therapeutic intervention. Given
the large number of patients who suffer a TIA/minor stroke, it is important to identify and
target those patients at highest risk for early recurrence.
Treatment of Minor Stroke/TIA: A logical approach to prevent early recurrence is aggressive
hyperacute antithrombotic therapy following TIA/minor stroke, as is now the standard of care
in acute coronary syndrome management. This treatment strategy is aimed at preventing both
recurrent thromboembolism and propagation of existing thrombi. In acute coronary syndrome
patients, antithrombotic therapy consists of both anticoagulants (low molecular weight
heparin) and combination antiplatelet agents (ASA+high dose clopidogrel, or more recently
prasugrel/ticagrelor). In ischemic stroke patients the benefits of traditional
anticoagulants, particularly heparin, have been consistently offset by an increased
incidence of intracranial hemorrhagic complications.5 Combination antiplatelet therapy is
sometimes used empirically following TIA/minor stroke, although this may not be an ideal
approach either. A previous trial in 392 patients demonstrated a trend towards reduction of
recurrent events by day 90 when patients were treated with a combination of ASA and
clopidogrel for 90 days (Absolute Risk Reduction = 3.3% [95% CI -1.9, 9.4]), but this was
also complicated by excess hemorrhagic events.
The direct thrombin inhibitor dabigatran is a very effective antithrombotic agent that has
been shown to be superior to warfarin in the prevention of cardioembolic ischemic stroke.
Dabigatran is unique in that unlike other antithrombotic drugs studied in cerebrovascular
disease, it appears to be associated with a much lower risk of intracranial hemorrhagic
complications, including intracerebral and subdural hemorrhages.7 This therefore appears to
be an ideal drug for treatment of acute cerebrovascular syndrome patients.
MRI as a Surrogate Outcome Marker in TIA/Minor Stroke: Our previous serial MRI study
indicates that the rate of new DWI lesion development in a TIA and minor stroke population
is 22% at 30 days and more importantly 92% of these lesions developed within the first 7
days after the initial symptoms.2 The majority (90%) of patients who developed new lesions
had baseline DWI lesions and all had areas of hypoperfusion evident on perfusion images.
Thus stroke 'recurrence' in fact appears to represent completion of the natural history of
an acute cerebrovascular syndrome. Having identified this high-risk group of patients, we
now aim to reduce the rate of development of new lesions. DWI lesion load has been shown to
be highly predictive of neurological and functional recovery following ischemic stroke,
making this an ideal surrogate outcome marker in smaller phase IIa studies.
The investigators have designed a two-phase study aimed at demonstrating the safety (phase
I) and efficacy (phase II) of acute dabigatran treatment following TIA/minor ischemic
stroke. Phase I is described below. The final design of phase II will be dependent on the
results of Phase I.
Study Aim and Design Phase I: The primary aim of phase I is to demonstrate the safety of
early use of dabigatran following TIA/minor stroke. Phase I is an open label, single arm
study. Patients with TIA/minor stroke (National Institutes of Health Stroke Scale (NIHSS)
score >/=3) who can be treated within 24 hours of symptom onset will be eligible. All
patients will be treated with dabigatran for 30 days. The dose of dabigatran will be
determined by age and renal function (patients >80 years old and/or with GFR 30-50 ml/min
will received 110 mg bid, and all other patients will receive 150 mg BID).The primary
endpoint is symptomatic hemorrhagic transformation. Patients (n=50) with TIA/minor stroke,
defined as having a National Institutes of Health Stroke Scale Score of </=3, will undergo
an MRI, including diffusion-weighted imaging (DWI), as well as gradient recall echo (GRE)
sequences, which will be used to assess for hemorrhagic transformation. Patients will have a
repeat MRI examination at 7 and 30 days to assess for hemorrhagic transformation and new
lesion development. The primary endpoint of of phase I is symptomatic hemorrhagic
transformation, defined as a parenchymal hematoma on the day 7 MRI scan (GRE sequence),
associated with clinical worsening (>/=4 point increase in National Institutes of Health
Stroke Scale (NIHSS) score).
Sample Size: Phase I is an open label, single arm study. The primary endpoint is symptomatic
hemorrhagic transformation. A total of 50 patients will be treated with dabigatran. A priori
stopping rules, based on the expected number of patients experiencing hemorrhagic
transformation in a group this size, will be employed.
;
Endpoint Classification: Safety Study, Intervention Model: Single Group Assignment, Masking: Open Label, Primary Purpose: Treatment
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