Ischemic Stroke Clinical Trial
Official title:
Cerebral Microbleeds as Predictor of Future Intra-Cerebral Hemorrhage During NOACs or Warfarin Therapy in NVAF Patients With Acute Ischemic Stroke (CMB-NOW)
Anticoagulants are generally recognized as a necessary therapy to prevent the recurrence of
ischemic stroke in patients with non-valvular atrial fibrillation (NVAF), but in some
patients they also cause bleedings, particularly intracranial hemorrhage. One of the
independent predictors of intracerebral hemorrhage is the presence of cerebral microbleeds
(CMBs); a high incidence of intracerebral hemorrhage is reported in patients with multiple
CMBs. Recent study suggested that patients who had CMBs at baseline developed more new CMBs
after 2 years (26%), compared with patients (12%) who did not have CMBs at baseline.
However, there has been no study on the progression of CMBs in patients receiving so-called
novel oral anticoagulants (NOACs).
This study tests the hypothesis that the incidence of hemorrhagic stroke is lower in
patients receiving NOACs (dabigatran, rivaroxaban, apixaban, and edoxaban) than in those
receiving warfarin, and this difference reflects the difference in the effects of warfarin
and NOACs on the progression of CMBs. Towards this goal, we enroll 200 patients with at
least one CMB detected by 1.5 T MRI (T2*WI) at baseline, who treated with NOACs or warfarin
for 12 months. Primary endpoint is the proportion of subjects with an increased number of
CMBs at Month 12 of treatment with NOACs or warfarin. If the results of this study support
the efficacy of NOACs in preventing increase of CMBs, this would be of great interest to
domestic and overseas clinicians, in view of the potential therapeutic impact, including
that for primary prevention of ischemic stroke.
1. Introduction Anticoagulants are generally recognized as a necessary therapy to prevent
the recurrence of ischemic stroke in patients with non-valvular atrial fibrillation
(NVAF), but in some patients they also cause bleedings, particularly intracranial
hemorrhage (including intracerebral hemorrhage). One of the independent predictors of
intracerebral hemorrhage is the presence of cerebral microbleeds (CMBs); a high
incidence of intracerebral hemorrhage is reported in patients with multiple CMBs (Soo
et al, J Neurol, 2008; Lee et al, Neurology, 2009) Also, the rate and absolute number
of CMBs increase in proportion to CHADS2 score in patients with cerebral infarction
accompanying NVAF (Song et al, Eur J Neurol, 2013). Among CMB-positive patients, a high
incidence of intracranial hemorrhage associated with oral anticoagulation therapy has
been reported (Song et al, Eur J Neurol, 2013); suggesting a relationship between the
occurrence or absolute number of CMBs and the development of intracranial hemorrhage
during oral anticoagulation therapy. Imaizumi et al. (J Stroke Cerebrovasc Dis, 2013)
found that warfarin alone did not increase the incidence of intracerebral hemorrhage in
all subjects with CMBs, but subjects with 3 or more deep CMBs did show an increased
incidence. Also, a meta-analysis conducted by Lovelock et al. (Stroke, 2010)
demonstrated a higher incidence of CMBs in patients with intracerebral hemorrhage
receiving warfarin than in patients with intracerebral hemorrhage not receiving
antithrombotic therapy. Recently, Orken et al (Clin Neurol Neurosurg, 2013) suggested
that patients who had CMBs at baseline developed more new CMBs after 2 years (26%),
compared with patients (12%) who did not have CMBs at baseline (p=0.03). However, there
has been no study on the progression of CMBs in patients receiving so-called novel oral
anticoagulants (NOACs).
NOACs, including dabigatran (Hart et al, Stroke 2012), rivaroxaban (Patel et al, N Engl
J Med 2011), apixaban (Granger CB et al, N Engl J Med 2011), and edoxaban (Giugliano et
al, N Engl J Med 2013), are superior to warfarin in preventing stroke or systemic
embolism in patients with NVAF, and have been reported to significantly reduce the
incidence of hemorrhagic stroke. Therefore, this study was designed to evaluate and
compare the absolute number of CMBs in patients with at least one CMB at baseline, who
receive anticoagulant therapy with NOACs and with warfarin. The correlation between
CMBs and intracranial hemorrhage, as well as the status of CMBs before commencement of
treatment and their progression during treatment, will be evaluated to determine
whether there are differences between the two groups.
2. The feature of this study Japan has a very high availability of MRI facilities, and
thus CMBs can be readily evaluated in multiple patients using T2*WI. As of January 1,
2013, the total population of Kanagawa Prefecture was 9.07 million, of whom the elderly
(≥65 years) comprised 1.95 million; therefore, a clinical observational study covering
this prefecture that revealed a significant difference between NOACs and warfarin
should have a substantial impact on drug-prescribing practice.
CMBs found on T2*-weighted gradient-echo MRI 1.5 Tesla should be evaluated. The imaging
data will be evaluated by the Cerebral Microbleeds Evaluation Committee using the
assessment scale of Gregoire et al. under a blinded condition.
3. Study design This study tests the hypothesis that the incidence of hemorrhagic stroke
is lower in patients receiving NOACs than in those receiving warfarin, and this
difference reflects the difference in the effects of warfarin and NOACs on the
progression of CMBs in patients with at least one CMB.
This study is an observational study, and the numbers of patients in the NOACs and
warfarin groups were not predetermined, though the total number of patients for the
study was limited to 200 for practical reasons. Primary endpoint is the proportion of
subjects with an increased number of CMBs at Month 12 of treatment with NOACs or
warfarin. If the results of this study support the efficacy of NOACs in preventing
increase of CMBs, this would be of great interest to domestic and overseas clinicians,
in view of the potential therapeutic impact, including that for primary prevention of
ischemic stroke.
For quality assurance, data validation and registry procedures including any plans for
site monitoring and auditing is performed.
4. Sample Size and Sample Size Justification Orken et al. (Clin Neurol Neurosurg, 2013)
suggested that more patients who had CMBs at baseline developed new CMBs (26%) after 2
years, compared with patients (12%) who did not have CMBs at baseline. Therefore, the
rate of new CMBs in warfarin-treated patients who had at least one CMB at baseline was
assumed to be 13% in 1-year follow-up. Meanwhile, in the ENGAGE AF-TIMI study, the
incidence of intracranial hemorrhage among patients receiving edoxaban (one of the
NOACs) was about half of that in patients receiving warfarin; the rate of appearance of
new CMBs was assumed to be 6.5%. Simulations (10,000 times) indicated that the
probability that the rank order of the rate of newly developed CMBs in 1 year would not
be reversed between the two groups was 92.7% (power: 19%, two-sided α= 0.05). As this
is a pilot study, the number of necessary subjects was estimated to be 100 subjects in
1 group and 200 in 2 groups combined, based on the above results.
5. Statistical Analysis plan For proportion with new CMBs at month 6 and at month 12,
number of new CMBs at months 6 and 12, and location of CMBs, major analyses will be
conducted according to the per protocol set (PPS) principle. In addition, for incidence
rate of adverse events, major analyses will be conducted according to the intention to
treat (ITT) principle. As the primary endpoints analyses (proportion with new CMBs at
month 12), the NOACs group and the warfarin group will be compared with respect to
total CMBs positive proportion. It' will be also compared between the NOACs group and
the warfarin group about the respective secondary endpoints (proportion with new CMBs
at month 6, number of new CMBs at months 6 and 12, location of CMBs, incidence rate of
adverse events). Proportion of subjects with an increased number of CMBs at month 12 is
compared among NOACs. As the need arises, such as the comparison among NOACs, it will
be stratified by the factors which are a patient background, the treatment contents and
etc., and will be analyzed.
;
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