The effects of alteplase 3 to 6 hours after stroke in the EPITHET-DEFUSE combined
dataset: post hoc case-control study.
Author(s): Ogata T(1), Christensen S, Nagakane Y, Ma H, Campbell BC, Churilov L, Lansberg
MG, Straka M, De Silva DA, Mlynash M, Bammer R, Olivot JM, Desmond PM, Albers GW,
Davis SM, Donnan GA; EPITHET and DEFUSE Investigators.
Affiliation(s): Author information:
(1)FRACP, Level 2 Alan Gilbert Bldg, 161 Barry St, Carlton S Victoria 3053,
Australia.
Publication date & source: 2013, Stroke. , 44(1):87-93
BACKGROUND AND PURPOSE: Two phase 2 studies of alteplase in acute ischemic stroke
3 to 6 hours after onset, Echoplanar Imaging Thrombolytic Evaluation Trial
(EPITHET; a randomized, controlled, double-blinded trial), and Diffusion and
Perfusion Imaging Evaluation for Understanding Stroke Evolution Study (DEFUSE;
open-label, treatment only) using MR imaging-based outcomes have been conducted.
We have pooled individual patient data from these to assess the response to
alteplase. The primary hypothesis was that alteplase would significantly
attenuate infarct growth compared with placebo in mismatch-selected patients
using coregistration techniques.
METHODS: The EPITHET-DEFUSE study datasets were pooled while retaining the
original inclusion and exclusion criteria. Significant hypoperfusion was defined
as a Tmax delay >6 seconds), and coregistration techniques were used to define MR
diffusion-weighted imaging/perfusion-weighted imaging mismatch. Neuroimaging,
parameters including reperfusion, recanalization, symptomatic intracerebral
hemorrhage, and clinical outcomes were assessed. Alteplase and placebo groups
were compared for the primary outcome of infarct growth as well for secondary
outcome measures.
RESULTS: From 165 patients with adequate MR scans in the EPITHET-DEFUSE pooled
data, 121 patients (73.3%) were found to have mismatch. For the primary outcome
analysis, 60 patients received alteplase and 41 placebo. Mismatch patients
receiving alteplase had significantly attenuated infarct growth compared with
placebo (P=0.025). The reperfusion rate was also increased (62.7% vs 31.7%;
P=0.003). Mortality and clinical outcomes were not different between groups.
CONCLUSIONS: The data provide further evidence that alteplase significantly
attenuates infarct growth and increases reperfusion compared with placebo in the
3- to 6- hour time window in patients selected based on MR penumbral imaging.
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