4.7 Article

Early apixaban therapy after ischemic stroke in patients with atrial fibrillation

Journal

JOURNAL OF NEUROLOGY
Volume 268, Issue 5, Pages 1837-1846

Publisher

SPRINGER HEIDELBERG
DOI: 10.1007/s00415-020-10335-2

Keywords

Atrial fibrillation; Ischemic stroke; Hemorrhagic transformation; Apixaban; Cardioembolic stroke; Intracerebral hemorrhage

Funding

  1. Pfizer Canada
  2. Canada Research Chairs Program
  3. Heart and Stroke Foundation of Alberta, Northwest Territories and Nunavut

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This study aimed to assess the impact of early anticoagulation on hemorrhagic transformation in atrial fibrillation (AF) patients after stroke. The results showed that early apixaban treatment did not lead to symptomatic HT, with all HT being asymptomatic on imaging. Recurrent ischemic events were common and clinically symptomatic.
Background The optimal timing of anticoagulation after stroke in patients with atrial fibrillation (AF) is unknown. We aimed to objectively assess the rate of radiological hemorrhagic transformation (HT) associated with early anticoagulation. Patients and methods A prospective, open label study (NCT04435418) of patients with AF treated with apixaban within 14 days of ischemic stroke/TIA onset was conducted. Baseline and follow-up CT scans were assessed for HT and graded using European Cooperative Acute Stroke Study (ECASS) criteria. The primary endpoint was symptomatic HT. Incident HT rates were assessed as Objective Performance Criteria. Results One-hundred AF stroke patients, with a mean age of 79 +/- 11 years were enrolled. Median infarct volume was 4 (0.5-10.75) ml. Median time from index event onset to apixaban initiation was 2 (1-6) days, and median baseline NIHSS was 4 (1-9). Asymptomatic HT on baseline imaging was present in 15 patients. Infarct volume (OR = 1.1, [1.02-1.12], p < 0.0001) and NIHSS (OR = 1.11, [1.03-1.20], p = 0.007) were both associated with baseline HT. No patients developed symptomatic HT or systemic hemorrhage. Incident asymptomatic HT was seen on follow-up CT scan in 3 patients. Patients with incident HT were functionally independent (mRS = 0-2) at 90 days. Recurrent ischemic events occurred within 90 days in 13 patients, 4 of which were associated with severe disability (mRS 3-5) and 4 with death. Discussion Early apixaban treatment did not precipitate symptomatic HT after stroke. All HT was asymptomatic identified on imaging. Recurrent ischemic events were common and clinically symptomatic. Conclusions Symptomatic HT rates are likely to be low in randomized trials of DOAC initiation post-stroke. Recurrent ischemic stroke may be the major clinical outcome. These data may be used as expected event rates when calculating sample size requirements for future safety/efficacy trials of early versus late DOAC initiation after AF-related stroke.

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