1.Acute Ischemic Stroke in Nonconvulsive Status Epilepticus–Underestimated? Results from an Eight-Year Cohort Study.
Christopher TRAENKA ; Gian Marco De MARCHIS ; Lisa HERT ; David J SEIFFGE ; Alexandros POLYMERIS ; Nils PETERS ; Leo H BONATI ; Stefan ENGELTER ; Philippe LYRER ; Stephan RÜEGG ; Raoul SUTTER
Journal of Stroke 2017;19(2):236-238
No abstract available.
Cohort Studies*
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Stroke*
2.Intravenous Thrombolysis in Patients with Stroke Taking Rivaroxaban Using Drug Specific Plasma Levels: Experience with a Standard Operation Procedure in Clinical Practice.
David J SEIFFGE ; Christopher TRAENKA ; Alexandros A POLYMERIS ; Sebastian THILEMANN ; Benjamin WAGNER ; Lisa HERT ; Mandy D MÜLLER ; Henrik GENSICKE ; Nils PETERS ; Christian H NICKEL ; Christoph STIPPICH ; Raoul SUTTER ; Stephan MARSCH ; Urs FISCH ; Raphael GUZMAN ; Gian Marco DE MARCHIS ; Philippe A LYRER ; Leo H BONATI ; Dimitrios A TSAKIRIS ; Stefan T ENGELTER
Journal of Stroke 2017;19(3):347-355
BACKGROUND AND PURPOSE: Standard operating procedures (SOP) incorporating plasma levels of rivaroxaban might be helpful in selecting patients with acute ischemic stroke taking rivaroxaban suitable for IVthrombolysis (IVT) or endovascular treatment (EVT). METHODS: This was a single-center explorative analysis using data from the Novel-Oral-Anticoagulants-in-Stroke-Patients-registry (clinicaltrials.gov:NCT02353585) including acute stroke patients taking rivaroxaban (September 2012 to November 2016). The SOP included recommendation, consideration, and avoidance of IVT if rivaroxaban plasma levels were < 20 ng/mL, 20‒100 ng/mL, and >100 ng/mL, respectively, measured with a calibrated anti-factor Xa assay. Patients with intracranial artery occlusion were recommended IVT+EVT or EVT alone if plasma levels were ≤100 ng/mL or >100 ng/mL, respectively. We evaluated the frequency of IVT/EVT, door-to-needle-time (DNT), and symptomatic intracranial or major extracranial hemorrhage. RESULTS: Among 114 acute stroke patients taking rivaroxaban, 68 were otherwise eligible for IVT/EVT of whom 63 had plasma levels measured (median age 81 years, median baseline National Institutes of Health Stroke Scale 6). Median rivaroxaban plasma level was 96 ng/mL (inter quartile range [IQR] 18‒259 ng/mL) and time since last intake 11 hours (IQR 4.5‒18.5 hours). Twenty-two patients (35%) received IVT/EVT (IVT n=15, IVT+EVT n=3, EVT n=4) based on SOP. Median DNT was 37 (IQR 30‒60) minutes. None of the 31 patients with plasma levels >100 ng/mL received IVT. Among 14 patients with plasma levels ≤100 ng/mL, the main reason to withhold IVT was minor stroke (n=10). No symptomatic intracranial or major extracranial bleeding occurred after treatment. CONCLUSIONS: Determination of rivaroxaban plasma levels enabled IVT or EVT in one-third of patients taking rivaroxaban who would otherwise be ineligible for acute treatment. The absence of major bleeding in our pilot series justifies future studies of this approach.
Arteries
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Hemorrhage
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Humans
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National Institutes of Health (U.S.)
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Plasma*
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Rivaroxaban*
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Stroke*