Intracranial bleeding under vitamin K antagonists or direct oral anticoagulants: results of the RADOA registry
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Published:2022-05-02
Issue:1
Volume:4
Page:
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ISSN:2524-3489
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Container-title:Neurological Research and Practice
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language:en
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Short-container-title:Neurol. Res. Pract.
Author:
Pfeilschifter WaltraudORCID, Lindhoff-Last Edelgard, Alhashim Ali, Zydek Barbara, Lindau Simone, Konstantinides Stavros, Grottke Oliver, Nowak-Göttl Ulrike, von Heymann Christian, Birschmann Ingvild, Beyer-Westendorf Jan, Meybohm Patrick, Greinacher Andreas, Herrmann Eva,
Abstract
Abstract
Background and purpose
The use of direct oral anticoagulants (DOAC) has increased sharply and DOAC are the oral anticoagulant therapy (OAT) of choice for the majority of patients with newly-diagnosed atrial fibrillation. Intracranial hemorrhage is the most severe adverse event of OAT. Systematic data on the course of intracranial hemorrhage under DOAC compared to vitamin K antagonists (VKA) are warranted to enable shared decision making in AF patients needing OAT.
Methods
This is a secondary analysis of the patients with intracranial bleedings from the prospective multicenter emergency department-based RADOA registry, which collected data on patients admitted with major bleeding while taking VKA or DOAC. The primary endpoint was in-hospital mortality until day 30. We evaluated hematoma volume and short-term clinical outcomes in relation to the extent of active OAT according to coagulation parameters and OAT plasma levels measured by UPLC-MS/MS.
Results
Of 193 patients with major bleeding, 109 (56.5%) had intracranial hemorrhage [52.3% intracerebral (ICH), 33.9% subdural (SDH), 11.0% subarachnoidal (SAH)]. 64 (58.7%) were on VKA and 45 (41.2%) were on DOAC. On admission, we could confirm active anticoagulation in 97.7% of VKA-treated patients based on either INR > 1.3 or phenprocoumon levels and in 75.8% of DOAC-treated patients based on DOAC levels. Patients suffering an intracranial hemorrhage under VKA showed significantly larger hematoma volumes and a higher in-hospital mortality. Especially in intracerebral hemorrhage, we observed a higher initial severity and numerically greater proportion of early changes towards palliative therapy under VKA, which coincided with a numerically higher case fatality.
Conclusions
We show significantly smaller hematoma volumes for ICH and SDH under DOAC in comparison to VKA and a significantly lower 30-day in-hospital mortality rate of DOAC-ICH, even before the introduction of specific antidotes. These data strongly support the use of DOAC whenever possible in patients requiring OAT.
Trial Registration: http://www.clinicaltrials.gov; Unique identifier: NCT01722786.
Funder
Bayer Bristol-Myers Squibb Daiichi-Sankyo CSL Behring
Publisher
Springer Science and Business Media LLC
Subject
Automotive Engineering
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