Emergencies on direct oral anticoagulants: Management, outcomes, and laboratory effects of prothrombin complex concentrate

Roisin Bavalia; Rahat Abdoellakhan; Herm Jan M Brinkman; Marjolein P A Brekelmans; Eva N Hamulyák; Marleen Zuurveld; Barbara A Hutten; Peter E Westerweel; Renske H Olie; Hugo Ten Cate; Marieke Kruip; Saskia Middeldorp; Karina Meijer; Michiel Coppens

doi:10.1002/rth2.12336

Emergencies on direct oral anticoagulants: Management, outcomes, and laboratory effects of prothrombin complex concentrate

Res Pract Thromb Haemost. 2020 Apr 23;4(4):569-581. doi: 10.1002/rth2.12336. eCollection 2020 May.

Affiliations

¹ Department of Vascular Medicine Amsterdam Cardiovascular Sciences Amsterdam UMC University of Amsterdam Amsterdam The Netherlands.
² Department of Hematology University Medical Center Groningen University of Groningen Groningen The Netherlands.
³ Department of Molecular and Cellular Hemostasis Sanquin Research Amsterdam The Netherlands.
⁴ Department of Clinical Epidemiology, Biostatistics and Bioinformatics Amsterdam UMC University of Amsterdam Amsterdam The Netherlands.
⁵ Department of Internal Medicine Albert Schweitzer Hospital Dordrecht The Netherlands.
⁶ Department of Internal Medicine Maastricht University Medical Center+ Maastricht The Netherlands.
⁷ Department of Hematology Erasmus University Medical Center Rotterdam The Netherlands.

Abstract

Background: In the initial absence of specific reversal agents for factor Xa inhibitors (FXa-Is), prothrombin complex concentrate (PCC) as a hemostatic agent has been recommended by guidelines. Since 2017, idarucizumab has been registered for dabigatran reversal. Still, data on the clinical outcome of direct oral anticoagulant (DOAC)-related emergencies (major bleeding or urgent interventions) is scarce. In addition, it is unknown to what extent PCC restores thrombin generation in FXa-I-related emergencies. Our aim was to describe management and clinical outcomes of DOAC-related emergencies and to assess the laboratory effect of PCC in patients with FXa-I emergencies.

Methods: In this prospective cohort study in 5 Dutch hospitals, patients presenting with DOAC-related emergencies were eligible. The primary outcome was effective hemostasis according to the ISTH definition. Safety outcomes were 30-day mortality and thromboembolic rate. In patients treated with PCC, additional blood samples were taken to assess the effect on thrombin generation.

Results: We included 101 patients with major bleeding (FXa-I, 76; dabigatran, 25) and 21 patients requiring an urgent intervention (FXa-I, 16; dabigatran, 5). Of patients with major bleeding, 67% were treated with PCC or idarucizumab. Effective hemostasis, 30-day mortality, and thromboembolism rate were 67%, 22%, and 1%, respectively. In a subset of bleeding patients on FXa-I managed with PCC, thrombin generation increased, with 96% immediately after PCC administration. In patients requiring an urgent intervention, effective hemostasis, 30-day mortality, and thromboembolic rate were 95%, 14%, and 5%.

Conclusions: Effective hemostasis was achieved in the majority of patients presenting with DOAC-related emergencies;, thromboembolic complications were rare, and mortality was quite high.

Keywords: dabigatran; emergencies; factor Xa inhibitors; hemorrhage; idarucizumab; prothrombin complex concentrates.