Case series of massive direct oral anticoagulant ingestion-Treatment and pharmacokinetics data

Maxime Delrue; Lucie Chevillard; Alain Stépanian; Alessandra Dragoni; Laurence Camoin-Jau; Sébastien Voicu; Isabelle Malissin; Nicolas Deye; Marc Gainnier; Virginie Siguret; Bruno Mégarbane

doi:10.1111/eci.13746

Case series of massive direct oral anticoagulant ingestion-Treatment and pharmacokinetics data

Eur J Clin Invest. 2022 Jun;52(6):e13746. doi: 10.1111/eci.13746. Epub 2022 Jan 12.

Authors

Maxime Delrue^{1

2}, Lucie Chevillard^{3

4}, Alain Stépanian^{1

2}, Alessandra Dragoni¹, Laurence Camoin-Jau⁵, Sébastien Voicu^{3

4}, Isabelle Malissin^{3

4}, Nicolas Deye³, Marc Gainnier⁶, Virginie Siguret^{1

7}, Bruno Mégarbane^{3

4}

Affiliations

¹ Hematology Laboratory, AP-HP Lariboisière Hospital, Paris University, Paris, France.
² EA 3518, Paris University, Paris, France.
³ Department of Medical and Toxicological Critical Care, AP-HP Lariboisière Hospital, Paris, France.
⁴ INSERM, UMRS-1144, Paris University, Paris, France.
⁵ Hematology Laboratory, APHM, la Timone Hospital, Marseille, France.
⁶ Department of Critical Care, APHM, la Timone Hospital, Marseille, France.
⁷ INSERM, UMRS-1140, Paris University, Paris, France.

PMID: 35000196
DOI: 10.1111/eci.13746

Abstract

Background: Direct oral anticoagulants (DOAC) are widely used due to favourable benefit/risk ratio. However, consequences of massive ingestion have been poorly investigated.

Objectives: We aimed to report outcome and pharmacokinetic parameters in patients who massively ingested DOACs.

Methods: We conducted a 5-year cohort study including consecutive massive DOAC ingestion patients admitted to two critical care departments. Patients were managed in accordance with standards of care. We collected the main history, clinical, laboratory, management and outcome data. The time-course of plasma DOAC concentrations measured using specific assays was modelled.

Results: Twelve patients (3F/9M; age, 55 years [41-63], median [25th-75th percentiles]) were included. Ingestions involved rivaroxaban (n = 7), apixaban (n = 3) and dabigatran (n = 2), with presumed doses of 9.4-fold [5.0-22.0] the full daily dose. Six patients received activated charcoal but no antidote nor blood-derived product. No bleeding was observed. One patient died due to refractory cardiogenic shock related to bisoprolol co-intoxication. Highest observed peak plasma concentrations were 1720 ng/ml (rivaroxaban), 750 ng/ml (apixaban) and 644 ng/ml (dabigatran). Times to reach DOAC concentration below 50 ng/ml were ~20-45 h (rivaroxaban), ~125 h (apixaban) and ~30-50 h (dabigatran). Elimination half-lives were 2.5-25.5 h (rivaroxaban), 22.0 and 36.5 h (apixaban), and 5.8 and 15.5 h (dabigatran), with substantial interindividual variability and prolongation in case of cardiovascular failure related to co-intoxicants. Charcoal administration, even if delayed, may have contributed to limit toxicity, possibly by reducing absorption and/or enteroenteric recycling.

Conclusion: No bleeding was observed in this series of massive DOAC ingestions despite elevated plasma concentrations. No patient required specific haemostatic agents. Charcoal administration should be considered to limit toxicity.

Keywords: Netherlands; apixaban; dabigatran; direct oral anticoagulant; pharmacokinetic modelling; poisoning.

MeSH terms

Administration, Oral
Anticoagulants
Atrial Fibrillation* / chemically induced
Atrial Fibrillation* / drug therapy
Charcoal / therapeutic use
Cohort Studies
Dabigatran*
Eating
Hemorrhage / chemically induced
Humans
Middle Aged
Pyridones / therapeutic use
Rivaroxaban / therapeutic use

Substances

Anticoagulants
Pyridones
Charcoal
Rivaroxaban
Dabigatran