Anticoagulant Reversal

Introduction

Anticoagulants reduce the risk of thrombosis but can lead to life-threatening bleeding. Reversal is indicated when there’s major bleeding, bleeding in critical sites (e.g., brain), or emergency surgery.

This guide reviews how common anticoagulants work, how they’re reversed, what lab values they affect, and how reversal works physiologically.


Vitamin K Antagonists (e.g., Warfarin)

  • Mechanism: Inhibits vitamin K–dependent clotting factors (II, VII, IX, X)
  • Lab Effects: Increase INR (very reliable)
  • Reversal: Replace clotting factors with PCC or FFP + give vitamin K to restore production.¹

Factor Xa Inhibitors (e.g., Apixaban, Rivaroxaban)

  • Mechanism: Directly inhibit factor Xa → decrease thrombin generation
  • Lab Effects: PT/INR may be slightly increased; anti-Xa assay (if available) is most accurate
  • Reversal: Andexanet alfa (preferred), or PCC if unavailable.²

Direct Thrombin Inhibitors (e.g., Dabigatran, Bivalirudin, Lepirudin)

  • Mechanism: Directly inhibit thrombin (factor IIa)
  • Lab Effects: Increase aPTT and thrombin time (TT); dilute thrombin time or ecarin clotting time most specific
  • Reversal: Idarucizumab; dialysis also effective due to renal clearance.³

Unfractionated Heparin (UFH)

  • Mechanism: Binds antithrombin → inhibits thrombin and Xa
  • Lab Effects: Increases aPTT (reliable); ACT* used during procedures
  • Reversal: Protamine sulfate (fully reverses if recent)⁴

Low Molecular Weight Heparin (e.g., Enoxaparin)

  • Mechanism: Primarily inhibits factor Xa via antithrombin
  • Lab Effects: aPTT minimally affected; anti-Xa assay best if available
  • Reversal: Protamine sulfate (partial reversal only)⁴

Fondaparinux

  • Mechanism: Indirect Xa inhibitor via antithrombin; long half-life
  • Lab Effects: Anti-Xa level elevated; PT/INR and aPTT usually normal
  • Reversal: No direct antidote; PCC or aPCC may offer partial effect⁵

Direct Thrombin Inhibitors (IV) — Argatroban, Bivalirudin

  • Mechanism: Directly inhibit thrombin (IIa)
  • Lab Effects: Increase aPTT, increase INR (especially argatroban)
  • Reversal: None needed — short half-life (~1 hr); stop infusion⁶

Anticoagulant Rapid Reversal Summary

AnticoagulantReversal AgentDose / NotesOther Options
WarfarinVitamin K + PCCVit K 5–10 mg IV slow + PCC 25–50 U/kg (max 3000 U)¹FFP if PCC unavailable
Apixaban / RivaroxabanAndexanet alfa400–800 mg IV bolus, then 4–8 mg/min infusion²PCC 50 U/kg if Andexanet not available²
DabigatranIdarucizumab (Praxbind)5 g IV (2 × 2.5 g vials)³Dialysis if renal failure³
Heparin (UFH)Protamine sulfate1 mg per 100 U UFH (max 50 mg)⁴Best if given <2 hrs from last dose; monitor ACT*
Enoxaparin (LMWH)Protamine (partial)1 mg protamine per 1 mg enoxaparin (if <8 hrs)⁴Second dose: 0.5 mg/mg if bleeding continues⁴
FondaparinuxNone specificPCC or aPCC empirically⁵Supportive measures⁵
Argatroban / BivalirudinNoneShort half-life; discontinue → clearance in 1–2 hrs⁶Supportive only⁶

ACT Footnote

ACT* = Activated Clotting Time

  • Point-of-care test used to monitor high-dose heparin during procedures like cardiopulmonary bypass, cath lab, or ECMO
  • Faster but less sensitive than aPTT
  • Normal: ~70–120 sec; therapeutic often >250–300 sec

References

  1. Holbrook A, et al. Evidence-based management of anticoagulant therapy. Chest. 2012;141(2_suppl):e152S-e184S. doi:10.1378/chest.11-2295
  2. Connolly SJ, et al. Andexanet alfa for bleeding with factor Xa inhibitors. NEJM. 2016;375(12):1131–1141. doi:10.1056/NEJMoa1607887
  3. Pollack CV Jr, et al. Idarucizumab for dabigatran reversal. NEJM. 2015;373(6):511–520. doi:10.1056/NEJMoa1502000
  4. Smythe MA, et al. Reversal of oral and parenteral anticoagulants. Am J Health Syst Pharm. 2016;73(10 Suppl 2):S27–S48. doi:10.2146/ajhp150658
  5. Spina M, et al. Reversal agents for NOACs: rapid evidence review. J Thromb Thrombolysis. 2020;49(2):220–231. doi:10.1007/s11239-019-01916-x
  6. Siegal DM, et al. Andexanet for reversal of Xa inhibitor activity. NEJM. 2015;373(25):2413–2424. doi:10.1056/NEJMoa1510991

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