Periprocedural management of oral anticoagulant therapy

Last updated: June 28, 2024

CME information and disclosures

To see contributor disclosures related to this article, hover over this reference: ^[1]

Physicians may earn CME/MOC credit by reading information in this article to address a clinical question, and then completing a brief evaluation, in which they will identify their question and report the impact of any information learned on their clinical practice.

AMBOSS designates this Internet point-of-care activity for a maximum of 0.5 AMA PRA Category 1 Credit(s)™. Physicians should claim only credit commensurate with the extent of their participation in the activity.

For answers to questions about AMBOSS CME, including how to redeem CME/MOC credit, see "Tips and Links" at the bottom of this article.

Summary

Oral anticoagulants include vitamin K antagonists (VKAs) and direct oral anticoagulants (DOACs). Periprocedural management of patients on long-term oral anticoagulants (e.g., for the prevention of stroke and systemic thromboembolism) is a field of ongoing research and there is currently no universal validated strategy. Management of anticoagulants in the periprocedural period should be tailored to the patient and the procedure in consultation with the proceduralist and anesthetist. Although invasive procedures performed on patients receiving anticoagulants are associated with an increased risk of bleeding, discontinuing anticoagulants increases the risk of thrombosis. Therefore, anticoagulant therapy should not be routinely interrupted periprocedurally, but instead, the decision should be based on the periprocedural bleeding risk and the periprocedural thrombotic risk. Once interrupted, VKAs take time to achieve therapeutic anticoagulation on reinitiation, and hence, bridging anticoagulation with a short-acting parenteral anticoagulant is required in patients at high thrombotic risk. Bridging anticoagulation is not routinely required for patients on DOACs, as they have a short half-life and, if discontinued, can rapidly achieve therapeutic anticoagulation on reinitiation.

For life-threatening periprocedural bleeding in patients on anticoagulants, see “Anticoagulant reversal.”

Approach

Consult the proceduralist and anesthetist early; follow local institutional protocols if available. ^[2]^[3]

The decision to interrupt anticoagulation therapy should weigh the risk of periprocedural thrombosis against the risk of periprocedural bleeding and be tailored to the patient and the procedure.

Elective procedures ^[2]^[3]

See “Periprocedural management of VKAs” and “Periprocedural management of DOACs” for further details.

7 days before the procedure ^[4]
- Assess periprocedural bleeding risk.
- Assess periprocedural thrombotic risk.
Low bleeding risk: minimal or no interruption of oral anticoagulants
Increased bleeding risk
- Low thrombotic risk: Interrupt oral anticoagulants (bridging anticoagulation not required).
- Moderate or high thrombotic risk
  - VKAs: Interrupt VKAs with bridging anticoagulation (use clinical judgment).
  - DOACs: Interrupt DOACs in most cases; preferably in consultation with specialists.

Parenteral bridging anticoagulation is not required for DOACs. ^[2]^[3]

Many recommendations are based on clinical experience and trials in patients with nonvalvular atrial fibrillation. Exercise caution when applying these recommendations to patients with a mechanical heart valve or a history of venous thromboembolism.

Emergency procedures ^[3]

Low bleeding risk: Anticoagulation may be continued; consult the proceduralist and anesthetist.
Increased bleeding risk
- Consider anticoagulation reversal before performing the procedure.
- Determine the need for postprocedural bridging anticoagulation based on the periprocedural thrombotic risk.

Bleeding risk assessment

Patient-related risk factors ^[3]^[5]^[6]

The following factors are associated with an increased risk of periprocedural bleeding.

Age > 65 years
Hypertension
Active cancer
Abnormal renal function ^[6]
Abnormal liver function ^[6]
History of alcohol consumption (≥ 8 drinks per week) or recreational drug use ^[6]
Chronic bleeding diathesis
Quantitative or qualitative platelet abnormality
Major bleeding or ICH < 3 months before planned procedure ^[5]
History of stroke (i.e., ischemic stroke, spontaneous or traumatic ICH)
History of or predisposition to major bleeding
History of bleeding due to a similar procedure
History of bleeding during bridging anticoagulation
Concomitant therapy with NSAIDs, steroids, antiplatelets, and/or anticoagulants
Labile INR or supratherapeutic INR

Consider delaying elective procedures until modifiable risk factors for periprocedural bleeding can be corrected or optimized.

Procedure-related risk factors

Procedure-related bleeding risk ^[2]^[3]^[7]^[8]
	High bleeding risk procedures	Low-to-moderate bleeding risk procedures	Minimal bleeding risk procedures
Urological procedures	Urological cancer surgery Transurethral resection of the prostate Transurethral bladder resection or tumor ablation Kidney biopsy Nephrectomy	Cystoscopy Hydrocele repair Bladder and prostate biopsies	N/A
Endoscopic procedures	Treatment of esophageal varices Biliary sphincterotomy Pneumatic dilation Percutaneous endoscopic gastrostomy tube placement Colon polypectomy Endoscopic retrograde cholangiopancreatography	Gastrointestinal endoscopy with or without biopsy Bronchoscopy with or without biopsy Biliary or pancreatic stenting without sphincterotomy Endosonography without fine needle aspiration	N/A
Vascular and cardiac surgery	Cardiac surgery Pulmonary surgery Abdominal aortic aneurysm repair Peripheral vascular surgery (e.g., varicose vein surgery, peripheral artery bypass surgery)	Angiography Percutaneous intravascular catheterization with or without intervention	Insertion of a pacemaker or cardioverter-defibrillator device
Orthopedic surgery	Total arthroplasty of major joint (e.g., THR or TKA) Spinal surgery	Hand surgery (including carpal tunnel repair) Arthroscopy	N/A
Neurosurgery	Intracranial surgery Spinal surgery	N/A	N/A
Gynecological procedures	Breast cancer surgery Radical hysterectomy	Cervical biopsy Hysteroscopy Abdominal hysterectomy	N/A
General, colon, and rectal surgery	Colorectal cancer surgery Bowel resection Surgery in highly vascular organs (e.g., spleen, liver, kidneys)	Diagnostic laparoscopy Laparoscopic cholecystectomy Hernioplasty	N/A
Other	Reconstructive plastic surgery Head and neck cancer surgery Any surgery lasting > 45 minutes Neuroaxial intervention (e.g., spinal or epidural anesthesia)	Axillary node dissection Skin, thyroid, breast, and lymph node biopsies	Cataract and other ophthalmic procedures Minor dermatological excisions Minor dental procedures

Even relatively minor bleeding in certain compartments (e.g., intraocular, spinal, pericardial) may cause significant morbidity and mortality. ^[3]

Thrombotic risk assessment

Risk factors for periprocedural thrombosis ^[2]^[6]

Patient-related factors
- Past history of stroke (especially within the past 3 months)
- Past history of VTE or risk factors for VTE
- Rheumatic valvular heart disease
- Atrial fibrillation
- Significant cardiovascular disease , especially within the past year
- Active cancer
- Thromboembolism during prior interruption of anticoagulation
Procedures, e.g.:
- Carotid endarterectomy
- Valve replacement
- Major vascular surgery

Common clinical scenarios ^[2]^[6]

Periprocedural thrombotic risk ^[2]^[3]^[6]
	High thrombotic risk	Moderate thrombotic risk	Low thrombotic risk
Atrial fibrillation	CHA₂DS₂-VASc score: ≥ 7 Rheumatic valvular heart disease Stroke or TIA < 3 months before planned procedure	CHA₂DS₂-VASc score: 5 or 6	CHA₂DS₂-VASc score: ≤ 4 (and no prior stroke or TIA)
Mechanical heart valve	Mitral valve prosthesis with additional stroke risk factors Caged ball or tilting disc mitral or aortic valve prosthesis Stroke or TIA < 3 months before planned procedure	Mitral valve prosthesis without additional risk factors Bileaflet aortic valve prosthesis with additional stroke risk factors	Bileaflet aortic valve prosthesis without additional stroke risk factors
Venous thromboembolism	VTE < 3 months before planned procedure Severe thrombophilia Active malignancy with increased VTE risk	VTE 3–12 months before planned procedure Nonsevere thrombophilia Recurrent VTE Active cancer or recent history of cancer	VTE > 12 months before planned procedure

Periprocedural management of DOACs

DOAC interruption ^[2]

The timing of periprocedural interruption of DOACs is based on procedure-related bleeding risk and the pharmacokinetics of DOACs. Selected patients with risk factors for impaired DOAC clearance (e.g., impaired renal or hepatic function) may require longer interruption intervals.

Timeframe for preprocedural interruption of DOACs ^[2]
DOAC		Procedure-related bleeding risk
DOAC		High	Low-to-moderate	Minimal
Factor Xa inhibitors		2 days	1 day	Day of procedure only
Dabigatran	CrCl ≥ 50 mL/min	2 days	1 day
Dabigatran	CrCl < 50 mL/min	4 days	2 days

Bridging anticoagulation with a parenteral agent is not required for DOACs. ^[2]^[9]

DOAC reinitiation ^[2]

Consult the proceduralist before reinitiating DOACs.
Ensure procedural site hemostasis.
The timing of postprocedural reinitiation is based on the procedure-related bleeding risk.
- High bleeding risk: 48–72 hours after the procedure
- Low-to-moderate bleeding risk: ≥ 24 hours after the procedure

Periprocedural management of VKAs

Approach ^[3]

Consult relevant specialists and follow institutional protocols if available.
Assess the need to interrupt VKAs based on periprocedural bleeding risk.
If VKAs are to be interrupted:
- Determine the timing of VKA interruption based on preprocedural INR levels.
- Determine the need for bridging anticoagulation based on periprocedural thrombotic risk.
Resume VKAs 12–24 hours after the procedure; consider delaying VKA resumption if postprocedural bleeding risk is high.

The decision of whether to interrupt VKAs is based on periprocedural bleeding risk. If VKAs are interrupted, the need for bridging anticoagulation is determined based on periprocedural thrombotic risk.

VKA interruption ^[2]^[3]^[6]

VKA interruption is the temporary discontinuation of VKAs before an elective invasive procedure to minimize periprocedural bleeding risk.

High periprocedural bleeding risk: Interrupt VKA.
Uncertain periprocedural bleeding risk
- Patient-related factors for periprocedural bleeding present: Interrupt VKA
- No patient-related factors for bleeding: Consider interruption.
Low periprocedural bleeding risk: VKAs may be continued.
- Patient-related factors for periprocedural bleeding present: Consider interruption.
- No patient-related factors for bleeding: Do not interrupt VKA.
Timing (if VKA is interrupted): Assess INR 5–7 days before the procedure.
- INR ≤ 3.5: Interrupt VKA 5 days before the procedure.
- INR > 3.5: Interrupt VKA ≥ 6 days before the procedure.

Bridging anticoagulation ^[3]

Periprocedural bridging anticoagulation involves the temporary administration of a short-acting parenteral anticoagulant after VKA interruption for an invasive procedure.

High periprocedural thrombotic risk: Bridging anticoagulation is typically required.
- Low periprocedural bleeding risk: Initiate preprocedural bridging anticoagulation.
- High periprocedural bleeding risk (e.g., ICH within the past 3 months)
  - Consider postprocedural bridging anticoagulation. ^[3]
  - If feasible, consider delaying the procedure in patients with a thromboembolic event in the past 3 months.
Moderate periprocedural thrombotic risk
- Low periprocedural bleeding risk: Use clinical judgment; consult the proceduralist.
- High periprocedural bleeding risk
  - Consider interrupting VKA without bridging anticoagulation.
  - OR consider postprocedural bridging anticoagulation.
Low periprocedural thrombotic risk: Do not bridge.

Preprocedural bridging anticoagulation ^[3]

Timing
- Initiate bridging anticoagulation when the patient's INR is in the subtherapeutic range.
- OR after 2–3 missed doses of VKA, if INR is not being monitored.
Agents
- LMWH, e.g., enoxaparin : Administer the last dose 24 hours before the procedure.
- UFH : Administer the last dose 4–6 hours before the procedure. ^[2]
- Nonheparin anticoagulants: indicated for patients with a history of heparin-induced thrombocytopenia
Reassess INR 24 hours before the procedure.
- INR normal or subtherapeutic: Procedure can be performed.
- Persistently elevated INR: Consider delaying the procedure till the desired INR is achieved.

Postprocedural bridging anticoagulation and resumption of VKA ^[2]^[3]

All patients
- Ensure procedural site hemostasis.
- Assess postprocedural bleeding risk based on the following:
  - Intraprocedural findings and adequacy of hemostasis (consult the proceduralist)
  - Patient-related factors for periprocedural bleeding
  - Procedure-related bleeding risk
- Low postprocedural bleeding risk: Resume VKAs 12–24 hours after the procedure. ^[2]^[3]
- High or uncertain postprocedural bleeding risk: Consider delaying VKA resumption. ^[3]
Additional measures in patients at moderate or high periprocedural thrombotic risk
- Consider overlapping VKAs with a parenteral anticoagulant (i.e., postprocedural bridging anticoagulation).
  - Low postprocedural bleeding risk: Initiate bridging anticoagulation 24 hours after the procedure. ^[3]
  - High or uncertain postprocedural bleeding risk: Consider delaying bridging anticoagulation until 48–72 hours after the procedure. ^[3]
- Agents and dosage: same as for preprocedural bridging anticoagulation ^[3]
- Monitor INR closely.
- Discontinue the parenteral agent once INR is in the therapeutic range.

Start your trial, and get 5 days of unlimited access to over 1,100 medical articles and 5,000 USMLE and NBME exam-style questions.

Start free trial

Evidence-based content, created and peer-reviewed by physicians. Read the disclaimer

Periprocedural management of oral anticoagulant therapy

CME information and disclosures

Summary

Approach

Elective procedures [2][3]

Emergency procedures [3]

Bleeding risk assessment

Patient-related risk factors [3][5][6]

Procedure-related risk factors

Thrombotic risk assessment

Risk factors for periprocedural thrombosis [2][6]

Common clinical scenarios [2][6]

Periprocedural management of DOACs

DOAC interruption [2]

DOAC reinitiation [2]