DECISION
- The senior clinician decides to anticoagulate orally, including duration and intensity of treatment
Choice of rapid or slow anticoagulation
Choose:
- Rapid anticoagulation with concurrent LMWH or heparin e.g. for VTE, follow RAPID ANTICOAGULATION
- Slow anticoagulation without concurrent LMWH or heparin e.g. for AF, follow SLOW ANTICOAGULATION
RAPID ANTICOAGULATION (WITH CONCURRENT HEPARIN)
Who initiates?
- Refer inpatients to an anticoagulation management service (AMS)
- Only if patient not referred to AMS, follow this guideline
Review clinical condition
Medication history
- Determine any significant interactions with warfarin
- remember herbal remedies
- Consider whether to discontinue or substitute medications
- particularly important for 'as required' medications e.g. NSAIDs, where the interaction may be inconsistent
- Seek further information from medicines information or AMS where necessary
Increased sensitivity to warfarin
- Frail, sick, have multiple comorbidities or take multiple medication
- Aged >80 yr
- Significantly underweight
- Congestive cardiac failure
- Abnormal liver function
- Receiving parenteral nutrition or drugs that potentiate warfarin significantly (see BNF Appendix 1)
Counsel patient
- Reason, risks and benefits of oral anticoagulation
- bleeding risk
- drug interactions (including alcohol)
- need for regular INR monitoring
- Provide anticoagulation information pack
Dose prediction
- Anticoagulation with warfarin takes effect only in 72-96 hrs after first dose
- The following algorithm allows the maintenance dose of warfarin to be predicted over 4 days by optimal interpretation of timed daily INR measurements
- Use INR to guide the selection of daily warfarin dose
- even during concurrent anticoagulant treatment with unfractionated heparin, dalteparin or any other low-molecular-weight heparin
- All warfarin tablets are scored, and
- any doses recommended can be administered by use of 1 mg, 3 mg and 5 mg tablets
Increased sensitivity to warfarin
- If patient has increased sensitivity to warfarin, use half the doses recommended below
Day 1
- Take blood for measurement of INR
- If INR ≥1.4, this predictive method cannot be used
- the choice of dose must rely on clinical judgement alone
- seek advice from AMS
- If INR <1.4 and no increased sensitivity to warfarin, give warfarin 10 mg before evening meal between 1700 and 1800 hr
- remember to halve doses in sensitive patients
Day 2
- Take blood between 0900 hr and 1000 hr (16 hr after first dose of warfarin)
- Measure INR and use the result to select next dose
- remember to halve doses suggested in sensitive patients
Dosage adjustment for rapid anticoagulation based on INR measurements day 2
| Day 2 (16 hr after first 10mg dose) | |
|---|---|
| INR | Wafarin dose (mg) |
| <1.8 | 10.0 |
| 1.8 | 1.0 |
| >1.8 | 0.5 |
Day 3
- Take blood between 0900 hr and 1000 hr (16 hr after second dose of warfarin)
- Measure INR and use the result to select next dose
- remember to halve doses suggested in sensitive patients
Dosage adjustment for rapid anticoagulation based on INR measurements day 3
| Day 3 (16 hr after second dose) | |
|---|---|
| INR | Wafarin dose (mg) |
| <2.0 | 10.0 |
| 2.0-2.1 | 5.0 |
| 2.2-2.3 | 4.5 |
| 2.4-2.5 | 4.0 |
| 2.6-2.7 | 3.5 |
| 2.8-2.9 | 3.0 |
| 3.0-3.1 | 2.5 |
| 3.2-3.3 | 2.0 |
| 3.4 | 1.5 |
| 3.5 | 1.0 |
| 3.6-4.0 | 0.5 |
| >4.0 | 0 |
Day 4
- Take blood between 0900 hr and 1000 hr (16 hr after third dose of warfarin)
- Measure INR and use the result to select next dose
- remember to halve doses suggested in sensitive patients
Dosage adjustment for rapid anticoagulation based on INR measurements (day 4)
| Day 4 (16 hr after third dose) | |
|---|---|
| INR | Wafarin dose (mg) |
| <1.4 | Discuss with haematology |
| 1.4 | 8.0 |
| 1.5 | 7.5 |
| 1.6-1.7 | 7.0 |
| 1.8 | 6.5 |
| 1.9 | 6.0 |
| 2.0-2.1 | 5.5 |
| 2.2-2.3 | 5.0 |
| 2.4-2.6 | 4.5 |
| 2.7-3.0 | 4.0 |
| 3.1-3.5 | 3.5 |
| 3.6-4.0 | 3.0 |
| 4.1-4.5 | 0 - give 2 mg from day 5 |
| >4.5 | 0 - give 1 mg from day 6 |
Subsequent management
- The dose selected on day 4 is the predicted maintenance dose necessary to achieve a stable INR in the range 2-4
- Watch for INR instability due to changing/starting/stopping of interacting medication or diet (se BNF Appendix 1)
- Make dose adjustments after end of initiation regimen onward intuitively
- If concerns of overanticoagulation, see Warfarin overanticoagulation
DISCHARGE
- Refer patients stabilised on warfarin to AMS for ongoing monitoring
- Order TTO for warfarin along with other medication
SLOW ANTICOAGULATION
Who initiates?
- Refer inpatients to an anticoagulation management service (AMS)
- Only if patient not referred to AMS, follow this guideline
Review clinical condition
Medication history
- Determine any significant interactions with warfarin
- remember herbal remedies
- Consider whether to discontinue or substitute medications
- particularly important for ‘as required’ medications e.g. NSAIDs, where the interaction may be inconsistent
- Seek further information from medicines information or AMS where necessary
Increased sensitivity to warfarin
- Frail, sick, have multiple comorbidities or take multiple medication
- Aged >80 yr
- Significantly underweight
- Congestive cardiac failure
- Abnormal liver function
- Receiving parenteral nutrition or drugs that potentiate warfarin significantly (see BNF Appendix 1)
Counsel patient
- Reason, risks and benefits of oral anticoagulation
- bleeding risk
- drug interactions (including alcohol)
- need for regular INR monitoring
- Provide anticoagulation information pack
Day 1
- Take blood for measurement of INR
- When INR result available:
- if INR ≤1.3 on day 1 and increased sensitivity to warfarin, choose Slow anticoagulation OATES regimen
- if INR <1.5 on day 1 and no factors likely to cause increased sensitivity to warfarin, choose Slow anticoagulation Tait regimen
- if INR fits neither of first two choices, seek senior advice
Slow anticoagulation OATES regimen
Rules for induction algorithm – Oates et al – (depending on INR on day 15)
| Female | Male | ||
|---|---|---|---|
| INR between | Dose (mg) | INR between | Dose (mg) |
| 1.0-1.1 | 5.0 | 1.0–1.0 | 6.0 |
| 1.2-1.3 | 4.0 | 1.1–1.2 | 5.0 |
| 1.4-1.9 | 3.0 | 1.3–1.5 | 4.0 |
| 2.0-3.0 | 2.0 | 1.6–2.1 | 3.0 |
| 3.1-4.0 | 1.0 | 2.2–3.0 | 2.0 |
| 3.1–4.0 | 1.0 | ||
Slow anticoagulation Tait regimen
Algorithm for dosage adjustment in slow anticoagulation Tait regimen
| Day 5 INR | Dosage (mg) for days 5–7 | Day 8 INR | Dosage (mg) from day 8 |
|---|---|---|---|
| ≤1.7 | 5 |
≤1.7 1.8-2.4 2.5-3.0 >3.0<5 ≥5 |
6 5 4 3 for 4 days Omit until INR<5 |
| 1.8-2.2 | 4 |
≤1.7 1.8-2.4 2.5-3.0 3.1-3.5 >3.5<5 ≥5 |
5 4 3.5 3 for 4 days 2.5 for 4 days Omit until INR<5 |
| 2.3-2.7 | 3 |
≤1.7 1.8-2.4 2.5-3.0 3.1-3.5 >3.5<5 ≥5 |
4 3.5 3 2.5 for 4 days 2 for 4 days Omit until INR<5 |
| 2.8-3.2 | 2 |
≤1.7 1.8-2.4 2.5-3.0 3.1-3.5 >3.5<5 ≥5 |
3 2.5 2 1.5 for 4 days 1 for 4 days Omit until INR<5 |
| 3.3-3.7 | 1 |
≤1.7 1.8-2.4 2.5-3.0 3.1-3.5 >3.5 |
2 1.5 1 0.5 for 4 days Omit for 4 days |
| >3.7 | 0 |
<2.0 2.0-2.9 3.0-3.5 |
1.5 for 4 days 1 for 4 days 0.5 for 4 days |
- At day 15 (or day 12) check INR and make fine dose adjustment as appropriate
Subsequent management
- Make dose adjustments after end of initiation regimen intuitively
- watch for INR instability due to changing/starting/stopping of interacting medication or diet (see BNF Appendix 1)
- If concerns of overcantioagulation, see Warfarin overanticoagulation
DISCHARGE
- Refer patients stabilised on warfarin to AMS for ongoing monitoring
- Order TTO for warfarin along with other medication
Date updated: 2024-01-10