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Please use current guidelines available on the UHNM intranet for patient treatment
Please use current guidelines available on the UHNM intranet for patient treatment
BACKGROUND
- Immune-mediated prothrombotic disorder occurring in patients on unfractioned heparin (UFH) or low molecular weight heparin (LMWH)
- If left untreated, associated with a 6% daily risk of thrombosis, amputation, or death
- Identify early, stop heparin and substitute alternative anticoagulation
- Over-diagnosis may cause harm due to unnecessary replacement of heparin by infrequently used, non-heparin anticoagulants
- Despite thrombocytopenia, bleeding in HIT is uncommon
MONITORING
- Inform all patients that HIT is a possible complication of heparin therapy
- UFH > LMWH risk
- Surgical > medical > obstetric risk
- Before starting heparin in all patients, check baseline platelet count
- Post-operative and cardiopulmonary bypass patients who have been exposed to heparin in the previous 100 days, check platelet count 24 hr after starting any type of heparin/UFH
Patients requiring routine monitoring for HIT (incidence >1%)
- Post-operative patients including obstetric cases receiving UFH
- Post-cardiopulmonary bypass patients receiving LMWH
Monitor platelet count at least every other day
- From days 4-14 of heparin treatment or until heparin is stopped
- if heparin is stopped for surgery, the day of restarting becomes day zero for the timing
The following patients do not require routine monitoring for HIT (incidence <1%)
- Post-operative patients (other than cardiopulmonary bypass patients) receiving LMWH
- Medical patients and obstetric patients receiving LMWH
RECOGNITION AND ASSESSMENT
Clinical features of HIT
- Consider HIT in a patient treated with heparin who has a platelet count fall of >30% and/or any of the following
- skin necrosis at sites of heparin injection
- venous and/or arterial thrombosis
- anaphylactoid response (cardiorespiratory, neurological or unusual symptoms) within 30 min of systemic heparin infusion
- extension of previous thrombosis
- adrenal haemorrhage
HIT suspected
- Perform pre-test probability scoring for HIT using the 4T score
Pre-test probability scoring for HIT (four Ts)
| Clinical feature | Score | ||
|---|---|---|---|
| 2 | 1 | 0 | |
| Thrombocytopenia | >50% fall from baseline and to nadir of >20 x 109/L | 30-50% fall from baseline or to nadir of 10-19 x 109/L | <30% fall from baseline or to nadir of <10 x 109/L |
| Timing of platelet count fall (after heparin exposure) | Clear onset between 5 and 10 days of present exposure to heparin OR if previous heparin exposure within 30 days, onset ≤1 day of present exposure to heparin |
Time of onset not clear (missing platelet counts etc) OR onset after day 10 of present exposure to heparin OR if previous herparin exposure was 30-100 days ago, onset ≤1 day of present exposure to heparin |
Without previous heparin exposure within last 100 days, onset within 4 days of present exposure to heparin |
| Thrombosis or other sequelae (e.g. skin lesions) |
New thrombosis
Skin necrosis Post-heparin acute systemic reaction |
Progressive or recurrent thrombosis;
Thrombosis not yet proven; erythematous skin lesions |
None |
| Other causes of thrombocytopenia evident | No other cause of thrombocytopenia evident | Possible other causes | Definite other cause present |
Pre-test probability score
Add score for each clinical category maximum score = 8
6-8 = High (~50% probability of HIT)
4-5 = Intermediate (~10% probability of HIT)
0-3 = Low (<<1% probability of HIT)
IMMEDIATE MANAGEMENT
Patients with low 4T score (0−3)
- Probability of HIT <<1%
- HIT excluded - continue heparin
- HIT antibody testing usually not required
- Contact haemostasis team regarding work up of alternative causes of thrombocytopenia and role of HIT antibody testing
Intermediate (4−5) or high (6−8) pre-test probability of HIT on 4T score
- Stop heparin immediately
- including line locks and flushes; remove any heparin coated lines
- Start alternative anticoagulant, usually at full treatment dose
Do not start warfarin
- Risk of skin necrosis
- If warfarin already started:
- omit further doses and
- give a single dose of vitamin K1 (phytomenadione) 5 mg by slow IV injection
- while introducing alternative anticoagulation
HIT antibody testing
- Do not order in patients with 4T score of 0-3
- Obtain blood sample for HIT antibody testing
- 6 mL clotted (red top) sample required
- complete HIT request form with 4T score and send with blood sample
- contact blood bank when sending sample
- If in doubt, contact the haemostasis team
- Discuss all HIT antibody results with consultant haematologist
Platelet transfusion is relatively contraindicated
- Discuss patients with bleeding or a need for urgent procedures with the haemostasis team
TRANSITION TO ORAL ANTICOAGULATION
- Prefer DOACs for clinically stable HIT patients (with or without thrombosis) at low to average bleeding risk
- Use is off licence but supported by major international guidelines
- Apply the same contraindications to their use in the treatment of acute VTE in determining their appropriateness for patients with HIT
- Rivaroxaban has been most studied in this area. If contraindicated, discuss alternative DOAC with a consultant haematologist
Rivaroxaban
- HIT with thrombosis: dose is 15 mg twice daily for 21 days then 20 mg once daily
- HIT without thrombosis: dose is 15 mg twice daily until platelet count >150 x 109/L then 20 mg once daily
- All doses to be taken with food
Switching from argatroban or fondaparinux to DOAC
Argatroban
- Stop infusion and start DOAC 2 hr after discontinuation
Fondaparinux
- Start DOAC 24 hr after last dose of fondaparinux
Switching from argatroban to warfarin
- Do not give warfarin until platelet count is >150 x 109/L
- if commenced too early, risk of warfarin induced skin necrosis and gangrene
- When assessing warfarin effect, remember argatroban prolongs INR
- Ask anticoagulation team for advice
Starting warfarin
- Start warfarin at 3 mg/day and monitor INR daily
- When INR is >4.0 for 2 days, stop argatroban infusion and check INR after 4 hr
- If INR >2 no further argatroban required
If INR <2 restart argatroban infusion and adjust warfarin dose with advice
Switching from fondaparinux to warfarin
- Do not give warfarin until the platelet count is >150 x 109/L
- if commenced too early, risk of warfarin induced skin necrosis and gangrene
- Start warfarin 3-5 mg daily (avoid large loading doses)
- Check INR daily - fondaparinux does not interfere with INR
- When INR >2 for 2 consecutive days, discontinue fondaparinux
DURATION OF ANTICOAGULATION
- After HIT associated with a thrombotic complication, give therapeutic anticoagulation for 3 months
- HIT without a thrombotic complication requires anticoagulation for 4 weeks. Discuss with haemostasis team
ANTICOAGULATION IN PATIENTS WITH A HISTORY OF HIT
- Avoid all forms of heparin and use an alternative anticoagulant
- Discuss with a haematologist if severe renal failure or planned cardiac surgery
SUBSEQUENT MANAGEMENT
- Platelet recovery in HIT usually occurs within 1 week of stopping heparin
- Screen all patients with HIT for asymptomatic proximal deep vein thrombosis
- by bilateral lower-extremity compression ultrasonography
- Screen all patients with an upper limb central line for asymptomatic DVT by an upper-extremity ultrasonography in the limb with the catheter
- In patients with an additional indication for antiplatelet therapy (e.g. recent PCI), decide on the balance of bleeding and thrombosis risk whether to continue antiplatelet therapy alongside anticoagulation
DISCHARGE AND FOLLOW-UP
- Document HIT in patient notes and electronic records (iPortal alert)
- Refer all patients being discharged on anticoagulation to the anticoagulation team
- Refer all patients to thrombosis clinic even if no thrombosis has developed
Inform patient and GP
- If given UFH or LMWH in the 100 days after HIT, increased risk of thrombosis
- If patient requires anticoagulation with heparin after more than 100 days, seek advice from haemostasis team
- Document HIT in discharge letter
- Ask GP to monitor platelet count where appropriate (see Monitoring above)