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Role of Anticoagulation in
Neurocritical Care
DR Ankit Gajjar
MD, Anesthesia, IDCCM, IFCCM, EDIC
Consultant Intensivist at INS Hospital
• Anticoagulation remains the main stay of
treatment for prevention and treatment of
thrombosis
• Aim of our lecture is to clear point about role
of anticoagulation in neurocritical care
Comparison
Features Heparin LMWH Fondaperinux
Target Xa=IIa Xa > iia Xa
Bioavailability 30 90 100
Half life (hr) 1 4 17
Renal Clearance No Yes Yes
Protamine reversal Complete Partial None
HIT < 5% <1% Case Reports
Advantage of UFH over LMWH is safe in Renal failure and
shorter duration of action
Prophylactic dose
• UFH – 5000 Unit SC bid/tid
• Enoxaparin
- 40 mg SC od
- If Cr CL < 30 ml/min,
Age > 75 years – 30 mg SC od
• Dalteparin 2500 units or 5000 units sc od
• Fondaparinux – 2.5 mg SC od
• LMWH IS PREFERRED OVER UFH
Therapeutic dose
• UFH – 80 U/kg bolus f/b 18 U/kg/hr
- Target aPTT 1.5 – 2 times normal (60 to 80
secs)
• Enoxaparin – 1 mg/kg SC bid or 1.5 mg/kg SC bid
- If CrCl<30 ml/min 1 mg/kg SC od
LMWH IS PREFERRED OVER UFH
Dalteparin and Fondaparinux is not
recommended.
• Patients with Neurologic disease or those
undergoing procedure for a neurologic or a
neurosurgical conditions, have very high risk of
VTE.
• DVTs may be present in 15-40% of all hospitalised
neurosurgical patients, 40-80% of head trauma
patients and 20-40% of hospitalised stroke
patients
• Thus, awareness of this risk is critical to prevent
the DVT and its complications.
• Among Neuro patients treated with
Mechanical Prophylaxis alone, DVTs rate is as
high as 32%
• Pharmacological thromboprophylaxis
associated with further 50% reduction in risk
of DVT
• Any patients who are immobilised for more
than 48 hours are candidates for DVT
prophylaxis
Ischemic stroke
• In patients with Acute Ischemic Stroke with
restricted mobility combined, Pharmacological
and Mechanical Prophylaxis
• In thrombolysed patients, should be delayed
upto 24 hours
Neurologic Critical Care
March 2017, Volume 45, No. 3
Ischemic Stroke
• Therapeutic anticoagulation
1) Cardio embolic stroke except large infarct
2) Spontaneous cerebral and cervical artery
dissection
3) Progressive or recurrent stroke despite of
antiplatelet therapy
Ischemic Stroke
• Early aggressive treatment with therapeutic
anticoagulation in other types of ischemic
stroke worsen the mortality by increasing risk
of intracranial haemorrhage
• Anticoagulant should be used as a DVT
prophylaxis
AHA Guideline 2018;49 eXXX-eXXX
Management of Acute Ischemic Stroke
Cerebral Venous Thrombosis
• Earliest to start Therapeutic Anticoagulation
• LMWH is preferred over UFH
• Presence of haemorrhagic venous infarct is
not a contraindication
• After Decompressive Hemicraniectomy,
Anticoagulant can be safely started within 24
hours
Curr Opin Crit Care 2016 22:113-119
ICH/SAH/TBI
• Can be started after 48 hours of documented
stoppage of bleeding
• Again combined prophylaxis is indicated
Post Surgical
• Can be start after 24 hours of Post
Craniotomy, if bleeding risk is not high
• Initially UFH is preferred over LMWH due to
ease of reversibility and shorter duration of
action
• Neuromuscular disease like GBS, Myasthenia
Gravis etc LMWH is indicated as a VTE is a
major risk factor for sudden death
Newer Oral Anticoagulants
Features Dabigatran Rivaroxaban Epixaban
Target Thrombin Factor Xa Factor Xa
Bioavailability (%) 6 80 90
Half life (h) 12-17 5-9 12
Onset of action 1-3 hr 2-4 hr 1-2 hr
Renal excretion 80 65 25
Coagulation
monitoring
No No No
Antidote Idarucizumab
(Praxbind)
No No
Dosage
Cr cl > 50 ml/min
15-50 ml/min
150 mg PO bd
75 mg PO bd
20 mg PO od with food
15 mg PO od
5 mg PO bd
2.5 mg PO bd
Monitoring Reversal Thrombin time Anti Xa level
Newer Oral Anticoagulants
• Advantage
• More effective than warfarin in prevention of
ischemic stroke in patients with non valvular AF
• No need of dietary restriction
• Less drug drug interaction
• Quick onset and offset of action
• No need of monitoring or dose titration
• No need of overlapping with parentral
anticoagulants
Newer Oral Anticoagulants
• Disadvantage
• No reversal agent
• Costly
• Not useful in renal failure and pregnancy

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A role of anticoagulation in neurocritical care jhjk

  • 1. Role of Anticoagulation in Neurocritical Care DR Ankit Gajjar MD, Anesthesia, IDCCM, IFCCM, EDIC Consultant Intensivist at INS Hospital
  • 2. • Anticoagulation remains the main stay of treatment for prevention and treatment of thrombosis • Aim of our lecture is to clear point about role of anticoagulation in neurocritical care
  • 3. Comparison Features Heparin LMWH Fondaperinux Target Xa=IIa Xa > iia Xa Bioavailability 30 90 100 Half life (hr) 1 4 17 Renal Clearance No Yes Yes Protamine reversal Complete Partial None HIT < 5% <1% Case Reports Advantage of UFH over LMWH is safe in Renal failure and shorter duration of action
  • 4. Prophylactic dose • UFH – 5000 Unit SC bid/tid • Enoxaparin - 40 mg SC od - If Cr CL < 30 ml/min, Age > 75 years – 30 mg SC od • Dalteparin 2500 units or 5000 units sc od • Fondaparinux – 2.5 mg SC od • LMWH IS PREFERRED OVER UFH
  • 5. Therapeutic dose • UFH – 80 U/kg bolus f/b 18 U/kg/hr - Target aPTT 1.5 – 2 times normal (60 to 80 secs) • Enoxaparin – 1 mg/kg SC bid or 1.5 mg/kg SC bid - If CrCl<30 ml/min 1 mg/kg SC od LMWH IS PREFERRED OVER UFH Dalteparin and Fondaparinux is not recommended.
  • 6. • Patients with Neurologic disease or those undergoing procedure for a neurologic or a neurosurgical conditions, have very high risk of VTE. • DVTs may be present in 15-40% of all hospitalised neurosurgical patients, 40-80% of head trauma patients and 20-40% of hospitalised stroke patients • Thus, awareness of this risk is critical to prevent the DVT and its complications.
  • 7. • Among Neuro patients treated with Mechanical Prophylaxis alone, DVTs rate is as high as 32% • Pharmacological thromboprophylaxis associated with further 50% reduction in risk of DVT
  • 8. • Any patients who are immobilised for more than 48 hours are candidates for DVT prophylaxis
  • 9. Ischemic stroke • In patients with Acute Ischemic Stroke with restricted mobility combined, Pharmacological and Mechanical Prophylaxis • In thrombolysed patients, should be delayed upto 24 hours Neurologic Critical Care March 2017, Volume 45, No. 3
  • 10. Ischemic Stroke • Therapeutic anticoagulation 1) Cardio embolic stroke except large infarct 2) Spontaneous cerebral and cervical artery dissection 3) Progressive or recurrent stroke despite of antiplatelet therapy
  • 11. Ischemic Stroke • Early aggressive treatment with therapeutic anticoagulation in other types of ischemic stroke worsen the mortality by increasing risk of intracranial haemorrhage • Anticoagulant should be used as a DVT prophylaxis AHA Guideline 2018;49 eXXX-eXXX Management of Acute Ischemic Stroke
  • 12. Cerebral Venous Thrombosis • Earliest to start Therapeutic Anticoagulation • LMWH is preferred over UFH • Presence of haemorrhagic venous infarct is not a contraindication • After Decompressive Hemicraniectomy, Anticoagulant can be safely started within 24 hours Curr Opin Crit Care 2016 22:113-119
  • 13. ICH/SAH/TBI • Can be started after 48 hours of documented stoppage of bleeding • Again combined prophylaxis is indicated
  • 14. Post Surgical • Can be start after 24 hours of Post Craniotomy, if bleeding risk is not high • Initially UFH is preferred over LMWH due to ease of reversibility and shorter duration of action
  • 15. • Neuromuscular disease like GBS, Myasthenia Gravis etc LMWH is indicated as a VTE is a major risk factor for sudden death
  • 16. Newer Oral Anticoagulants Features Dabigatran Rivaroxaban Epixaban Target Thrombin Factor Xa Factor Xa Bioavailability (%) 6 80 90 Half life (h) 12-17 5-9 12 Onset of action 1-3 hr 2-4 hr 1-2 hr Renal excretion 80 65 25 Coagulation monitoring No No No Antidote Idarucizumab (Praxbind) No No Dosage Cr cl > 50 ml/min 15-50 ml/min 150 mg PO bd 75 mg PO bd 20 mg PO od with food 15 mg PO od 5 mg PO bd 2.5 mg PO bd Monitoring Reversal Thrombin time Anti Xa level
  • 17. Newer Oral Anticoagulants • Advantage • More effective than warfarin in prevention of ischemic stroke in patients with non valvular AF • No need of dietary restriction • Less drug drug interaction • Quick onset and offset of action • No need of monitoring or dose titration • No need of overlapping with parentral anticoagulants
  • 18. Newer Oral Anticoagulants • Disadvantage • No reversal agent • Costly • Not useful in renal failure and pregnancy