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Enoxaparin (Appendix)
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Purpose
To provide details about enoxaparin use
 
Indication
Enoxaparin is used for the treatment and prevention of thrombosis.
 

USE 
 
Initiating Therapy

 
Pharmacokinetics

Half-life4 h
Time to peak3 to 5 h following SC injection
ExcretionRenal cleared

 
Therapeutic dosing without renal compromise (Max dose 150 mg)

  Age 0-2 months Age >2 months to ≤ 6 months Age > 6 months to adult
Dosing
  • 1.5 mg/kg/dose SC q12h
  • Consider higher dosing in full-term neonates 0-1 mo of age: 1.7 mg/kg/dose SC q 12h and titrate dose to achieve anti-Xa levels of 0.5 -1.0 units/mL
  • Consider higher dosing in premature infants: 2 mg/kg/dose SC q12h and titrate dose to achieve anti-Xa levels of 0.5 -1.0 units/mL
1.2 mg/kg/dose SC q12h and titrate dose to achieve anti-Xa levels of 0.5 -1.0 units/mL
  • 1 mg/kg/dose (max 150 mg per dose) SC q12h and titrate dose to achieve anti-Xa levels of 0.5 -1.0 units/mL
  • If BMI >40 (or >120 kg), then adjusted body weight should be used, Consider starting at lower dose ~ 0.8 mg/kg for obese patients with BMI >30

 
Prophylactic dosing without renal compromise

  < 60 kg 60 kg to < 120 kg 120 kg or greater
Dosing
  • 0.5 mg/kg/dose (max 30 mg) SC q12h
  • Consider higher dosing in infants up to 2 mo of age: 0.75 mg/kg/dose SQ q12h
40 mg SC q24h or 30 mg SC q12h
  • 40 mg SC q12h and titrate dose to achieve goal anti-factor Xa levels of 0.1-0.3 units/mL. Can consider anti-Xa level of 0.2-0.49 Units/mL as well.
  • See obese patient notes above.

Dosage Adjustment for Renal Impairment +/- Dialysis
See Appendix 1.

Monitoring Therapy

Goal anti-Xa level 0.5-1 units/mL for twice daily Therapeutic dosing, or once daily Prophylactic dosing at 4-6 hours post dose, and applies to those without bleeding. Note: Therapeutic anti-Xa levels up to 1.2 unit/mL have been targeted for patients with high risk of thrombosis

Anti-XaDose changeRepeat peak anti-Xa level
< 0.35 units/mLIncrease dose by 25%4 h after 2nd dose
0.35-0.49 units/mLIncrease dose by 10%4 h after 2nd dose
0.5-1 units/mLNoneOnce per week while inpatient, one week after discharge, and then monthly (4 h after morning dose)
1.1-1.5 units/mLDecrease dose by 20%4 h after 2nd dose
1.6-2 units/mLDelay next dose by 3h and decrease dose by 30%Trough prior to the next dose, then 4 h after 2nd dose
> 2 units/mLHold all doses until <0.5 units/mL, then decrease dose by 40%Trough prior to the next dose and every 12h until <0.5 units/mL.

Goal anti-Xa level 0.2-0.49 units/mL for twice daily Prophylactic dosing, or once daily Prophylactic dosing 12 hours post dose, and applies to those without bleeding. This table should only be applied if strict anti-Xa monitoring indicated.

Anti-XaDose changeRepeat peak anti-Xa level
<0.15 units/mLIncrease by 25%4 h after 2nd dose
0.15-0.19 units/mLIncrease by 10%4 h after 2nd dose
0.2-0.49 units/mLNoneOnce per week while inpatient (4 h after morning dose)
0.5-0.74 units/mLDecrease by 20%4 h after 2nd dose
0.75-1 units/mLDelay next dose by 3h and decrease dose by 30%Trough prior to the next dose, then 4 h after 2nd dose
>1 units/mLHold all doses until <0.5 units/mL, then decrease dose by 40%Trough prior to the next dose and every 12h until <0.5 units/mL

Goal anti-Xa level 0.1-0.3 units/mL for twice daily Prophylactic dosing. The below table applies to those without bleeding. This table should only be applied if strict anti-Xa monitoring indicated. 

Anti-XaDose changeRepeat peak anti-Xa level
<0.1 units/mLIncrease by 10%4 h after 2nd dose
0.1-0.3 units/mLNoneOnce per week while inpatient (4 h after morning dose)
0.4-0.49 units/mLDecrease by 20%4 h after 2nd dose
0.5-0.75 units/mLDelay next dose by 3h and decrease dose by 30%Trough prior to the next dose, then 4 h after 2nd dose
>0.75 units/mLHold all doses until <0.5 units/mL, then decrease dose by 40%Trough prior to the next dose and every 12h until <0.5 units/mL

Administration
Enoxaparin should not be administered in areas where the skin is damaged/edematous. It is recommend to NOT use an insuflon catheter for the administration of enoxaparin given the risk of hematoma.
 
 
Safety Precautions


Bleeding Precautions & Warnings

 
Perioperative Management


Reversal Information

Time Since Last Enoxaparin DoseProtamine Dose per 1 mg Enoxaparin Received
< 4 hours1 mg per 1 mg (100 units) enoxaparin received
4-8 hours0.5-0.75 mg per 1 mg (100 units) enoxaparin received
>8-12 hours0.25-0.5 mg per 1 mg (100 units) enoxaparin received
>12 hoursDo not give protamine

Critical site bleeds: Intracranial hemorrhage, including intraparenchymal, subdural, epidural, and subarachnoid hemorrhages; Other CNS hemorrhage, including intraocular, intra- or extra-axial spinal hemorrhages; Pericardial tamponade; Airway, including posterior epistaxis; Hemothorax, intraabdominal bleeding, and retroperitoneal hemorrhage; Extremity bleeds, including intramuscular and intraarticular bleeding concerning for compartment syndrome, bleeding associated with hemodynamic instability, bleeding in a noncompressible vessel (e.g., subclavian)

Transition Information

FromToAction
EnoxaparinArgatroban/ Bivalirudin/ Dalteparin/ Fondaparinux/ HeparinFrom therapeutic enoxaparin: Stop enoxaparin, and initiate parenteral anticoagulant no earlier than 8 hours after the last enoxaparin dose. If UFH is started ≥12 hours following last enoxaparin dose, an UFH bolus dose is generally indicated. In cases of increased bleeding risk, consider a risk benefit analysis before omitting initial bolus when transitioning to heparin infusion.  

From prophylactic enoxaparin: Initiate parenteral anticoagulant as clinically needed irrespective of time of last enoxaparin dose. In cases of increased bleeding risk, consider a risk benefit analysis before omitting initial bolus when transitioning to heparin infusion.
Apixaban, Betrixaban Dabigatran, Edoxaban, or RivaroxabanFrom therapeutic enoxaparin: Stop enoxaparin and initiate apixaban, betrixaban, dabigatran, edoxaban, or rivaroxaban when next enoxaparin dose is expected to be given.
From prophylactic enoxaparin doses: Stop enoxaparin and initiate apixaban, betrixaban, dabigatran, edoxaban, or rivaroxaban as clinically indicated irrespective of time of last enoxaparin dose.
WarfarinFrom therapeutic enoxaparin: Overlap therapeutic dose enoxaparin with warfarin for at least 5 days AND until INR is in therapeutic range. Consider waiting for 2 consecutive therapeutic INRs for higher risk patients or when initiating warfarin.
From prophylactic enoxaparin AND assuming patient does not have a new thrombosis: If immediate therapeutic anticoagulation is not desired, stop enoxaparin and initiate warfarin as clinically needed irrespective of time of last enoxaparin dose.

Pregnancy
Currently, only Lovenox (enoxaparin) and unfractionated heparin are advised for use in pregnant women. 
 
 
Patient Education and Ongoing Management
Discharging IHTC physician/APP is responsible for ensuring adequate follow-up for anticoagulation management has been scheduled prior to patient leaving the hospital.
 
 
Ordering Enoxaparin

Appendix 1: Enoxaparin Guidelines for Patients with Renal Insufficiency or Failure


Dosage Adjustment for Renal Impairment
Algorithm 1: CrCl < 30 mL/min +/- peritoneal dialysis

Table 1. Nomogram for adjusting enoxaparin dose based on peak anti-Xa level

Anti-Factor XaDose changeTime to Repeat Anti-Factor Xa Level
< 0.35 units/mLIncrease by 25%4 h after 2nd dose
0.35-0.49 units/mLIncrease by 10%4 h the 2nd dose
0.5-1 units/mLNoneOnce level is within target range, then check anti-Xa every 3 days for at least 2 levels, then weekly.
1.1-1.5 units/mLDecrease dose by 20%4 h after 2nd dose
1.6-2 units/mLDelay next dose by 3h and decrease dose by 30%4 h after 2nd dose
> 2 units/mLHold doseMeasure every 12 h until anti-Xa level is < 0.5 units/mL. Then resume at 40% dose and recheck 4 h after 2nd dose

Algorithm 2: patients on intermittent hemodialysis

Table 2. Nomogram for adjusting enoxaparin dose based on peak anti-Xa level

Anti-Factor XaDose changeTime to Repeat Anti-Factor Xa Level
< 0.35 units/mLIncrease by 25%4 h after 2nd dose
0.35-0.49 units/mLIncrease by 10%4 h after 2nd dose
0.5-1 units/mLNoneOnce level is within target range, then check anti-Xa trough 20-24 hours after last dose and adjust dose based on Table 3 and give every 24 hours
1.1-1.5 units/mLDecrease dose by 20%4 h after 2nd dose
1.6-2 units/mLDelay next dose by 3h and decrease dose by 30%4 h after 2nd dose
> 2 units/mLHold doseMeasure every 12 h until anti-Xa level is < 0.5 units/mL. Then resume at 40% dose and recheck 4 h after 2nd dose

Table 3. Nomogram for adjusting enoxaparin dose for trough anti-Xa level in patients with renal impairment as outpatient (20-24 h after dose)

Trough Anti-Xa LevelPeak Anti-Xa LevelDose changeTime to Repeat Anti-Xa Level
< 0.1 units/mL0.5-0.75 units/mLIncrease by 10%4 h after 2nd dose
> 0.75 units/mLDiscuss with clinical pharmacy
0.1-0.3 units/mL0.5-1 units/mLNoneOnce levels are in the target range, check peak and trough every 3 days for at least 2 levels, then weekly 
>0.3 units/mL0.5-0.75 units/mLRecheck both peak and trough within 48 h. If repeat peak and trough are similar to initial peak and trough, then adjust/monitoring according to peak recommendation. If different, then use nomogram for adjusting based on trough.
>0.75-1 units/mLDecrease by 10%4h after the 2nd dose
>1 units/mLDiscuss with clinical pharmacy 

 
Monitoring Anti-Xa for Renal Impairment

References
1.     Lovenox (enoxaparin sodium) injection [Prescribing Information]. Bridgewater, New Jersey, Sanofi-aventis U.S. LLC; April 2022.

2.     Monagle, P.; Chan, A.K.C.; Goldenberg, N.A.; Ichord, R.N.; Journeycake, J.M.; Nowak-Gottl, U.; and Vesely, S.K. Antithrombotic therapy in neonates and children: antithrombobotic therapy and prevention of thrombosis, 9 th ed: American College of Chest Physicians Evidence Based Clinical Practice Guidelines. Chest, 2012: 141(2)(Suppl): e737se801s

3.     Protamine. Lexi-Drugs AHFS Drug Information [Internet database]. Lexi-Comp, Inc.; Accessed September 18, 2023. 

4.     Children’s Hospital of Philadelphia Enoxaparin Clinical Practice Guidelines 2018.

5.     Douketis, J.D.; Spyropoulos, A.C.; Spencer, F.A.; Mayr, M.; Jaffer, A.K.; Eckman, M.H.; Dunn, A.S.; and Kunz, R. Perioperative management of antithrombotic therapy: antithrombotic therapy and prevention of thrombosis, 9th ed: American College of Chest Physicians Evidence Based Clinical Practice Guidelines. Chest, 2012: 141 (2)(Suppl): e326Se350S

6.     Garcia, D.A.; Baglin, T.P.; Weitz, J.I.; and Samama, M.M. Parenteral anticoagulants: antithrombotic therapy and prevention of thrombosis, 9 th ed: American College of Chest Physicians Evidence-Based Clinical Practice Guidelines. Chest, 2012: 141(2)(Suppl): e24S-e43S.

7.     Linkins, L.A.; Dans, A.L.; Moores, L.K.; Bona, R.; Davidson, B.L.; Schulman, S.; and Crowther, M. Treatment and prevention of heparininduced thrombocytopenia: antithrombotic therapy and prevention of thrombosis, 9th ed: American College of Chest Physicians Evidence Based Clinical Practice Guidelines. Chest,2012: 141(2)(Suppl): e495Se530S

8.     Giglia TM, Massicotte MP, Tweddell JS et al. Prevention and treatment of thrombosis in pediatric and congenital heart disease: a scientific statement from the American Heart Association. Circulation 2013;128:2622-703.

9.     Duplaga BA, et al. Dosing and Monitoring of Low-Molecular-Weight Heparins in Special Populations. Pharmacotherapy 2001; 21(2): 218-34

10.  Moffett BS, Lee-Kim Y, Galati M, et al. Population Pharmacokinetics of Enoxaparin in Pediatric Patients. Ann Pharmacother. 2018;52(2):140-146. doi:10.1177/1060028017734234

11.  Malowany JI, Monagle P, Knoppert DC, et al. Enoxaparin for neonatal thrombosis: a call for a higher dose for neonates. Thromb Res. 2008;122(6):826-830. doi:10.1016/j.thromres.2007.11.009