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Drug Monograph

Enoxaparin (Lovenox)

Enoxaparin sodium — generic formulations widely available
Low Molecular Weight Heparin (LMWH) · Subcutaneous, Intravenous
Pharmacokinetic Profile
Half-Life
~4.5 h (single dose); ~7 h (repeated dosing)
Metabolism
Hepatic desulfation & depolymerisation
Protein Binding
Low (minimal plasma protein binding)
Bioavailability
~100% (SC)
Volume of Distribution
~4.3 L (anti-Xa basis)
Clinical Information
Drug Class
Low Molecular Weight Heparin (LMWH)
Available Doses
30 mg, 40 mg, 60 mg, 80 mg, 100 mg, 120 mg, 150 mg (prefilled syringes); 300 mg/3 mL (multidose vial)
Route
Subcutaneous, Intravenous (STEMI bolus only)
Renal Adjustment
Required: CrCl <30 mL/min
Hepatic Adjustment
Use with caution
Pregnancy
Does not cross placenta; considered safe (avoid multidose vials with benzyl alcohol)
Lactation
Unknown excretion in human milk; weigh benefit vs risk
Schedule / Legal Status
Rx only
Generic Available
Yes
Reversal Agent
Protamine sulfate (partial: ~60% anti-Xa neutralisation)
Rx

Indications

IndicationApproved PopulationTherapy TypeStatus
DVT prophylaxis — hip replacement surgeryAdultsMonotherapyFDA Approved
DVT prophylaxis — knee replacement surgeryAdultsMonotherapyFDA Approved
DVT prophylaxis — abdominal surgeryAdults at risk of thromboembolic complicationsMonotherapyFDA Approved
DVT prophylaxis — acutely ill medical patientsAdults with severely restricted mobilityMonotherapyFDA Approved
Treatment of acute DVT (with or without PE)Adults (inpatient and outpatient)Bridge to warfarinFDA Approved
Unstable angina / NSTEMIAdults (with aspirin)Combination (with ASA)FDA Approved
Acute STEMI (with thrombolysis or PCI)Adults (with aspirin)Combination (with ASA ± fibrinolytic)FDA Approved

Enoxaparin is the most widely used low molecular weight heparin worldwide. Its predictable pharmacokinetics, high subcutaneous bioavailability, and established trial data make it the standard choice for both venous thromboembolism prevention and treatment, as well as adjunctive anticoagulation in acute coronary syndromes. The MEDENOX trial established its role in medical prophylaxis, while ExTRACT-TIMI 25 demonstrated superiority over unfractionated heparin as adjunctive therapy with fibrinolysis in STEMI.

Off-Label Uses

VTE prophylaxis in pregnancy: ACOG recommends enoxaparin 40 mg SC once daily for antepartum thromboprophylaxis in high-risk women. Dose-adjusted regimens (0.5–1 mg/kg q12h) are used for therapeutic anticoagulation. Evidence: High

Bridge anticoagulation for warfarin interruption: Commonly used periprocedurally to bridge patients with atrial fibrillation or mechanical heart valves who require temporary warfarin cessation, though the BRIDGE trial tempered enthusiasm for routine bridging in AF. Evidence: Moderate

Cerebral venous sinus thrombosis: LMWH is first-line anticoagulation per AHA/ASA guidelines, even in the presence of haemorrhagic infarction. Evidence: High

Dose

Dosing

VTE Prophylaxis by Clinical Scenario

Clinical ScenarioStarting DoseMaintenance DoseMaximum DoseNotes
Hip replacement surgery30 mg SC q12h (start 12–24 h post-op) or 40 mg SC once daily (start 9–15 h pre-op)Same as starting40 mg/day or 60 mg/dayContinue 10–14 days; extended prophylaxis up to 35 days reduces late VTE
Once-daily regimen common in Europe; q12h regimen common in US
Knee replacement surgery30 mg SC q12h (start 12–24 h post-op)30 mg SC q12h60 mg/dayContinue 10–14 days or until ambulatory
Ensure haemostasis at wound site before first dose
Abdominal / colorectal surgery40 mg SC once daily (start 2 h pre-op)40 mg SC once daily40 mg/dayContinue 7–10 days (up to 12 days studied)
In cancer surgery, consider extended prophylaxis up to 28 days
Acutely ill medical patients (restricted mobility)40 mg SC once daily40 mg SC once daily40 mg/dayContinue 6–11 days or until mobile
MEDENOX trial: 40 mg reduced VTE vs placebo; 20 mg did not

VTE Treatment and Acute Coronary Syndromes

Clinical ScenarioStarting DoseMaintenance DoseMaximum DoseNotes
Acute DVT/PE — inpatient treatment1 mg/kg SC q12h or 1.5 mg/kg SC once dailySame as startingWeight-based (no cap)Initiate warfarin within 72 h; continue enoxaparin for ≥5 days AND until INR 2.0–3.0 for ≥24 h
Average treatment duration 7 days; up to 17 days studied
Acute DVT without PE — outpatient treatment1 mg/kg SC q12h1 mg/kg SC q12hWeight-basedBridge to warfarin; same INR targets as inpatient
Suitable patients: haemodynamically stable, no massive PE, adequate home support
Unstable angina / NSTEMI1 mg/kg SC q12h (with aspirin 100–325 mg daily)1 mg/kg SC q12hWeight-basedContinue for ≥2 days until clinical stabilisation; usual duration 2–8 days
ESSENCE trial: enoxaparin superior to UFH for composite ischaemic endpoint
STEMI — age <75 years30 mg IV bolus + 1 mg/kg SC simultaneously1 mg/kg SC q12h100 mg per dose (first 2 SC doses only)Give with fibrinolytic (15 min before to 30 min after); continue for hospitalisation or up to 8 days
ExTRACT-TIMI 25: 17% RRR in death/MI vs UFH at 30 days
STEMI — age ≥75 years0.75 mg/kg SC q12h (NO IV bolus)0.75 mg/kg SC q12h75 mg per dose (first 2 SC doses only)Omit IV bolus to reduce bleeding risk in elderly
Age-adjusted regimen from ExTRACT-TIMI 25 protocol

Renal Dose Adjustment (CrCl <30 mL/min)

Clinical ScenarioStarting DoseMaintenance DoseMaximum DoseNotes
DVT prophylaxis (all surgical & medical)30 mg SC once daily30 mg SC once daily30 mg/dayReduced from standard 40 mg daily or 30 mg q12h
Consider UFH if CrCl <15 or on dialysis
DVT/PE treatment1 mg/kg SC once daily1 mg/kg SC once dailyWeight-basedChanged from q12h to once daily; monitor anti-Xa levels
Clearance reduced ~44% in severe renal impairment
UA/NSTEMI1 mg/kg SC once daily (with aspirin)1 mg/kg SC once dailyWeight-basedChanged from q12h to once daily
Monitor anti-Xa if prolonged therapy
STEMI <75 years30 mg IV bolus + 1 mg/kg SC1 mg/kg SC once dailyWeight-basedChanged from q12h to once daily after initial dose
FDA PI does not specify separate dose cap for renal regimen
STEMI ≥75 years1 mg/kg SC once daily (NO IV bolus)1 mg/kg SC once dailyWeight-basedNo IV bolus; changed from 0.75 mg/kg q12h to 1 mg/kg once daily
Dual adjustment for age AND renal impairment
Clinical Pearl: PCI Dosing Considerations

If the last SC dose of enoxaparin was administered <8 hours before balloon inflation, no additional anticoagulation is needed in the catheterisation laboratory. If >8 hours have elapsed since the last SC dose, give an IV bolus of 0.3 mg/kg enoxaparin. Do not switch between enoxaparin and unfractionated heparin, as this increases bleeding risk. If a manual compression method is used post-PCI, remove the sheath 6 hours after the last IV/SC enoxaparin dose. The next scheduled dose should be given no sooner than 6–8 hours after sheath removal.

PK

Pharmacology

Mechanism of Action

Enoxaparin is derived from unfractionated porcine heparin through controlled alkaline depolymerisation, yielding fragments with a mean molecular weight of approximately 4,500 daltons. Like all LMWHs, enoxaparin exerts its anticoagulant effect by binding to antithrombin III (AT-III) via a specific pentasaccharide sequence, potentiating AT-III’s inhibition of factor Xa. Because the shorter chain fragments of enoxaparin are generally too small to form the ternary complex required for efficient thrombin (factor IIa) inhibition, enoxaparin exhibits a higher ratio of anti-Xa to anti-IIa activity (~3.8:1) compared to unfractionated heparin (~1:1). This preferential anti-Xa activity provides effective antithrombotic action with a more predictable dose-response relationship, less platelet factor 4 binding (reducing HIT risk), and minimal effect on conventional clotting assays such as aPTT.

ADME Profile

ParameterValueClinical Implication
Absorption~100% bioavailability (SC); Tmax 3–5 h (SC), 5–10 min (IV); linear dose-proportional pharmacokineticsNear-complete SC absorption enables reliable weight-based dosing without routine laboratory monitoring in most patients; absorbed much more predictably than UFH
DistributionVd ~4.3 L (anti-Xa basis); low plasma protein binding; does not significantly cross the placentaLow Vd reflects largely intravascular distribution; minimal placental transfer makes it a preferred anticoagulant in pregnancy
MetabolismHepatic desulfation and depolymerisation to lower molecular weight fragments with reduced biological activity; not CYP-metabolisedHepatic metabolism is minor; no significant CYP-mediated drug interactions; use with caution in severe hepatic impairment due to altered haemostasis rather than impaired clearance
EliminationPrimarily renal; ~40% as active and inactive fragments in urine over 24 h; t½ 4.5 h (single dose), ~7 h (steady state) based on anti-Xa activityRenal-dependent clearance necessitates dose reduction at CrCl <30 mL/min; clearance reduced ~44% in severe renal impairment; not removed by haemodialysis
SE

Side Effects

≥10% Very Common
Adverse EffectIncidenceClinical Note
Injection site haematoma / ecchymosis10–18%Most common adverse effect; minimise by alternating injection sites (left/right anterolateral and posterolateral abdominal wall); do not rub the site after injection
Anaemia<1% to 16%Incidence varies by indication; highest in hip replacement trials; monitor haemoglobin; may reflect occult bleeding rather than direct haematological effect
1–10% Common
Adverse EffectIncidenceClinical Note
Elevated hepatic transaminases (AST/ALT)5–6%Generally asymptomatic and reversible; elevations >3× ULN occur in ~5% of patients; rarely requires discontinuation; monitor if persistent or symptomatic
Minor bleeding (haematuria, epistaxis, wound oozing)3–7%Incidence increases with therapeutic (vs prophylactic) dosing; manage conservatively; assess for supratherapeutic anti-Xa levels in renal impairment
Thrombocytopenia (mild, non-immune)1–3%Type I: mild, transient, occurs within first few days; non-immune mediated; does not require discontinuation; distinguish from HIT (type II)
Nausea / diarrhoea1–3%Generally mild and self-limiting
Peripheral oedema2–6%More common in surgical prophylaxis trials; distinguish from DVT recurrence
Fever1–5%Common in post-surgical setting; rule out infection and thrombotic complications
Serious Serious (Regardless of Frequency)
Adverse EffectEstimated FrequencyTypical OnsetRequired Action
Major haemorrhage (GI, retroperitoneal, intracranial)1–4% (therapeutic dosing); <1% (prophylactic dosing)Any time during treatmentDiscontinue enoxaparin; administer protamine sulfate 1 mg per 1 mg enoxaparin given in last 8 h (max 60% reversal); transfuse as needed; surgical haemostasis if required
Heparin-induced thrombocytopenia (HIT type II)<1% (lower than UFH at 1–5%)5–10 days after initiation (or within hours if prior heparin exposure)Discontinue ALL heparin products immediately; initiate non-heparin anticoagulant (argatroban, bivalirudin, or fondaparinux); send PF4/heparin antibodies and functional assay; do NOT transfuse platelets (risk of thrombosis)
Spinal / epidural haematomaRare (estimated 1 in 3,000–150,000)Hours to days after neuraxial procedureEmergency MRI and neurosurgical decompression within 8–12 h of symptom onset to prevent permanent paralysis; monitor for back pain, numbness, weakness, bowel/bladder dysfunction
Skin necrosis at injection siteRareDays to weeksDiscontinue enoxaparin; may indicate underlying HIT; evaluate for anti-PF4 antibodies; switch to alternative anticoagulant
Hyperkalaemia1–5% (patients with renal impairment or diabetes)Days to weeksMonitor potassium in at-risk patients (renal failure, diabetes, acidosis, concurrent K+-sparing agents); treat per standard hyperkalaemia protocols
Osteoporosis (with prolonged use)Uncommon; less than UFHMonths of continuous useConsider DEXA scan for patients on >3 months of therapy (e.g., pregnancy); LMWH has less osteoporotic effect than UFH; ensure adequate calcium and vitamin D
Discontinuation Discontinuation Rates
Prophylactic Dosing
<3% due to adverse events
Top reasons: Bleeding, thrombocytopenia, injection site reactions
Therapeutic Dosing
3–7% due to adverse events
Top reasons: Major bleeding, HIT, patient preference (injection burden)
Reason for DiscontinuationIncidenceContext
Clinically significant bleeding1–4%Highest at therapeutic doses; may require reversal with protamine
Suspected or confirmed HIT<1%Mandates immediate discontinuation of all heparin products and switch to alternative anticoagulant
Transition to oral anticoagulantExpectedStandard clinical course: bridge to warfarin (INR 2–3) or transition to DOAC per guideline
Recognising Heparin-Induced Thrombocytopenia (HIT)

Suspect HIT when the platelet count falls by ≥50% from baseline, typically 5–10 days after starting heparin/LMWH, or immediately in patients with prior heparin exposure within the last 100 days. The 4T scoring system (Thrombocytopenia, Timing, Thrombosis, oTher causes) should be applied. A high pre-test probability warrants immediate cessation of all heparin products and initiation of a non-heparin anticoagulant (argatroban, bivalirudin, or fondaparinux) before confirmatory results (PF4/heparin ELISA, serotonin release assay) return. Do NOT use another LMWH as a substitute. Warfarin should NOT be started until the platelet count has recovered to ≥150,000/mcL.

Int

Drug Interactions

Enoxaparin is not metabolised by cytochrome P450 enzymes, so classic CYP-mediated drug interactions are not a concern. However, its anticoagulant activity means that any co-administered drug affecting haemostasis substantially increases bleeding risk. The FDA PI recommends discontinuing agents that enhance haemorrhage risk prior to starting enoxaparin, or conducting close clinical and laboratory monitoring if co-administration is essential.

Major Warfarin / DOACs
MechanismAdditive anticoagulant effect through complementary inhibition of coagulation factors
EffectSubstantially increased bleeding risk during overlap period
ManagementDuring warfarin bridging, overlap for ≥5 days and until INR ≥2.0 for 24 h; when transitioning to DOAC, start DOAC at the time of next scheduled enoxaparin dose
FDA PI
Major Antiplatelet Agents (ASA, clopidogrel, ticagrelor, prasugrel)
MechanismAdditive impairment of haemostasis: anticoagulant + antiplatelet
EffectIncreased risk of major bleeding, particularly GI and procedural bleeding
ManagementConcurrent aspirin is part of standard ACS therapy but requires heightened bleeding surveillance; use lowest effective aspirin dose; add PPI for GI protection in high-risk patients
ACC/AHA Guidelines
Major NSAIDs (ibuprofen, naproxen, ketorolac)
MechanismNSAIDs impair platelet function and promote GI mucosal injury; additive bleeding risk with enoxaparin
EffectSignificantly increased risk of GI and surgical bleeding
ManagementAvoid concurrent use whenever possible; use paracetamol for analgesia; if NSAID essential, use shortest duration and lowest dose with GI protection
FDA PI
Major Thrombolytics (alteplase, tenecteplase, reteplase)
MechanismFibrinolysis combined with anticoagulation produces profound haemostatic impairment
EffectSubstantially increased major bleeding including intracranial haemorrhage
ManagementExpected combination in STEMI; administer enoxaparin 15 min before to 30 min after fibrinolytic per ExTRACT-TIMI 25 protocol; strict adherence to age-adjusted dosing is critical
ExTRACT-TIMI 25
Moderate SSRIs / SNRIs
MechanismSerotonin reuptake inhibition impairs platelet aggregation
EffectIncreased bleeding tendency, particularly GI
ManagementMonitor for signs of bleeding; consider PPI co-therapy if high GI bleeding risk
Lexicomp
Moderate Potassium-Sparing Diuretics / ACE Inhibitors / ARBs
MechanismEnoxaparin can suppress aldosterone secretion; combined with K+-retaining agents, risk of hyperkalaemia increases
EffectHyperkalaemia, especially in patients with renal impairment or diabetes
ManagementMonitor serum potassium at baseline and periodically during therapy; highest risk in patients with CrCl <30 mL/min
FDA PI
Mon

Monitoring

  • Platelet Count Baseline; then q2–3 days for 2 weeks
    Routine     Essential for HIT surveillance; suspect HIT if platelet count drops ≥50% from baseline or falls below 100,000/mcL, typically day 5–10; earlier onset possible with prior heparin exposure within 100 days
  • CBC with Haemoglobin Baseline; periodic
    Routine     Monitor for occult bleeding manifesting as unexplained haemoglobin decline; stool occult blood tests recommended during treatment course per FDA PI
  • Renal Function Baseline; during therapy
    Routine     Calculate CrCl (Cockcroft-Gault) before initiating; dose adjustment required at CrCl <30 mL/min; repeat if clinical status changes (acute kidney injury, dehydration, sepsis)
  • Anti-Factor Xa Level PRN: obesity, renal impairment, extremes of weight, pregnancy
    Trigger-based     Draw 4–6 hours after 3rd dose (steady state); therapeutic target: 0.5–1.0 IU/mL (q12h dosing) or 1.0–2.0 IU/mL (once-daily dosing); prophylactic target: 0.2–0.5 IU/mL; not needed for routine prophylaxis in normal-weight patients with preserved renal function
  • Serum Potassium Baseline; periodic in at-risk patients
    Trigger-based     Risk of heparin-induced aldosterone suppression causing hyperkalaemia; monitor in patients with renal failure, diabetes, concurrent ACE inhibitor/ARB/K+-sparing diuretic use
  • Neurological Status Post-neuraxial procedure
    Trigger-based     Monitor for signs of spinal/epidural haematoma (new back pain, lower limb weakness, sensory changes, bowel/bladder dysfunction) after spinal anaesthesia or lumbar puncture while on enoxaparin; urgent MRI if suspected
  • Signs of Bleeding Every assessment
    Routine     Assess for unexplained bruising, haematuria, melaena, haematemesis, prolonged bleeding from puncture sites, or sudden haemoglobin drop; particular vigilance after PCI, surgery, or invasive procedures
CI

Contraindications & Cautions

Absolute Contraindications

  • Active major bleeding: Any uncontrolled haemorrhage is an absolute contraindication to anticoagulation
  • History of HIT with enoxaparin or any heparin product: Anti-PF4/heparin antibodies show high in vitro cross-reactivity with all LMWHs; guidelines recommend against substituting one LMWH for another in confirmed HIT
  • Hypersensitivity to enoxaparin, heparin, or porcine products: Includes anaphylaxis, severe urticaria, or bronchospasm
  • Hypersensitivity to benzyl alcohol: Applies to multidose vial formulation only; use preservative-free prefilled syringes as alternative

Relative Contraindications (Specialist Input Recommended)

  • Severe renal impairment (CrCl <30 mL/min): If enoxaparin is used, dose must be reduced and anti-Xa levels monitored; UFH may be preferred for CrCl <15 mL/min or patients on dialysis
  • Severe uncontrolled hypertension: Increased risk of intracranial haemorrhage
  • Active peptic ulcer disease or recent GI haemorrhage: Risk of recurrent or worsened bleeding
  • Diabetic retinopathy (proliferative): Risk of intraocular haemorrhage
  • Mechanical prosthetic heart valves in pregnancy: Inadequate anticoagulation reported; fatalities documented in clinical study; requires intensive anti-Xa monitoring
  • Recent neuraxial anaesthesia or lumbar puncture: Risk of spinal/epidural haematoma; strict timing of dosing relative to catheter insertion/removal is mandatory

Use with Caution

  • Elderly patients (≥75 years): Age-related decline in renal function may increase enoxaparin exposure; use age-adjusted STEMI dosing (no IV bolus, 0.75 mg/kg q12h); monitor renal function
  • Low body weight (<45 kg women, <57 kg men): Increased exposure with fixed prophylactic dosing; observe closely for bleeding
  • Obesity (BMI >40 kg/m²): Standard prophylactic doses may be subtherapeutic; consider 40 mg q12h or weight-based dosing with anti-Xa monitoring
  • Severe hepatic impairment: Altered haemostasis and bleeding risk; limited clinical data; use with caution
  • Concurrent antiplatelet or anticoagulant therapy: Substantially increased bleeding risk; ensure clinical benefit outweighs risk
FDA Boxed Warning Spinal/Epidural Haematomas with Neuraxial Anaesthesia

Epidural or spinal haematomas may occur in patients anticoagulated with LMWH or heparinoids who are receiving neuraxial anaesthesia or undergoing spinal puncture. These haematomas may result in long-term or permanent paralysis. Risk is increased by the use of indwelling epidural catheters, concurrent use of drugs affecting haemostasis (NSAIDs, antiplatelet agents, other anticoagulants), traumatic or repeated epidural/spinal puncture, and a history of spinal deformity or spinal surgery. Patients should be frequently monitored for signs of neurological impairment. If neurological compromise is noted, urgent treatment is necessary. The clinician should consider the potential benefit versus risk before neuraxial intervention in patients anticoagulated or to be anticoagulated for thromboprophylaxis.

Neuraxial Timing Guidelines (ASRA 2018)

Prophylactic dose (30–40 mg daily): Wait ≥12 hours after last dose before needle placement or catheter removal. Resume enoxaparin ≥4 hours after catheter removal.

Therapeutic dose (1 mg/kg q12h or 1.5 mg/kg daily): Wait ≥24 hours after last dose before needle placement or catheter removal. Resume enoxaparin ≥4 hours after catheter removal.

CrCl <30 mL/min: Double the time intervals above (at least 24 h for prophylactic, 48 h for therapeutic dosing).

Pt

Patient Counselling

Purpose of Therapy

Explain that enoxaparin is a blood-thinning medication given by injection under the skin to prevent or treat blood clots. Blood clots can form in the legs (deep vein thrombosis) and travel to the lungs (pulmonary embolism), which can be life-threatening. In patients with heart conditions, enoxaparin helps prevent further clot formation in coronary arteries. It is essential to take the medication exactly as prescribed and to attend all follow-up appointments for blood tests.

How to Administer

For patients self-injecting at home, demonstrate the correct technique: pinch a fold of skin on the lower abdomen (alternating left and right sides, at least 5 cm from the navel), insert the entire needle at a 90-degree angle, depress the plunger fully, and release the skin fold only after the needle is withdrawn. Do not rub the injection site afterward, as this increases bruising. Each prefilled syringe is single-use. Dispose of used syringes in a sharps container.

Bruising at Injection Sites
Tell patient Some bruising at the injection site is normal and expected. You can reduce bruising by alternating injection sites on either side of the abdomen and by not rubbing the area after injection. Applying gentle pressure with a cotton ball for 1–2 minutes may help.
Call prescriber If bruises are very large, growing, or if hard lumps form under the skin at injection sites.
Bleeding Risk
Tell patient Because enoxaparin thins the blood, you may bleed more easily. Use caution with sharp objects, and avoid activities with a high risk of injury. Use an electric razor instead of a blade. Avoid over-the-counter pain medications like ibuprofen or naproxen, as these increase bleeding risk. Paracetamol (acetaminophen) is a safer alternative for pain relief while on enoxaparin.
Call prescriber If you notice blood in urine or stool, black or tarry stools, vomiting blood, nosebleeds that do not stop within 10 minutes, severe or unexplained bruising, or any fall or head injury.
Signs of Blood Clots
Tell patient Even while on enoxaparin, blood clots can still occasionally occur. Stay mobile as much as possible. Watch for new swelling, pain, warmth, or redness in a leg, or sudden shortness of breath, chest pain, or rapid heartbeat, which could indicate a clot in the lungs.
Call prescriber Seek emergency medical attention immediately if you develop sudden shortness of breath, chest pain, coughing up blood, or new leg swelling and pain.
Spinal or Epidural Procedures
Tell patient If you have recently had or are planning any spinal or epidural injection or procedure, it is critical that your anaesthetist and surgeon know you are taking enoxaparin. Rare but serious bleeding near the spine can occur, which could lead to permanent nerve damage.
Call prescriber If you develop sudden back pain, leg numbness, tingling, or weakness, or loss of bladder or bowel control after a spinal or epidural procedure.
Missed Dose
Tell patient If you miss a dose, take it as soon as you remember. If it is almost time for the next dose, skip the missed dose and take the next one as scheduled. Never take a double dose to make up for a missed one.
Call prescriber If you miss more than one dose or are unsure about when to take your next injection.
Ref

Sources

Regulatory (PI / SmPC)
  1. Lovenox (enoxaparin sodium) Prescribing Information. Sanofi-Aventis U.S. LLC. Revised March 2026. https://www.drugs.com/pro/lovenox.html Primary FDA-approved label with complete dosing, renal adjustments, adverse reactions, and boxed warning for spinal/epidural haematoma.
  2. Lovenox (enoxaparin sodium) FDA Label 2021. https://www.accessdata.fda.gov/drugsatfda_docs/label/2021/020164s129lbl.pdf Full prescribing information with pharmacokinetic data, clinical trial results tables, and adverse reactions by indication.
Key Clinical Trials
  1. Antman EM, Morrow DA, McCabe CH, et al. Enoxaparin versus unfractionated heparin with fibrinolysis for ST-elevation myocardial infarction (ExTRACT-TIMI 25). N Engl J Med. 2006;354(14):1477–1488. doi:10.1056/NEJMoa060898 Landmark RCT (n=20,479) demonstrating enoxaparin superiority over UFH for death/MI in STEMI with fibrinolysis; established age-adjusted dosing for elderly patients.
  2. Cohen M, Demers C, Gurfinkel EP, et al. A comparison of low-molecular-weight heparin with unfractionated heparin for unstable coronary artery disease (ESSENCE). N Engl J Med. 1997;337(7):447–452. doi:10.1056/NEJM199708143370702 Pivotal trial establishing enoxaparin as superior to UFH in UA/NSTEMI for the composite endpoint of death, MI, or recurrent angina at 14 and 30 days.
  3. Samama MM, Cohen AT, Darmon JY, et al. A comparison of enoxaparin with placebo for the prevention of venous thromboembolism in acutely ill medical patients (MEDENOX). N Engl J Med. 1999;341(11):793–800. doi:10.1056/NEJM199909093411103 Double-blind RCT demonstrating 40 mg enoxaparin daily significantly reduced VTE in acutely ill medical patients vs placebo without increasing major bleeding.
  4. Bergqvist D, Agnelli G, Cohen AT, et al. Duration of prophylaxis against venous thromboembolism with enoxaparin after surgery for cancer (ENOXACAN II). N Engl J Med. 2002;346(13):975–980. doi:10.1056/NEJMoa012385 Extended prophylaxis trial showing 4 weeks of enoxaparin post abdominal/pelvic cancer surgery reduced VTE from 12% to 4.8% vs 1 week of treatment.
Guidelines
  1. Kearon C, Akl EA, Ornelas J, et al. Antithrombotic Therapy for VTE Disease: CHEST Guideline and Expert Panel Report. Chest. 2016;149(2):315–352. doi:10.1016/j.chest.2015.11.026 ACCP guideline providing recommendations on LMWH dosing for VTE treatment and prophylaxis, including renal adjustment thresholds.
  2. Horlocker TT, Vandermeuelen E, Kopp SL, et al. Regional Anesthesia in the Patient Receiving Antithrombotic or Thrombolytic Therapy: ASRA 2018 Guidelines. Reg Anesth Pain Med. 2018;43(3):263–309. doi:10.1097/AAP.0000000000000763 Consensus guidelines on timing of neuraxial procedures relative to LMWH dosing, establishing the 12-hour and 24-hour windows for prophylactic and therapeutic dosing.
  3. Lawton JS, Tamis-Holland JE, Bangalore S, et al. 2025 ACC/AHA/ACEP/NAEMSP/SCAI Guideline for the Management of Patients With Acute Coronary Syndromes. Circulation. 2025. doi:10.1161/CIR.0000000000001309 Most current ACS guideline with enoxaparin dosing recommendations for STEMI and NSTE-ACS, including PCI transition guidance.
Mechanistic / Basic Science
  1. Fareed J, Hoppensteadt DA, Bick RL. An update on heparins at the beginning of the new millennium. Semin Thromb Hemost. 2000;26(Suppl 1):5–21. doi:10.1055/s-2000-9488 Comprehensive review of LMWH pharmacology including anti-Xa:anti-IIa ratios, AT-III binding kinetics, and differentiation from UFH.
Pharmacokinetics / Special Populations
  1. Enoxaparin. In: StatPearls [Internet]. Treasure Island (FL): StatPearls Publishing; 2023. https://www.ncbi.nlm.nih.gov/books/NBK539865/ Comprehensive clinical review covering mechanism, pharmacokinetics, dosing by indication, adverse effects, and monitoring recommendations.
  2. Hulot JS, Vantelon C, Urien S, et al. Effect of renal function on the pharmacokinetics of enoxaparin and consequences on dose adjustment. Ther Drug Monit. 2004;26(3):305–310. doi:10.1097/00007691-200406000-00014 Population PK study demonstrating 44% clearance reduction in severe renal impairment and 31% reduction in moderate impairment, forming the basis for dose adjustments.
  3. Bazinet A, Bhatt M, Bhatt DK, et al. Dosing of enoxaparin in renal impairment. Pharmacy (Basel). 2017;5(1):1. doi:10.3390/pharmacy5010001 Review of enoxaparin pharmacokinetics in renal impairment with analysis of dose adjustment strategies and anti-Xa monitoring targets.