My Dashboard
Courses
Articles Evidence Reviews Practice Updates Cases News Presentations
About Us
My Dashboard
Drug Monograph

Heparin (Unfractionated Heparin)

Heparin sodium β€” derived from porcine intestinal mucosa
Anticoagulant (Glycosaminoglycan) Β· Intravenous, Subcutaneous
Pharmacokinetic Profile
Half-Life
0.5–2 h (dose-dependent)
Metabolism
Reticuloendothelial system (liver, macrophages)
Protein Binding
Extensive (AT-III, fibrinogen, plasma proteins, endothelial cells)
Bioavailability
~30% SC (variable); 100% IV
Volume of Distribution
~0.07 L/kg (approximates intravascular volume)
Clinical Information
Drug Class
Unfractionated Heparin (UFH)
Available Formulations
1,000–20,000 units/mL (vials); premixed bags (25,000 units/250–500 mL in D5W or NS); flush 10–100 units/mL
Route
IV continuous infusion, IV bolus, SC
Renal Adjustment
No formal adjustment; clearance may decrease β€” monitor aPTT closely
Hepatic Adjustment
Caution; clearance may decrease β€” dose adjustment may be required
Pregnancy
Does not cross placenta; preferred parenteral anticoagulant in pregnancy (use preservative-free)
Lactation
Not excreted in breast milk; compatible
Schedule / Legal Status
Rx only
Generic Available
Yes
Reversal Agent
Protamine sulfate (complete reversal: 1 mg per 100 units heparin)
Therapeutic Index
Narrow β€” HIGH-ALERT medication (ISMP)
Rx

Indications

IndicationApproved PopulationTherapy TypeStatus
Treatment of DVT and PEAdults, PaediatricsMonotherapy (bridge to warfarin or DOAC)FDA Approved
Prevention of DVT and PEAdults (perioperative)Monotherapy (low-dose SC)FDA Approved
Atrial fibrillation with embolisationAdultsMonotherapy or bridgeFDA Approved
Peripheral arterial embolismAdultsMonotherapyFDA Approved
Anticoagulation during cardiac surgery / extracorporeal circulationAdults, PaediatricsMonotherapyFDA Approved
Diagnosis and treatment of DIC (consumptive coagulopathy)AdultsMonotherapyFDA Approved
Prevention of clotting in blood sampling and heparin lock flushAll agesFlushFDA Approved

Unfractionated heparin remains the parenteral anticoagulant of choice in settings requiring rapid onset, short duration of action, and complete reversibility with protamine. Its short half-life and titrability make it indispensable in the ICU, operating theatre, and cardiac catheterisation laboratory. While LMWH has largely replaced UFH for standard VTE prophylaxis and treatment in haemodynamically stable patients, UFH is preferred in severe renal impairment, high bleeding risk scenarios, and when urgent procedures may require rapid reversal of anticoagulation.

Off-Label Uses

ACS (UA/NSTEMI/STEMI): IV heparin is widely used per ACC/AHA guidelines as adjunctive anticoagulation in ACS. The 2025 ACC/AHA ACS guideline recommends parenteral anticoagulation for all patients with ACS to reduce major adverse cardiovascular events. Evidence: High

Continuous renal replacement therapy (CRRT): Heparin is used for circuit anticoagulation in CRRT, though regional citrate anticoagulation is increasingly preferred. Evidence: Moderate

Acute limb ischaemia: Immediate systemic heparinisation is recommended at diagnosis per 2024 ACC/AHA PAD guidelines. Evidence: High

Dose

Dosing

Therapeutic Anticoagulation by Clinical Scenario

Clinical ScenarioStarting DoseMaintenance DoseMaximum DoseNotes
VTE treatment (DVT/PE)80 units/kg IV bolus18 units/kg/hr continuous infusionWeight-based (institution-specific caps)Titrate to aPTT 1.5–2.5Γ— control (or anti-Xa 0.3–0.7 IU/mL)
Raschke nomogram: superior to fixed-dose (5000 U bolus, 1000 U/hr)
UA / NSTEMI (ACS)60 units/kg IV bolus (max 5,000 units)12 units/kg/hr (max 1,000 units/hr)Bolus max 5,000 U; infusion max 1,000 U/hrTarget aPTT 50–70 sec; co-administer with aspirin and P2Y12 inhibitor
Lower dose than VTE to reduce bleeding with concurrent antiplatelets
STEMI with fibrinolysis (alteplase)60 units/kg IV bolus (max 4,000 units)12 units/kg/hr (max 1,000 units/hr)Bolus max 4,000 U; infusion max 1,000 U/hrTarget aPTT 50–70 sec; continue for 48 h or until revascularisation
Per ACC/AHA STEMI guidelines; lower bolus cap than UA/NSTEMI
PCI (without GP IIb/IIIa inhibitor)70–100 units/kg IV bolusAdditional boluses PRNWeight-basedTarget ACT 250–350 sec (HemoTec) or 300–350 sec (Hemochron)
Additional bolus if ACT below target during procedure
PCI (with GP IIb/IIIa inhibitor)50–70 units/kg IV bolusAdditional boluses PRNWeight-basedTarget ACT 200–250 sec
Lower target to reduce bleeding with concurrent GP IIb/IIIa
Cardiopulmonary bypass300–400 units/kg IVPRN to maintain ACT400 units/kgTarget ACT >480 sec; 300 U/kg for procedures <60 min, 400 U/kg for >60 min
Reverse with protamine post-bypass (1 mg per 100 U given)

Prophylaxis and Other Uses

Clinical ScenarioStarting DoseMaintenance DoseMaximum DoseNotes
Postoperative VTE prophylaxis (low-dose)5,000 units SC 2 h before surgery5,000 units SC q8–12h5,000 units per doseContinue for 7 days or until fully ambulatory; deep SC into abdominal fat
aPTT monitoring not required at prophylactic doses
Medical VTE prophylaxis5,000 units SC q8–12h5,000 units SC q8–12h5,000 units per doseFor acutely ill hospitalised patients with restricted mobility
LMWH generally preferred over UFH for medical prophylaxis (MEDENOX)
Paediatric therapeutic anticoagulation75–100 units/kg IV bolus over 10 minInfants: 25–30 units/kg/hr; Children >1 yr: 18–20 units/kg/hrWeight-basedTitrate to aPTT or anti-Xa; neonates <2 months may require ~28 U/kg/hr
Use preservative-free formulations in neonates (avoid benzyl alcohol)
Catheter lock flush10–100 units/mLInstil to fill catheter lumen; flush q6–8hPer catheter volumeDo not use full-strength heparin vials for flush β€” fatal overdoses reported
ISMP high-alert: verify concentration before use
HIGH-ALERT Medication: Concentration Verification

Heparin is available in numerous concentrations (from 1 unit/mL flush solution to 20,000 units/mL vials). Fatal haemorrhages have occurred from medication errors involving wrong concentration selection. The FDA and ISMP mandate that all heparin products be carefully examined to confirm the correct container choice prior to administration. Use independent double checks for all heparin infusion calculations. Heparin lock flush vials must never be confused with therapeutic heparin vials.

Clinical Pearl: Heparin Resistance

Heparin resistance is defined as requiring >35,000 units/day to achieve a therapeutic aPTT. Common causes include antithrombin III (AT-III) deficiency (congenital or acquired), elevated factor VIII or fibrinogen (acute-phase reactants), increased heparin clearance, and concurrent medications. When resistance is suspected, check AT-III levels and consider switching to anti-Xa-based monitoring. AT-III concentrate supplementation may restore heparin sensitivity in AT-III-deficient patients.

PK

Pharmacology

Mechanism of Action

Unfractionated heparin is a heterogeneous mixture of glycosaminoglycan chains with molecular weights ranging from 3,000 to 30,000 daltons (mean ~15,000 Da). Its anticoagulant activity depends on a specific pentasaccharide sequence that binds to antithrombin III (AT-III), inducing a conformational change that accelerates AT-III’s inactivation of coagulation serine proteases by approximately 1,000-fold. Unlike LMWHs, UFH chains are long enough to simultaneously bridge AT-III and thrombin (factor IIa), enabling potent inhibition of both factor Xa and thrombin in approximately equal measure (anti-Xa:anti-IIa ratio ~1:1). Heparin also prevents fibrin clot stabilisation by inhibiting factor XIIIa activation but does not possess fibrinolytic activity and will not dissolve existing clots. The broad spectrum of plasma protein binding accounts for its unpredictable dose-response and the necessity for laboratory-guided dose titration.

ADME Profile

ParameterValueClinical Implication
AbsorptionNot absorbed orally; IV onset immediate; SC onset 1–2 h; SC bioavailability ~30% (variable and unpredictable)IV route preferred for therapeutic anticoagulation due to immediate onset and predictable delivery; SC reserved for prophylaxis where precise anticoagulation is less critical
DistributionVd ~0.07 L/kg (~60 mL/kg); distributes primarily within intravascular space; binds extensively to AT-III, fibrinogen, globulins, lipoproteins, endothelial cells, and macrophagesHighly variable protein binding is the principal reason for unpredictable dose-response; acute-phase proteins (factor VIII, fibrinogen) compete for binding sites, contributing to heparin resistance in acute illness
MetabolismPrimarily by reticuloendothelial system (liver sinusoidal endothelial cells and macrophages); partially depolymerised and desulfated; not metabolised by CYP enzymesSaturable binding to endothelial cells and macrophages creates dose-dependent (zero-order) clearance at lower doses; at higher doses, non-saturable renal excretion (first-order) predominates, producing the characteristic non-linear pharmacokinetics
EliminationBiphasic: rapid saturable phase (RES uptake) then slower first-order renal phase; tΒ½ 0.5–2 h (dose-dependent); not removed by haemodialysisShort half-life is a key clinical advantage: allows rapid reversal by simply stopping the infusion (~4 h to clear); protamine provides immediate full reversal in emergencies; longer aPTT observed in patients β‰₯60 years
SE

Side Effects

β‰₯10% Very Common
Adverse EffectIncidenceClinical Note
Bleeding (any site, therapeutic dosing)10–33%Varies widely by intensity and concurrent therapy; most common with supratherapeutic aPTT; risk increases with age β‰₯60, concurrent antiplatelets, and renal impairment
Thrombocytopenia (type I, non-immune)10–30%Mild, transient (platelet count rarely <100,000); occurs within first 2 days; non-immune direct platelet activation; does not require discontinuation; distinguish from HIT
1–10% Common
Adverse EffectIncidenceClinical Note
Elevated hepatic transaminases (AST/ALT)5–9%Transient and typically asymptomatic; occurs in the first week; rarely requires discontinuation; not predictive of hepatic injury
Injection site haematoma (SC dosing)5–10%Minimise with proper deep SC technique into abdominal fat fold; avoid IM administration (higher haematoma risk)
Minor bleeding (epistaxis, haematuria, ecchymosis)3–8%More common at therapeutic than prophylactic doses; manage conservatively; check aPTT and adjust dose
Serious Serious (Regardless of Frequency)
Adverse EffectEstimated FrequencyTypical OnsetRequired Action
Major haemorrhage (GI, retroperitoneal, intracranial, adrenal)1–5% (therapeutic dosing)Any time during therapyStop heparin immediately; give protamine sulfate (1 mg per 100 units given in last 2–2.5 h; max 50 mg slow IV over 10 min); transfuse as indicated; evaluate for adrenal haemorrhage if hypotension
Heparin-induced thrombocytopenia type II (HIT)1–5% (surgical patients); 0.1–1% (medical patients)Day 5–10 (or within hours if prior heparin exposure in last 100 days)Stop ALL heparin immediately (including flushes and coated catheters); start non-heparin anticoagulant (argatroban, bivalirudin, or fondaparinux); send PF4/heparin antibodies + functional assay; do NOT give platelets; do NOT start warfarin until platelets β‰₯150,000
HIT with thrombosis (HITT)~50% of HIT patients develop thrombosisDuring or shortly after HIT episodeFull therapeutic non-heparin anticoagulation; imaging for DVT/PE; may result in stroke, MI, limb ischaemia, amputation, or death if not promptly treated
Osteoporosis~2–3% with prolonged use (>6 months)Months of continuous therapyConsider switching to LMWH (lower osteoporotic risk) for prolonged anticoagulation (e.g., pregnancy); DEXA monitoring for patients on >3 months of therapy
HyperkalaemiaUncommon; higher risk in renal impairment / diabetesDays to weeksMonitor potassium in patients with renal failure, diabetes, or concurrent K+-sparing drugs; heparin suppresses aldosterone secretion
Anaphylactoid reactionsRareMinutes to hours after first doseDiscontinue heparin; manage as anaphylaxis with epinephrine; patients with pork allergy at higher risk; consider synthetic alternatives (fondaparinux, argatroban)
Discontinuation Discontinuation Rates
Therapeutic Dosing
5–10% due to adverse events
Top reasons: Bleeding, HIT, transition to oral anticoagulant, difficulty maintaining therapeutic aPTT
Prophylactic Dosing
<3% due to adverse events
Top reasons: Bleeding, injection site reactions, thrombocytopenia
Protamine Reversal: Key Dosing Principles

Protamine sulfate fully neutralises heparin’s anti-IIa and anti-Xa activity (unlike ~60% neutralisation of LMWH). Dose is based on the amount of heparin given and elapsed time. If given within 30 minutes of the last heparin dose, use 1 mg protamine per 100 units heparin. If 30–60 minutes have elapsed, use 0.5–0.75 mg per 100 units. If >2 hours, protamine may not be needed. For continuous infusion, calculate the dose based on heparin given in the preceding 2–2.5 hours. Maximum single dose: 50 mg administered slowly over 10 minutes. Monitor for protamine-related hypotension and anaphylactoid reactions (especially in patients with fish allergy, prior protamine exposure, or vasectomy).

Int

Drug Interactions

Heparin is not metabolised by CYP enzymes, so pharmacokinetic drug interactions are uncommon. However, any agent affecting haemostasis has the potential to amplify or attenuate heparin’s anticoagulant effect. The FDA PI specifically notes that drugs interfering with platelet aggregation represent the main haemostatic defence of heparinised patients and should be used with caution.

MajorAntiplatelet Agents (ASA, clopidogrel, GP IIb/IIIa inhibitors)
MechanismAdditive impairment of haemostasis: anticoagulant + antiplatelet
EffectSubstantially increased bleeding risk; concurrent use is standard in ACS but requires dose adjustment and close monitoring
ManagementUse ACS-specific lower heparin doses (60 U/kg bolus, 12 U/kg/hr); lower ACT targets with GP IIb/IIIa (200–250 sec); PPI for GI protection
ACC/AHA Guidelines
MajorWarfarin / DOACs
MechanismOverlapping anticoagulant effect through different pathways
EffectIncreased bleeding during overlap; heparin prolongs PT/INR and may give falsely elevated warfarin readings
ManagementDraw INR β‰₯5 h after last IV heparin dose or β‰₯24 h after last SC dose for valid reading; overlap for β‰₯5 days during warfarin bridge; when transitioning to DOAC, start DOAC at time infusion is stopped
FDA PI
MajorThrombolytics (alteplase, tenecteplase)
MechanismFibrinolysis + anticoagulation produces profound haemostatic compromise
EffectSubstantially increased major bleeding including intracranial haemorrhage
ManagementExpected combination in STEMI; use lower ACS heparin dosing with caps (60 U/kg max 4,000 U bolus; 12 U/kg/hr max 1,000 U/hr); strict aPTT monitoring at 3, 6, 12, 24 h
ACC/AHA STEMI Guideline
ModerateNSAIDs (ibuprofen, ketorolac)
MechanismNSAIDs impair platelet function and promote GI mucosal injury
EffectIncreased risk of GI and surgical bleeding
ManagementDiscontinue NSAIDs prior to starting heparin when possible; use paracetamol for analgesia; if concurrent use essential, reduce heparin dose and add PPI
FDA PI
ModerateIV Nitroglycerin
MechanismIV nitroglycerin may reduce heparin’s anticoagulant effect through unclear mechanism (possibly enhanced heparin clearance)
EffectSubtherapeutic aPTT during co-administration; rebound supratherapeutic aPTT when nitroglycerin is stopped
ManagementMonitor aPTT closely when starting, adjusting, or stopping IV nitroglycerin; increase heparin dose during co-administration and reduce when nitroglycerin is discontinued
FDA PI
MinorDigitalis, tetracyclines, nicotine, antihistamines
MechanismMay partially counteract heparin’s anticoagulant effect through unclear pharmacodynamic mechanisms
EffectPossible reduction in heparin efficacy
ManagementMonitor aPTT and adjust heparin dose accordingly; clinical significance is generally limited
FDA PI
Mon

Monitoring

  • aPTTBaseline; 6 h after initiation; q6h until stable; then q12–24h
    Routine    Primary monitoring parameter for IV continuous infusion; therapeutic target 1.5–2.5Γ— control (typically 60–100 sec, institution-specific); draw from non-heparinised line; not reliable in lupus anticoagulant, elevated factor VIII, or DIC
  • Anti-Factor XaPRN: heparin resistance, discordant aPTT
    Trigger-based    Therapeutic target 0.3–0.7 IU/mL; draw 4–6 h after dose change; not affected by lupus anticoagulant or elevated factor VIII; increasingly used as primary monitoring parameter at some institutions
  • ACTDuring PCI and cardiac surgery
    Routine    Point-of-care test for high-dose heparin (procedures); target ACT varies by procedure and concurrent GP IIb/IIIa use; measured within minutes at bedside
  • Platelet CountBaseline; q2–3 days for first 2 weeks
    Routine    Essential for HIT surveillance; suspect HIT if platelet drop β‰₯50% from baseline, typically day 5–10; apply 4T score; higher risk with UFH than LMWH (1–5% vs <1%)
  • Haemoglobin / HaematocritBaseline; periodic
    Routine    Unexplained drop may indicate occult bleeding; stool occult blood testing recommended during therapy per FDA PI
  • Serum PotassiumBaseline; periodic in at-risk patients
    Trigger-based    Risk of heparin-induced aldosterone suppression causing hyperkalaemia; highest risk in renal impairment, diabetes, concurrent ACE inhibitors/ARBs/K+-sparing diuretics
  • Signs of BleedingEvery assessment
    Routine    Assess for unexpected blood pressure drops, tachycardia, unexplained back/flank pain (retroperitoneal bleed), abdominal distension (adrenal haemorrhage), haematuria, haematemesis, or prolonged oozing from puncture sites
CI

Contraindications & Cautions

Absolute Contraindications

  • Active uncontrolled bleeding: Any uncontrolled haemorrhage (except DIC, where heparin may be indicated)
  • Severe thrombocytopenia: Platelets <20,000/mcL (relative risk assessment required)
  • History of HIT or HITT: Absolute contraindication to all heparin products including LMWH; use non-heparin alternative
  • Hypersensitivity to heparin or pork products: Heparin is derived from porcine intestinal mucosa
  • Inability to perform coagulation monitoring: Full-dose heparin requires aPTT or anti-Xa monitoring; this does not apply to low-dose prophylaxis

Relative Contraindications (Specialist Input Recommended)

  • Recent CNS surgery or active intracranial bleeding: Extremely high risk of catastrophic haemorrhage
  • Severe uncontrolled hypertension: Increased intracranial haemorrhage risk
  • Active peptic ulcer disease: GI bleeding risk markedly increased
  • Subacute bacterial endocarditis: Risk of mycotic aneurysm rupture
  • Threatened abortion: Bleeding risk must be weighed against thrombotic risk
  • Recent spinal tap or spinal anaesthesia: Risk of spinal/epidural haematoma

Use with Caution

  • Elderly (β‰₯60 years): May have higher plasma levels and prolonged aPTT for equivalent doses; increased bleeding risk; may require lower starting doses
  • Renal or hepatic impairment: Decreased clearance may prolong anticoagulant effect; no formal dose adjustment but increased monitoring required
  • Recent surgery or invasive procedures: Risk of procedural bleeding; hold heparin per institutional protocols
  • Concurrent use of antiplatelet agents: Standard in ACS but requires lower heparin doses and vigilant monitoring
FDA Safety Alert Heparin Concentration Errors: Fatal Haemorrhage Risk

Heparin is supplied in numerous concentrations. Fatal haemorrhages have occurred due to errors in selecting the correct vial or premixed bag. The FDA and ISMP classify heparin as a HIGH-ALERT medication. All healthcare facilities must implement safeguards including independent double checks, barcode scanning, standardised concentrations, and clear labelling. Heparin lock flush solutions (1–100 units/mL) must be stored separately from therapeutic concentrations (1,000–20,000 units/mL) to prevent inadvertent overdose.

Pt

Patient Counselling

Purpose of Therapy

Explain that heparin is a blood-thinning medication administered by injection or continuous drip to prevent existing blood clots from growing larger and to reduce the risk of new clots forming. It works rapidly and is closely monitored with frequent blood tests to ensure the correct level of anticoagulation. Heparin is typically a short-term treatment while other longer-term blood thinners are being started.

How It Works in Hospital

Heparin is usually given through an IV line as a continuous drip. The nursing team will draw blood samples every few hours (from the opposite arm) to check the level of anticoagulation and adjust the dose accordingly. You may also receive heparin as injections under the skin in the abdomen after surgery to prevent clots during recovery.

Bleeding Risk
Tell patientWhile on heparin, you will bleed more easily. Inform your nurse or doctor about any new bruising, blood in your urine or stool, nosebleeds that do not stop, or bleeding from your gums. Use caution with sharp objects and avoid activities that could cause injury.
Call prescriberReport immediately any sudden severe headache, confusion, vision changes, severe abdominal or back pain, or blood in your vomit, as these could indicate serious internal bleeding.
Blood Test Monitoring
Tell patientFrequent blood draws are necessary to make sure the heparin dose is keeping your blood at the right level of thinness. This is a normal part of heparin treatment and is essential for your safety. The tests help prevent both clotting and excessive bleeding.
Call prescriberIf you notice signs of a new blood clot (new leg swelling, chest pain, shortness of breath) despite being on heparin, notify your care team immediately as this may indicate a need for dose adjustment or a rare complication called HIT.
Heparin-Induced Thrombocytopenia (HIT)
Tell patientIn rare cases, heparin can cause an immune reaction that lowers your platelet count and paradoxically increases clot risk. Your platelet levels will be checked regularly. If you have ever had a reaction to heparin before, it is critical that you inform every healthcare provider before any future medical treatments.
Call prescriberIf you develop new pain, redness, or swelling in a leg, sudden chest pain, shortness of breath, or a skin rash or darkening at heparin injection sites, notify your team immediately.
Transition to Oral Blood Thinner
Tell patientHeparin is typically a bridge medication. You will likely be transitioned to an oral blood thinner (such as warfarin or a newer oral anticoagulant) before discharge. There will be a period when you take both medications together. It is important to take the oral medication exactly as prescribed and attend follow-up appointments for INR monitoring if you are started on warfarin.
Call prescriberDo not stop any blood thinner without consulting your prescriber. If you are unsure about your medication schedule after discharge, contact your care team for clarification.
Ref

Sources

Regulatory (PI / SmPC)
  1. Heparin Sodium Injection Prescribing Information. FDA-approved label, revised 2024. https://www.accessdata.fda.gov/drugsatfda_docs/label/2024/017029s178lbl.pdfPrimary regulatory label with dosing recommendations, adverse reactions, contraindications, and full prescribing information for heparin sodium injection.
  2. Heparin Sodium in 0.9% Sodium Chloride Injection Prescribing Information. FDA label, revised 2025. https://www.accessdata.fda.gov/drugsatfda_docs/label/2025/019953s048lbl.pdfPremixed bag formulation label with pharmacokinetic data, clinical pharmacology, and dose-dependent half-life information.
Key Clinical Trials
  1. Raschke RA, Reilly BM, Guidry JR, et al. The weight-based heparin dosing nomogram compared with a “standard care” nomogram: a randomized controlled trial. Ann Intern Med. 1993;119(9):874–881. doi:10.7326/0003-4819-119-9-199311010-00002Landmark RCT establishing the 80 U/kg bolus, 18 U/kg/hr weight-based nomogram as superior to fixed-dose heparin for achieving therapeutic aPTT.
  2. 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.2015.11.026ACCP guidelines on VTE treatment including UFH dosing, aPTT targets, and comparison with LMWH for initial anticoagulation.
Guidelines
  1. 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.0000000000001309Most current ACS guideline with UFH dosing for UA/NSTEMI (60 U/kg, 12 U/kg/hr) and STEMI with fibrinolysis; recommends parenteral anticoagulation for all ACS patients.
  2. Menon V, Berkowitz SD, Antman EM, et al. New heparin dosing recommendations for patients with acute coronary syndromes. Am J Med. 2001;110(8):641–650. doi:10.1016/s0002-9343(01)00715-xReview establishing the ACS-specific lower heparin dosing (60 U/kg bolus max 4000-5000 U, 12 U/kg/hr max 1000 U/hr) to reduce bleeding with concurrent antiplatelets.
  3. Witt DM, Nieuwlaat R, Clark NP, et al. American Society of Hematology 2018 guidelines for management of venous thromboembolism: optimal management of anticoagulation therapy. Blood Adv. 2018;2(22):3257–3291. doi:10.1182/bloodadvances.2018024893ASH guideline on anticoagulation management including transition from heparin to warfarin and monitoring recommendations.
  4. Gornik HL, Aronow HD, Goodney PP, et al. 2024 ACC/AHA/AACVPR/APMA/ABC/SCAI/SVM/SVN/SVS/SIR/VESS Guideline for the Management of Lower Extremity Peripheral Artery Disease. Circulation. 2024. doi:10.1161/CIR.0000000000001251PAD guideline recommending immediate systemic heparinisation at diagnosis for acute limb ischaemia.
Mechanistic / Basic Science
  1. Hirsh J, Anand SS, Halperin JL, Fuster V. Mechanism of action and pharmacology of unfractionated and low molecular weight heparin. Arterioscler Thromb Vasc Biol. 2001;21(7):1094–1096. doi:10.1161/hq0701.093686Authoritative review of heparin’s AT-III binding mechanism, anti-Xa:anti-IIa ratio, protein binding, and pharmacological differences from LMWH.
Pharmacokinetics / Special Populations
  1. Heparin. In: StatPearls [Internet]. Treasure Island (FL): StatPearls Publishing; 2025. https://www.ncbi.nlm.nih.gov/books/NBK538247/Comprehensive clinical review covering mechanism, biphasic pharmacokinetics, dosing by indication, HIT management, and adverse effects.
  2. Estes JW. Clinical pharmacokinetics of heparin. Clin Pharmacokinet. 1980;5(3):204–220. doi:10.2165/00003088-198005030-00002Classic PK reference describing heparin’s dose-dependent half-life, plasma protein binding, volume of distribution, and non-linear clearance.
  3. Kandrotas RJ. Heparin pharmacokinetics and pharmacodynamics. Clin Pharmacokinet. 1992;22(5):359–374. doi:10.2165/00003088-199222050-00003Detailed review of heparin’s intravascular distribution, saturable and non-saturable clearance mechanisms, and concave-convex elimination curves.
  4. Garcia DA, Baglin TP, Weitz JI, Samama MM. Parenteral anticoagulants: Antithrombotic Therapy and Prevention of Thrombosis, 9th ed: ACCP Evidence-Based Clinical Practice Guidelines. Chest. 2012;141(2 Suppl):e24S–e43S. doi:10.1378/chest.11-2291ACCP guideline chapter on parenteral anticoagulants including UFH monitoring, HIT risk factors, and protamine reversal dosing.