Acute coronary syndromes (unstable angina and NSTEMI [non-Q-wave myocardial infarction] in conjunction with aspirin):
Initial:
Weight-based dosing: IV: 86 anti-Xa units/kg one time bolus (maximum dose: 9,500 anti-Xa units).
Fixed dosing: IV:
<50 kg: 3,800 anti-Xa units one time bolus.
50 to 59 kg: 4,750 anti-Xa units one time bolus.
60 to 69 kg: 5,700 anti-Xa units one time bolus.
70 to 79 kg: 6,650 anti-Xa units one time bolus.
80 to 89 kg: 7,600 anti-Xa units one time bolus.
90 to 99 kg: 8,550 anti-Xa units one time bolus.
≥100 kg: 9,500 anti-Xa units one time bolus.
Maintenance: Note: Begin 12 hours after initial bolus. Usual treatment duration: 6 days; plasma anti-Xa levels should be <1.2 anti-Xa units/mL 3 to 4 hours postinjection.
Weight-based dosing: SUBQ: 86 anti-Xa units/kg every 12 hours (maximum dose: 19,000 anti-Xa units/day).
Fixed dosing: SUBQ:
<50 kg: 3,800 anti-Xa units every 12 hours.
50 to 59 kg: 4,750 anti-Xa units every 12 hours.
60 to 69 kg: 5,700 anti-Xa units every 12 hours.
70 to 79 kg: 6,650 anti-Xa units every 12 hours.
80 to 89 kg: 7,600 anti-Xa units every 12 hours.
90 to 99 kg: 8,550 anti-Xa units every 12 hours.
≥100 kg: 9,500 anti-Xa units every 12 hours.
Anticoagulation during hemodialysis: Note: Administer into arterial line at start of each dialysis session; may give additional dose if session lasts longer than 4 hours; adjust dose during subsequent dialysis sessions to plasma anti-Xa levels of 0.5 to 1 anti-Xa units/mL.
Weight-based dosing: SUBQ: Initial: ~65 anti-Xa units/kg single dose (initial maximum dose: 5,700 anti-Xa units).
Fixed dosing: SUBQ: Initial:
<50 kg: 2,850 anti-Xa units single dose.
50 to 69 kg: 3,800 anti-Xa units single dose.
≥70 kg: 5,700 anti-Xa units single dose.
Patients at risk of hemorrhage: Note: Doses may be halved. Administer into arterial line at start of each dialysis session; may give additional smaller dose if session lasts longer than 4 hours; adjust dose during subsequent dialysis sessions to plasma anti-Xa levels of 0.2 to 0.4 anti-Xa units/mL.
Weight-based dosing: SUBQ: Initial: ~32.5 anti-Xa units/kg single dose (initial maximum dose: 2,850 anti-Xa units).
Fixed dosing: SUBQ: Initial:
<50 kg: 1,425 anti-Xa units single dose.
50 to 69 kg: 1,900 anti-Xa units single dose.
≥70 kg: 2,850 anti-Xa units single dose.
Deep vein thrombosis treatment:
Note: For timing of initiating oral anticoagulant, see "Transitioning Between Anticoagulants."
Inpatient treatment:
Patients with standard bleeding risk:
Weight-based dosing: SUBQ: 171 anti-Xa units/kg once daily.
Fixed dosing: SUBQ:
40 to 49 kg: 7,600 anti-Xa units once daily.
50 to 59 kg: 9,500 anti-Xa units once daily.
60 to 69 kg: 11,400 anti-Xa units once daily.
70 to 79 kg: 13,300 anti-Xa units once daily.
80 to 89 kg: 15,200 anti-Xa units once daily.
≥90 kg: 17,100 anti-Xa units once daily.
Patients with increased risk for bleeding: Note: For patients with higher-than-average bleeding risk, may administer the same total daily dose in 2 equally divided doses:
Weight-based dosing: SUBQ: 86 anti-Xa units/kg every 12 hours.
Fixed dosing: SUBQ:
40 to 49 kg: 3,800 anti-Xa units every 12 hours.
50 to 59 kg: 4,750 anti-Xa units every 12 hours.
60 to 69 kg: 5,700 anti-Xa units every 12 hours.
70 to 79 kg: 6,650 anti-Xa units every 12 hours.
80 to 89 kg: 7,600 anti-Xa units every 12 hours.
≥90 kg: 8,550 anti-Xa units every 12 hours.
Duration of therapeutic anticoagulation (first episode, general recommendations): Optimal duration of therapy is unknown and depends on many factors, such as whether provoking events were present, patient risk factors for recurrence and bleeding, and individual preference.
Provoked deep vein thrombosis: 3 months (provided the provoking risk factor is no longer present) (ACCP [Stevens 2021]).
Unprovoked deep vein thrombosis or provoked venous thromboembolism with a persistent risk factor: ≥3 months depending on risk of venous thromboembolism (VTE) recurrence and bleeding (ACCP [Stevens 2021]; ISTH [Baglin 2012]).
Note: All patients receiving indefinite therapeutic anticoagulation with no specified stop date should be reassessed at periodic intervals.
Thromboprophylaxis:
General surgery: SUBQ: Initial: 2,850 anti-Xa units administered 2 to 4 hours preoperatively; Maintenance: 2,850 anti-Xa units once daily. Continue therapy for at least 7 days and until ambulant or no longer at deep vein thrombosis (DVT) risk.
High-risk medical patients (respiratory failure and/or respiratory infection and/or cardiac failure): Note: Continue for length of hospital stay or until patient is fully ambulatory and risk of VTE has diminished (ACCP [Kahn 2012]). Extended prophylaxis beyond acute hospital stay is not routinely recommended (ACCP [Kahn 2012]; Sharma 2012). However, in high-risk coronavirus disease 2019 (COVID-19) patients who are discharged from the hospital, some experts would consider extended prophylaxis with a direct oral anticoagulant (eg, rivaroxaban) (Cuker 2020).
≤70 kg: SUBQ: 3,800 anti-Xa units once daily during the risk period of thromboembolism.
>70 kg: SUBQ: 5,700 anti-Xa units once daily during the risk period of thromboembolism.
Hip replacement surgery:
Note: Continue therapy for at least 10 days and until ambulant or no longer at DVT risk.
Weight-based dosing: SUBQ: Initial: 38 anti-Xa units/kg (maximum dose: 3,800 anti-Xa units) 12 hours before and after surgery, followed by 38 anti-Xa units/kg once daily (maximum: 3,800 anti-Xa units/day) up to and including postoperative day 3; on postoperative day 4, begin 57 anti-Xa units/kg once daily (maximum dose: 5,700 anti-Xa units/day).
Fixed dosing: SUBQ:
<50 kg: 1,900 anti-Xa units 12 hours before and after surgery, followed by 1,900 anti-Xa units once daily up to and including postoperative day 3; on postoperative day 4, begin 2,850 anti-Xa units once daily.
50 to 69 kg: 2,850 anti-Xa units 12 hours before and after surgery, followed by 2,850 anti-Xa units once daily up to and including postoperative day 3; on postoperative day 4, begin 3,800 anti-Xa units once daily.
≥70 kg: 3,800 anti-Xa units 12 hours before and after surgery, followed by 3,800 anti-Xa units once daily up to and including postoperative day 3; on postoperative day 4, begin 5,700 anti-Xa units once daily.
Transitioning between anticoagulants : Note: This provides general guidance on transitioning between anticoagulants; also refer to local protocol for additional detail:
Transitioning from another anticoagulant to nadroparin:
Transitioning from therapeutic IV unfractionated heparin infusion to therapeutic-dose nadroparin: Discontinue unfractionated heparin (UFH) and begin nadroparin within 1 hour. Note: If aPTT is not in therapeutic range at the time UFH is discontinued, consult local protocol (Nutescu 2007).
Transitioning from nadroparin to another anticoagulant:
Transitioning from therapeutic-dose nadroparin to therapeutic IV unfractionated heparin infusion: Start IV UFH (rate based on indication) 1 to 2 hours before the next dose of nadroparin would have been due. Note: Omit IV UFH loading dose (Nutescu 2007).
Transitioning from prophylactic nadroparin to therapeutic IV unfractionated heparin: UFH should be started without delay. A UFH bolus/loading dose may be used if indicated.
Transitioning from therapeutic-dose nadroparin to warfarin: Start warfarin and continue nadroparin until INR is within therapeutic range (Wittkowsky 2018). Note: Overlap nadroparin with warfarin until INR is ≥2 for at least 2 measurements taken ~24 hours apart (duration of overlap is ~5 days) (ACCP [Ageno 2012]).
Transitioning from therapeutic-dose nadroparin to a direct oral anticoagulant: Start direct oral anticoagulant within 2 hours prior to the next scheduled dose of nadroparin.
Dosage adjustment for concomitant therapy: Significant drug interactions exist, requiring dose/frequency adjustment or avoidance. Consult drug interactions database for more information.
CrCl ≥50 mL/minute: No dosage adjustment necessary.
CrCl ≥30 to <50 mL/minute: Decrease dose by 25% to 33%. Some have suggested that no dose adjustment is needed when used for prophylaxis; one small clinical trial found no change in peak anti-Xa activity after 5 days of nadroparin at prophylactic doses (Atiq 2015).
CrCl <30 mL/minute:
Prophylaxis: Reduce dose by 25% to 33%.
Treatment: Use is contraindicated.
Hemodialysis: Not dialyzable (NCS/SCCM [Frontera 2016])
There are no dosage adjustments provided in the manufacturer's labeling (has not been studied).
Refer to adult dosing; use with caution (increased risk of bleeding in the elderly). Close monitoring necessary, especially in patients with low body weight (ie, <45 kg) or predisposed to renal impairment.
Thromboprophylaxis in high-risk medical patients (respiratory failure and/or respiratory infection and/or cardiac failure), immobilized due to acute illness or in ICU: Consider dose reduction to 2,850 anti-Xa units once daily during the risk period of thromboembolism.
Deep vein thrombosis treatment: Some experts do not recommend a fixed upper dose limit (Nutescu 2009). Consider anti-factor Xa monitoring to ensure a therapeutic dose (ACCP [Garcia 2012]).
Thromboprophylaxis: In patients with BMI ≥40 kg/m2, increasing dose by 30% may be appropriate for some indications (Nutescu 2009).
Yes
Excipient information presented when available (limited, particularly for generics); consult specific product labeling.
Solution Prefilled Syringe, Injection:
Fraxiparine: 1900 units/0.2 mL (0.2 mL); 2850 units/0.3 mL (0.3 mL); 3800 units/0.4 mL (0.4 mL); 5700 units/0.6 mL (0.6 mL); 9500 units/mL (1 mL)
Fraxiparine Forte: 11,400 units/0.6 mL (0.6 mL); 15,200 units/0.8 mL (0.8 mL); 19,000 units/mL (1 mL)
Not available in the US
SubQ: Administer by SubQ injection into anterolateral abdominal wall with subsequent doses to be administered alternately on right and left side of abdominal wall. The thigh may also be used as an alternative site. Do not administer intramuscularly.
IV: May be administered IV only as initial bolus dose for acute coronary syndromes (unstable angina and NSTEMI [ie, non-Q-wave myocardial infarction]).
Hemodialysis: Inject into arterial line at start of dialysis session.
Note: Not approved in the United States.
Fraxiparine:
Acute coronary syndromes: Treatment of unstable angina and non-ST-elevation myocardial infarction (NSTEMI) myocardial infarction (ie, non-Q wave MI)
Anticoagulation during hemodialysis: Prevention of clotting during hemodialysis
Deep vein thrombosis: Treatment of deep vein thrombosis (DVT). Note: In patients with venous thromboembolism (VTE) (ie, DVT or PE) and without cancer, oral anticoagulants are preferred over LMWH (unless LMWH is used as initial parenteral anticoagulation prior to dabigatran, edoxaban, or while initiating warfarin).
Thromboprophylaxis: Prophylaxis of thromboembolic disorders (particularly DVT and pulmonary embolism [PE]) in general and orthopedic surgery, high-risk medical patients (respiratory failure and/or respiratory infection and/or cardiac failure) immobilized due to acute illness or hospitalized in ICU
Fraxiparine Forte: Treatment of deep vein thrombosis (DVT)
This medication is in a class the Institute for Safe Medication Practices (ISMP) includes among its list of drug classes which have a heightened risk of causing significant patient harm when used in error.
The following adverse drug reactions and incidences are derived from product labeling unless otherwise specified. As with all anticoagulants, bleeding is the major adverse effect of nadroparin. Hemorrhage may occur at virtually any site. Risk is dependent on multiple variables.
Frequency not defined:
Cardiovascular: Arterial thrombosis, thromboembolism, venous thrombosis
Dermatologic: Skin necrosis
Endocrine & metabolic: Calcinosis, hypoaldosteronism (causing hyperkalemia and/or hyponatremia)
Genitourinary: Priapism
Hematological & oncologic: Eosinophilia, hemorrhage, thrombocythemia, thrombocytopenia
Hepatic: Increased serum alanine aminotransferase, increased serum aspartate aminotransferase
Hypersensitivity: Angioedema, hypersensitivity reaction, nonimmune anaphylaxis
Local: Hematoma at injection site, injection site reaction
Neuromuscular & skeletal: Osteopenia
Postmarketing: Erythema of skin, headache, migraine, pruritus, skin rash, urticaria
Hypersensitivity to nadroparin, any component of the formulation, or to other low molecular weight heparins and/or heparin; acute infective endocarditis; active bleeding or increased risk of hemorrhage (hemostasis disorder); history of confirmed or suspected immunologically mediated heparin-induced thrombocytopenia (HIT) (delayed-onset severe thrombocytopenia) or positive in vitro test for antiplatelet antibodies in the presence of nadroparin; major blood clotting disorders; hemorrhagic tendency or other conditions involving increase risk of bleeding; organic lesions likely to bleed (active peptic ulceration); hemorrhagic cerebrovascular event; severe uncontrolled hypertension; diabetic or hemorrhagic retinopathy; injuries to or operations on the CNS, eyes, or ears; severe renal insufficiency (creatinine clearance <30 mL/minute when used for treatment); concomitant use of spinal/epidural anesthesia with repeated high-dose nadroparin (eg, 171 anti-Xa units/kg/day).
Note: Use of nadroparin in patients with current HIT or HIT with thrombosis is not recommended and considered contraindicated due to high cross-reactivity to heparin-platelet factor-4 antibody (ACCP [Guyatt 2012]; Warkentin 1999).
Concerns related to adverse effects:
• Bleeding: Bleeding may occur at any site during therapy. Monitor patient closely for signs or symptoms of bleeding. Certain patients are at increased risk of bleeding. Risk factors include bacterial endocarditis; congenital or acquired bleeding disorders; active ulcerative or angiodysplastic GI diseases; severe uncontrolled hypertension; hemorrhagic stroke; use shortly after brain, spinal, or ophthalmology surgery; in patients treated concomitantly with other drugs known to cause bleeding (eg, platelet inhibitors); recent GI bleeding or ulceration; vascular disorder of the chorio-retina; thrombocytopenia or platelet defects; severe liver disease; hypertensive or diabetic retinopathy; in patients undergoing invasive procedures; and in the elderly. Discontinue if bleeding occurs. Protamine infusion may be necessary for serious bleeding (consult Protamine monograph for dosing recommendations).
• Cutaneous necrosis: Cutaneous necrosis preceded by purpura or infiltrated or painful erythematous blotches has been reported rarely; discontinue treatment immediately if suspected.
• Hyperkalemia: Monitor for hyperkalemia; can cause hyperkalemia possibly by suppressing aldosterone production. Most commonly occurs in patients with risk factors for the development of hyperkalemia (eg, renal dysfunction, concomitant use of potassium-sparing diuretics or potassium supplements, hematoma in body tissues).
• Thrombocytopenia: Cases of thrombocytopenia including thrombocytopenia with thrombosis have occurred. Use with caution in patients with history of thrombocytopenia (drug-induced or congenital) or platelet defects; monitor platelet count closely. Use is contraindicated in patients with a history of confirmed or suspected heparin-induced thrombocytopenia (HIT) or positive in vitro test for antiplatelet antibodies in the presence of nadroparin. Discontinue therapy and consider alternative treatment if platelets are <100,000/mm3 and/or thrombosis develops.
Disease-related concerns:
• Cardiovascular disease: Use with caution in patients with severe arterial hypertension.
• GI disease: Use with caution in patients with history of GI ulceration; contraindicated in patients with active peptic ulceration.
• Hepatic impairment: Use with caution in patients with hepatic impairment (has not been studied); patients with hepatic failure are at an increased risk of bleeding.
• Prosthetic heart valves: Prosthetic valve thrombosis has been reported in patients receiving thromboprophylaxis therapy with low-molecular-weight heparins (LMWHs).
• Renal impairment: Use with caution in patients with renal impairment; primarily renally excreted. Dose reductions may be required. Use is contraindicated in severe renal impairment when treating thromboembolic disorders, unstable angina, and NSTEMI.
Special populations:
• Elderly: Use with caution in the elderly; dosage reduction may be needed.
• Obesity: There is no consensus for adjusting/correcting the weight-based dosage of LMWH for patients who are morbidly obese (BMI ≥40 kg/m2). The American College of Chest Physicians Practice Guidelines suggest consulting with a pharmacist regarding dosing in bariatric surgery patients and other obese patients who may require higher doses of LMWH (Gould 2012).
Dosage form specific issues:
• Latex: Packaging (needle cover of prefilled syringe) may contain natural latex rubber.
Other warnings/precautions:
• Appropriate use: Do not administer intramuscularly.
• Conversion to other products: Not to be used interchangeably (unit for unit) with heparin or any other LMWHs.
• Knee surgery: Risk of bleeding may be increased in patients undergoing knee surgery and receiving LMWHs. Consider risk versus benefit in this population.
• Neuraxial anesthesia: Epidural or spinal hematomas, including subsequent long-term or permanent paralysis, may occur in patients anticoagulated with LMWH or heparinoids who are receiving neuraxial anesthesia (epidural or spinal anesthesia) or undergoing spinal puncture. Consider risk versus benefit prior to spinal procedures; risk is increased by concomitant agents which may alter hemostasis, the use of indwelling epidural catheters, a history of spinal deformity or spinal surgery, or a history of traumatic or repeated epidural or spinal punctures. Avoid lumbar puncture or spinal or epidural anesthesia for 12 hours following the last nadroparin prophylactic dose or 24 hours following the last nadroparin treatment dose. The timing of subsequent nadroparin doses following catheter removal should be based on careful risk assessment for thrombosis and bleeding. Longer intervals should be considered for patients with renal impairment (doubling the timing of catheter removal). Observe patient closely for bleeding and signs and symptoms of neurological impairment if therapy is administered. If spinal hematoma is suspected, diagnose and treat immediately; spinal cord decompression may be considered although it may not prevent or reverse neurological sequelae.
None known.
Acalabrutinib: May enhance the anticoagulant effect of Anticoagulants. Risk C: Monitor therapy
Agents with Antiplatelet Properties (e.g., P2Y12 inhibitors, NSAIDs, SSRIs, etc.): May enhance the anticoagulant effect of Anticoagulants. Risk C: Monitor therapy
Alemtuzumab: May enhance the anticoagulant effect of Anticoagulants. Risk C: Monitor therapy
Aliskiren: Heparins (Low Molecular Weight) may enhance the hyperkalemic effect of Aliskiren. Risk C: Monitor therapy
Angiotensin II Receptor Blockers: Heparins (Low Molecular Weight) may enhance the hyperkalemic effect of Angiotensin II Receptor Blockers. Risk C: Monitor therapy
Angiotensin-Converting Enzyme Inhibitors: Heparins (Low Molecular Weight) may enhance the hyperkalemic effect of Angiotensin-Converting Enzyme Inhibitors. Risk C: Monitor therapy
Antithrombin: May enhance the anticoagulant effect of Heparins (Low Molecular Weight). Risk C: Monitor therapy
Apixaban: May enhance the anticoagulant effect of Anticoagulants. Refer to separate drug interaction content and to full drug monograph content regarding use of apixaban with vitamin K antagonists (eg, warfarin, acenocoumarol) during anticoagulant transition and bridging periods. Risk X: Avoid combination
Bromperidol: May enhance the adverse/toxic effect of Anticoagulants. Risk C: Monitor therapy
Caplacizumab: May enhance the anticoagulant effect of Anticoagulants. Risk C: Monitor therapy
Collagenase (Systemic): Anticoagulants may enhance the adverse/toxic effect of Collagenase (Systemic). Specifically, the risk of injection site bruising and/or bleeding may be increased. Risk C: Monitor therapy
Dabigatran Etexilate: May enhance the anticoagulant effect of Anticoagulants. Refer to separate drug interaction content and to full drug monograph content regarding use of dabigatran etexilate with vitamin K antagonists (eg, warfarin, acenocoumarol) during anticoagulant transition and bridging periods. Risk X: Avoid combination
Dasatinib: May enhance the anticoagulant effect of Anticoagulants. Risk C: Monitor therapy
Deferasirox: Anticoagulants may enhance the adverse/toxic effect of Deferasirox. Specifically, the risk for GI ulceration/irritation or GI bleeding may be increased. Risk C: Monitor therapy
Deoxycholic Acid: Anticoagulants may enhance the adverse/toxic effect of Deoxycholic Acid. Specifically, the risk for bleeding or bruising in the treatment area may be increased. Risk C: Monitor therapy
Desirudin: Anticoagulants may enhance the anticoagulant effect of Desirudin. Management: Discontinue treatment with other anticoagulants prior to desirudin initiation. If concomitant use cannot be avoided, monitor patients receiving these combinations closely for clinical and laboratory evidence of excessive anticoagulation. Risk D: Consider therapy modification
Edoxaban: May enhance the anticoagulant effect of Anticoagulants. Refer to separate drug interaction content and to full drug monograph content regarding use of edoxaban with vitamin K antagonists (eg, warfarin, acenocoumarol) during anticoagulant transition and bridging periods. Management: Some limited combined use may be indicated during periods of transition from one anticoagulant to another. See the full edoxaban drug monograph for specific recommendations on switching anticoagulant treatment. Risk X: Avoid combination
Eplerenone: Heparins (Low Molecular Weight) may enhance the hyperkalemic effect of Eplerenone. Risk C: Monitor therapy
Factor X (Human): Anticoagulants (Inhibitors of Factor Xa) may diminish the therapeutic effect of Factor X (Human). Risk C: Monitor therapy
Hemin: May enhance the anticoagulant effect of Anticoagulants. Risk X: Avoid combination
Herbal Products with Anticoagulant/Antiplatelet Effects (eg, Alfalfa, Anise, Bilberry): May enhance the adverse/toxic effect of Anticoagulants. Bleeding may occur. Risk C: Monitor therapy
Ibritumomab Tiuxetan: Anticoagulants may enhance the adverse/toxic effect of Ibritumomab Tiuxetan. Both agents may contribute to an increased risk of bleeding. Risk C: Monitor therapy
Ibrutinib: May enhance the adverse/toxic effect of Anticoagulants. Risk C: Monitor therapy
Icosapent Ethyl: May enhance the anticoagulant effect of Anticoagulants. Risk C: Monitor therapy
Inotersen: May enhance the anticoagulant effect of Anticoagulants. Risk C: Monitor therapy
Kanamycin: May enhance the anticoagulant effect of Anticoagulants. Risk C: Monitor therapy
Limaprost: May enhance the adverse/toxic effect of Anticoagulants. The risk for bleeding may be increased. Risk C: Monitor therapy
Lipid Emulsion (Fish Oil Based): May enhance the anticoagulant effect of Anticoagulants. Risk C: Monitor therapy
Mesoglycan: May enhance the anticoagulant effect of Anticoagulants. Risk C: Monitor therapy
MiFEPRIStone: May enhance the adverse/toxic effect of Anticoagulants. Specifically, the risk of bleeding may be increased. Risk X: Avoid combination
Nintedanib: Anticoagulants may enhance the adverse/toxic effect of Nintedanib. Specifically, the risk for bleeding may be increased. Risk C: Monitor therapy
Nonsteroidal Anti-Inflammatory Agents (COX-2 Selective): May enhance the anticoagulant effect of Anticoagulants. Risk C: Monitor therapy
Nonsteroidal Anti-Inflammatory Agents (Topical): May enhance the anticoagulant effect of Anticoagulants. Risk C: Monitor therapy
Obinutuzumab: Anticoagulants may enhance the adverse/toxic effect of Obinutuzumab. Specifically, the risk of serious bleeding-related events may be increased. Risk C: Monitor therapy
Omacetaxine: Anticoagulants may enhance the adverse/toxic effect of Omacetaxine. Specifically, the risk for bleeding-related events may be increased. Management: Avoid concurrent use of anticoagulants with omacetaxine in patients with a platelet count of less than 50,000/uL. Risk X: Avoid combination
Omega-3 Fatty Acids: May enhance the anticoagulant effect of Anticoagulants. Risk C: Monitor therapy
Palifermin: Heparins (Low Molecular Weight) may increase the serum concentration of Palifermin. Risk C: Monitor therapy
Pentosan Polysulfate Sodium: May enhance the anticoagulant effect of Anticoagulants. Risk C: Monitor therapy
Pentoxifylline: May enhance the anticoagulant effect of Heparins (Low Molecular Weight). Risk C: Monitor therapy
Potassium Salts: Heparins (Low Molecular Weight) may enhance the hyperkalemic effect of Potassium Salts. Risk C: Monitor therapy
Potassium-Sparing Diuretics: Heparins (Low Molecular Weight) may enhance the hyperkalemic effect of Potassium-Sparing Diuretics. Management: Monitor serum potassium concentrations closely. The spironolactone Canadian product monograph lists its combination with heparin or low molecular weight heparins as contraindicated. Risk C: Monitor therapy
Prostacyclin Analogues: May enhance the adverse/toxic effect of Anticoagulants. Specifically, the antiplatelet effects of these agents may lead to an increased risk of bleeding with the combination. Risk C: Monitor therapy
Rivaroxaban: Anticoagulants may enhance the anticoagulant effect of Rivaroxaban. Refer to separate drug interaction content and to full drug monograph content regarding use of rivaroxaban with vitamin K antagonists (eg, warfarin, acenocoumarol) during anticoagulant transition and bridging periods. Risk X: Avoid combination
Salicylates: May enhance the anticoagulant effect of Anticoagulants. Risk C: Monitor therapy
Sugammadex: May enhance the anticoagulant effect of Anticoagulants. Risk C: Monitor therapy
Sulodexide: May enhance the anticoagulant effect of Anticoagulants. Risk C: Monitor therapy
Thrombolytic Agents: May enhance the anticoagulant effect of Anticoagulants. Management: Monitor for signs and symptoms of bleeding if these agents are combined. For the treatment of acute ischemic stroke, avoidance with anticoagulants is often recommended, see full Lexicomp or drug interaction monograph for details. Risk C: Monitor therapy
Tibolone: May enhance the anticoagulant effect of Anticoagulants. Risk C: Monitor therapy
Tipranavir: May enhance the anticoagulant effect of Anticoagulants. Risk C: Monitor therapy
Urokinase: May enhance the anticoagulant effect of Anticoagulants. Risk X: Avoid combination
Vitamin E (Systemic): May enhance the anticoagulant effect of Anticoagulants. Risk C: Monitor therapy
Vitamin K Antagonists (eg, warfarin): Anticoagulants may enhance the anticoagulant effect of Vitamin K Antagonists. Risk C: Monitor therapy
Vorapaxar: May enhance the adverse/toxic effect of Anticoagulants. More specifically, this combination is expected to increase the risk of bleeding. Risk X: Avoid combination
Zanubrutinib: May enhance the adverse/toxic effect of Anticoagulants. Risk C: Monitor therapy
Prophylaxis with LMWH is not routinely recommended for women undergoing assisted reproduction therapy; however, LMWH therapy is recommended for women who develop severe ovarian hyperstimulation syndrome. For women who require long-term anticoagulation with warfarin and who are considering pregnancy, LMWH substitution should be done prior to conception when possible. When choosing therapy, fetal outcomes (ie, pregnancy loss, malformations), maternal outcomes (ie, VTE, hemorrhage), burden of therapy, and maternal preference should be considered (Bates 2012; Linnemann 2016).
Information related to placental transfer is limited.
Prosthetic valve thrombosis has been reported in patients receiving thromboprophylaxis therapy with low-molecular-weight heparins (LMWHs); pregnant women may be at increased risk. LMWH is recommended over unfractionated heparin for the treatment of acute venous thromboembolism (VTE) in pregnant women. LMWH is also recommended over unfractionated heparin for VTE prophylaxis in pregnant women with certain risk factors (eg, homozygous factor V Leiden, antiphospholipid antibody syndrome with ≥3 previous pregnancy losses). LMWH should be discontinued ≥24 hours prior to induction of labor or a planned cesarean delivery. For women undergoing cesarean section and who have additional risk factors for developing VTE, the prophylactic use of LMWH may be considered. When choosing LMWH therapy, fetal outcomes (ie, pregnancy loss, malformations), maternal outcomes (ie, VTE, hemorrhage), burden of therapy, and maternal preference should be considered (Bates 2012; Linnemann 2016).
Small amounts of low molecular weight heparins (LMWHs) may be present in breast milk; however, because they have a low oral bioavailability, LMWHs are unlikely to cause adverse events in a breastfeeding infant. Breastfeeding is not recommended by the manufacturer; however, antithrombotic guidelines note the use of LMWH may be continued in breastfeeding women (Guyatt 2012).
Platelet counts (at baseline and then twice weekly during therapy), bleeding complications including stool occult blood tests, hemoglobin, antifactor Xa levels (recommended to obtain levels 4 hours postdose); renal and hepatic function; potassium in patients at risk for hyperkalemia; signs/symptoms of neurological impairment.
When used for anticoagulation during hemodialysis, carefully monitor patients for signs of bleeding or clotting in the dialysis session.
Anti-Xa level target (measured 4 hours after administration): Treatment of venous thromboembolism (Garcia 2012):
Once-daily dosing: 1.3 Anti-Xa units/mL.
Twice-daily dosing: 0.6 to 1 Anti-Xa units/mL.
Nadroparin is a low molecular weight heparin (LMWH) (average molecular weight is ~4,300 daltons, distributed as 2,000 to 8,000 daltons [75% to 85%]) that binds antithrombin III, enhancing the inhibition of several clotting factors, particularly factor Xa. Nadroparin anti-Xa activity (85 to 110 units/mg) is greater than anti-IIa activity (~27 units/mg) and it has a higher ratio of antifactor Xa to antifactor IIa activity compared to unfractionated heparin. LMWHs have a small effect on the activated partial thromboplastin time.
Note: Values reflective of anti-Xa activity.
Duration: Anti-Xa activity: ≥18 hours
Distribution: Vd: 3.59 L
Metabolism: Hepatic
Bioavailability: SubQ: ~98%
Half-life elimination: ~3.5 hours (prolonged in renal impairment)
Time to peak, serum: SubQ: 3 to 6 hours
Excretion: Urine (primarily)
Renal function impairment: Clearance is decreased. In patients with moderate impairment (CrCl 36 to 43 mL/minute), mean AUC and half-life increased 52% and 39% respectively; in severe impairment (CrCl 10 to 20 mL/minute), mean AUC and half-life increased 95% and 112% respectively. Patients with CrCl <10 mL/minute receiving hemodialysis had mean increases in AUC and half-life of 62% and 65% respectively.
Geriatric: Mean anti-Xa peak and total exposure increased 22% and 45% respectively when compared to younger subjects.