Bemiparin sodium 2,500units/0.2ml solution for injection pre-filled syringes
Bemiparin is an antithrombotic and belongs to the group of drugs known as the low molecular weight heparins (LMWH).
Active ingredients:
Bemiparin
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Source: MHRA Products DatabaseOGL 3.0
Updated 3 months ago(16 Jan 2026)Safety monitoring data
Yellow Card reports
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The MHRA Yellow Card scheme collects reports of suspected side effects from healthcare professionals and patients. View the Drug Analysis Profile (iDAP) for real-world adverse reaction data.
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Data from the MHRA Yellow Card scheme. A reported reaction does not necessarily mean the medicine caused it. Contains public sector information licensed under the Open Government Licence v3.0.
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EudraVigilance data is published by the European Medicines Agency (EMA). A suspected adverse reaction is not necessarily caused by the medicine.
2 branded products available
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2 products
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Zibor 2,500units/0.2ml solution for injection pre-filled syringes
Discontinued
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WHO defined daily dose (DDD)
2500 unit
Not a recommended dose. The DDD is the assumed average maintenance dose per day for a drug used for its main indication in adults. It is a statistical measure used for research and comparison purposes only.
Source: WHO Collaborating Centre for Drug Statistics Methodology, distributed via NHS dm+d BNF mapping files. Contains public sector information licensed under the Open Government Licence v3.0.
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Antithrombin III 500unit powder and solvent for solution for infusion vials
Infusion
500unit
Same therapeutic group
Similarity based on WHO Anatomical Therapeutic Chemical (ATC) classification and NHS BNF section grouping. Source data: NHS dm+d via TRUD (OGL v3.0), WHO ATC/DDD Index.
NHS prescribing volume and spending trends
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Clinical guidelines and formulary information
British National Formulary
Bemiparin
BNF
Drug monograph — bnf.nice.org.ukSource: British National Formulary, NICE. Joint Formulary Committee. Contains public sector information licensed under the Open Government Licence v3.0.
Check stock at pharmacies and supply information
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Supply & product information
Official product databases and supply status monitoring
Pharmacy links redirect to the retailer's own search and do not represent real-time stock levels. emc (electronic medicines compendium) is operated by Datapharm Ltd. Shortage information sourced from NHS Specialist Pharmacy Service (SPS), sps.nhs.uk.
Codes for healthcare professionals and prescribing systems
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These codes are used by healthcare IT systems and prescribers to identify this medicine.
NHS UK identifiers
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SNOMED CT and dm+d codes from NHS TRUD (Technology Reference data Update Distribution), licensed under the Open Government Licence v3.0. BNF codes from NHS Business Services Authority (NHSBSA). ATC codes from the WHO Collaborating Centre for Drug Statistics Methodology (whocc.no).
Active and completed clinical studies from ClinicalTrials.gov
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Searching UK clinical trials...
Source: ClinicalTrials.gov, a database of the U.S. National Library of Medicine (NLM), National Institutes of Health (NIH). Data accessed via ClinicalTrials.gov API v2. Trial information is provided for research purposes and does not constitute medical advice.
Pharmacology and chemical data from DrugBank
Key facts
Drug status
Approved
Major interactions
157 found
Half-life
5-6 hours
Mechanism
This drug is a second-generation low molecular weight heparin (LMWH).
Food interactions
1 warning
Human targets
3 targets
Data: DrugBank · CC BY-NC 4.0
Pharmacokinetics at a glance
Absorption
96%
Hemiparin sodium is rapidly absorbed following its subcutaneous dose of injection, and the bioavailability is estimated to be 96% .
[L1462]
[L1462]
Half-life
5-6 hours
Bemiparin, when administered in the dose range of 2,500 IU to 12,500 (therapeutic dosing), it has an approximate half-life of 5-6 hours .
[L1462]
[L1462]
Protein binding
There are currently no data available with regards to plasma protein binding, metabolism and excretion of bemiparin in humans .
[L1465]
[L1465]
Volume of distribution
5.1 L
5.1 L .
[A32018]
[A32018]
Metabolism
3h
In a study of healthy volunteers, bemiparin 3500 IU achieved more anti-Xa activity than enoxaparin 4000 IU, measured by the area under the curve.…
Elimination
This drug is eliminated by the renal and hepatic routes. Elimination is prolonged in those with renal or hepatic impairment .
[L1466]
[L1466]
Clearance
7 h
Elimination occurs in a linear fashion, with a mean clearance time of over 7 h and total clearance of 0.9 L/h .
[A32018]
[A32018]
Pharmacokinetic data: DrugBank · CC BY-NC 4.0
Status:
Approved
Investigational
Withdrawn
Small molecule
About this compound
Bemiparin is an antithrombotic and belongs to the group of drugs known as the low molecular weight heparins (LMWH). Like semuloparin, bemiparin is classified as an ultra-LMH because of its low mean molecular mass of 3600 daltons, which is a unique property of this class [A7866]. These heparins have lower anti-thrombin activity than the traditional low molecular weight heparins and act mainly on factor-Xa, reducing the risk of bleeding due to selectivity for this specific clotting factor. Interestingly, current research is underway for the potential benefit of bemiparin in the treatment of tumors and diabetic foot ulcers [L1468][A7866].
Properties:
solid
DrugBank indication
Bemiparin is indicated in the following cases: To prevent blood clots in the veins after general abdominal surgery in patients with a moderate risk of venous thromboembolism; in the prevention of the thromboembolic disease in non-surgical patients; prevention of clotting in the extracorporeal circuit during hemodialysis; to prevent blood clots in the veins after a major orthopedic surgery in patients with high risk of venous thromboembolism; secondary prevention of venous thromboembolism; recurrence in patients with deep vein thrombosis; transient prevention and treatment of deep vein thrombosis (DVT) .
[L1463]
[L1463]
Also known as(13)
Bemiparin
3.4.21.6
Stuart factor
Stuart-Prower factor
AT3
ATIII
Serpin C1
HC-II
Dosage forms(21)
Solution (Subcutaneous) — 500 UI
Injection, solution (Parenteral) — 10000 IU/0.4mL
Injection (Intravenous) — 10000 iu/0.4ml
Injection, solution (Parenteral) — 2500 IU/0.2mL
Injection (Intravenous) — 2500 iu/0.2ml
Injection, solution (Parenteral) — 3500 IU/0.2mL
Injection (Intravenous) — 3500 iu/0.2ml
Injection, solution (Parenteral) — 5000 IU/0.2mL
Drug interactions(863)
Known interactions with other medications. Always consult a healthcare professional.
Apixaban may increase the anticoagulant activities of Bemiparin.
Dabigatran etexilate
Moderate
Dabigatran etexilate may increase the anticoagulant activities of Bemiparin.
The risk or severity of bleeding and hemorrhage can be increased when Dasatinib is combined with Bemiparin.
Deferasirox
Unknown severity
The risk or severity of gastrointestinal bleeding can be increased when Bemiparin is combined with Deferasirox.
Ursodeoxycholic acid
Unknown severity
The risk or severity of bleeding and bruising can be increased when Bemiparin is combined with Ursodeoxycholic acid.
Glycochenodeoxycholic Acid
Unknown severity
The risk or severity of bleeding and bruising can be increased when Bemiparin is combined with Glycochenodeoxycholic Acid.
Cholic Acid
Unknown severity
The risk or severity of bleeding and bruising can be increased when Bemiparin is combined with Cholic Acid.
Glycocholic acid
Unknown severity
The risk or severity of bleeding and bruising can be increased when Bemiparin is combined with Glycocholic acid.
Deoxycholic acid
Unknown severity
The risk or severity of bleeding and bruising can be increased when Bemiparin is combined with Deoxycholic acid.
Taurocholic acid
Unknown severity
The risk or severity of bleeding and bruising can be increased when Bemiparin is combined with Taurocholic acid.
Obeticholic acid
Unknown severity
The risk or severity of bleeding and bruising can be increased when Bemiparin is combined with Obeticholic acid.
Chenodeoxycholic acid
Unknown severity
The risk or severity of bleeding and bruising can be increased when Bemiparin is combined with Chenodeoxycholic acid.
Taurochenodeoxycholic acid
Unknown severity
The risk or severity of bleeding and bruising can be increased when Bemiparin is combined with Taurochenodeoxycholic acid.
Tauroursodeoxycholic acid
Unknown severity
The risk or severity of bleeding and bruising can be increased when Bemiparin is combined with Tauroursodeoxycholic acid.
The risk or severity of bleeding and bruising can be increased when Bemiparin is combined with Bamet-UD2.
Dehydrocholic acid
Unknown severity
The risk or severity of bleeding and bruising can be increased when Bemiparin is combined with Dehydrocholic acid.
Hyodeoxycholic Acid
Unknown severity
The risk or severity of bleeding and bruising can be increased when Bemiparin is combined with Hyodeoxycholic Acid.
The risk or severity of bleeding can be increased when Edoxaban is combined with Bemiparin.
The risk or severity of bleeding and hemorrhage can be increased when Ibrutinib is combined with Bemiparin.
Obinutuzumab
Major
The risk or severity of bleeding and hemorrhage can be increased when Bemiparin is combined with Obinutuzumab.
Rivaroxaban
Moderate
Bemiparin may increase the anticoagulant activities of Rivaroxaban.
Sugammadex
Major
The risk or severity of bleeding and hemorrhage can be increased when Bemiparin is combined with Sugammadex.
Tibolone may increase the anticoagulant activities of Bemiparin.
Tipranavir
Major
The risk or severity of bleeding and hemorrhage can be increased when Tipranavir is combined with Bemiparin.
Urokinase may increase the anticoagulant activities of Bemiparin.
Vitamin E may increase the anticoagulant activities of Bemiparin.
The risk or severity of bleeding and hemorrhage can be increased when Vorapaxar is combined with Bemiparin.
Trandolaprilat
Unknown severity
The risk or severity of hyperkalemia can be increased when Trandolaprilat is combined with Bemiparin.
Moexiprilat
Unknown severity
The risk or severity of hyperkalemia can be increased when Moexiprilat is combined with Bemiparin.
Cilazaprilat
Unknown severity
The risk or severity of hyperkalemia can be increased when Cilazaprilat is combined with Bemiparin.
Ginkgo biloba
Moderate
Ginkgo biloba may increase the anticoagulant activities of Bemiparin.
Ifosfamide
Unknown severity
The risk or severity of bleeding can be increased when Ifosfamide is combined with Bemiparin.
The therapeutic efficacy of Bemiparin can be increased when used in combination with Quinine.
The therapeutic efficacy of Bemiparin can be increased when used in combination with Quinidine.
The risk or severity of bleeding can be increased when Tamoxifen is combined with Bemiparin.
Toremifene
Unknown severity
The risk or severity of bleeding can be increased when Toremifene is combined with Bemiparin.
The risk or severity of hypotension and sinus node depression can be increased when Bemiparin is combined with Corticorelin ovine triflutate.
Oritavancin
Moderate
The therapeutic efficacy of Bemiparin can be decreased when used in combination with Oritavancin.
Streptokinase
Moderate
Streptokinase may increase the anticoagulant activities of Bemiparin.
Telavancin
Moderate
The therapeutic efficacy of Bemiparin can be decreased when used in combination with Telavancin.
Palifermin
Unknown severity
The serum concentration of Palifermin can be increased when it is combined with Bemiparin.
Pentoxifylline
Moderate
The therapeutic efficacy of Bemiparin can be increased when used in combination with Pentoxifylline.
Pentosan polysulfate
Moderate
Pentosan polysulfate may increase the anticoagulant activities of Bemiparin.
Levocarnitine
Moderate
The therapeutic efficacy of Bemiparin can be increased when used in combination with Levocarnitine.
Diethylstilbestrol
Moderate
Diethylstilbestrol may decrease the anticoagulant activities of Bemiparin.
Chlorotrianisene
Moderate
Chlorotrianisene may decrease the anticoagulant activities of Bemiparin.
Conjugated estrogens
Moderate
Conjugated estrogens may decrease the anticoagulant activities of Bemiparin.
The risk or severity of adverse effects can be increased when Mestranol is combined with Bemiparin.
Estrone sulfate
Moderate
Estrone sulfate may decrease the anticoagulant activities of Bemiparin.
Quinestrol
Moderate
Quinestrol may decrease the anticoagulant activities of Bemiparin.
Showing 50 of 863 interactions
Food & lifestyle interactions
Advice
Avoid herbs and supplements with anticoagulant/antiplatelet activity. Examples include garlic, ginger, bilberry, danshen, piracetam, and ginkgo biloba.
Toxicity & overdose
Bemiparin, like other drugs in its class, may suppress adrenal secretion of aldosterone, leading to elevated potassium (hyperkalemia). This may occur more frequently in patients with conditions such as diabetes mellitus, chronic renal failure, metabolic acidosis, an increased plasma potassium, and those ingesting potassium sparing drugs. There is a linear relationship between duration of therapy and adverse effects, but this is usually reversible with cessation of treatment. Serum electrolytes should be measured in at-risk patients before starting bemiparin, and these patients should be monitored regularly thereafter particularly if treatment is prolonged beyond 1 week.
In rare cases, mild transient thrombocytopenia (HIT type I) at the beginning of therapy with heparin with platelet counts between 100,000/mm3 and 150,000/mm3 due to temporary platelet activation has been noted in clinical studies.
On rare occasions, antibody-mediated severe thrombocytopenia (HIT type II) with platelet counts clearly below
100,000/mm3 has been observed (see section 4.8). This effect usually occurs within 5-21 days after the initiation of treatment, although in patients with a history of heparin-induced thrombocytopenia this may occur more rapidly.
Platelet count studies are recommended before the administration of bemiparin, on the first day of therapy and then every 3-4 days, in addition to repeating platelet studies at the end of therapy.
Treatment must be discontinued immediately and an alternate therapy initiated if significant reductions in platelet counts are observed ( 30% decrease and above) .
[L1462]
As with other heparin products, cases of cutaneous necrosis, often preceded by purpura or painful erythematous, ecchymose-like lesions have been reported with bemiparin. In these cases, treatment should cease immediately .
[L1462]
Overdosage after subcutaneous or other routes of administration of bemiparin may lead to hemorrhagic complications. Neutralization can be obtained by slow intravenous of a suitable dose of the antidote protamine sulphate .
[L1463]
In rare cases, mild transient thrombocytopenia (HIT type I) at the beginning of therapy with heparin with platelet counts between 100,000/mm3 and 150,000/mm3 due to temporary platelet activation has been noted in clinical studies.
On rare occasions, antibody-mediated severe thrombocytopenia (HIT type II) with platelet counts clearly below
100,000/mm3 has been observed (see section 4.8). This effect usually occurs within 5-21 days after the initiation of treatment, although in patients with a history of heparin-induced thrombocytopenia this may occur more rapidly.
Platelet count studies are recommended before the administration of bemiparin, on the first day of therapy and then every 3-4 days, in addition to repeating platelet studies at the end of therapy.
Treatment must be discontinued immediately and an alternate therapy initiated if significant reductions in platelet counts are observed ( 30% decrease and above) .
[L1462]
As with other heparin products, cases of cutaneous necrosis, often preceded by purpura or painful erythematous, ecchymose-like lesions have been reported with bemiparin. In these cases, treatment should cease immediately .
[L1462]
Overdosage after subcutaneous or other routes of administration of bemiparin may lead to hemorrhagic complications. Neutralization can be obtained by slow intravenous of a suitable dose of the antidote protamine sulphate .
[L1463]
How it works
Mechanism of action
This drug is a second-generation low molecular weight heparin (LMWH). It has a very low mean molecular weight (3600 Dalton), a long half-life (5.3 hrs) and a large anti-Xa: anti-IIa ratio (8:1)[L1463]. The mechanism of action of bemiparin is inhibition of factor Xa, which is a necessary step in the clotting cascade. Factor-Xa is necessary for the propagation of a thrombus.
Combined with various co-factors that bind to activated platelets, Factor-Xa increases coagulation by converting prothrombin to thrombin [L1467]. Activated Factor-X, bound as part of the prothrombinase complex on the external surface of activated platelets, converts significant amounts of prothrombin to thrombin, promoting the so-called ‘thrombin burst’, referring to a burst of thrombin release [L1467].
A secondary but less potent mechanism of action of this drug is binding to antithrombin III and activated factor II (Factor IIa), which further prevents the propagation of thrombi [L1472].
Due to its excellent pharmacological profile-the second-generation LMWH with the lowest molecular weight, the longest half-life and the highest anti-Factor Xa/anti-Factor IIa activity ratio-it can be safely used in special categories of patients (children, elderly, patients with renal impairment and congestive heart failure). Several studies demonstrated its safety and efficacy, while cost analyses show the economic benefits of bemiparin treatment as compared to other heparins [A7866][A7867].
Combined with various co-factors that bind to activated platelets, Factor-Xa increases coagulation by converting prothrombin to thrombin [L1467]. Activated Factor-X, bound as part of the prothrombinase complex on the external surface of activated platelets, converts significant amounts of prothrombin to thrombin, promoting the so-called ‘thrombin burst’, referring to a burst of thrombin release [L1467].
A secondary but less potent mechanism of action of this drug is binding to antithrombin III and activated factor II (Factor IIa), which further prevents the propagation of thrombi [L1472].
Due to its excellent pharmacological profile-the second-generation LMWH with the lowest molecular weight, the longest half-life and the highest anti-Factor Xa/anti-Factor IIa activity ratio-it can be safely used in special categories of patients (children, elderly, patients with renal impairment and congestive heart failure). Several studies demonstrated its safety and efficacy, while cost analyses show the economic benefits of bemiparin treatment as compared to other heparins [A7866][A7867].
Pharmacodynamics
Bemiparin is an anticoagulant classified under the broad category of low molecular weight heparins.
In humans, bemiparin has been proven to possess antithrombotic activity and, at therapeutic doses, does not significantly prolong global clotting laboratory tests [L1465].
In humans, bemiparin has been proven to possess antithrombotic activity and, at therapeutic doses, does not significantly prolong global clotting laboratory tests [L1465].
Pharmacokinetics
How the body processes this drug — absorption, distribution, metabolism, and elimination
Absorption
Hemiparin sodium is rapidly absorbed following its subcutaneous dose of injection, and the bioavailability is estimated to be 96% .
[L1462]
[L1462]
Half-life
Bemiparin, when administered in the dose range of 2,500 IU to 12,500 (therapeutic dosing), it has an approximate half-life of 5-6 hours .
[L1462]
[L1462]
Protein binding
There are currently no data available with regards to plasma protein binding, metabolism and excretion of bemiparin in humans .
[L1465]
[L1465]
Volume of distribution
5.1 L .
[A32018]
[A32018]
Metabolism
In a study of healthy volunteers, bemiparin 3500 IU achieved more anti-Xa activity than enoxaparin 4000 IU, measured by the area under the curve. The peak of anti-Xa activity was reached at 3h post-administration, and there were anti-Xa measurable levels up to 16 h after subcutaneous injection .
[A32030]
[A32030]
Route of elimination
This drug is eliminated by the renal and hepatic routes. Elimination is prolonged in those with renal or hepatic impairment .
[L1466]
[L1466]
Clearance
Elimination occurs in a linear fashion, with a mean clearance time of over 7 h and total clearance of 0.9 L/h .
[A32018]
[A32018]
Drug targets(3)
Proteins and enzymes this drug interacts with in the body
Coagulation factor X
F10
antagonist
Specific functioncalcium ion binding
Cellular location
Secreted
General function & pharmacology
Factor Xa is a vitamin K-dependent glycoprotein that converts prothrombin to thrombin in the presence of factor Va, calcium and phospholipid during blood clotting .
PMID:22409427
Factor Xa activates pro-inflammatory signaling pathways in a protease-activated receptor (PAR)-dependent manner .
PMID:24041930 PMID:30568593 PMID:34831181 PMID:18202198
Up-regulates expression of protease-activated receptors (PARs) F2R, F2RL1 and F2RL2 in dermal microvascular endothelial cells .
PMID:35738824
Triggers the production of pro-inflammatory cytokines, such as MCP-1/CCL2 and IL6, in cardiac fibroblasts and umbilical vein endothelial cells in PAR-1/F2R-dependent manner .
PMID:30568593 PMID:34831181
Triggers the production of pro-inflammatory cytokines, such as MCP-1/CCL2, IL6, TNF-alpha/TNF, IL-1beta/IL1B, IL8/CXCL8 and IL18, in endothelial cells and atrial tissues .
PMID:24041930 PMID:35738824 PMID:9780208
Induces expression of adhesion molecules, such as ICAM1, VCAM1 and SELE, in endothelial cells and atrial tissues .
PMID:24041930 PMID:35738824 PMID:9780208
Increases expression of phosphorylated ERK1/2 in dermal microvascular endothelial cells and atrial tissues .
PMID:24041930 PMID:35738824
Triggers activation of the transcription factor NF-kappa-B in dermal microvascular endothelial cells and atrial tissues .
PMID:24041930 PMID:35738824
Activates pro-inflammatory and pro-fibrotic responses in dermal fibroblasts and enhances wound healing probably via PAR-2/F2RL1-dependent mechanism .
PMID:18202198
Activates barrier protective signaling responses in endothelial cells in PAR-2/F2RL1-dependent manner; the activity depends on the cleavage of PAR-2/F2RL1 by factor Xa .
PMID:22409427
Up-regulates expression of plasminogen activator inhibitor 1 (SERPINE1) in atrial tissues PMID:24041930
PMID:22409427
Factor Xa activates pro-inflammatory signaling pathways in a protease-activated receptor (PAR)-dependent manner .
PMID:24041930 PMID:30568593 PMID:34831181 PMID:18202198
Up-regulates expression of protease-activated receptors (PARs) F2R, F2RL1 and F2RL2 in dermal microvascular endothelial cells .
PMID:35738824
Triggers the production of pro-inflammatory cytokines, such as MCP-1/CCL2 and IL6, in cardiac fibroblasts and umbilical vein endothelial cells in PAR-1/F2R-dependent manner .
PMID:30568593 PMID:34831181
Triggers the production of pro-inflammatory cytokines, such as MCP-1/CCL2, IL6, TNF-alpha/TNF, IL-1beta/IL1B, IL8/CXCL8 and IL18, in endothelial cells and atrial tissues .
PMID:24041930 PMID:35738824 PMID:9780208
Induces expression of adhesion molecules, such as ICAM1, VCAM1 and SELE, in endothelial cells and atrial tissues .
PMID:24041930 PMID:35738824 PMID:9780208
Increases expression of phosphorylated ERK1/2 in dermal microvascular endothelial cells and atrial tissues .
PMID:24041930 PMID:35738824
Triggers activation of the transcription factor NF-kappa-B in dermal microvascular endothelial cells and atrial tissues .
PMID:24041930 PMID:35738824
Activates pro-inflammatory and pro-fibrotic responses in dermal fibroblasts and enhances wound healing probably via PAR-2/F2RL1-dependent mechanism .
PMID:18202198
Activates barrier protective signaling responses in endothelial cells in PAR-2/F2RL1-dependent manner; the activity depends on the cleavage of PAR-2/F2RL1 by factor Xa .
PMID:22409427
Up-regulates expression of plasminogen activator inhibitor 1 (SERPINE1) in atrial tissues PMID:24041930
Antithrombin-III
SERPINC1
antagonist
Specific functionheparin binding
Cellular location
Secreted, extracellular space
General function & pharmacology
Most important serine protease inhibitor in plasma that regulates the blood coagulation cascade .
PMID:15140129 PMID:15853774
AT-III inhibits thrombin, matriptase-3/TMPRSS7, as well as factors IXa, Xa and XIa .
PMID:15140129
Its inhibitory activity is greatly enhanced in the presence of heparin
PMID:15140129 PMID:15853774
AT-III inhibits thrombin, matriptase-3/TMPRSS7, as well as factors IXa, Xa and XIa .
PMID:15140129
Its inhibitory activity is greatly enhanced in the presence of heparin
Heparin cofactor 2
SERPIND1
antagonist
Specific functionendopeptidase inhibitor activity
General function & pharmacology
Thrombin inhibitor activated by the glycosaminoglycans, heparin or dermatan sulfate. In the presence of the latter, HC-II becomes the predominant thrombin inhibitor in place of antithrombin III (AT-III). Also inhibits chymotrypsin, but in a glycosaminoglycan-independent manner
Scientific references(6)
Chapman T.M., Goa K.L.
Bemiparin.
Drugs
200363(21):2357-2377. doi: 10.2165/00003495-200363210-00009
Planes A.
Review of bemiparin sodium a new second-generation low molecular weight heparin and its applications in venous thromboembolism.
Expert Opinion on Pharmacotherapy
20034(9):1551-1561. doi: 10.1517/eoph.4.9.1551.21062
Jeske W.P., Hoppensteadt D., Gray A., Walenga J.M., Cunanan J., Myers L., Fareed J., Bayol A., Rigal H., Viskov C.
A common standard is inappropriate for determining the potency of ultra low molecular weight heparins such as semuloparin and bemiparin.
Thromb Research
2011 Oct128(4):361-7. doi: 10.1016/j.thromres.2011.03.001. Epub 2011 Apr 2
Sanchez-Ferrer C.F.
Bemiparin: pharmacological profile.
Drugs
2010 Dec 1470 Suppl 2:19-23. doi: 10.2165/1158581-S0-000000000-00000
Hoffman M., Monroe D.M.
Coagulation 2006: a modern view of hemostasis.
Hematology Oncology Clinical North American
2007 Feb21(1):1-11. doi: 10.1016/j.hoc.2006.11.004
Antonijoan R.M., Rico S., Martinez-Gonzalez J., Borrell M., Valcarcel D., Fontcuberta J., Barbanoj M.J.
Comparative pharmacodynamic time-course of bemiparin and enoxaparin in healthy volunteers.
International
Journal of Clinical Pharmacology and Therapeutics. 200947(12):726-732. doi: 10.5414/cpp47726
ATC classification(1 code)
ATC B01AB12
Affected organisms(1)
Humans
International brands(4)
Salt forms(1)
Bemiparin sodium(DBSALT001275)
Experimental properties(1)
Chemical identifiers
CAS, UNII, InChI Key and database cross-references
Show
Chemical identifiers
CAS, UNII, InChI Key and database cross-references
Linked compound data from DrugBank Open Data (CC BY-NC 4.0)
Bemiparin
Additional database identifiers
HUGO Gene Nomenclature Committee (HGNC)
HGNC:3528
GenAtlas
F10
GeneCards
F10
GenBank Gene Database
K03194
GenBank Protein Database
182841
Guide to Pharmacology
2359
UniProt Accession
FA10_HUMAN
HUGO Gene Nomenclature Committee (HGNC)
HGNC:775
GenAtlas
SERPINC1
GeneCards
SERPINC1
GenBank Gene Database
M21642
GenBank Protein Database
179161
Guide to Pharmacology
2632
UniProt Accession
ANT3_HUMAN
HUGO Gene Nomenclature Committee (HGNC)
HGNC:4838
GenAtlas
SERPIND1
GeneCards
SERPIND1
GenBank Gene Database
M12849
GenBank Protein Database
183910
UniProt Accession
HEP2_HUMAN
DrugBank citations
If you use DrugBank data in your research, please cite the following publications:
Knox C., Wilson M., Klinger C.M., et al
DrugBank 6.
0: the DrugBank Knowledgebase for 2024
Nucleic Acids Res. 2024 Jan 552(D1):D1265-D1275
Wishart D.S., Feunang Y.D., Guo A.C., et al
DrugBank 5.
0: a major update to the DrugBank database for 2018
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Updated 27 days ago(8 Mar 2026)