Brands, Medical Use, Clinical Data
Drug Category
- Rodenticides
- Anticoagulants
- Coumarin and Indandione Derivatives
Dosage Forms
- Powder for solution
- Tablet
Brands / Synonyms
200 Coumarin; Athrombin; Athrombin-K; Athrombine-K; Brumolin; Co-Rax; Compound 42; Coumadin; Coumafen; Coumafene; Coumaphen; Coumaphene; Coumarins; Coumefene; D-Con; Dethmor; Dethnel; Dicusat E; Eastern States Duocide; Fasco Fascrat Powder; Frass-Ratron; Jantoven; Killgerm Sewarin P; Kumader; Kumadu; Kumatox; Kypfarin; Latka 42; Liqua-Tox; Maag Rattentod Cum; Mar-Frin; Marevan; Martin's Mar-Frin; Maveran; Mice Bait; Mouse Pak; Panwarfin; Place-Pax; Prothromadin; RAX; Rodafarin; Rodafarin C; Rodex; Rodex Blox; Rosex; Sofarin; Solfarin; Sorexa Plus; Temus W; Tintorane; Tox-Hid; Vampirinip II; Vampirinip III; W.A.R.F. 42; Waran; Warf 42; Warf Cmpd. 42; Warf Compound 42; Warfarat; Warfarin; Warfarin Plus; Warfarin Q; Warfarin sodium; Warfarine; Warficide; Warfilone; Zoocoumarin
Indications
For the treatment of retinal vascular occlusion, pulmonary embolism, cardiomyopathy, atrial fibrillation and flutter, cerebral embolism, transient cerebral ischaemia, arterial embolism and thrombosis.
Pharmacology
Warfarin, a coumarin anticoagulant, is a racemic mixture of two active isomers. It is used in the prevention and treatment of thromboembolic disease including venous thrombosis, thromboembolism, and pulmonary embolism as well as for the prevention of ischemic stroke in patients with atrial fibrillation (AF).
Mechanism of Action
Warfarin inhibits vitamin K reductase, resulting in depletion of the reduced form of vitamin K (vitamin KH2). As vitamin K is a cofactor for the carboxylation of glutamate residues on the N-terminal regions of vitamin K-dependent proteins, this limits the gamma-carboxylation and subsequent activation of the vitamin K-dependent coagulant proteins. The synthesis of vitamin K-dependent coagulation factors II, VII, IX, and X and anticoagulant proteins C and S is inhibited. Depression of three of the four vitamin K-dependent coagulation factors (factors II, VII, and X) results in decresed prothrombin levels and a decrease in the amount of thrombin generated and bound to fibrin. This reduces the thrombogenicity of clots.
Absorption
Not Available
Toxicity
LD50=374 (orally in mice)
Biotrnasformation / Drug Metabolism
Metabolized by hepatic microsomal enzymes.
Contraindications
Anticoagulation is contraindicated in any localized or general physical condition or personal
circumstance in which the hazard of hemorrhage might be greater than the potential clinical benefits of
anticoagulation, such as:
Pregnancy
COUMADIN is contraindicated in women who are or may become pregnant because the drug passes through
the placental barrier and may cause fatal hemorrhage to the fetus in utero. Furthermore, there have been
reports of birth malformations in children born to mothers who have been treated with warfarin during pregnancy.
Embryopathy characterized by nasal hypoplasia with or without stippled epiphyses (chondrodysplasia
punctata) has been reported in pregnant women exposed to warfarin during the first trimester. Central nervous system
abnormalities also have been reported, including dorsal midline dysplasia characterized by agenesis of the corpus
callosum, Dandy-Walker malformation, and midline cerebellar atrophy. Ventral midline dysplasia, characterized by
optic atrophy, and eye abnormalities have been observed. Mental retardation, blindness,a nd other central nervous
system abnormalities have been reported in association with second and third trimester exposure. Although rare,
teratogenic reports following in utero exposure to warfarin include urinary tract anomalies such as single
kidney, asplenia, anencephaly, spina bifida, cranial nerve palsy, hydrocephalus, cardiac defects and congenital heart
disease, polydactyly, deformities of toes, diaphragmatic hernia, corneal leukoma, cleft palate, cleft lip,
schizencephaly, and microcephaly.
Spontaneous abortion and stillbirth are known to occur and a higher risk of fetal mortality is
associated with the use of warfarin. Low birth weight and growth retardation have also been reported.
Women of childbearing potential who are candidates for anticoagulant therapy should be carefully
evaluated and the indications critically reviewed with the patient. If the patient becomes pregnant while taking this
drug, she should be apprised of the potential risks to the fetus, and the possibility of termination of the pregnancy
should be discussed in light of those risks.
Hemorrhagic tendencies or blood dyscrasias.
Recent or contemplated surgery of: (1) central nervous system; (2) eye; (3) traumatic surgery
resulting in large open surfaces.
Bleeding tendencies associated with active ulceration or overt bleeding of: (1) gastrointestinal,
genitourinary or respiratory tracts; (2) cerebrovascular hemorrhage; (3) aneurysms-cerebral, dissecting aorta; (4)
pericarditis and pericardial effusions; (5) bacterial endocarditis.
Threatened abortion, eclampsia and preeclampsia.
Inadequate laboratory facilities.
Unsupervised patients with senility, alcoholism,or psychosis or other lack of patient cooperation.
Spinal puncture and other diagnostic or therapeutic procedures with potential for uncontrollable
bleeding.
Miscellaneous major regional, lumbar block anesthesia, malignant hypertension and known
hypersensitivity to warfarin or to any other components of this product.
Drug Interactions
Drugs may interact with COUMADIN through pharmacodynamic or pharmacokinetic mechanisms.
Pharmacodynamic mechanisms for drug interactions with COUMADIN are synergism (impaired hemostasis, reduced clotting
factor synthesis), competitive antagonism (vitamin K), and altered physiologic control loop for vitamin K metabolism
(hereditary resistance). Pharmacokinetic mechanisms for drug interactions with COUMADIN are mainly enzyme induction,
enzyme inhibition, and reduced plasma protein binding. It is important to note that some drugs may interact by more
than one mechanism.
The following factors, alone or in combination, may be responsible for INCREASED PT/INR response
ENDOGENOUS FACTORS
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blood dyscrasias —
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diarrhea
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hyperthyroidism
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see CONTRAINDICATIONS
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elevated temperature
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poor nutritional state
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cancer
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hepatic disorders
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steatorrhea
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collagen vascular disease
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infectious hepatitis
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vitamin K deficiency
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congestive heart failure
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jaundice
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EXOGENOUS FACTORS
Potential drug interactions with COUMADIN are listed below by drug class and by specific drugs.
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Classes of Drugs
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5-lipoxygenase Inhibitor
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Antiparasitic/Antimicrobials
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HMG-CoA Reductase
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Adrenergic Stimulants, Central
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Antiplatelet Drugs/Effects
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Inhibitors†
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Alcohol Abuse Reduction
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Antithyroid Drugs†
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Leukotriene Receptor Antagonist
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Preparations
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Beta-Adrenergic Blockers
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Monoamine Oxidase Inhibitors
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Analgesics
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Cholelitholytic Agents
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Narcotics,prolonged
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Anesthetics, Inhalation
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Diabetes Agents, Oral
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Nonsteroidal Anti-Inflammatory
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Antiandrogen
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Diuretics†
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Agents
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Antiarrhythmics†
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Fungal Medications, Intravaginal,
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Psychostimulants
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Antibiotics†
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Systemic†
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Pyrazolones
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Aminoglycosides (oral)
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Gastric Acidity and Peptic
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Salicylates
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Cephalosporins, parenteral
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Ulcer Agents†
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Selective Serotonin
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Macrolides
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Gastrointestinal
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Reuptake Inhibitors
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Miscellaneous
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Prokinetic Agents
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Steroids, Adrenocortical†
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Penicillins, intravenous,
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Ulcerative Colitis Agents
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Steroids, Anabolic (17-Alkyl
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high dose
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Gout Treatment Agents
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Testosterone Derivatives)
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Quinolones (fluoroquinolones)
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Hemorrheologic Agents
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Thrombolytics
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Sulfonamides, long acting
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Hepatotoxic Drugs
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Thyroid Drugs
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Tetracyclines
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Hyperglycemic Agents
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Tuberculosis Agents†
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Anticoagulants
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Hypertensive Emergency Agents
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Uricosuric Agents
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Anticonvulsants†
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Hypnotics†
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Vaccines
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Antidepressants†
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Hypolipidemics†
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Vitamins†
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Antimalarial Agents
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Bile Acid-Binding Resins†
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Antineoplastics†
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Fibric Acid Derivatives
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Specific Drugs Reported
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acetaminophen
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fluconazole
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penicillin G,intravenous
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alcohol†
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fluorouracil
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pentoxifylline
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allopurinol
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fluoxetine
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phenylbutazone
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aminosalicylic acid
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flutamide
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phenytoin†
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amiodarone HCl
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fluvastatin
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piperacillin
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aspirin
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fluvoxamine
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piroxicam
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atorvastatin†
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gemfibrozil
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pravastatin†
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azithromycin
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glucagon
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prednisone†
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capecitabine
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halothane
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propafenone
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cefamandole
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heparin
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propoxyphene
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cefazolin
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ibuprofen
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propranolol
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cefoperazone
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ifosfamide
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propylthiouracil†
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cefotetan
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indomethacin
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quinidine
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cefoxitin
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influenza virus vaccine
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quinine
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ceftriaxone
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itraconazole
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ranitidine†
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celecoxib
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ketoprofen
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rofecoxib
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cerivastatin
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ketorolac
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sertraline
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chenodiol
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levamisole
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simvastatin
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chloramphenicol
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levofloxacin
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stanozolol
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chloral hydrate†
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levothyroxine
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streptokinase
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chlorpropamide
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liothyronine
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sulfamethizole
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cholestyramine†
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lovastatin
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sulfamethoxazole
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cimetidine
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mefenamic acid
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sulfinpyrazone
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ciprofloxacin
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methimazole†
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sulfisoxazole
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cisapride
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methyldopa
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sulindac
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clarithromycin
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methylphenidate
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tamoxifen
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clofibrate
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methylsalicylate ointment
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tetracycline
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COUMADIN overdose
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(topical)
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thyroid
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cyclophosphamide†
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metronidazole
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ticarcillin
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danazol
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miconazole
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ticlopidine
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dextran
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(intravaginal,systemic)
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tissue plasminogen
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dextrothyroxine
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moricizine hydrochloride†
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activator (t-PA)
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diazoxide
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nalidixic acid
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tolbutamide
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diclofenac
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naproxen
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tramadol
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dicumarol
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neomycin
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trimethoprim/sulfamethoxazole
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diflunisal
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norfloxacin
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urokinase
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disulfiram
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ofloxacin
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valproate
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doxycycline
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olsalazine
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vitamin E
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erythromycin
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omeprazole
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zafirlukast
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ethacrynic acid
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oxaprozin
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zileuton
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fenofibrate
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oxymetholone
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fenoprofen
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paroxetine
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also: other medications affecting blood elements which may modify hemostasis dietary deficiencies
prolonged hot weather unreliable PT/INR determinations
† increased and decreased PT/INR responses have been reported.
The following factors, alone or in combination, may be responsible for DECREASED PT/INR response
ENDOGENOUS FACTORS
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edema
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hypothyroidism
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hereditary coumarin resistance
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nephrotic syndrome
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hyperlipemia
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EXOGENOUS FACTORS
Potential drug interactions with COUMADIN (Warfarin Sodium) are listed below by drug class and by
specific drugs.
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Classes of Drugs
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Adrenal Cortical Steroid Inhibitors
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Antithyroid Drugs†
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HMG-CoA Reductase Inhibitors†
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Antacids
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Barbiturates
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Immunosuppressives
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Antianxiety Agents
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Diuretics†
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Oral Contraceptives,
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Antiarrhythmics†
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Enteral Nutritional Supplements
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Estrogen Containing
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Antibiotics†
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Fungal Medications, Systemic†
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Selective Estrogen Receptor
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Anticonvulsants†
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Gastric Acidity and
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Modulators
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Antidepressants†
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Peptic Ulcer Agents†
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Steroids, Adrenocortical†
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Antihistamines
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Hypnotics†
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Tuberculosis Agents†
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Antineoplastics†
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Hypolipidemics†
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Vitamins†
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Antipsychotic Medications
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Bile Acid-Binding Resins†
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Specific Drugs Reported
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alcohol†
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COUMADIN underdosage
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phenytoin†
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aminoglutethimide
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cyclophosphamide†
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pravastatin†
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amobarbital
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dicloxacillin
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prednisone†
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atorvastatin†
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ethchlorvynol
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primidone
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azathioprine
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glutethimide
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propylthiouracil†
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butabarbital
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griseofulvin
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raloxifene
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butalbital
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haloperidol
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ranitidine†
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carbamazepine
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meprobamate
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rifampin
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chloral hydrate†
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6-mercaptopurine
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secobarbital
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chlordiazepoxide
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methimazole†
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spironolactone
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chlorthalidone
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moricizine hydrochloride†
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sucralfate
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cholestyramine†
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nafcillin
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trazodone
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clozapine
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paraldehyde
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vitamin C (high dose)
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corticotropin
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pentobarbital
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vitamin K
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cortisone
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phenobarbital
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also: diet high in vitamin K unreliable PT/INR determinations
†Increased and decreased PT/INR responses have been reported.
Because a patient may be exposed to a combination of the above factors, the net effect of COUMADIN on
PT/INR response may be unpredictable. More frequent PT/INR monitoring is therefore advisable. Medications of unknown
interaction with coumarins are best regarded with caution. When these medications are started or stopped, more
frequent PT/INR monitoring is advisable.
It has been reported that concomitant administration of warfarin and ticlopidine may be associated
with cholestatic hepatitis.
Botanical (Herbal) Medicines
Caution should be exercised when botanical medicines (botanicals) are taken concomitantly with
COUMADIN. Few adequate, well-controlled studies exist evaluating the potential for metabolic and/or pharmacologic
interactions between botanicals and COUMADIN. Due to a lack of manufacturing standardization with botanical medicinal
preparations, the amount of active ingredients may vary. This could further confound the ability to assess potential
interactions and effects on anticoagulation. It is good practice to monitor the patient’s response with
additional PT/INR determinations when initiating or discontinuing botanicals.
Specific botanicals reported to affect COUMADIN therapy include the following:
• Bromelains, danshen, dong quai (Angelica sinensis), garlic, Ginkgo biloba, and ginseng are
associated most often with an INCREASE in the effects of COUMADIN.
• Coenzyme Q10 (ubidecarenone) and St. John’s wort are associated most often with a
DECREASE in the effects of COUMADIN.
Some botanicals may cause bleeding events when taken alone (e.g., garlic and Ginkgo biloba) and may
have anti-coagulant, antiplatelet, and/or fibrinolytic properties. These effects would be expected to be additive to
the anticoagulant effects of COUMADIN. Conversely, other botanicals may have coagulant properties when taken alone or
may decrease the effects of COUMADIN.
Some botanicals that may affect coagulation are listed below for reference; however, this list should
not be considered all-inclusive. Many botanicals have several common names and scientific names. The most widely
recognized common botanical names are listed.
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Botanticals that contain coumarins with potential anticoagulant effects:
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Alfalfa
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Celery
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Parsley
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Angelica (Dong Quai)
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Chamomile
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Passion Flower
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Aniseed
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(German and Roman)
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Prickly Ash (Northern)
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Arnica
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Dandelion3
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Quassia
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Asa Foetida
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Fenugreek
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Red Clover
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Bogbean1
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Horse Chestnut
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Sweet Clover
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Boldo
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Horseradish
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Sweet Woodruff
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Buchu
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Licorice3
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Tonka Beans
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Capsicum2
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Meadowsweet1
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Wild Carrot
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Cassia3
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Nettle
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Wild Lettuce
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Miscellaneous botanticals with anticoagulant properties:
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Bladder Wrack (Fucus)
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Pau d’arco
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Botanicals that contain salicylate and/or have antiplatelet properties:
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Agrimony4
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Dandelion3
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Meadowsweet1
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Aloe Gel
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Feverfew
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Onion5
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Aspen
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Garlic5
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Policosanol
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Black Cohosh
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German Sarsaparilla
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Poplar
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Black Haw
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Ginger
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Senega
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Bogbean1
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Ginkgo Biloba
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Tamarind
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Cassia3
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Ginseng (Panax)5
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Willow
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Clove
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Licorice3
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Wintergreen
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Botanticals with fibrinolytic properties:
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Bromelains
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Garlic5
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Inositol Nicotinate
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Capsicum2
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Ginseng (Panax)5
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Onion5
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Botanticals with coagulant properties:
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Agrimony4 Mistletoe
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Yarrow
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Goldenseal
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1 Contains coumarins and salicylate.
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2 Contains coumarins and has fibrinolytic properties.
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3 Contains coumarins and has antiplatelet properties.
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4 Contains salicylate and has coagulant properties.
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5 Has antiplatelet and fibrinolytic properties.
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Effect on Other Drugs
Coumarins may also affect the action of other drugs. Hypoglycemic agents (chlorpropamide and
tolbutamide) and anticonvulsants (phenytoin and phenobarbital) may accumulate in the body as a result of interference
with either their metabolism or excretion.
Special Risk Patients
COUMADIN (Warfarin Sodium) is a narrow therapeutic range (index) drug, and caution should be observed
when warfarin sodium is administered to certain patients such as the elderly or debilitated or when administered in
any situation or physical condition where added risk of hemorrhage is present.
Intramuscular (I.M.) injections of concomitant medications should be confined to the upper extremities
which permits easy access for manual compression, inspections for bleeding and use of pressure bandages.
Caution should be observed when COUMADIN (or warfarin) is administered concomitantly with nonsteroidal
antiinflammatory drugs (NSAIDs), including aspirin, to be certain that no change in anticoagulation dosage is
required. In addition to specific drug interactions that might affect PT/INR, NSAIDs, including aspirin, can inhibit
platelet aggregation, and can cause gastrointestinal bleeding, peptic ulceration and/or perforation.
Acquired or inherited warfarin resistance should be suspected if large daily doses of COUMADIN are
required to maintain a patient’s PT/INR within a normal therapeutic range.
Potential adverse reactions to COUMADIN may include:
• Fatal or nonfatal hemorrhage from any tissue or organ. This is a consequence of the anticoagulant effect.
The signs, symptoms, and severity will vary according to the location and degree or extent of the bleeding.
Hemorrhagic complications may present as paralysis; paresthesia; headache, chest, abdomen, joint, muscle or other
pain; dizziness; shortness of breath, difficult breathing or swallowing; unexplained swelling; weakness;
hypotension; or unexplained shock. Therefore, the possibility of hemorrhage should be considered in evaluating the
condition of any anticoagulated patient with complaints which do not indicate an obvious diagnosis. Bleeding during
anticoagulant therapy does not always correlate with PT/INR.
• Bleeding which occurs when the PT/INR is within the therapeutic range warrants diagnostic investigation
since it may unmask a previously unsuspected lesion, e.g., tumor, ulcer, etc.
• Necrosis of skin and other tissues.
• Adverse reactions reported infrequently include: hypersensitivity/allergic reactions, systemic
cholesterol microembolization, purple toes syndrome, hepatitis, cholestatic hepatic injury, jaundice, elevated
liver enzymes, vasculitis, edema, fever, rash, dermatitis, including bullous eruptions, urticaria, abdominal pain
including cramping, flatulence/bloating, fatigue, lethargy, malaise, asthenia, nausea, vomiting, diarrhea, pain,
headache, dizziness, taste perversion, pruritus, alopecia, cold intolerance, and paresthesia including feeling cold
and chills.
Rare events of tracheal or tracheobronchial calcification have been reported in association with
long-term warfarin therapy. The clinical significance of this event is unknown.
Priapism has been associated with anticoagulant administration, however, a causal relationship has not
been established.
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