Warfarin

B01A - Antithrombotic agents ATC B01AA03 Small molecule approved 1954 Oral Parenteral Natural product Narrow therapeutic index Black-box warning

JFDA label: ORFARIN 5MG TABLET

⚠ Black-Box Warning

Bleeding risk:

Mechanism of Action

Hepatic synthesis of coagulation factors II (half-life 42 to 72 hours), VII (half-life 4 to 6 hours), IX, and X (half-life 27 to 48 hours), as well as proteins C and S, requires the presence of vitamin K. These clotting factors are biologically activated by the addition of carboxyl groups to key glutamic acid residues within the proteins’ structure. In the process, “active” vitamin K is oxidatively converted to an “inactive” form, which is then subsequently reactivated by vitamin K epoxide reductase complex 1 (VKORC1). Warfarin competitively inhibits the subunit 1 of the multi-unit VKOR complex, thus depleting functional vitamin K reserves and hence reduces synthesis of active clotting factors.

Indications

Approved

Mechanical prosthetic cardiac valves
Myocardial infarction
Nonvalvular AF or atrial flutter
Thromboembolic complications
Valvular AF
Venous thromboembolism (VTE)

Off-label

Recurrent stroke/Transient ischemic attacks (secondary prevention)

Contraindications

Source: Curated · Lexicomp

Active major bleeding or high risk of clinically significant bleeding Absolute
CNS hemorrhage Absolute
Hypersensitivity to warfarin or any component of the formulation Absolute
Pregnancy (teratogenic — category X; causes fetal warfarin syndrome) Absolute
Unsupervised patients with senility, alcoholism, or psychosis Absolute
bacterial endocarditis Absolute
blood dyscrasias Absolute
cerebral aneurysm Absolute
dissecting aortic aneurysm Absolute
eclampsia/preeclampsia, threatened abortion, pregnancy (except in women with mechanical heart valves at high risk for thromboembolism) Absolute
hemorrhagic tendencies (eg, active GI ulceration, patients bleeding from the GI, respiratory, or GU tract Absolute
major regional lumbar block anesthesia or traumatic surgery resulting in large, open surfaces Absolute
malignant hypertension Absolute
pericarditis or pericardial effusion Absolute
recent or potential surgery of the eye or CNS Absolute
spinal puncture and other diagnostic or therapeutic procedures with potential for significant bleeding) Absolute
unsupervised patients with conditions associated with a high potential for noncompliance Absolute

Adverse Reactions

Very Common >10%Common 1–10%Uncommon 0.1–1% Rare 0.01–0.1%Very Rare <0.01%Not Known

Cardiac disorders (3)

Not Known Purple-toe syndrome · systemic cholesterol micro-embolism · vasculitis

Vascular disorders (1)

Rare Purple toe syndrome

Nervous system disorders (2)

Uncommon Intracranial haemorrhage

Not Known Chills

Hepatobiliary disorders (1)

Not Known Hepatitis

Renal and urinary disorders (1)

Not Known Acute renal failure (in patients with altered glomerular integrity or with a history of kidney disease)

Blood and lymphatic system disorders (2)

Common Major hemorrhage

Not Known Minor hemorrhage

Immune system disorders (2)

Not Known Anaphylaxis · hypersensitivity reaction

Gastrointestinal disorders (8)

Uncommon Nausea

Not Known Abdominal pain · bloating · diarrhea · dysgeusia · flatulence · nausea · vomiting

Skin and subcutaneous tissue disorders (8)

Uncommon Alopecia

Rare Skin necrosis (protein C/S deficiency)

Not Known Alopecia · bullous rash · dermatitis · pruritus · skin necrosis · urticaria

Injury, poisoning and procedural complications (2)

Very Common Bleeding (minor: bruising, epistaxis)

Common Bleeding (major: GI, urological)

Respiratory, thoracic and mediastinal disorders (1)

Not Known Tracheobronchial calcification

Dosing

Source: Lexicomp

Note: Coumadin injection has been discontinued in the US for more than 1 year. Note: Labeling identifies genetic factors which may increase patient sensitivity to warfarin. Specifically, genetic variations in the proteins CYP2C9 and VKORC1, responsible for warfarin's primary metabolism and pharmacodynamic activity, respectively, have been identified as predisposing factors associated with decreased dose requirement and increased bleeding risk. Genotyping tests are available, and may provide guidance on initiation of anticoagulant therapy. The American College of Chest Physicians recommends against the use of routine pharmacogenomic testing to guide dosing (Guyatt 2012). For management of elevated INRs as a result of warfarin therapy, see Additional Information/Pharmacotherapy Pearls for guidance. Thromboembolic complications (prophylaxis/treatment) or myocardial infarction (risk reduction): IV (administer as a slow bolus injection): 2 to 5 mg/day Oral: Initial dosing must be individualized. Consider the patient (hepatic function, cardiac function, age, nutritional status, concurrent therapy, risk of bleeding) in addition to prior dose response (if available) and the clinical situation. Start 2 to 5 mg once daily or for healthy individuals, 10 mg once daily for 2 days; lower doses (eg, 5 mg once daily) recommended for patients with confirmed HIT once platelet recovery has occurred (Guyatt 2012). In patients with acute venous thromboembolism, initiation may begin on the first or second day of low molecular weight heparin or unfractionated heparin therapy (Guyatt 2012). Adjust dose according to INR results; usual maintenance dose ranges from 2 to 10 mg daily (individual patients may require loading and maintenance doses outside these general guidelines). Note: Lower starting doses may be required for patients with hepatic impairment, poor nutrition, CHF, elderly, high risk of bleeding, or patients who are debilitated, or those with reduced function genomic variants of the catabolic enzymes CYP2C9 (*2 or *3 alleles) or VKORC1 (-1639 polymorphism); see table. Higher initial doses may be reasonable in selected patients (ie, receiving enzyme-inducing agents and with low risk of bleeding). Overlapping a parenteral anticoagulant and warfarin therapy by at least 5 days is necessary in treatment of DVT/PE even if the INR is therapeutic earlier. Although an elevation in INR (due to factor VII depletion) may be seen early (within the first 24 to 48 hours) in warfarin therapy, it does not represent adequate anticoagulation. Factors II and X must also be depleted which takes considerably longer (ACCP [Guyatt 2012]). Range1 of Expected Therapeutic Maintenance Dose Based on CYP2C92 and VKORC13 Genotypes VKORC1 CYP2C9 Note: Must also take into account other patient related factors when determining initial dose (eg, age, body weight, concomitant medications, comorbidities). The American College of Chest Physicians recommends against the use of routine pharmacogenom

(For additional information see "Warfarin: Pediatric drug information") Note: Coumadin injection has been discontinued in the US for more than 1 year. Note: Labeling identifies genetic factors which may increase patient sensitivity to warfarin. Specifically, genetic variations in the proteins CYP2C9 and VKORC1, responsible for warfarin's primary metabolism and pharmacodynamic activity, respectively, have been identified as predisposing factors associated with decreased dose requirement and increased bleeding risk. Genotyping tests are available, and may provide guidance on initiation of anticoagulant therapy. The American College of Chest Physicians recommends against the use of routine pharmacogenomic testing to guide dosing (Guyatt 2012). For management of elevated INRs as a result of warfarin therapy, see Additional Information/Pharmacotherapy Pearls for guidance. Prevention/treatment of thrombosis: Infants and Children (off-label use): Oral: Initial loading dose (if baseline INR is 1-1.3): 0.2 mg/kg (maximum: 10 mg/dose); adjust dose based on INR (reported ranges to maintain INR of 2 to 3: 0.09 to 0.33 mg/kg/day). Infants

Thromboembolic complications (prophylaxis/treatment) or myocardial infarction (risk reduction): Oral: Initial dose ≤5 mg. Usual maintenance dose: 2 to 5 mg/day. Patients >60 years of age tend to require lower dosages to produce a therapeutic level of anticoagulation (due to changes in the pattern of warfarin metabolism).

No dosage adjustment necessary. However, patients with renal impairment have an increased risk for bleeding diathesis; monitor INR closely. Hemodialysis: Not dialyzable (NCS/SCCM [Frontera 2016])

There are no dosage adjustments provided in the manufacturer's labeling. However, the response to oral anticoagulants may be markedly enhanced in obstructive jaundice, hepatitis, and cirrhosis. INR should be closely monitored.

Warnings & Precautions

Source: Lexicomp

Acute kidney injury

Acute kidney injury, possibly as a result of episodes of excessive anticoagulation and hematuria, may occur in patients with a history of kidney disease or in patients with altered glomerular integrity.

Anaphylaxis/hypersensitivity

May cause hypersensitivity reactions, including anaphylaxis; use with caution in patients with anaphylactic disorders.

Bleeding

May cause major or fatal bleeding. Perform regular INR monitoring in all treated patients. INR levels achieved with warfarin therapy may be affected by concomitant medication, dietary modifications and/or other factors (eg, smoking). Risk factors for bleeding include high intensity anticoagulation (INR >4), age (≥65 years), variable INRs, history of GI bleeding, hypertension, cerebrovascular disease, serious heart disease, anemia, severe diabetes, malignancy, trauma, renal insufficiency, polycythemia vera, vasculitis, open wound, history of PUD, indwelling catheters, menstruating and postpartum women, drug-drug interactions, long duration of therapy, or known genetic deficiency in CYP2C9 activity. Patient must be instructed to report bleeding, accidents, or falls as well as any new or discontinued medications, herbal or alternative products used, or significant changes in smoking or dietary habits. Unrecognized bleeding sites (eg, colon cancer) may be uncovered by anticoagulation.

Calciphylaxis

Fatal and serious calciphylaxis (calcium uremic arteriolopathy) has been reported in patients with and without end-stage renal disease. If calciphylaxis is diagnosed, discontinue therapy and treat calciphylaxis as appropriate. Consider alternative anticoagulation therapy.

Skin necrosis/gangrene

Necrosis or gangrene of the skin and other tissue can occur (rarely, • Atheroemboli/cholesterol microemboli: Warfarin therapy may release atheromatous plaque emboli; symptoms depend on site of embolization, most commonly kidneys, pancreas, liver, and spleen. In some cases may lead to necrosis or death. “Purple toe” syndrome, due to cholesterol microembolization, has been rarely described with coumarin-type anticoagulants. Typically, this occurs after several weeks of therapy, and may present as a dark, purplish, mottled discoloration of the plantar and lateral surfaces. Other manifestations of cholesterol microembolization may include rash; livedo reticularis; gangrene; abrupt and intense pain in lower extremities; abdominal, flank, or back pain; hematuria, renal insufficiency; hypertension; cerebral ischemia; spinal cord infarction; or other symptoms of vascular compromise. Disease-related concerns:

Dietary insufficiency

Use with caution in patients with prolonged dietary insufficiencies (vitamin K deficiency).

Heparin-induced thrombocytopenia

Use with caution in patients with heparin-induced thrombocytopenia and DVT; limb ischemia, necrosis, and gangrene have occurred when warfarin was started or continued after heparin was stopped. Warfarin monotherapy is contraindicated in the initial treatment of active HIT; warfarin initially inhibits the synthesis of protein C, potentially accelerating the underlying active thrombotic process.

Hepatic impairment

Reduced liver function, regardless of etiology, may impair synthesis of coagulation factors leading to increased warfarin sensitivity.

Infection

Use with caution in patients with acute infection or active TB or any disruption of normal GI flora; antibiotics and fever may alter response to warfarin.

Renal impairment

Use with caution in patients with renal impairment. Patients with renal impairment are at increased risk for bleeding diathesis; frequent INR monitoring is recommended.

Thyroid disease

Use with caution in patients with thyroid disease; warfarin responsiveness may increase (Ageno 2012). Special populations:

Elderly

The elderly may be more sensitive to anticoagulant therapy.

Patients with genomic variants in CYP2C9 and/or VKORC1

Presence of the CYP2C9*2 or *3 allele and/or polymorphism of the vitamin K oxidoreductase (VKORC1) gene may increase the risk of bleeding. The *2 allele is reported to occur with a frequency of 4% to 11% in African-Americans and Caucasians, respectively, while the *3 allele frequencies are 2% to 7% respectively. Other variant 2C9 alleles (eg, *5, *6, *9, and *11) are also associated with reduced metabolic activity and thus may increase risk of bleeding, but are much less common. Lower doses may be required in these patients; genetic testing may help determine appropriate dosing. Other warnings/precautions:

Appropriate use

Surgical patients: When temporary interruption is necessary before surgery, discontinue for approximately 5 days before surgery; when there is adequate hemostasis, may reinstitute warfarin therapy ~12 to 24 hours after surgery (evening of or next morning). Decision to safely continue warfarin therapy through the procedure and whether or not bridging of anticoagulation is necessary is dependent upon risk of perioperative bleeding and risk of thromboembolism, respectively. If risk of thromboembolism is elevated, consider bridging warfarin therapy with an alternative anticoagulant (eg, unfractionated heparin, LMWH) (Guyatt 2012).

Patient selection

Use care in the selection of patients appropriate for this treatment; ensure patient cooperation especially from the alcoholic, illicit drug user, demented, or psychotic patient; ability to comply with routine laboratory monitoring is essential.

Pregnancy & Lactation

Pregnancy

FDA category X Teratogenic Contraindicated

Contraindicated

Replace with LMWH throughout pregnancy; warfarin may be used in selected cases in 2nd trimester with careful monitoring by specialist

Lactation

Based on available data, warfarin is not present in breast milk. Breastfeeding women may be treated with warfarin. According to the American College of Chest Physicians (ACCP), warfarin may be used in lactating women who wish to breastfeed their infants (ACCP [Bates 2012]). The manufacturer recommends monitoring of breastfeeding infants for bruising or bleeding.

Monitoring

Efficacy	INR (target 2–3 for most indications; 2.5–3.5 for mechanical heart valves); PT every 1–4 weeks once stable
Toxicity	Signs of bleeding (haematuria, melena, bruising, prolonged bleeding from minor cuts); INR > 5 → increased bleeding risk
Clinical pearl	Many drug-drug and drug-food interactions alter INR significantly. Consistent vitamin K intake is essential. Check INR 3–5 days after any change in dose or interacting drug.
Counseling	Do not change diet drastically. Report unusual bleeding or bruising immediately. Carry anticoagulant alert card.

Chemistry & Properties

Formula	C19H16O4
Molecular weight	308.33 g/mol
IUPAC name	4-hydroxy-3-(3-oxo-1-phenylbutyl)chromen-2-one
CAS	81-81-2
PubChem CID	54678486
InChIKey	`PJVWKTKQMONHTI-UHFFFAOYSA-N`
logP	3.61 (XLogP 2.7)
Polar surface area	67.51 Å²
H-bond acceptors / donors	4 / 1
Drug-likeness (QED)	0.75
Lipinski violations	0

SMILES

CC(=O)CC(c1ccccc1)c1c(O)c2ccccc2oc1=O

Biology & Pharmacokinetics

Pharmacokinetics predicted

Bioavailability	10.0%
Half-life	1.252 h
Volume of distribution	0.127 L/kg
Protein binding	98.2%
BBB penetrant	No

Enzyme interactions

Enzyme	Role	Detail
CYP1A2	Substrate	—
CYP2B6	Substrate	—
CYP2C19	Substrate	—
CYP2C9	Inhibitor	Ki 20.000000000000004 µM
CYP2C9	Substrate	—
CYP2D6	Substrate	—
CYP3A4	Substrate	—

Receptor binding (top 1)

Target	Action	Affinity
vitamin K epoxide reductase complex subunit 1 (VKORC1)	Inhibitor	pKi 5.6

Transporters

BCRP (Inhibitor)BCRP (Inhibitor)BSEP (Inhibitor)BSEP (Inhibitor)MRP1 (Inhibitor)MRP2 (Inhibitor)MRP3 (Inhibitor)MRP4 (Inhibitor)NTCP (Inhibitor)OAT1 (Inhibitor)OAT3 (Inhibitor)OATP1B1 (Inhibitor)OATP1B1 (Inhibitor)OATP1B3 (Inhibitor)OATP1B3 (Inhibitor)OATP2B1 (Inhibitor)OCT1 (Inhibitor)P-gp (Inhibitor)MDR1 (Substrate)OATP1B3 (Substrate)P-gp (Substrate)

Drug–drug interactions (100+, DDInter)

Interacting drug	Severity	Management
Abciximab	major
Acalabrutinib	major
Acetylsalicylic acid	major
Alteplase	major
Amiodarone	major
Amobarbital	major
Anistreplase	major
Apixaban	major
Ardeparin	major
Argatroban	major
Avapritinib	major
Betrixaban	major
Bivalirudin	major
Bromfenac	major
Butabarbital	major
Butalbital	major
Cabozantinib	major
Cangrelor	major
Capecitabine	major
Caplacizumab	major
Cinoxacin	major
Ciprofloxacin	major
Clarithromycin	major
Clofibrate	major
Clopidogrel	major
Dalteparin	major
Danaparoid	major
Danazol	major
Dasatinib	major
Deferasirox	major
Defibrotide	major
Desirudin	major
Diclofenac	major
Dicloxacillin	major
Diflunisal	major
Drotrecogin alfa	major
Edoxaban	major
Enoxacin	major
Enoxaparin	major
Eptifibatide	major

Showing 40 of 100+.

Registered Products (3)

Brand	Form / strength	Pack	Agent	Citizen (JOD)
ORFARIN	Tablet 3 mg	100 tab	Awtar Pharmaceutical Co	3.240
ORFARIN	Tablet 5 mg	100 tab	Awtar Pharmaceutical Co	4.540
macfarin	Tablet 5 mg	100 tab	Pharma Care Drug Store	4.720