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Digoxin

    DEA Class; Rx

    Common Brand Names; Lanoxin

    • Antidysrhythmics, V; 
    • Inotropic Agents
    Oral and parenteral cardiac glycoside
    Used for CHF and treatment/prophylaxis of supraventricular tachyarrhythmias
    Use in patients with WPW increases the risk of rapid ventricular response

    Indicated for the treatment of heart failure.

    For ventricular rate control in patients with chronic atrial fibrillation and/or atrial flutter; or for the treatment of narrow-complex paroxysmal supraventricular tachycardia (PSVT) or for paroxysmal supraventricular tachycardia (PSVT) prophylaxis in patients without a delta wave on ECG during sinus rhythm.

    Hypersensitivity

    Ventricular fibrillation

    Dizziness (4.9%)

    Mental disturbances (4.1%)

    Diarrhea (3.2%)

    Headache (3.2%)

    Nausea (3.2%)

    Vomiting (1.6%)

    Maculopapular rash (1.6%)

    Anorexia

    Cardiac dysrhythmia

    Arrhythmia in children (consider a toxicity)

    Visual disturbance (blurred or yellow vision)

    Heart block (1°/2°/3°)

    Asystole

    Tachycardia

    Use caution in chronic constrictive pericarditis, electrical cardioversion, severe bradycardia, severe heart failure, severe pulmonary disease, sick sinus syndrome, ventricular tachycardia, ventricular premature contractions, Wolff-Parkinson-White syndrome, electrolyte imbalance, hypothyroidism or hyperthyroidism, hypoxia, idiopathic hypertrophic subaortic stenosis, renal disease, concomitant diuretics

    Not recommended in patients with acute myocardial infarction

    Avoid in patients with myocarditis

    Risk of advanced or complete heart block in patients with sinus node disease and AV block

    Very narrow margin between effective therapeutic and toxic dosages: Therapeutic range, 0.5-2 ng/mL (target 0.5-1 ng/mL); toxic range, >2.5 ng/mL

    Generally avoid if left ventricular systolic function preserved, although may be used for ventricular rate control in subgroup with chronic atrial fibrillation

    Less effective in presence of hypokalemia or hypocalcemia; avoid hypercalcemia or hypomagnesemia, which may predispose to serious arrhythmias

    Heart failure patients with preserved ventricular function, including acute cor pulmonale, amyloid heart disease, and constrictive pericarditis may be susceptible to digoxin toxicity

    May cause false-positive ST-T changes during exercise testing

    Do not switch between different PO forms or between brand and generic forms of digoxin; bioavailability varies

    Serum levels drawn within 6-8 hours of dose will be falsely high because of prolonged distribution phase

    Increased risk of estrogen-like effects in geriatric patients

    Beriberi heart disease may not respond adequately if underlying thiamine deficiency not corrected

    Atrial arrhythmias are difficult to treat if associated with hypermetabolic (hyperthyroidism) or hyperdynamic (hypoxia) states; treat underlying condition before initiating therapy

    Experience with digoxin in pregnant women over several decades, based on published retrospective clinical studies and case reports, has not led to the identification of a drug associated risk of major birth defects, miscarriage or adverse maternal and fetal outcomes

    The digoxin dose received through breastfeeding is up to 4% of the neonatal maintenance dosage, which is unlikely to be clinically relevant

    There are no data on the effects of digoxin on the breastfed infant or the effects on milk production

    Digoxin has a narrow therapeutic index. In all populations, the dosage is individualized based on patient weight, renal function, clinical goals, patient response, and when needed, serum digoxin concentrations.

    Digoxin

    oral solution

    • 0.05mg/mL

    injectable solution

    • 0.1mg/mL
    • 0.25mg/mL

    tablet

    • 0.0625mg (Lanoxin only)
    • 0.125mg
    • 0.1875mg (Lanoxin only)
    • 0.25mg