Digoxin toxicity
(Redirected from Digoxen Toxicity)
Background
- Digoxin (digitalis) is a cardiac glycoside used for atrial fibrillation rate control and heart failure
- Narrow therapeutic index (therapeutic level: 0.5-2.0 ng/mL)
- Mechanism of action: inhibits Na/K-ATPase → increased intracellular calcium → increased contractility
- Also increases vagal tone (AV nodal blockade)
- Toxicity occurs from:
- Acute ingestion (intentional overdose, accidental)
- Chronic accumulation (most common — renal insufficiency, drug interactions, dehydration)
- Drug interactions that increase digoxin levels:
- Amiodarone (increases level by ~50%), verapamil, diltiazem, quinidine
- Macrolide antibiotics (erythromycin, clarithromycin)
- Cyclosporine, itraconazole
- Conditions that increase sensitivity to digoxin:
- Hypokalemia (most important — K and digoxin compete for same binding site)
- Hypomagnesemia, hypercalcemia, hypothyroidism, renal failure
- Mortality without antidote: up to 20-30% in significant poisoning
Clinical Features
GI (Often Earliest)
- Nausea, vomiting, anorexia (most common symptoms)
- Abdominal pain, diarrhea
Cardiac (Most Dangerous)
- Almost ANY dysrhythmia can occur
- Classic: increased automaticity + decreased conduction
- Most common arrhythmia: PVCs
- Highly suggestive rhythms:
- Bidirectional ventricular tachycardia (nearly pathognomonic)[1]
- Atrial tachycardia with AV block (PAT with block)
- Accelerated junctional rhythm
- Regularized atrial fibrillation (AF with complete heart block + junctional escape)
- Sinus bradycardia, AV block (1st, 2nd, 3rd degree)
- Ventricular fibrillation / asystole (in severe toxicity)
Neurologic
- Visual disturbances: xanthopsia (yellow-green halo vision), blurred vision, photophobia
- Confusion, delirium, weakness, fatigue
- Drowsiness
Metabolic
- Hyperkalemia in acute toxicity (Na/K-ATPase inhibition → K moves extracellularly)
- K >5.0 in acute digoxin poisoning is a marker of severe toxicity
- In chronic toxicity, K is often low (from concurrent diuretic use)
Differential Diagnosis
- Other causes of bradycardia with heart block
- Beta-blocker or calcium channel blocker overdose
- Hyperkalemia
- Oleander or foxglove poisoning (contain cardiac glycosides)
- Other causes of bidirectional VT: catecholaminergic polymorphic VT, aconitine
Evaluation
- ECG (look for dysrhythmias, ST changes)
- Digitalis effect (scooped ST depression, "Salvador Dali mustache") ≠ toxicity
- Digitalis toxicity = arrhythmias
- Digoxin level:
- Therapeutic: 0.5-2.0 ng/mL
- Draw level ≥6 hours after last dose (allows tissue distribution)
- Level >2.0 suggests toxicity but clinical correlation is essential
- Level may be falsely elevated after Digibind (measures bound + unbound)
- BMP: potassium (critical — hypokalemia worsens toxicity), creatinine, magnesium, calcium
- Magnesium level (hypomagnesemia increases digoxin sensitivity)
Management
Digoxin-Specific Antibody Fragments (DigiFab/Digibind)
- Definitive antidote — highly effective
- Indications for empiric dosing:
- Life-threatening arrhythmias (VT, VF, symptomatic bradycardia, high-grade AV block)
- Hyperkalemia >5.0 mEq/L in acute poisoning
- Hemodynamic instability
- Digoxin level >10 ng/mL (acute) or >4 ng/mL (chronic) with symptoms
- Dosing:
- If amount ingested known: # vials = (body load in mg × 0.8) / 0.5
- If level known: # vials = (level ng/mL × weight kg) / 100
- Empiric dosing: 10-20 vials for acute life-threatening toxicity; 3-6 vials for chronic toxicity
- Onset: 30-60 minutes
- Each vial binds ~0.5 mg digoxin
- Post-Digibind: total digoxin level rises (bound to antibody) but free digoxin decreases
Supportive Measures
- Correct hypokalemia to >4.0 mEq/L (in chronic toxicity)
- Correct hypomagnesemia: magnesium sulfate 2g IV
- Calcium: CONTROVERSIAL in digoxin toxicity
- Traditional teaching: avoid calcium (risk of "stone heart")
- Recent evidence suggests risk may be overstated, but use with extreme caution
- If hyperkalemic arrest, may give calcium but administer Digibind simultaneously
- Atropine for symptomatic bradycardia: 0.5-1 mg IV (may repeat)
- Activated charcoal if acute ingestion within 1-2 hours and protected airway
- Avoid electrical cardioversion if possible (may precipitate VF in digitalis toxicity)
- If cardioversion unavoidable: use lowest effective energy
What to Avoid
- No calcium (controversial — may worsen toxicity)
- No Class IA antiarrhythmics (procainamide, quinidine — worsen conduction)
- Minimize cardioversion
- No beta-blockers (worsen bradycardia/AV block)
Refractory Cases
- Lidocaine (for ventricular arrhythmias not responsive to Digibind)
- Phenytoin (can improve conduction through AV node; historical use)
- Temporary pacing for complete heart block refractory to atropine and Digibind
- Consider hemodialysis — does NOT effectively remove digoxin (highly protein/tissue bound) but may help if Digibind unavailable
Disposition
- Admit all symptomatic patients to monitored bed or ICU
- ICU for arrhythmias, hemodynamic instability, or Digibind administration
- Continuous telemetry for minimum 12-24 hours
- Serial digoxin levels are NOT useful post-Digibind (measures total, not free)
- Poison control: 1-800-222-1222
See Also
- Toxicology
- Atrial fibrillation
- Heart failure
- Hyperkalemia
- Cardiac arrest
- Beta-blocker toxicity
- Calcium channel blocker overdose
References
- Hauptman PJ, Kelly RA. Digitalis. Circulation. 1999;99(9):1265-1270. PMID 10069797
- Hack JB, Lewin NA. Cardioactive steroids. In: Goldfrank's Toxicologic Emergencies. 10th ed. McGraw-Hill. 2015.
- Chan BS, Buckley NA. Digoxin-specific antibody fragments in the treatment of digoxin toxicity. Clin Toxicol. 2014;52(8):824-836. PMID 25089630
- Levine M, et al. The effects of intravenous calcium in patients with digoxin toxicity. J Emerg Med. 2011;40(1):41-46. PMID 18814997
- ↑ Smith TW. Digitalis: Mechanisms of action and clinical use. N Engl J Med. 1988;318(6):358-365. PMID 3277052