Digoxin toxicity: Difference between revisions

Latest revision as of 10:25, 22 March 2026

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

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

[1] Smith TW. Digitalis: Mechanisms of action and clinical use. N Engl J Med. 1988;318(6):358-365. PMID 3277052

[1]

@@ Line 1: / Line 1: @@
-== Background ==
+==Background==
-*Mechanism of action
+*Digoxin (digitalis) is a cardiac glycoside used for [[atrial fibrillation]] rate control and [[heart failure]]
-**Positive inotropic effect
+*Narrow therapeutic index (therapeutic level: 0.5-2.0 ng/mL)
-***Inhibits Na-K pump -> incr extracelluar K, incr intracellular Na -> incr intracellular Ca
+*Mechanism of action: inhibits Na/K-ATPase → increased intracellular calcium → increased contractility
-**Increases vagal tone
+*Also increases vagal tone (AV nodal blockade)
-***Can lead to bradyarrhythmias (esp in young)
+*Toxicity occurs from:
-**Increases automaticity
+**Acute ingestion (intentional overdose, accidental)
-***Can lead to tachyarrhythmias (esp in elderly)
+**Chronic accumulation (most common — renal insufficiency, drug interactions, dehydration)
-*Renally cleared
+*Drug interactions that increase digoxin levels:
-*Hemodialysis does not work
+**Amiodarone (increases level by ~50%), verapamil, diltiazem, quinidine
-*Can also be found in nature: Foxglove, Oleander, certain toads
+**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
-=== Risk Factors  ===
+==Clinical Features==
+===GI (Often Earliest)===
+*Nausea, vomiting, anorexia (most common symptoms)
+*Abdominal pain, diarrhea
-#Electrolyte Imbalance
+===Cardiac (Most Dangerous)===
-##[[Hypokalemia|Hyperkalemia]], [[Hypomagnesemia]], [[Hypercalcemia]]
+*Almost ANY dysrhythmia can occur
-#Hypovolemia
+*Classic: increased automaticity + decreased conduction
-#Renal insufficiency
+*Most common arrhythmia: PVCs
-#[[Cardiac Ischemia]]
+*Highly suggestive rhythms:
-#[[Hypothyroidism]]
+**Bidirectional ventricular tachycardia (nearly pathognomonic)<ref>Smith TW. Digitalis: Mechanisms of action and clinical use. N Engl J Med. 1988;318(6):358-365. PMID 3277052</ref>
-#Meds
+**Atrial tachycardia with AV block (PAT with block)
-##CCBs, amiodarone
+**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)
-== Clinical Manifestations ==
+===Neurologic===
-===Cardiac===
+*Visual disturbances: xanthopsia (yellow-green halo vision), blurred vision, photophobia
-#[[Syncope]]
+*Confusion, delirium, weakness, fatigue
-#Dysrhythmias
+*Drowsiness
-##PVCs
-##[[Bradycardia]]
-##SVT w/ AV block
-##Junctional escape
-##Ventricular dysrhythmia, including bidirectional V-tach (esp in chronic toxicity)
-#Digitalis Effect (seen with therapeutic levels; not indicative of toxicity)
-##T wave changes (flattening or inversion)
-##QT interval shortening
-##Scooped ST segments with depression in lateral leads
-##Increased U-wave amplitude
-[[File:Digtox.jpg|center|700px]]
-===GI===
+===Metabolic===
-#Often the earliest manifestation of toxicity
+*Hyperkalemia in acute toxicity (Na/K-ATPase inhibition → K moves extracellularly)
-##[[Nausea/vomiting]]
+**K >5.0 in acute digoxin poisoning is a marker of severe toxicity
-##[[Abdominal Pain]]
+**In chronic toxicity, K is often low (from concurrent diuretic use)
-===Neuro===
+==Differential Diagnosis==
-#[[Confusion]]
+*Other causes of bradycardia with heart block
-#[[Weakness]]
+*[[Beta-blocker]] or [[calcium channel blocker overdose]]
-#Visual disturbances
+*[[Hyperkalemia]]
-##Yellow halos
+*Oleander or foxglove poisoning (contain cardiac glycosides)
-##Scotomas
+*Other causes of bidirectional VT: catecholaminergic polymorphic VT, aconitine
-#Delirium
-==Work-Up==
+==Evaluation==
-#Dig level
+*ECG (look for dysrhythmias, ST changes)
-##Only useful prior to administration of [[Fab]] (otherwise becomes falsely elevated)
+**'''Digitalis effect''' (scooped ST depression, "Salvador Dali mustache") ≠ toxicity
-#Chemistry
+**Digitalis toxicity = arrhythmias
-#Urine output
+*Digoxin level:
-#ECG (serial)
+**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)
-== Diagnosis ==
+==Management==
-#Must use H&P and labs in combination; no single element excludes or confirms the dx
+===Digoxin-Specific Antibody Fragments (DigiFab/Digibind)===
-#Digoxin level
+*Definitive antidote — highly effective
-##Normal = 0.5-2 ng/mL (ideal = 0.7-1.1)
+*Indications for empiric dosing:
-###May have toxicity even with "therapeutic" levels (esp w/ chronic toxicity)
+**'''Life-threatening arrhythmias''' (VT, VF, symptomatic bradycardia, high-grade AV block)
-##Measure at least 6hr after acute ingestion (if stable); immediately for chronic ingestion
+**Hyperkalemia >5.0 mEq/L in acute poisoning
-###If measure before this may be falsely elevated due to incomplete drug distribution
+**Hemodynamic instability
-#Potassium level
+**Digoxin level >10 ng/mL (acute) or >4 ng/mL (chronic) with symptoms
-##Acute toxicity: Degree of [[Hyperkalemia]] correlates w/ degree of toxicity
+*Dosing:
-##Chronic toxicity: K+ may be normal/low (concomitant diuretic use) or high (renal failure)
+**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
-==DDX==
+===Supportive Measures===
-#CCB/BB toxicity
+*Correct hypokalemia to >4.0 mEq/L (in chronic toxicity)
-#Clonidine toxicity
+*Correct hypomagnesemia: magnesium sulfate 2g IV
-#[[Organophosphate Toxicity]]
+*Calcium: CONTROVERSIAL in digoxin toxicity
-#Sick sinus syndrome
+**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
-== Treatment ==
+===What to Avoid===
-'''Calcium is theoretically contradindicated in Dig Toxicity (see [[Stone Heart]])'''
+*No calcium (controversial — may worsen toxicity)
-#'''[[Digoxin Immune Fab]]'''
+*No Class IA antiarrhythmics (procainamide, quinidine — worsen conduction)
-##Indications
+*Minimize cardioversion
-### Ventricular dysrhythmias (ventricular fibrillation, ventricular tachycardia)
+*No beta-blockers (worsen bradycardia/AV block)
-### Symptomatic bradycardias unresponsive to atropine
-### Hyerkalemia >5.0 mEq/L secondary to digitalis intoxicaiton
-### Coningestions of cardiotoxic drugs (beta-blockers, cyclic antidepressants)
-### Acute digoxin ingestion of greater than 10mg in adults or greater than 4mg in children
-### Acute digoxin ingestions with post distribution digoxin >10ng/mL (by 6 hours post ingestion)
-### Chronic digoxin ingestion leading to steady state serum digoxin concentrations of >4ng/ml
-#[[Activated Charcoal]]
+===Refractory Cases===
-##Questionable efficacy
+*Lidocaine (for ventricular arrhythmias not responsive to Digibind)
-##Only an adjunctive tx; NOT an alternative to fab fragment therapy
+*Phenytoin (can improve conduction through AV node; historical use)
-##Consider only if present within 1 hr of ingestion
+*Temporary pacing for complete heart block refractory to atropine and Digibind
-##1g/kg (max 50g)
+*Consider hemodialysis — does NOT effectively remove digoxin (highly protein/tissue bound) but may help if Digibind unavailable
-===Dysrhythmias===
-#[[Digoxin Immune Fab]] is the agent of choice for all dysrhythmias!
-#[[Cardioversion]] should only be used as a last resort (may precipitate V-Fib)
-##Consider lower energy settings (25-50J)
-#Bradyarrhythmias (symptomatic)
-##[[Atropine]] 0.5mg IV
-##[[Pacing]]
-#Ventricular dysrhythmias
-##[[Dilantin Load|Phenytoin]]
-###Enhances AV conduction
-###Phenytoin: 15-20mg/kg at 50mg/min
-###Fosphenytoin: 15-20mg PE/kg at 100-150mg/min
-##[[Lidocaine]]
-###Decreases ventricular automaticity
-###1-3mg/kg over several minutes; follow by 1-4mg/min
-##[[Magnesium]]
-###Many patients have [[Hypomagnesemia]] and labs can be unreliable.
-###2-4 g IV over 20-60 mins
-===[[Hyperkalemia]]===
-#Treat with [[Fab]], not with usual meds
-##Once Fab is given hyperkalemia will rapidly correct
-#If [[Fab]] unavailable and hyperkalemia is life-threatening then treat with:
-##Glucose-insulin
-##Sodium bicarb
-##Kayexelate
-##Dialysis
-##Calcium (controversial: some say dangerous, others say not)
-===[[Hypokalemia]]===
-#Chronic intoxication
-##Raise level to 3.5-4
-#Acute intoxication
-##Do not treat (likely that potassium level is rapidly rising)
-===[[Hypomagnesemia]]===
-#Treat with 1-2g over 10-20 min
-##Monitor for resp depresion
-##Avoid in pts with:
-###Renal failure
-###Bradydysrhythmias/conduction blocks
 ==Disposition==
-*Admit for signs of toxicity or history of large ingested dose; admit to ICU if [[Fab]] given
+*Admit all symptomatic patients to monitored bed or ICU
-*Discharge after 12hr observation if asymptomatic after accidental overdose
+*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==
-*[[Digoxin Immune Fab]]
+*[[Toxicology]]
-*[[Toxidromes]]
+*[[Atrial fibrillation]]
-*[[Digoxin]]
+*[[Heart failure]]
+*[[Hyperkalemia]]
+*[[Cardiac arrest]]
+*[[Beta-blocker toxicity]]
+*[[Calcium channel blocker overdose]]
-== Source ==
+==References==
-*Rosen's
+*Hauptman PJ, Kelly RA. Digitalis. ''Circulation''. 1999;99(9):1265-1270. PMID 10069797
-*Tintinalli
+*Hack JB, Lewin NA. Cardioactive steroids. In: ''Goldfrank's Toxicologic Emergencies''. 10th ed. McGraw-Hill. 2015.
-*ECG image by Dr. James Heilman
+*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
-[[Category:Cards]]
+[[Category:Toxicology]]
-[[Category:Drugs]]
+[[Category:Cardiology]]
-[[Category:Tox]]