Acetaminophen toxicity: Difference between revisions
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==Background==
==Background==
*Recommended maximum total daily dose:
*'''Most common cause of acute liver failure''' in the United States and UK
**Adults: 4gm/day
*Found in >600 OTC and prescription products (Tylenol, Percocet, Vicodin, NyQuil, etc.)
**Peds: 75mg/kg/day  
*Therapeutic dose: 10-15 mg/kg per dose (max 4g/day in adults; 2g/day in chronic alcoholics)
*Toxic dose
*Toxic dose: >150 mg/kg (single ingestion) or > 7.5 g total in adults
**>10gm or >200mg/kg as single ingestion or over 24hr period OR
*Mechanism:
**>6gm or >150mg/kg per 24hr period x2d
**Normal metabolism: 90% glucuronidation/sulfation → nontoxic → renally excreted
*Peak serum levels seen within 2hr
**~5% oxidized by CYP2E1 → NAPQI (toxic metabolite) → detoxified by glutathione
===The 150 Rule ===
**In overdose: glucuronidation/sulfation saturated → excess NAPQI production → glutathione depletion → hepatocellular necrosis
*Toxic dose is 150 mg/kg
*N-acetylcysteine (NAC) is a glutathione precursor and is nearly 100% effective when given within 8 hours of ingestion<ref>Smilkstein MJ, et al. Efficacy of oral N-acetylcysteine in the treatment of acetaminophen overdose. ''N Engl J Med''. 1988;319(24):1557-1562. PMID 3059186</ref>
*Give NAC if level is >150 mcg/mL four hours post-ingestion
*Initial loading dose of NAC is 150 mg/kg IV (140mg/kg PO)


==Pharmacology==
===Risk Factors for Enhanced Toxicity===
===Mechanism of action===
*Chronic alcohol use (CYP2E1 induction + depleted glutathione stores)
*Poorly understood
*Fasting / malnutrition (depleted glutathione)
*Possibly through inhibition of Cyclooxygenase-3 (COX-3)
*CYP2E1 inducers: isoniazid, phenobarbital, carbamazepine, rifampin
**Decreases synthesis of prostaglandins
*Lower threshold for treatment in these patients
*Antipyresis through inhibition of hypothalamic heat center
===Pharmacokinetics===
*A - Rapid and near complete absorption
*D - Vd = 0.95 L/kg
*M - T 1/2 = 1.5-2hrs
**40-60% - Glucuronidation
**20-40% - Sulfuronidation
**5-10% - Metabolism through CYP450 '''(Forms NAPQI)'''<ref>Hendrickson RG, Bizovi KE. Acetaminophen. In: Flomenbaum NE, Goldfrank LR, Hoffman RS, et al, eds. Goldfrank’s Toxicologic Emergencies. 8th ed. New York: McGraw-Hill; 2002:523-543. (Textbook chapter)</ref>
*E - Conjugated and unconjugated excreted through kidneys


== Toxicology ==
==Clinical Features==
=== Pathophysiology ===
===Four Stages of Toxicity===
*APAP toxic metabolite NAPQI usually quickly detoxified by glutathione stores in liver
*Stage 1 (0-24h): Often asymptomatic or nonspecific (nausea, vomiting, anorexia, diaphoresis)
**In overdose, glutathione runs out, NAPQI accumulates -> liver injury
*Stage 2 (24-72h): RUQ pain, elevated transaminases, rising INR; may appear to improve clinically
*NAC increases availability of glutathione
*Stage 3 (72-96h): Peak hepatotoxicity — markedly elevated AST/ALT (can exceed 10,000), coagulopathy, [[jaundice]], [[acute kidney injury]], [[hepatic encephalopathy]]
**NAC is a precursor
**Fulminant hepatic failure: [[cerebral edema]], [[DIC]], [[multi-organ failure]], death
*Stage 4 (4-14 days): Recovery phase in survivors (hepatocytes regenerate)


=== Clinical Features ===
===Chronic/Repeated Supratherapeutic Ingestion===
#Stage 1 (first 24hr)
*More common than acute overdose in clinical practice
##Mild N/V/malaise
*Presents with hepatotoxicity without early Stage 1 symptoms
##Hypokalemia (a/w high 4-hr level)
*Rumack-Matthew nomogram does NOT apply
#Stage 2 (days 2-3)
*Treat based on APAP level + ALT elevation
##Improvement in symptoms
##RUQ abd pain
##Elevated transaminases
##Elevated bilirubin, PT (if severe)
#Stage 3 (days 3-4)
##Recurrence of N/V
##Hepatic failure
##Jaundice
##Coagulopathy
##Encephalopathy (esp w/ massive ingestions)
##Renal failure (1-2%; usually after hepatic failure is evident)
##Pancreatitis (rare)
#Stage 4 (after day 5)
##Clinical improvement and recovery (7-8d) OR
##Deterioration to multi-organ failure and death OR
##Continued deterioration


== Work-Up ==
==Differential Diagnosis==
#APAP level
*[[Viral hepatitis]]
#Chemistry
*Alcoholic hepatitis
##Metabolic acidos seen w/ extremely large ingestion
*Other drug-induced hepatitis
#LFT
*[[Ischemic hepatitis]] (shock liver)
#PT/PTT/INR
*[[Wilson disease]] (acute presentation)
#Acetaminophen level: 4 hours post ingestion and repeat in 4 hours
*Amanita phalloides (mushroom) poisoning
#ASA levels and other co-ingestants
*[[Salicylate toxicity]]
*Other ingestions causing liver failure


==Diagnosis==
==Evaluation==
#APAP level
*'''Serum APAP level''': draw at '''4 hours post-ingestion''' (or immediately if >4 hours)
##Obtain 4hrs post-ingestion
**Plot on Rumack-Matthew nomogram at time since ingestion
##Obtaining multiple levels is rarely indicated in the absence of hepatotoxicity
**Treatment line: starts at 150 mcg/mL at 4 hours (US uses this; original line at 200)
#Nomogram (see below)
**Below treatment line = low risk; above = treat with NAC
##Only indicated for single, acute ingestion occurring <24hr prior to presentation
*AST/ALT: may be normal initially; any elevation warrants NAC
*INR/PT: coagulopathy = hepatic failure; INR is the best prognostic marker
*BMP: creatinine (renal injury occurs in ~25% of severe cases), bicarbonate, glucose
*Lipase, bilirubin, CBC
*Salicylate level (coingestion screening)
*Lactate: elevated lactate = poor prognosis
*VBG/ABG: pH <7.30 after resuscitation = poor prognosis


===King's College Criteria (Liver Transplant Referral)===
*Acetaminophen-induced ALF:
**pH <7.30 after adequate fluid resuscitation (regardless of grade of encephalopathy) OR
**All three: INR >6.5, creatinine >3.4 mg/dL, and Grade III-IV hepatic encephalopathy
*Consider early transfer to a liver transplant center


===Rumack-Matthew Nomogram===
==Management==
[[File:APAP_nomogram.jpg]]
===GI Decontamination===
*<big><big>'''Not useful for chronic ingestion (patients who take supratherapeutic doses for several days) or if time of ingestion is unknown'''</big></big>
*Activated charcoal 1 g/kg (max 50g) if within 1-2 hours of ingestion and patient is alert with protected airway
*'''Make sure you use the correct units!'''
*May benefit up to 4 hours post-ingestion
*Do NOT delay NAC for charcoal


==Treatment==
===N-Acetylcysteine (NAC) — The Antidote===
*'''Very important to identify time of ingestion'''
*Give NAC if:
===<4hr after ingestion===
**APAP level above treatment line on Rumack-Matthew nomogram
#GI decontamination
**Time of ingestion unknown and APAP level detectable
##[[Activated Charcoal]] if <3 hr post-ingestion (no role for multidose activated charcoal)
**Elevated transaminases with history of APAP ingestion
##[[Gastric Lavage]] if high-morbidity coingestants and <1 hr post-ingestion
**Ingestion of > 150 mg/kg and level will not be available within 8 hours
#Send 4hr APAP level
**Any doubt → give NAC (minimal side effects, potentially life-saving)
##Toxic level: Give NAC
##Nontoxic level: No treatment necessary
===Between 4-24hr after ingestion===
#Send APAP level
##If level will be available within 8hr post-ingestion: wait for level before treating
##If level will not be available within 8hr post-ingestion: do not wait for level before treating
###Discontinue treatment if level returns non-toxic
===Unknown or >24hr after ingestion===
#Consider GI decontamination for unknown ingestion time
#Give 1st dose of NAC
#Send APAP level, LFT, coags
##APAP level >10 OR elevated transaminases? If yes then continue NAC
###pH <7.3 or PT >100 or Cr >3.3 or AMS? If yes refer to liver transplant unit
##APAP level and LFT both normal? If yes then stop NAC (treatment not indicated)
===Extended release overdose===
*Extended-release acetaminophen (Tylenol ER) consists of acetaminophen 325 mg in immediate release (IR) form surrounding a matrix of acetaminophen 325 mg
**Several studies show that the elimination of ER and IR APAP preparations is nearly identical after 4 hours. However, some case reports have documented APAP levels that are above the potential toxicity and treatment line on the nomogram as late as 11-14 hours after the ingestion of the ER preparation.
**Recommended management includes the measurement of 4-, 6-, and 8-hour APAP concentrations. Begin NAC therapy if any level crosses above the nomogram treatment line. If the 6-hour level is greater than the 4-hour level, begin NAC therapy.


==N-acetylcysteine (NAC)==
====IV NAC Protocol (21-hour Protocol — Preferred)====
===Background===
*Loading dose: 150 mg/kg IV in 200 mL D5W over 60 minutes (or 15 minutes if used to be over 15 min)
#Almost 100% effective if given <8 hr post-ingestion; less effective if 16-24 hr post-ingestion
*Second infusion: 50 mg/kg IV in 500 mL D5W over 4 hours
#May still be useful >24 hr post-ingestion, even with fulminant hepatic failure. Give NAC until LFTs improve (not until APAP level is 0) <ref>Keays R, Harrison PM, Wendon JA, et al. Intravenous acetylcysteine in paracetamol-induced fulminant hepatic failure: a prospective controlled trial. BMJ. 1991;303(6809):1026-1029. (Prospective randomized controlled trial; 50 patients)</ref> <ref>Harrison PM, Keays R, Bray GP, et al. Improved outcome of paracetamol-induced fulminant hepatic failure by late administration of N-acetylcysteine. Lancet. 1990;335(8705):1572- 1573. (Retrospective analysis; 100 patients)</ref>
*Third infusion: 100 mg/kg IV in 1000 mL D5W over 16 hours
*Total: 300 mg/kg over 21 hours
*Anaphylactoid reactions (flushing, urticaria, bronchospasm) most common during loading dose
**Slow or pause infusion; treat with antihistamines/bronchodilators; '''do not stop NAC permanently'''


===Dosing:===
====Oral NAC Protocol (72-hour)====
====PO====
*Loading dose: 140 mg/kg PO
#140mg/kg PO load
*Maintenance: 70 mg/kg PO every 4 hours × 17 additional doses
#70mg/kg PO q4hr x17 doses additional; dilute to 5% soln
*Total: 1,330 mg/kg over 72 hours
*Mixed with cola or juice to improve palatability
*If patient vomits within 1 hour of dose, repeat the dose


;Side Effects: sulfur-smell causes nausea and vomiting. Consider mixing with juice or soda, in a cup with a lid and straw
====Two-Bag Modified Prescott Protocol====
*Some centers use a simplified 2-bag protocol: 200 mg/kg IV over 4 hours then 100 mg/kg IV over 16 hours
*Lower rate of anaphylactoid reactions<ref>Wong A, et al. Comparison of two- versus three-bag IV acetylcysteine protocols. ''Clin Toxicol''. 2013;51(7):676-679.</ref>


====IV====
===When to Stop NAC===
#Loading dose: 150mg/kg in 100 mL D5W over 60min
*APAP level undetectable, AST/ALT normalizing/improving, INR ≤1.3, clinically well
#Second (maintenance) dose: 50mg/kg in 250 mL D5W over 4hr
*If AST/ALT still elevated or INR elevated: continue NAC beyond standard protocol
#Third dose: 100mg/kg in 500 mL D5W over 16hr


;Side Effects: Anaphylactoid reaction but also associated with seizures, cerebral edema, & herniation. <ref>http://journals.lww.com/em-news/Fulltext/2012/02000/Toxicology_Rounds__Lessons_from_the_Courtroom_.9.aspx</ref>
===Fulminant Hepatic Failure===
*Continue IV NAC indefinitely (has benefit even in established liver failure)
*Contact liver transplant center early
*Manage: coagulopathy (FFP only if active bleeding), [[cerebral edema]] (elevate HOB, hypertonic saline, mannitol), [[hypoglycemia]], [[infection]], [[electrolyte imbalances]]


== King's College Criteria ==
==Disposition==
* criteria for predicting fulminant hepatic failure, and thus referral to transplant center
*'''Admit''' if NAC initiated, elevated transaminases, or altered mental status
* PPV 70-90% and sensitivity 69%
*ICU for evidence of liver failure (coagulopathy, encephalopathy, acidosis, renal failure)
* includes:
*Consider discharge if:
# pH<7.3 or lactate>3 at 12hrs after full fluid resuscitation, OR all of the following:
**APAP level below treatment line at ≥4 hours post-ingestion
# Cr>3.4
**Normal AST/ALT, INR, creatinine
# INR>6.5
**4-6 hour observation complete
# grade 3 or 4 [[Hepatic Encephalopathy]]
**Psychiatric evaluation for intentional ingestions
*Poison control: 1-800-222-1222


* other predictors of APAP-induced hepatic failure include:
==See Also==
# lactate>3.5 4hrs after fluid resusciation
*[[Toxicology]]
# phos>3.8 at 48hrs, OR
*[[Acute liver failure]]
# APACHE II >15
*[[Salicylate toxicity]]
*[[Hepatic encephalopathy]]


== Disposition ==
==References==
* Consider discharge for asymptomatic pts who do not require NAC
<references/>
* Admission if requiring NAC or other ingestions, injuries
*Heard KJ. Acetylcysteine for acetaminophen poisoning. ''N Engl J Med''. 2008;359(3):285-292. PMID 18635433
* Transfer to transplant center based on above criteria
*Rumack BH. Acetaminophen hepatotoxicity: the first 35 years. ''J Toxicol Clin Toxicol''. 2002;40(1):3-20. PMID 11990202
* Psych consult if pt has suicidal ideation
*Chun LJ, et al. Acetaminophen hepatotoxicity and acute liver failure. ''J Clin Gastroenterol''. 2009;43(4):342-349. PMID 19169150


==External Links==
[[Category:Toxicology]]
*[http://www.mdcalc.com/acetaminophen-overdose-and-iv-nac-dosing/ MDCalc - Acetaminophen Overdose & NAC Dosing]
[[Category:GI]]
*[http://www.mdcalc.com/kings-college-criteria-for-acetaminophen-toxicity/ MDCalc - King's College Criteria for Acetaminophen Toxicity]
 
== References ==
<references />
 
[[Category:Tox]]

Latest revision as of 09:29, 22 March 2026

Background

  • Most common cause of acute liver failure in the United States and UK
  • Found in >600 OTC and prescription products (Tylenol, Percocet, Vicodin, NyQuil, etc.)
  • Therapeutic dose: 10-15 mg/kg per dose (max 4g/day in adults; 2g/day in chronic alcoholics)
  • Toxic dose: >150 mg/kg (single ingestion) or > 7.5 g total in adults
  • Mechanism:
    • Normal metabolism: 90% glucuronidation/sulfation → nontoxic → renally excreted
    • ~5% oxidized by CYP2E1 → NAPQI (toxic metabolite) → detoxified by glutathione
    • In overdose: glucuronidation/sulfation saturated → excess NAPQI production → glutathione depletion → hepatocellular necrosis
  • N-acetylcysteine (NAC) is a glutathione precursor and is nearly 100% effective when given within 8 hours of ingestion[1]

Risk Factors for Enhanced Toxicity

  • Chronic alcohol use (CYP2E1 induction + depleted glutathione stores)
  • Fasting / malnutrition (depleted glutathione)
  • CYP2E1 inducers: isoniazid, phenobarbital, carbamazepine, rifampin
  • Lower threshold for treatment in these patients

Clinical Features

Four Stages of Toxicity

  • Stage 1 (0-24h): Often asymptomatic or nonspecific (nausea, vomiting, anorexia, diaphoresis)
  • Stage 2 (24-72h): RUQ pain, elevated transaminases, rising INR; may appear to improve clinically
  • Stage 3 (72-96h): Peak hepatotoxicity — markedly elevated AST/ALT (can exceed 10,000), coagulopathy, jaundice, acute kidney injury, hepatic encephalopathy
  • Stage 4 (4-14 days): Recovery phase in survivors (hepatocytes regenerate)

Chronic/Repeated Supratherapeutic Ingestion

  • More common than acute overdose in clinical practice
  • Presents with hepatotoxicity without early Stage 1 symptoms
  • Rumack-Matthew nomogram does NOT apply
  • Treat based on APAP level + ALT elevation

Differential Diagnosis

Evaluation

  • Serum APAP level: draw at 4 hours post-ingestion (or immediately if >4 hours)
    • Plot on Rumack-Matthew nomogram at time since ingestion
    • Treatment line: starts at 150 mcg/mL at 4 hours (US uses this; original line at 200)
    • Below treatment line = low risk; above = treat with NAC
  • AST/ALT: may be normal initially; any elevation warrants NAC
  • INR/PT: coagulopathy = hepatic failure; INR is the best prognostic marker
  • BMP: creatinine (renal injury occurs in ~25% of severe cases), bicarbonate, glucose
  • Lipase, bilirubin, CBC
  • Salicylate level (coingestion screening)
  • Lactate: elevated lactate = poor prognosis
  • VBG/ABG: pH <7.30 after resuscitation = poor prognosis

King's College Criteria (Liver Transplant Referral)

  • Acetaminophen-induced ALF:
    • pH <7.30 after adequate fluid resuscitation (regardless of grade of encephalopathy) OR
    • All three: INR >6.5, creatinine >3.4 mg/dL, and Grade III-IV hepatic encephalopathy
  • Consider early transfer to a liver transplant center

Management

GI Decontamination

  • Activated charcoal 1 g/kg (max 50g) if within 1-2 hours of ingestion and patient is alert with protected airway
  • May benefit up to 4 hours post-ingestion
  • Do NOT delay NAC for charcoal

N-Acetylcysteine (NAC) — The Antidote

  • Give NAC if:
    • APAP level above treatment line on Rumack-Matthew nomogram
    • Time of ingestion unknown and APAP level detectable
    • Elevated transaminases with history of APAP ingestion
    • Ingestion of > 150 mg/kg and level will not be available within 8 hours
    • Any doubt → give NAC (minimal side effects, potentially life-saving)

IV NAC Protocol (21-hour Protocol — Preferred)

  • Loading dose: 150 mg/kg IV in 200 mL D5W over 60 minutes (or 15 minutes if used to be over 15 min)
  • Second infusion: 50 mg/kg IV in 500 mL D5W over 4 hours
  • Third infusion: 100 mg/kg IV in 1000 mL D5W over 16 hours
  • Total: 300 mg/kg over 21 hours
  • Anaphylactoid reactions (flushing, urticaria, bronchospasm) most common during loading dose
    • Slow or pause infusion; treat with antihistamines/bronchodilators; do not stop NAC permanently

Oral NAC Protocol (72-hour)

  • Loading dose: 140 mg/kg PO
  • Maintenance: 70 mg/kg PO every 4 hours × 17 additional doses
  • Total: 1,330 mg/kg over 72 hours
  • Mixed with cola or juice to improve palatability
  • If patient vomits within 1 hour of dose, repeat the dose

Two-Bag Modified Prescott Protocol

  • Some centers use a simplified 2-bag protocol: 200 mg/kg IV over 4 hours then 100 mg/kg IV over 16 hours
  • Lower rate of anaphylactoid reactions[2]

When to Stop NAC

  • APAP level undetectable, AST/ALT normalizing/improving, INR ≤1.3, clinically well
  • If AST/ALT still elevated or INR elevated: continue NAC beyond standard protocol

Fulminant Hepatic Failure

Disposition

  • Admit if NAC initiated, elevated transaminases, or altered mental status
  • ICU for evidence of liver failure (coagulopathy, encephalopathy, acidosis, renal failure)
  • Consider discharge if:
    • APAP level below treatment line at ≥4 hours post-ingestion
    • Normal AST/ALT, INR, creatinine
    • 4-6 hour observation complete
    • Psychiatric evaluation for intentional ingestions
  • Poison control: 1-800-222-1222

See Also

References

  1. Smilkstein MJ, et al. Efficacy of oral N-acetylcysteine in the treatment of acetaminophen overdose. N Engl J Med. 1988;319(24):1557-1562. PMID 3059186
  2. Wong A, et al. Comparison of two- versus three-bag IV acetylcysteine protocols. Clin Toxicol. 2013;51(7):676-679.
  • Heard KJ. Acetylcysteine for acetaminophen poisoning. N Engl J Med. 2008;359(3):285-292. PMID 18635433
  • Rumack BH. Acetaminophen hepatotoxicity: the first 35 years. J Toxicol Clin Toxicol. 2002;40(1):3-20. PMID 11990202
  • Chun LJ, et al. Acetaminophen hepatotoxicity and acute liver failure. J Clin Gastroenterol. 2009;43(4):342-349. PMID 19169150
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