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Acetaminophen

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Acetaminophen N-acetyl-P-aminophenol (APAP) Paracetamol Overdose -Most common drug taken in overdose -As little as 12g can be fatal (therapeutic dose = 2.6 gm/24 hour ... – PowerPoint PPT presentation

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Title: Acetaminophen


1
Acetaminophen N-acetyl-P-aminophenol (APAP)
2
Paracetamol Overdose
  • -Most common drug taken in overdose
  • -As little as 12g can be fatal (therapeutic dose
    2.6 gm/24 hour)
  • -It is a hepatic and renal toxin (Centrolobular
    necrosis)
  • -More toxic if liver enzymes are induced or with
    reduced ability to conjugate toxin (alcoholics,
    phenytoin, phenobarbitone)
  • -The safety of acetaminophen depends on the
    availability of electron donors such as reduced
    glutathione (GSH) and other thiol-containing
    substances required to detoxify NAPQI.

3
Met pathways of APAP
  • 1- Hepatic glucuronide conjugation(40-65)
    Hepatic
    sulfat conjugation(20 - 45)
  • 90 inactive metabolites excreted in
    the urine.
  • 2- Excretion of unchanged APAP in the urine
    (5).
  • 3- Oxidation by P450 cytochromes to NAPQI
    (5-15)
  • ? GSH combines with NAPQI
  • ? nontoxic cysteine/mercaptate
    conjugates
  • ? excreted in urine.
  • Hepatic glucuronide conjugation(40-65)
  • Hepatic sulfat conjugation(20 - 45)

4
Mechanism of Toxicity
  • The ingested APAP undergo oxidative metabolism by
    CYP- 450 to reactive intermediate metabolite
    (N-acetyl P-benzoquinone imineNAPQI) which is
    rapidly bounded to glutathion ,detoxified
    through conjugation pathway ,and excreted. In the
    presence of adequate GSH stores , there is no
    fear from any toxicity. However, overdose of APAP
    saturate the conjugation pathways and NAPQI
    overwhelms the GSH detoxifi-cation mechanism ,
    finally leading to liver necrosis and may be
    death.

5
Paracetamol Metabolism
6
What happens to APAP metabolism in an OD
situation?
  • 1-Saturation of glucuronidation and sulfation
    pathways
  • 2-Amount of APAP metabolized by p450 cytochromes
    to NAPQI increases.
  • 3-Normally NAPQI is detoxified by reduced GSH
    (glutathione) and thiol containing substances.
  • 4-In OD rate and quantity of NAPQI formation
    overwhelms GSH supply and regeneration
  • ? elimination of NAPQI prolonged
  • ? free NAPQI binds critical intracellular
    proteins with sulfhydryl groups
  • ? cellular dysfunction and cell death.

7
Factors which adversely affect APAP metabolism
  • 1-Upregulation (i.e. induction) of CYP 2E1 enzyme
    activity
  • smoking, barbituates, rifampin, carbamazepine,
    phenytoin, ethanol
  • 2-Decreased glutathione stores (malnutrition)
  • 3-Frequent dosing interval of APAP.
  • 4-Prolonged duration of excessive dosing.

8
GSH stores
  • Glutathione stores are determined by
  • -Age
  • -Diet
  • -Liver disease
  • -Fasting prior ingestion
  • -Chronic malnutrition
  • -Anorexia
  • -Gastroenteritis
  • -Chronic alcoholism
  • -HIV
  • Glutathione replacement by sulfhydryl compounds
  • -Eating
  • -NAC

9
Renal toxicity
  • Organ dysfunction results everywhere where local
    oxidative metabolism (via p450) creates NAPQI
    that cannot be detoxified ? direct toxicity
  • cytochrome P-450 enzymes produce NAPQI in the
    renal tubules ? NAPQI binds cellular
    macromolecules ? acute tubular necrosis.
  • (25 of hepatotoxic cases) Hepatorenal
    Syndrome Volume depletion

10
Other organs damaged
  • Heart ? myocarditis
  • Pancreas ? pancreatitis
  • It is controversial whether these entities are
    part of multisystem organ failure (MSOF) from
    fulminant hepatic failure (FHF) or from the local
    accumulation of toxic metabolites.

11
Clinical presentation
  • Phase 1 (few hrs after ingestion up to 24 hr)
    Malaise , nausea , vomiting and diaphoresis.
  • Phase 2 (24-72 hrs after ingestion) Increase in
    liver enzymes, serum bilirubin , prothrombin time
    , and pain in the right upper abdominal quadrant.
  • Phase 3 (72-96 hrs after ingestion) Peak in the
    liver function, altered consciousness,
    hypoglycemia, jaundice , and coagulation
    abnormalities. Hepatic failure can develops in
    4th or in the 5th day if hepatic damage is sever.
  • Myocardial necrosis, pancreatitis , heamolytic
    anemia and skin rashes may develop but are rare.
  • Phase 4 (7-10 days after ingestion) Liver
    enzymes abnormalities reaching resolution. If
    hepatic damage is massively sever sepsis and
    death may occure at 7-10 days

12
Laboratory analysis
  • 1-Determination of plasma APAP level.
  • 2-Monitoring liver profile including serum ALT,
    AST , bilirubin , glucose , prothrombin time,
    platelet countetc
  • 3- Determination of kideny functions by measuring
    plasma creatinine and BUN.
  • 4-ECG for assessment of myocardial injury.
  • 5- Urine analysis.

13
Management Steps
  • General measures
  • (if the patient is presented to ER within 4 hrs
    of ingestion
  • -Gastric lavage
  • -Activated charcoal ,cathartics (saline sulfate
    are prefered to enhance sulfate metabolic
    pathway).
  • glucose, bicarbonate, Vit K for elevated
    prothrombin time
  • lt8 hours
  • -Take level of APAP after four hours (Peak
    concentration at 4 hrs then hepatic metabolism)
  • -Start N-aceylcysteine (antidote) if APAP
    concentration is high APAP is on or above
    nomogram tx line.
  • -Patients should be advised to return to hospital
    if vomiting or abdominal pain develop or reoccur.

14
Nomogram
15
Management 2
  • gt8 hours
  • Urgent action required because the efficacy of
    NAC declines progressively from 8 hours after the
    overdose
  • Therefore, if gt 150mg/kg or gt 12g (whichever is
    the smaller) has been ingested, start NAC
    immediately, without waiting for the result of
    the plasma paracetamol concentration
  • gt24 hours
  • Still benefit from starting NAC

16
N-acetylcysteine (Antidote)
  • Supplies glutathione precursor (cysteine)
  • Dosage for NAC infusion
  • (1) 150mg/kg IV infusion in 200ml 5 dextrose
    over 15 minutes, then
  • (2) 50mg/kg IV infusion in 500ml 5 dextrose over
    4 hours, then
  • (3) 100mg/kg IV infusion in 1000ml 5 dextrose
    over 16 hours
  • Side-effects
  • Flushing, hypotension, wheezing, anaphylactoid
    reaction
  • -Alternative is methionine PO , it increase GSH
    synthesis.
  • -Hemodialysis and hemoperfusion can be considered
    in extremly elevated APAP level.
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