Rosen & Barkin's 5-Minute Emergency Medicine Consult (619 page)

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Authors: Jeffrey J. Schaider,Adam Z. Barkin,Roger M. Barkin,Philip Shayne,Richard E. Wolfe,Stephen R. Hayden,Peter Rosen

Tags: #Medical, #Emergency Medicine

BOOK: Rosen & Barkin's 5-Minute Emergency Medicine Consult
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DESCRIPTION
  • Reversible clinicopathologic syndrome of unknown etiology
  • Primary mitochondrial injury
  • Decreased enzyme activity:
    • Krebs cycle
    • Gluconeogenesis
    • Urea biosynthesis
  • Fatty infiltration:
    • Liver:
      • Hyperammonemia due to decreased conversion from ammonia to urea
      • Hepatorenal syndrome may be the end result.
      • Rapid recovery of liver function in survivors
    • Brain:
      • Encephalopathy of unclear etiology
      • Cytotoxic edema
      • Deteriorating level of consciousness reflects increasing intracranial pressure (ICP).
      • Herniation is the most common cause of death.
      • Normal recovery of neurologic function in survivors
    • Skeletal and myocardial muscle
    • Fatty infiltration and distorted mitochondria
  • <10% of cases occur before the age of 1 yr:
    • Average age is 7 yr
    • Peak age is 4–11 yr
    • Extremely rare in age >18 yr.
  • Regional differences:
    • Highest incidence in the Midwestern states
    • Lower incidence in the states of the Southeast and far West
  • More common in whites than in blacks
  • Peak incidence in winter and early spring
  • Reye-like syndrome:
    • Describes conditions resulting in defects in urea and fatty acid metabolism, toxicologic injury, and impaired gluconeogenesis
ETIOLOGY
  • Not known with certainty
  • Multifactorial causes have been epidemiologically implicated:
    • Antecedent viral syndrome
    • Influenza A or B
    • Varicella
    • Diarrhea illness
    • Genetic predisposition
    • Exposure to salicylates
    • Other undefined factors
DIAGNOSIS
SIGNS AND SYMPTOMS
  • Usually the patient is afebrile.
  • Tachycardia
  • Hyperventilation
History
  • Biphasic history marked by an infectious phase (viral illness or prodrome) followed by an encephalopathic stage
  • Profuse and repeated vomiting:
    • Typically 4–5 days after the start of the viral illness
  • Marked behavioral changes, including delirium and combativeness, disorientation, and hallucination
Physical-Exam
  • No focal neurologic signs
  • Hepatomegaly in 40% of cases
  • Pancreatitis
  • Clinical staging of Reye syndrome with Lovejoy classification:
    • Stage 0:
      • Wakeful
    • Stage I:
      • Vomiting
      • Lethargy
      • Sleepiness
    • Stage II:
      • Disorientation
      • Delirium
      • Combative/stuporous
      • Hyperventilation
      • Hyperreflexia
      • Appropriate response to noxious stimuli
    • Stage III:
      • Obtunded
      • Coma
      • Hyperventilation
      • Inappropriate response to noxious stimuli
      • Decorticate posturing
      • Preservation of pupillary light reflexes
      • Preservation of oculovestibular light reflexes
    • Stage IV:
      • Deeper coma
      • Decerebrate rigidity
      • Loss of oculovestibular reflexes
      • Dilated, fixed pupils
      • Disconjugate eye movements in response to caloric stimulation
    • Stage V:
      • Seizures
      • Absent deep tendon reflexes
      • Respiratory arrest
      • Flaccid paralysis
      • No papillary response
  • Infants: Atypical presentation:
    • Tachypnea
    • Apnea
    • Irritability
    • Seizures
    • Hypoglycemia
ESSENTIAL WORKUP
  • Establish the presence of encephalopathy and liver abnormalities.
  • Lab testing to assess for characteristic biochemical abnormalities
  • Liver biopsy confirms the diagnosis.
DIAGNOSIS TESTS & NTERPRETATION
Lab
  • Liver function tests:
    • ≥3× rise in aspartate aminotransferase, alanine aminotransferase
    • Serum ammonia level >1.5–3× normal:
      • Transient 24–48 hr after mental status changes
      • Level >300 μg/dL is associated with poor prognosis.
    • Serum bilirubin should be normal or slightly elevated.
  • Hypoglycemia may be present, especially in infants.
  • Elevated BUN
  • Ketonuria
  • The prothrombin time may be prolonged due to decreased liver-dependent clotting factors (II, VII, IX, X).
  • Normal platelet count and blood smear
  • Negative toxicology screen
Imaging

Head CT scan:

  • May show diffuse cerebral edema
  • Edema is diffuse, and lumbar puncture is not contraindicated.
Diagnostic Procedures/Surgery
  • Lumbar puncture:
    • Perform after head CT
    • Measure opening pressure
    • <8 leukocytes/mm
      3
  • Percutaneous liver biopsy:
    • Useful in patients with atypical presentation (1 yr old, recurrent, familial)
DIFFERENTIAL DIAGNOSIS
  • Inborn errors of metabolism:
    • Disorders of the urea cycle
    • Disorders of fatty acid oxidation
    • Systemic carnitine deficiency
    • Organic acidemias
    • Disorders of the electron transport chain
  • Hypoglycemia
  • Toxin exposure:
    • Toxic encephalopathy without liver dysfunction (Gall syndrome)
    • Lead
    • Hydrocarbons
  • Drug intoxication:
    • Acetaminophen
    • Salicylates
    • Ethanol
  • Infection:
    • Sepsis
    • Meningitis
    • Encephalitis
    • Varicella hepatitis
  • Trauma, head
TREATMENT
PRE HOSPITAL
  • Decreased mental status:
    • Glucose
    • Narcan
  • Coma:
    • Assist respirations with bag-valve mask.
INITIAL STABILIZATION/THERAPY
  • Place on a cardiorespiratory monitor.
  • Supplemental oxygen
  • Rapid-sequence intubation if airway management required
  • Glucose if mental status is altered:
    • 10% glucose solution IV
    • Rate of 2/3 maintenance requirement after dehydration is corrected
    • Follow serum glucose hourly; maintain glucose 125–175 mg/dL.
  • Avoid early overhydration.
ED TREATMENT/PROCEDURES
  • Institute treatment before the liver biopsy.
  • Vitamin K:
    • Indicated if prothrombin time is elevated.
  • Fresh-frozen plasma:
    • To control bleeding
    • To correct a severe coagulopathy
  • Interventions aimed at lowering ICP:
    • Stage III or greater
    • Stage II with serum ammonia >300 μg/L:
      • Intubation using rapid-sequence protocol
      • Hyperventilation
      • Fluid restriction
      • Barbiturate coma
  • Osmotically active agents:
    • Mannitol
    • Furosemide
  • Monitor ICP:
    • Subarachnoid bolt
    • Intraventricular cannula
MEDICATION
  • D
    50
    W: 1–2 mL/kg/dose (0.5–1 g/kg) IV for age >3 yr
  • D
    25
    W: 2–4 mL/kg/dose (0.5–1 mg/kg) IV for age of <3 yr; maintenance infusion 10% dextrose solution at a rate of 2/3 maintenance
  • Fresh-frozen plasma: 10 mL/kg/dose q12–24h IV or PRN
  • Lasix: 1 mg/kg IV
  • Mannitol: 0.25–1 g/kg IV q4–6h
  • Pentobarbital: 3–5 mg/kg IV slowly while monitoring BP; maintenance infusion 1–2 mg/kg/h; maintain level at 2–5 mg/L
  • Vitamin K: 1–2 mg/dose IV slowly (infants and children); 2–10 mg/dose IV (adolescents)
FOLLOW-UP
DISPOSITION
Admission Criteria
  • All children with suspected Reye syndrome should be admitted to the ICU.
  • Hospital capable of ICP monitoring
Discharge Criteria

Hospital discharge criteria are individualized for each case:

  • Mental status and lab values have improved and stabilized.
Issues for Referral

Close follow-up with specialists in gastroenterology (hepatology) and neurology

FOLLOW-UP RECOMMENDATIONS

Long-term psychological and neuropsychological testing

PEARLS AND PITFALLS
  • Aspirin and salicylates are found in many medications and combination products.
  • All efforts must be directed at identifying other possible causes of illness in the patient with suspected Reye syndrome.
  • Monitoring and control of intracranial pressure is a key component of treatment.
ADDITIONAL READING

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