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Kevin Maskell, MD Division of Toxicology VCU Medical Center Virginia Poison Center With slides adapted from B-Wills SHAMELESSLY PILFERED!
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By the end you will know: Mechanism of toxicity Types of ingestion Diagnostic keys Management/Antidotes How not to kill your patient
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Why do we care? Common Deadly We can fix it
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APAP Glucuronidation/ Sulfation Safe MercaptateNAPQI 2E1 GSH Lipid peroxidation Death
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APAP is just APAP right? Acute Repeat supratherapeutic Late presenter
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Stages (acute) 1) Nonspecific NV, malaise (0-24) 2) Hepatic injury (8-36) 3) Fulminant failure (3-4 d) 4) Recovery (weeks?)
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Rumack-Mathew nomogram
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Nomogram When can we use? Extended release? Coingestants?
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..
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Repeat Supratherapeutic APAP ingestion Stratify by Risk High Risk: 1. APAP >10 and AST > normal 2. APAP 2x or symptomatic 3. APAP level > expected for appropriate dose Minimal Risk: APAP <10 + normal AST Low Risk: APAP <10 + AST nml to 2x nml and asymptomatic
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Antidote N-Acetylcysteine NAC is universally effective if given within ___ hours?
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Delay (hrs) in NAC admin vs hepatotoxicity 0 4 8 12 16 20 24(hrs) % 0% 0-8hrs 6% 8-10hrs 26% 10-24hrs 41% 16-24hrs Smilkstein M: NEJM 1988
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N-Acetylcysteine Indications Acute ingestion plotted ______ treatment nomogram Time unknown and APAP level is __________ Non-reassuring repeated supratherapeutic ingestion ( ↑ APAP level and/ or ↑ LFT’s) ED presentation > ___ hours post ingestion above 8 detectable
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IV vs PO NAC? Dosing regimen PO intolerant? Anaphylactoid reactions? Other reasons?
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What if we fail? pH < 7.3 after 12 hrs resuscitation Lactate >3.5 after 4 hrs Cr > 3.4 INR >6.5 Grade 3 or 4 encephalopathy Phosphorus >3.75 at 48 hrs
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Survival Points: APAP 1.Doses > 150-200 mg/kg could be concerning (> 200 mg/kg in peds) 2.Can only plot single acute OD’s on the nomogram 3.Repeated supratherapeutic OD: ND APAP + Nl AST = YOU’re DONE 4.NAC within 8 hrs is ~100% effective (in preventing hepatic failure) 5.Sick patients: refer to King’s College criteria of who might lose their liver 6.IV NAC is 150 mg/kg over 60 minutes 7.Get 2 nd level for co-ingestants with opioids/ diphenhydramine 8.Allergy is likely anaphylactoid rather than anaphylaxis (this means you can can Rx with benadryl and usually restart the infusion with no problems)
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In 8 minutes…ish…
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Why does ASA kill you? ASA ASA - pH low pH high
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Why is pH the key for treatment? Answers: 1. Protects the CNS 2. Enhances ASA elimination Acidic Environment ASA Alkaline Environment ASA ASA - “Ion Trapping”
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Clinical Features Early 1.Tinnitus/ Vertigo 2.Fever 3.N/V/D 4.Hyperpnea Late 1.AMS / Coma 2.Seizures 3.ARDS 4.Death
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Labs ASA level (Q2 hrs) Urine pH (also Q2 if able) Blood gas Chemistry
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Treatment Airway/Breathing: Intubation? Circulation : Fluids, electrolytes Decontamination? Enhanced elimination? Disposition?
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Why is pH the key for treatment? Answers: 1. Protects the CNS 2. Enhances ASA elimination Acidic Environment ASA Alkaline Environment ASA ASA - “Ion Trapping”
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Alkalinization of Urine 1.Urine pH of 7.5-8.0, avoid serum pH >7.60 2.1-2 mEq/kg NaHCO start ggt 3.Correct K+ depletion
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Chronic Salicylism? Old and dwindling with… Gastroenteritis Urosepsis Metabolic acidosis of unknown etiology AMS/ encephalopathy Influenza (ARDS)
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Survival Points: ASA 1.ASA overdose generates M&M’s because its underappreciated 2.Units screw people up; use mg/dl for salicylates 3.Salicylate levels should be obtained Q2h until they peak and start to fall 4.Consider urinary alkalinization for levels > 30 mg/dl (Reasonable infusion is 3 amps in 1L D5W at 2x maintenance) 5.Consider dialysis when levels > 80 mg/dl for acute cases 6.Keep sick patients breathing: allow them to hyperventilate; if you over-sedate or intubate them, you could kill them if you don’t maintain a high minute ventilation 7.Protect the CNS with bicarb 8.Chronic salicylism is more likely to be diagnosed as: old person with gastroenteritis, urosepsis, influenza, or metabolic acidosis of unknown etiology…
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