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Transcript 
ACETAMINOPHEN,
SALICYLATES & NSAID TOXICITY
Amy Gutman MD
[email protected]
COMMON PRESCRIBED
MEDICATIONS & OVERDOSES*
• Opioids
• Sedatives-HypnoticsAntipsychotics
• Cardiovascular drugs
• Antidepressants
• Stimulants
• Acetaminophen
*Intentional & unintentional
WHAT A DIFFERENCE A
DECADE MAKES…
• American Association of Poison Control Centers 2006
• Among analgesics, acetaminophen & salicylate are 40% of
overdose cases
• American Association of Poison Control Centers 2016
• Among analgesics, opiates are 70% of overdose cases
PREVALENCE & UTILIZATION
• Acetaminophen, ibuprofen & aspirin are the most commonly
used analgesic medications among US adults
• In any given week, 23% adults (48 million) use
acetaminophen-containing products, 17% use aspirin, 17%
use ibuprofen, & 4% use naproxen
One-Week Prevalence of Most Commonly Used Analgesic Products in the US Adult Population (n= 209 million); Slone Survey of Medication Use
ACETAMINOPHEN
N–ACETYL–P–AMINOPHENOL (APAP)
• 1st synthesized in 1800’s
• Synthetic non-opiate analgesic
O
H
C
N
• MOI:
• CNS prostaglandin inhibition
• Blocks generation of peripheral pain impulses
• Antipyresis via inhibiting hypothalamic heat
regulation
OH
CH 3
UBIQUITOUS!
Arthritis Foundation Pain Reliever Aspirin Free Aspirin Free Pain Relief Aspirin Free Anacid Maximum
Strength Atasol Atasol Forte Genapap Extra Strength Genebs Extra Strength Caplets Panadol
Panadol Junior Strength Tapanol Extra Strength Tylenol Arthritis Extended Relief Tylenol Caplets
Capsules: Dapacin Meda Cap Aceta Genapap Children's Mapap Children's Oraphen-PD Ridenol
Silapap Children's Tylenol Children's Aspirin Free Anacid Maximum Strength Tapanol Extra Strength
Tylenol Extra Strength Atasol Children's Acetaminophen Elixir Drops Halenol Children's Panadol
Children's Pediatrix Tempra Tempra 2 Syrup Tempra Children's Syrup Tylenol Extra Strength Oral
Solution: Acetaminophen Drops Apacet Atasol Children's Acetaminophen Oral Solution Genapap
Infants' Drops Mapap Infant Drops Panadol Infants' Drops Pediatrix PMS-Acetaminophen Silapap
Infants Tempra 1 Tylenol Infants' Drops Uni-Ace Tylenol Children's Suspension Tylenol Infants'
Suspension Sprinkle Capsules: Feverall Children's Feverall Junior Strength Suppositories: Abenol 120,
325, 650 mg Acephen Acetaminophen Uniserts Children's Feverall Infant's Feverall Junior Strength
Feverall Neopap Aceta A.F. Anacin A.F. Anacin Extra Strength Apo-Acetaminophen Aspirin Free
Pain Relief Aspirin Free Anacin Maximum Strength Atasol
Atasol Forte
Extra Strength
Acetaminophen Fem-Etts Genapap Genapap Extra Strength Genebs Genebs Extra Strength Mapap
Regular Strength Mapap Extra Strength Maranox Meda Tab Panadol Redutemp Regular Strength
Acetaminophen Tapanol Regular Strength Tapanol Extra Strength Tempra Tylenol Regular Strength
Tylenol Extra Strength Tylenol Junior Strength Tylenol Tablets 325 mg, 500 mg Tablets, Chewable:
Apacet Children's Chewable Acetaminophen Children's Genapap Children's Panadol Children's
Tylenol Tempra Tempra 3 Tylenol Chewable Tablets Fruit Tylenol Junior Strength Chewable Tablets
Fruit Acetaminophen, buffered (Bromo Seltzer)
APAP METABOLISM
• Rapidly absorbed from GIT
• Primarily small intestine
• Peak serum concentrations
2 hours post-ingestion
• With acute OD, peak serum
concentration at 4 hours
• Coingestants delaying gastric
emptying, or extendedrelease APAP increases time
to peak serum concentrations
APAP METABOLISM
• 90-95% in liver
• Primary metabolic pathways are
sulfation (children) & glucuronidation
• 2% renally excreted
• Water-soluble by-products of hepatic
metabolism
• 4% biotransformed by CYP-450 system
• Creates reactive toxic metabolite Nacetyl-p-benzoquinone imine (NAPQI)
APAP METABOLISM
• Hepatic glutathione binds NAPQI producing
non-toxic renally excreted byproduct
• Acute APAP OD depletes liver glutathione
stores by 70-80% limiting NAPQI metabolism
• NAPQI buildup causes hepatic injury by
binding to hepatocyte lipid bilayer, causing
centrilobular necrosis (zone 3)
• N-Acetylcysteine (NAC) limits liver injury by
replenishing glutathione to metabolize
excess NAPQI
CLINICAL
EVIDENCE OF
TOXICITY
TOXICICITY
• Fatalities uncommon
• Chronic ingestion has low mortality, moderate morbidity
• High risk: APAP > 10mcg/ml, AST 2X normal
• Low risk: APAP <10mcg/ml, AST <2X normal
• Severe toxicity related to acuity of OD, co-ingestants & PMH
• Pediatric: single dose >250 mg/kg
• Adult: single dose >150 mg/kg or >12 g
RUMACK-MATTHEW NOMOGRAM
Only useful for 24 hours post ingestion
LABORATORY PROGNOSIS PREDICTORS
• King’s College Criteria
pH < 7.30, or
PT >100sec
Creatinine > 3.4 mg/dL
Grade III+
encephalopathy
• PPV= 98%, NPV=82%
•
•
•
•
Chung PY, Sitrin MD, Te HS. Serum phosphorus level predict clinical outcome in fulminant
hepatic failure. Liver Transplantation. 2003;9:248-253
MANAGEMENT
Limit GI absorption, provide supportive care, control symptoms
• GI decontamination
• Rapid GI absorption
limits effective gastric
lavage
• Activated charcoal
• Very early presentation
• Co-ingestants
• Adsorbs to NAC
NAC TREATMENT
• Reduces hepatotoxic metabolite NAPQI via bio-transformation
• NAC becomes cysteine & mercapturic acid, replenishing glutathione stores,
serving as sulfation substrate
• Dosing: 140mg/kg bolus followed by 17 doses of 70mg/kg Q4º
• Pregnancy:
• APAP crosses placenta
• 2nd trimester fetal cytochrome P450 enzymes present
• IV NAC achieves higher maternal-fetal NAC gradient than oral
LATE NAC THERAPY
• Decreased hepatotoxicity when treatment begins 16-24 hours post ingestion
• IV NAC post onset of fulminant hepatic failure decreases vasopressor
requirements, & lowers incidence of cerebral edema & death
• Improved extra-hepatic oxygen delivery & utilization including cerebral
blood flow due to preservation of microvascular tone
SALICYLATES
Apo-Asa
Asaphen
Aspergum Aspirin Aspirin
Regimen Bayer 81 mg with Calcium Bayer Children's
Aspirin Easprin Ecotrin Caplets and Tablets Ecotrin
Maximum Strength Caplets and Tablets Empirin
Entrophen
Excedrin Geltabs Genprin Genuine Bayer
Aspirin Caplets and Tablets Halfprin 8-Hour Bayer
Timed-Release Caplets Maximum Bayer Aspirin
Caplets
and
Tablets
MSD
Enteric
Coated
ASA
Norwich Extra Strength Novasen
St. Joseph
Adult Chewable Aspirin Therapy Bayer Caplets ZORprin (Easprin and ZOR-prin are Rx) Acetylsalicylic acid,
buffered
(Ascriptin
Regular
Strength,
Bufferin)
Acetylsalicylic acid, buffered Alka-Seltzer with Aspirin
Alka-Seltzer with Aspirin (flavored) Alka-Seltzer Extra
Strength with Aspirin Arthritis Pain Formula Ascriptin
Regular Strength Ascriptin A/D Bayer Buffered Buffered
Aspirin Bufferin Buffex Cama Arthritis Pain Reliever
Magnaprin Magnaprin Arthritis Strength Captabs TriBuffered Bufferin Caplets and Tablets
OH
C O
O
O C CH3
Acetyl-salicylic acid
PHARMACOKINETICS
• Decreased prostaglandins &
thromboxane TXA2 production
• Irreversible inactivation of
cyclooxygenase (COX) enzyme
• Acetylating agent uncouples
mitochondiral oxidative
phosphorylation
• At toxic levels (>30mg/dL),
elimination routes saturated, with
decreased fraction protein
bound
SALICYLATE UNCOUPLING
Krebs cycle inhibition causes increased amounts of lactic & pyruvic acid
ATP
Glycolysis
Glucose
Lactate
• Uremia
• DKA, SKA, AKA
• INH, Iron, Infection
• Lactate
• Ethylene glycol
• Salicylates
Pyruvate
Kreb’s
Cycle
CO2
• Methanol
• Paraldehyde
Pyruvate
decarboxylase
H2O
Oxidative Phosphorylation
SALICYLATES
ATP
NADH2
MECHANISM OF TOXICITY
• High ASA levels depress medullary
respiratory center
• Uncoupling ETC
• High metabolism & temperature
• Increased CO2 production & O2 use
• Increased glycolysis with
hypoglycemia
• Hypokalemia from inhibition of active
transport
• Renal losses:
• Urinary ASA excretion pH-sensitive
• Hypokalemia from vomiting
• Increased renal losses of Na+ & HCO3
• Increased renal tubercle permeability
with intracellular H2O, Na+ retention
• Decreased renal blood flow, causes
ARI & SIADH from negative feedback
loop
SERUM LEVELS & ACUTE TOXICITY
• Absorbed well in small intestine
• Slow absorption in stomach
• Peak serum levels 30 minutes
• Toxic dose ½ life 15-30 hours
• Adult toxic ingestion 200-300mg/kg
• 500mg/kg often lethal
• Serum levels = tissue levels
• Follow levels with arterial pH,
clinical condition
Done nomogram (1960)
TOXICITY
•
•
•
•
•
Tinnitus
N/V
Pylorospasm
Diaphoresis
AMS
• Bleeding risk
• Decreased Factor VI & platelet
aggregation
• Death from:
• Metabolic acidosis
• Hypoglycemia
• Seizure
• Hyperthermia
• Pulmonary edema
• Cerebral edema
• Renal failure
*Increased CNS glucose utilization
CHRONIC SALICYLISM
• Common in elderly
• SSX consistent with acute toxicity
• May also present as:
• Delirium
• Encephalopathy
• CHF
• Mortality of chronic toxicity 25%
vs 1% for acute
ASA CHRONIC TOXICITY
• Any decreased blood flow to liver decreases ASA biotransformation
• Any decreased kidney function decreases salicylate clearance
• Decreased albumin binding leads to free salicylate
• Free salicylate enters cells causing symptoms with lower serum
concentration
• Chronic toxicity at 40mg/dL may be more ill than in an acute ingestion
at 80mg/dL
ABG = TOXICITY
• Early:
• Pure respiratory alkalosis
• 7.50 – 7.60 / 20 - 30
• Later:
• Respiratory alkalosis with compensated anion gap
metabolic acidosis
• 7.47 / 25
• Late
• Severe toxicity
• 7.40 / 15
TYPICAL ABG*
• High anion gap metabolic acidosis
• Concomitant normal anion gap
metabolic acidosis
• Respiratory alkalosis
• Decreased delta ratio
• Mixed acid-base order exists in elevated
AG acidosis
*Lifeinthefastlane.com
ASA TOXICITY ~ PULMONARY EDEMA
• MOA unknown
• At risk adults
•
•
•
•
•
•
•
•
Smoking
30+ y/o
Chronic use
Metabolic acidosis
CNS symptoms
Salicylate > 40mg/dL
Hypokalemia
Hypocapnea
MANAGEMENT
Limit absorption, increase excretion, correct fluid & acid-base abnormalities
• Laboratory
• ABG
• CBC / CMP
• ASA level (mg/dL) 6 & 8 hours post ingestion
• GI decontamination with multiple dose charcoal
• ASA is slow release, clumping in GIT where it is poorly souable with
delayed absorbtion
• Fluid resuscitation & electrolyte repletion
• Forced alkaline diuresis
• Hemodialysis
URINARY ALKALINIZATION
• Acidemia facilitates transfer of ASA into tissue
• Alkalinizing urine from pH 5 to 8 increases renal ASA elimination from
1.3 mL/min to 100 mL/min (10-20 times)
• Serum half-life decreases from 48 hours to 6 hours
• Acetazolamide creates alkyluria & metabolic acidosis while avoiding
systemic alkalosis
• NaHCO3 increases urinary elimination 10-20x
• Bolus 1-2 mEq/kg followed by 3 amps
• Goal: urine pH 7.5-8.0
• Serum pH not to exceed 7.55
• Must avoid hypokalemia
URINARY ALKALINIZATION
Prior to Alkalinization
Tissue pH 6.8
Plasma pH 7.1
Urine pH 6.5
HA
HA
HA
H+ + A-
H+ + A-
H+ + A-
URINARY ALKALINIZATION
After Alkalinization
Tissues pH 6.8
Plasma pH 7.4
Urine pH 8
HA
HA
HA
H+ + A-
H+ + A-
H+ + A-
Temple AR. Acute and chronic effects of aspirin toxicity and their treatment. Arch Intern Med 1981;141:367
EXTRACORPOREAL REMOVAL
• ASA primarily protein-bound with small VOD
• Binding site saturation leads to large levels of
free drug, which is easily dialyzable
• Indications
• Critically ill /
• Severe fluid / electrolyte disturbance
• High serum levels / unable to eliminate
salicylates
• Hemoperfusion
• Better clearance than hemodialysis for
protein-bound & lipid-soluble drugs
• Hemodialysis
• Better clearance for water-soluble & small
molecules
• Fluid, electrolyte, acid-base correction
NONSTEROIDAL ANTI-INFLAMMATORY
DRUGS (NSAIDS)
• Common indications & adverse
effects based upon common
mechanism of action
• Cyclooxygenase inhibition
• Different selectivity to COX I & II =
different pharmacokinetics &
potency
• Same toxicity management
PHARMACOLOGIC EFFECTS
• Analgesic
• CNS & peripheral
• Antipyretic
• CNS
• Anti-inflammatory
• Prostaglandin inhibition
• Inhibit activation, aggregation,
adhesion of neutrophils &
release of lysosomal enzymes
COMMON ADVERSE EFFECTS
• Platelet dysfunction
• Gastritis & peptic ulceration
• Nephropathy
• Na+ & H2O retention with edema
• Inhibition of labor
• Hypersenstivity (PG inhibition)
NSAID TOXICITY
• Toxicity based on COX selectivity
• COX-1: concentrated in platelets, gastric mucosa, renal collecting tubules,
vascular endothelium
• COX-2: anti-inflammatory with fewer GI side effects, primarily kidney &
platelet toxicity with increased risk of thrombotic events
- Most OD have only minor CNS or GI disturbances
- N/V, abdominal pain, drowsiness
- Severe*
-
Renal dysfunction
Bleeding dyscrasias
Acidosis
AMS / Coma
Seizure
Fever
Respiratory / cardiac arrest
Arrhythmias
*Does not correlate with serum level
MANAGEMENT
• Laboratory
•
•
•
•
•
•
CBC, LFTS, CMP, Magnesium, Phosphorus
PTT / PT / INR
ABG
Lactate
NSAID concentrations NOT useful
Salicylates, APAP, drug screen, alcohol
• High protein binding & rapid metabolism
• There is no role for urinary alkalinization or forced diuresis
• Multidose charcoal decreases elimination half-life by 30%
• Hemodialysis against an alkaline bath facilitates correction of
acid-base & electrolyte abnormalities & management of volume
status
MANAGEMENT
• NSAIDs acidic (i.e. carboxylic acid) or metabolized to acidic
compounds
• Anion gap acidosis from accumulation of parent compound &
metabolites, inhibition of mitochondrial respiration & distributive shock
in the setting of progressive acidosis
• Sodium bicarbonate
•
•
•
•
•
Not a specific antidote for NSAID toxicity
Consider with other supportive cares in an acidotic patient
Transient acidosis moderate toxicity typically self-limiting
Lactic secondary to tissue hypoperfusion refractory to bicarbonate
Supportive cares aimed at restoring normal tissue oxygenation &
perfusion are key
NITROASPIRINS DECREASE NSAID
TOXICITY
SUMMARY
• Management of acute APAP, ASA, NSAID poisoning is
supportive & symptom-specific
• Initial stabilization always consists of ABCs
• No evidence exists that empiric administration of
activated charcoal in drug OD improves clinical
outcome
• Be wary of chronic toxicity & co-ingestants
REFERENCES
• Acetaminophen and Salicylates Toxicity and Management. Joseph Rella, MD. NJMS
• Morgan AG, Polak A. The excretion of salicylate in salicylate poisoning. Clin Sci
1971;41:475-484
• Smilkstein, Knapp, Kulig, Rumack. Efficacy of oral N-Acetylcysteine in the treatment
of acetaminophen overdose: Analysis of the national multicenter study. N Engl J
Med 1988;319:1557-1562
• Smilkstein, Knapp, Kulig, Rumack. N-Acetylcysteine in the treatment of
acetaminophen overdose. N Engl J Med 1989;320:1418
• Keays, Harrison, Wendon, et al. Intravenous acetylcysteine in paracetamol induced
fulminant hepatic failure: A prospective trial. Br Med J 1991;303:1026-1029
• Defendi G. Consultant: Volume 12 - Issue 7 - July 2013. Acetaminophen toxicity in
children: diagnosis, clinical assessment, and treatment of acute overingestion. July
24, 2013
• Mottram AR, Kumar AM. Focus on: acetaminophen toxicity and treatment. ACEP
News. May 200712
• Temple AR, Baggish JS. Guidelines for the Management of Acetaminophen
Overdose. Fort Washington, PA: McNeil Consumer & Specialty Pharmaceuticals. 2005
• Blackford MG, Felter T, Gothard MD, Reed MD. Assessment of the clinical use of
intravenous and oral N-acetylcysteine in the treatment of acute acetaminophen
poisoning in children: a retrospective review. Clin Ther. 2011;33(9):1322-1330.
• Temple AR. Acute and chronic effects of aspirin toxicity and their treatment. Arch
Intern Med 1981;141:367
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