Carbamate poisoning

Background

• Carbamates are N-methyl carbamate insecticides derived from carbamic acid
• Structurally and mechanistically similar to organophosphates (OPs) but with critical differences in duration and reversibility^[1]
• Common agents:

• Absorption via dermal, inhalational, and gastrointestinal routes^[1]

Mechanism of Action

• Carbamates carbamylate the serine active site of acetylcholinesterase (AChE), preventing breakdown of acetylcholine
• This results in acetylcholine accumulation → cholinergic toxicity (identical toxidrome to Organophosphate toxicity)

Key Differences from Organophosphates

^[1][3]

• Clinical pearl: Despite being "reversible," severe carbamate poisoning (especially aldicarb) can absolutely be fatal — respiratory failure can occur before spontaneous enzyme reactivation^[4]

Special Considerations: Tres Pasitos

• Tres Pasitos ("Three Little Steps") is an illegally imported rodenticide containing aldicarb, one of the most toxic carbamates
• Sold unlabeled in small groceries, particularly in Dominican, Caribbean, and Latin American communities in the US^[2]
• Patients may present without knowing what they ingested — ask about rat poison specifically
• Has caused mass poisoning events; patients may require high-dose atropine (>10 mg) and ICU admission^[5]

Autonomic Nervous System Receptors and Their Effects

• Parasympathetic - ACh is transm
  • Muscarinic
    • receptors in heart, eye, lung, GI, skin and sweat glands
    • Bradycardia
    • Miosis
    • Bronchorrhea / Bronchospasm
    • Hyperperistalsis (SLUDGE)
    • Sweating
    • Vasodilation
  • Nicotinic
    • receptors in both sympathetic and parasympathetic nervous systems
    • fasciculations, flaccid paralysis
    • ?Mild bradycardia, hypotension
• Sympathetic
  • Alpha effects (vessels, eye, skin)
    • Mydriasis, hypertension, sweating
  • Beta effects (heart, lungs)
    • Tachycardia, bronchodilation

Clinical Features

• Identical cholinergic toxidrome to Organophosphate toxicity, but generally shorter duration and less CNS involvement^[1]
• Onset: minutes to hours depending on route (inhalation fastest, dermal slowest)
• Duration: usually self-limited within 6-12 hours; rarely up to 24 hours (due to spontaneous AChE reactivation)

Muscarinic Effects

• SLUDGE(M) = Salivation, Lacrimation, Urination, Diarrhea, GI pain, Emesis, Miosis
• DUMBELLS = Diarrhea/Diaphoresis, Urination, Miosis, Bradycardia/Bronchorrhea, Emesis, Lacrimation, Lethargic, Salivation
• Killer B's = Bradycardia, Bronchorrhea, Bronchospasm (leading causes of death)

Nicotinic Effects (NMJ)

• MTWThF (days of week) = Mydriasis/Muscle cramps, Tachycardia, Weakness, Twitching, Hypertension/Hyperglycemia, Fasciculations
• Note: Nicotinic effects (tachycardia, mydriasis) may mask classic muscarinic findings — do not rule out carbamate poisoning based on normal pupils or heart rate

CNS Effects

• Generally less prominent than with OPs because most carbamates cross the blood-brain barrier poorly^[6]
• When present: headache, confusion, agitation, seizures (more common with highly toxic agents like aldicarb)
• Respiratory depression — central drive suppression can still occur and is life-threatening

Cause of Death

• Respiratory failure from the combination of:
  • Bronchospasm and bronchorrhea (drowning in secretions)
  • Respiratory muscle weakness/paralysis (nicotinic effect)
  • Central respiratory depression (with agents that cross BBB)
• Patients can die before spontaneous enzyme reactivation occurs — do not be falsely reassured by the "reversible" label^[4]

Differential Diagnosis

• Carbamate and OP poisoning are clinically indistinguishable — differentiation requires history, product identification, or lab testing^[1]

SLUDGE Syndrome

• Carbamate toxicity
• Mushroom toxicity, especially:
  • Amanita muscaria
  • Inocybe
  • Clitocybe
• Organophosphate toxicity
• Nerve agent
  • Sarin
  • VX
  • Novichok agent
• Nicotine toxicity (look alike)
• Acetylcholinesterase inhibitor overdose (e.g in myasthenia gravis or post anesthesia reversal)

Weakness

• Neuromuscular weakness
  • Upper motor neuron:
    • CVA
    • Hemorrhagic stroke
    • Multiple sclerosis
    • Amyotrophic Lateral Sclerosis (ALS) (upper and lower motor neuron)
  • Lower motor neuron:
    • Spinal and bulbar muscular atrophy (Kennedy's syndrome)
  • Spinal cord disease:
    • Infection (Epidural abscess)
    • Infarction/ischemia
    • Trauma (Spinal Cord Syndromes)
    • Inflammation (Transverse Myelitis)
      • Acute flaccid myelitis
    • Degenerative (Spinal muscular atrophy)
    • Tumor
  • Peripheral nerve disease:
    • Guillain-Barre syndrome
    • Toxins (Ciguatera)
    • Tick paralysis
    • Diabetic peripheral neuropathy
  • Neuromuscular junction disease:
    • Myasthenia gravis crisis
    • Botulism
    • Organophosphate toxicity
    • Lambert-Eaton myasthenic syndrome
  • Muscle disease:
    • Rhabdomyolysis
    • Dermatomyositis
    • Polymyositis
    • Alcoholic myopathy
• Non-neuromuscular weakness
  • Can't miss diagnoses:
    • ACS
    • Arrhythmia/Syncope
    • Severe infection/Sepsis
    • Hypoglycemia
    • Periodic paralysis (electrolyte disturbance, K, Mg, Ca)
      • Hypokalemic periodic paralysis
      • Thyrotoxic periodic paralysis
    • Respiratory failure
  • Emergent Diagnoses:
    • Symptomatic Anemia
    • Severe dehydration
    • Hypothyroidism
    • Polypharmacy
    • Malignancy
    • Aortic disease - occlusion, stenosis, dissection
  • Other causes of weakness and paralysis
    • Acute intermittent porphyria (ascending weakness)

Chemical weapons

• Blister chemical agents (Vesicants)
  • Lewisite (L)
  • Sulfur mustard (H)
  • Phosgene oxime (CX)
• Pulmonary chemical agents (Choking agents)
  • Ammonia toxicity
  • Methyl isocyanate
  • Methyl bromide
  • Hydrochloric acid
  • Chlorine gas
  • Phosgene
• Incendiary agents
  • Agent orange
  • White phosphorus
• Cyanide chemical weapon agents (Blood agents)
  • Prussic acid (AKA hydrogen cyanide, hydrocyanic acid, or formonitrile)
• Nerve Agents (organophosphates)
  • Acetylcholinesterase inhibitors
  • Household and commercial pesticides (diazinon and parathion)
  • G-series (sarin, tabun, soman)
  • V-series (VX)
• Lacrimating or riot-control agents
  • Pepper spray
  • Chloroacetophenone
  • CS

Symptomatic bradycardia

• Cardiac
  • Inferior MI (involving RCA)
  • Sick sinus syndrome
• Neurocardiogenic/reflex-mediated
  • Increased ICP
  • Vasovagal reflex
  • Hypersensitive carotid sinus syndrome
  • Intra-abdominal hemorrhage (i.e. ruptured ectopic)
• Metabolic/endocrine/environmental
  • Hyperkalemia
  • Hypothermia (Osborn waves on ECG)
  • Hypothyroidism
    • Myxedema coma
  • Hypoglycemia (neonates)
• Toxicologic
  • B-blocker
  • Ca-channel blocker
  • Clonidine
  • Digoxin toxicity
  • Ethanol
  • Opioids
  • Organophosphates
  • Xylazine toxicity
• Infectious/Postinfectious
  • Chagas disease
  • Lyme disease
  • Syphilis
• Other
  • Brash syndrome

Evaluation

Workup

• Point-of-care glucose — nicotinic-mediated hyperglycemia may occur; exclude hypoglycemia in altered patients
• CBC — may show leukocytosis
• Comprehensive Metabolic Panel
• VBG/ABG — assess for respiratory failure, acidosis
• CXR — pulmonary edema in severe cases
• ECG
  • Sinus bradycardia, QT prolongation, AV block, ventricular dysrhythmias
  • Continuous cardiac monitoring is essential

Diagnosis

• Clinical diagnosis based on history + cholinergic toxidrome
• Attempt to identify the specific product:
  • Ask EMS to bring containers, labels, or Material Safety Data Sheets (MSDS)
  • Distinguish carbamate vs OP whenever possible — this guides pralidoxime decisions
  • Ask specifically about rat poisons, especially "Tres Pasitos" in appropriate populations^[2]
• Atropine challenge: If diagnosis is uncertain, a trial dose of atropine (1 mg IV) that produces improvement supports the diagnosis of cholinesterase inhibitor poisoning^[3]
• Laboratory cholinesterase levels:
  • RBC AChE and plasma butyrylcholinesterase (BuChE) can be obtained but are rarely available in time to guide acute management
  • Important caveat: In carbamate poisoning, RBC AChE levels rapidly normalize in vitro because the carbamate-AChE bond is reversible — samples must be obtained quickly and cooled/frozen immediately, or false-negative results will occur^[1]
  • Levels may be more useful for retrospective confirmation and medicolegal purposes

Management

Staff Safety and Decontamination

• Don PPE before patient contact — nitrile or neoprene gloves (latex is insufficient), gown, eye protection^[3]
• Remove ALL clothing and bag separately
• Wash skin thoroughly with soap and water
• GI decontamination: Generally not recommended
  • Rapid absorption and profuse vomiting/diarrhea limit utility of activated charcoal and lavage^[3]
  • If very early presentation (<1 hour) with large ingestion and protected airway, single-dose activated charcoal may be considered

Atropine

• First-line and most important antidote — muscarinic antagonist^[7]
• Does NOT reverse nicotinic symptoms (weakness, fasciculations, paralysis)
• Starting dose: 1-2 mg IV (pediatric: 0.02-0.05 mg/kg, minimum 0.1 mg)
• Doubling protocol: If inadequate response after 5 minutes, double the dose (1 → 2 → 4 → 8 mg...) until adequate atropinization
• Severe cases (e.g. aldicarb) may require >10 mg total^[2]
• Endpoints of adequate atropinization:
  • Drying of bronchial secretions (most important endpoint)
  • Heart rate >80 bpm
  • Systolic BP >80 mmHg
• Do NOT target: Fully dilated pupils, absent bowel sounds, or HR >150 (these indicate atropine toxicity)
• After initial atropinization: consider atropine infusion (10-20% of loading dose per hour)
• Total atropine requirements are generally LESS than with OP poisoning due to shorter duration of carbamate toxicity
• Optimize oxygenation before giving atropine to reduce risk of dysrhythmias

Pralidoxime (2-PAM): The Controversy

• Pralidoxime is generally NOT indicated for confirmed carbamate poisoning^[8]
• Rationale:
  • Carbamate-AChE binding is reversible and spontaneously regenerates → oximes are theoretically unnecessary
  • Pralidoxime has a different binding mechanism to carbamates than to OPs → no reactivation benefit^[6]
  • Historical concern: Animal studies with carbaryl showed that pralidoxime alone worsened outcomes (protective ratio <1)^[9]
• However, important nuances:
  • The carbaryl concern was from a single carbamate tested with pralidoxime ALONE (without atropine) — when atropine was co-administered, outcomes improved^[9]
  • Recent case reports suggest pralidoxime may be safe and possibly beneficial in some carbamate poisonings when given with atropine^[10]
  • Mixed exposures (carbamate + OP) are common (up to 35% of insecticide exposures) — pralidoxime is indicated for the OP component^[9]
• Bottom line for the ED:

Benzodiazepines

• Diazepam 5-10 mg IV or midazolam for seizures
• Pediatric: diazepam 0.2-0.5 mg/kg IV
• Do NOT use phenytoin — ineffective for cholinergic seizures^[7]

Supportive Care

• Airway management: Early intubation for copious secretions, respiratory failure, or altered mental status
  • Large-bore suction is critical — patients may drown in secretions^[11]
  • Avoid succinylcholine — metabolized by plasma cholinesterase (inhibited by carbamates) → prolonged paralysis
  • Use non-depolarizing agents (e.g. rocuronium) if RSI is needed
• IV fluid resuscitation for hypotension (from fluid losses, vasodilation)
• Vasopressors if refractory hypotension
• Continuous cardiac monitoring and pulse oximetry
• Avoid: morphine, theophylline, aminophylline, phenothiazines, reserpine^[11]

Medication Dosing

Atropine 1-2mg IV, double dose q5min until drying of secretions IV Atropine 0.02-0.05mg/kg IV (min 0.1mg), double q5min until drying of secretions IV Diazepam 5-10mg IV IV Diazepam 0.2-0.5mg/kg IV IV Pralidoxime 20mg/kg (max 2g) IV over 30min, then 8-10mg/kg/hr (max 650mg/hr) IV

Disposition

• Most carbamate poisonings resolve within 6-12 hours (some up to 24 hours) due to spontaneous AChE reactivation^[1]
• Asymptomatic patients with minimal exposure: observe for a minimum of 6 hours; may discharge if remains asymptomatic
• Admit all symptomatic patients — ICU admission for:
  • Need for atropine infusion or repeated dosing
  • Respiratory distress or intubation
  • Hemodynamic instability
  • Seizures or altered mental status
  • Aldicarb or other highly toxic carbamate exposure
• Unlike OP poisoning, intermediate syndrome and delayed neuropathy (OPIDN) are not expected — prolonged monitoring beyond 24 hours is usually not needed for confirmed carbamate-only exposures
• If agent is unidentified: monitor as for OP poisoning (at least 24 hours; watch for delayed toxicity)
• If evidence of deliberate self-harm → psychiatric hold and consult psychiatry
• Poison Control: 1-800-222-1222 (US) for all exposures

Consultant Pearls

• Toxicology: Call early — especially if agent is unknown or if considering pralidoxime. Ask about the specific product and whether it is carbamate, OP, or mixed
• ICU/Critical Care: For any patient requiring intubation, atropine infusion, or hemodynamic support
• Psychiatry: Mandatory for intentional ingestions
• If EMS or family can identify the product label or MSDS: This is extremely valuable — it distinguishes carbamate from OP and determines whether pralidoxime is indicated^[1]

See Also

• Organophosphate toxicity
• Toxidromes
• Cholinergic crisis
• Nerve agent
• Atropine
• Pralidoxime
• Acetylcholinesterase inhibitors

External Links

• Carbamate Toxicity — StatPearls
• Tres Pasitos — National Pesticide Information Center
• N-Methyl Carbamate Insecticides — EPA

References