3584 PART 14 Poisoning, Drug Overdose, and Envenomation
light remains. The anticholinergic toxidrome is also distinguished by
hot, dry, flushed skin; decreased bowel sounds; and urinary retention.
Other stimulant syndromes increase sympathetic activity and cause
diaphoresis, pallor, and increased bowel activity with varying degrees
of nausea, vomiting, abnormal distress, and occasionally diarrhea. The
absolute and relative degree of vital-sign changes and neuromuscular
hyperactivity can help distinguish among stimulant toxidromes. Since
sympathetics stimulate the peripheral nervous system more directly
than do hallucinogens or drug withdrawal, markedly increased vital
signs and organ ischemia suggest sympathetic poisoning. Findings
helpful in suggesting the particular drug or class causing physiologic
stimulation include reflex bradycardia from selective α-adrenergic
stimulants (e.g., decongestants), hypotension from selective β-adrenergic stimulants (e.g., asthma therapeutics), limb ischemia from
ergot alkaloids, rotatory nystagmus from phencyclidine and ketamine
(the only physiologic stimulants that cause this finding), and delayed
cardiac conduction from high doses of cocaine and some anticholinergic agents (e.g., antihistamines, cyclic antidepressants, and antipsychotics). Seizures suggest a sympathetic etiology, an anticholinergic
agent with membrane-active properties (e.g., cyclic antidepressants,
phenothiazines), or a withdrawal syndrome. Close attention to core
temperature is critical in patients with grade 4 physiologic stimulation
(Table 459-2).
The Depressed Physiologic State Decreased pulse, blood pressure, respiratory rate, temperature, and neuromuscular activity are
indicative of the depressed physiologic state caused by “functional”
sympatholytics (agents that decrease cardiac function and vascular
tone as well as sympathetic activity), cholinergic (muscarinic and
nicotinic) agents, opioids, and sedative-hypnotic γ-aminobutyric acid
(GABA)-ergic agents (Tables 459-1 and 459-2). Miosis is also common
and is most pronounced in opioid and cholinergic poisoning. Miosis
TABLE 459-1 Differential Diagnosis of Poisoning Based on Physiologic State
STIMULATED DEPRESSED DISCORDANT NORMAL
Sympathetics
Sympathomimetics
Ergot alkaloids
Methylxanthines
Monoamine oxidase inhibitors
Thyroid hormones
Anticholinergics
Antihistamines
Antiparkinsonian agents
Antipsychotics
Antispasmodics
Belladonna alkaloids
Cyclic antidepressants
Mushrooms and plants
Hallucinogens
Cannabinoids (marijuana)
LSD and analogues
Mescaline and analogues
Mushrooms
Phencyclidine and analogues
Withdrawal syndromes
Barbiturates
Benzodiazepines
Ethanol
GHB products
Opioids
Sedative-hypnotics
Sympatholytics
Sympatholytics
α1
-Adrenergic antagonists
α2
-Adrenergic agonists
ACE inhibitors
Angiotensin receptor blockers
Antipsychotics
β-Adrenergic blockers
Calcium channel blockers
Cardiac glycosides
Cyclic antidepressants
Cholinergics
Acetylcholinesterase inhibitors
Muscarinic agonists
Nicotinic agonists
Opioids
Analgesics
GI antispasmodics
Heroin
Sedative-hypnotics
Alcohols
Anticonvulsants
Barbiturates
Benzodiazepines
GABA precursors
Muscle relaxants
Other agents
GHB products
Asphyxiants
Cytochrome oxidase inhibitors
Inert gases
Irritant gases
Methemoglobin inducers
Oxidative phosphorylation inhibitors
AGMA inducers
Alcohol (ketoacidosis)
Ethylene glycol
Iron
Methanol
Other alcohols
Salicylate
Toluene
CNS syndromes
Extrapyramidal reactions
Hydrocarbon inhalation
Isoniazid
Lithium
Neuroleptic malignant syndrome
Serotonin syndrome
Strychnine
Membrane-active agents
Amantadine
Antiarrhythmics
Antihistamines
Antipsychotics
Carbamazepine
Cyclic antidepressants
Local anesthetics
Opioids (some)
Quinoline antimalarials
Nontoxic exposure
Psychogenic illness
“Toxic time-bombs”
Slow absorption
Anticholinergics
Carbamazepine
Concretion formers
Extended-release phenytoin sodium
capsules (Dilantin Kapseals)
Drug packets
Enteric-coated pills
Diphenoxylate-atropine (Lomotil)
Opioids
Salicylates
Sustained-release pills
Valproate
Slow distribution
Cardiac glycosides
Lithium
Metals
Salicylate
Valproate
Toxic metabolite
Acetaminophen
Carbon tetrachloride
Cyanogenic glycosides
Ethylene glycol
Methanol
Methemoglobin inducers
Mushroom toxins
Organophosphate insecticides
Paraquat
Metabolism disruptors
Antineoplastic agents
Antiviral agents
Colchicine
Hypoglycemic agents
Immunosuppressive agents
MAO inhibitors
Metals
Other oral anticoagulants
Salicylate
Warfarin
Abbreviations: ACE, angiotensin-converting enzyme; AGMA, anion-gap metabolic acidosis; CNS, central nervous system; GABA, γ-aminobutyric acid; GHB,
γ-hydroxybutyrate; GI, gastrointestinal; LSD, lysergic acid diethylamide; MAO, monoamine oxidase.
3585Poisoning and Drug Overdose CHAPTER 459
is distinguished from other depressant syndromes by muscarinic and
nicotinic signs and symptoms (Table 459-1). Pronounced cardiovascular depression in the absence of significant CNS depression suggests
a direct or peripherally acting sympatholytic. In contrast, in opioid
and sedative-hypnotic poisoning, vital-sign changes are secondary to
depression of CNS cardiovascular and respiratory centers (or consequent hypoxemia), and significant abnormalities in these parameters do
not occur until there is a marked decrease in the level of consciousness
(grade 3 or 4 physiologic depression; Table 459-2). Other clues that suggest the cause of physiologic depression include cardiac arrhythmias and
conduction disturbances (due to antiarrhythmics, β-adrenergic antagonists, calcium channel blockers, digitalis glycosides, propoxyphene,
and cyclic antidepressants), mydriasis (due to tricyclic antidepressants, some antiarrhythmics, meperidine, and diphenoxylate-atropine
[Lomotil]), nystagmus (due to sedative-hypnotics), and seizures (due
to cholinergic agents, propoxyphene, and cyclic antidepressants).
The Discordant Physiologic State The discordant physiologic
state is characterized by mixed vital-sign and neuromuscular abnormalities, as observed in poisoning by asphyxiants, CNS syndromes,
membrane-active agents, and anion-gap metabolic acidosis (AGMA)
inducers (Table 459-1). In these conditions, manifestations of physiologic stimulation and physiologic depression occur together or at
different times during the clinical course. For example, membraneactive agents can cause simultaneous coma, seizures, hypotension,
and tachyarrhythmias. Alternatively, vital signs may be normal while
the patient has an altered mental status or is obviously sick or clearly
symptomatic. Early, pronounced vital-sign and mental-status changes
suggest asphyxiant or membrane-active agent poisoning; the lack of
such abnormalities suggests an AGMA inducer; and marked neuromuscular dysfunction without significant vital-sign abnormalities
suggests a CNS syndrome. The discordant physiologic state may also
be evident in patients poisoned with multiple agents.
The Normal Physiologic State A normal physiologic status and
physical examination may be due to a nontoxic exposure, psychogenic
illness, or poisoning by “toxic time-bombs”: agents that are slowly
absorbed, are slowly distributed to their sites of action, require metabolic activation, or disrupt metabolic processes (Table 459-1). Because
so many medications have now been reformulated into once-a-day
preparations for the patient’s convenience and adherence, toxic timebombs are increasingly common. Diagnosing a nontoxic exposure
requires that the identity of the exposure agent be known or that a toxic
time-bomb exposure be excluded and the time since exposure exceed
the longest known or predicted interval between exposure and peak
toxicity. Psychogenic illness (fear of being poisoned, mass hysteria)
may also follow a nontoxic exposure and should be considered when
symptoms are inconsistent with exposure history. Anxiety reactions
resulting from a nontoxic exposure can cause mild physiologic stimulation (Table 459-2) and be indistinguishable from toxicologic causes
without ancillary testing or a suitable period of observation.
■ LABORATORY ASSESSMENT
Laboratory assessment may be helpful in the differential diagnosis.
Increased AGMA is most common in advanced methanol, ethylene
glycol, and salicylate intoxication but can occur with any poisoning that
results in hepatic, renal, or respiratory failure; seizures; or shock. The
serum lactate concentration is more commonly low (less than the anion
gap) in the former and high (nearly equal to the anion gap) in the latter.
An abnormally low anion gap can be due to elevated blood levels of
bromide, calcium, iodine, lithium, or magnesium. An increased osmolal gap—a difference of >10 mmol/L between serum osmolality (measured by freezing-point depression) and osmolality calculated from
serum sodium, glucose, and blood urea nitrogen levels—suggests the
presence of a low-molecular-weight solute such as acetone; an alcohol
(benzyl, ethanol, isopropanol, methanol); a glycol (diethylene, ethylene,
propylene); ether (ethyl, glycol); or an “unmeasured” cation (calcium,
magnesium) or sugar (glycerol, mannitol, sorbitol). Ketosis suggests
acetone, isopropyl alcohol, salicylate poisoning, or alcoholic ketoacidosis. Hypoglycemia may be due to poisoning with β-adrenergic
blockers, ethanol, insulin, oral hypoglycemic agents, quinine, and salicylates, whereas hyperglycemia can occur in poisoning with acetone,
β-adrenergic agonists, caffeine, calcium channel blockers, iron, theophylline, or N-3-pyridylmethyl-N′-p-nitrophenylurea (PNU [Vacor]).
Hypokalemia can be caused by barium, β-adrenergic agonists, caffeine,
diuretics, theophylline, or toluene; hyperkalemia suggests poisoning
with an α-adrenergic agonist, a β-adrenergic blocker, cardiac glycosides, or fluoride. Hypocalcemia may be seen in ethylene glycol,
fluoride, and oxalate poisoning. Prothrombin time and international
normalized ratio are useful for risk stratification in cases of warfarin or
rodenticide poisoning but are not to be relied on when evaluating overdose or complications from novel oral anticoagulant pharmaceuticals
(direct thrombin inhibitors and direct factor Xa inhibitors).
The electrocardiogram (ECG) can be useful for rapid diagnostic
purposes. Bradycardia and atrioventricular block may occur in patients
poisoned by α-adrenergic agonists, antiarrhythmic agents, beta blockers, calcium channel blockers, cholinergic agents (carbamate and
organophosphate insecticides), cardiac glycosides, lithium, or tricyclic
antidepressants. QRS- and QT-interval prolongation may be caused
by hyperkalemia, various antidepressants, and other membrane-active
drugs (Table 459-1). Ventricular tachyarrhythmias may be seen in
poisoning with cardiac glycosides, fluorides, membrane-active drugs,
methylxanthines, sympathomimetics, antidepressants, and agents that
cause hyperkalemia or potentiate the effects of endogenous catecholamines (e.g., chloral hydrate, aliphatic and halogenated hydrocarbons).
Radiologic studies may occasionally be useful. Pulmonary edema
(adult respiratory distress syndrome [ARDS]) can be caused by poisoning with carbon monoxide, cyanide, an opioid, paraquat, phencyclidine, a sedative-hypnotic, or salicylate; by inhalation of irritant
gases, fumes, or vapors (acids and alkali, ammonia, aldehydes, chlorine, hydrogen sulfide, isocyanates, metal oxides, mercury, phosgene,
polymers); or by prolonged anoxia, hyperthermia, or shock. Aspiration
pneumonia is common in patients with coma, seizures, and petroleum
distillate aspiration. Chest x-ray is useful for identifying complications
from metal fume fever or elemental mercury. The presence of radiopaque densities on abdominal x-rays or abdominal computed tomography (CT) scan suggests the ingestion of chloral hydrate, chlorinated
hydrocarbons, heavy metals, illicit drug packets, iodinated compounds,
potassium salts, enteric-coated tablets, or salicylates.
Toxicologic analysis of urine and blood (and occasionally of gastric contents and chemical samples) can sometimes confirm or rule
out suspected poisoning. Interpretation of laboratory data requires
TABLE 459-2 Severity of Physiologic Stimulation and Depression in
Poisoning and Drug Withdrawal
Physiologic Stimulation
Grade 1 Anxious, irritable, tremulous; vital signs normal; diaphoresis,
flushing or pallor, mydriasis, and hyperreflexia sometimes
present
Grade 2 Agitated; may have confusion or hallucinations but can converse
and follow commands; vital signs mildly to moderately increased
Grade 3 Delirious; unintelligible speech, uncontrollable motor
hyperactivity; moderately to markedly increased vital signs;
tachyarrhythmias possible
Grade 4 Coma, seizures, cardiovascular collapse
Physiologic Depression
Grade 1 Awake, lethargic, or sleeping but arousable by voice or tactile
stimulation; able to converse and follow commands; may be
confused
Grade 2 Responds to pain but not voice; can vocalize but not converse;
spontaneous motor activity present; brainstem reflexes intact
Grade 3 Unresponsive to pain; spontaneous motor activity absent;
brainstem reflexes depressed; motor tone, respirations, and
temperature decreased
Grade 4 Unresponsive to pain; flaccid paralysis; brainstem reflexes and
respirations absent; cardiovascular vital signs decreased
3586 PART 14 Poisoning, Drug Overdose, and Envenomation
knowledge of the qualitative and quantitative tests used for screening
and confirmation (enzyme-multiplied, fluorescence polarization, and
radio-immunoassays; colorimetric and fluorometric assays; thin-layer,
gas-liquid, or high-performance liquid chromatography; gas chromatography; mass spectrometry), their sensitivity (limit of detection)
and specificity, the preferred biologic specimen for analysis, and the
optimal time of specimen sampling. Personal communication with
the hospital laboratory is essential to an understanding of institutional
testing capabilities and limitations.
Rapid qualitative hospital-based urine tests for drugs of abuse are only
screening tests that cannot confirm the exact identity of the detected
substance and should not be considered diagnostic or used for forensic
purposes. False-positive and false-negative results are common. A positive screen may result from other pharmaceuticals that interfere with
laboratory analysis (e.g., fluoroquinolones commonly cause false-positive opiate screens). Confirmatory testing with gas chromatography/
mass spectrometry can be requested, but it often takes weeks to obtain a
reported result. A negative screening result may mean that the responsible substance is not detectable by the test used or that its concentration
is too low for detection at the time of sampling. For instance, recent new
drugs of abuse that often result in emergency department evaluation for
unexpected complications, such as synthetic cannabinoids (spice), cathinones (bath salts), and opiate substitutes (kratom), are not detectable by
hospital-based tests. In cases where a drug concentration is too low to be
detected early during clinical evaluation, repeating the test at a later time
may yield a positive result. Patients symptomatic from drugs of abuse
often require immediate management based on the history, physical
examination, and observed toxidrome without laboratory confirmation
(e.g., apnea from opioid intoxication). When the patient is asymptomatic or when the clinical picture is consistent with the reported history,
qualitative screening is neither clinically useful nor cost-effective. Thus,
qualitative drug screens are of greatest value for the evaluation of patients
with severe or unexplained toxicities, such as coma, seizures, cardiovascular instability, metabolic or respiratory acidosis, and nonsinus cardiac
rhythms. In contrast to qualitative drug screens, quantitative serum
tests are useful for evaluation of patients poisoned with acetaminophen
(Chap. 340), alcohols (including ethylene glycol and methanol), anticonvulsants, barbiturates, digoxin, heavy metals, iron, lithium, salicylate, and theophylline, as well as for the presence of carboxyhemoglobin
and methemoglobin. The serum concentration in these cases guides
clinical management, and results are often available within an hour.
The response to antidotes is sometimes useful for diagnostic purposes. Resolution of altered mental status and abnormal vital signs
within minutes of IV administration of dextrose, naloxone, or flumazenil is virtually diagnostic of hypoglycemia, opioid poisoning, and
benzodiazepine intoxication, respectively. The prompt reversal of
dystonic (extrapyramidal) signs and symptoms following an IV dose of
benztropine or diphenhydramine confirms a drug etiology. Although
complete reversal of both central and peripheral manifestations of
anticholinergic poisoning by physostigmine is diagnostic of this condition, physostigmine may cause some arousal in patients with CNS
depression of any etiology.
TREATMENT
Poisoning and Drug Overdose
GENERAL PRINCIPLES
Treatment goals include support of vital signs, prevention of further poison absorption (decontamination), enhancement of poison
elimination, administration of specific antidotes, and prevention
of reexposure (Table 459-3). Specific treatment depends on the
identity of the poison, the route and amount of exposure, the time
of presentation relative to the time of exposure, and the severity of
poisoning. Knowledge of the offending agents’ pharmacokinetics
and pharmacodynamics is essential.
During the pretoxic phase, prior to the onset of poisoning, decontamination is the highest priority, and treatment is based solely on
the history. The maximal potential toxicity based on the greatest
possible exposure should be assumed. Since decontamination is
more effective when accomplished soon after exposure and when
the patient is asymptomatic, the initial history and physical examination should be focused and brief. It is also advisable to establish
IV access and initiate cardiac monitoring, particularly in patients
with potentially serious ingestions or unclear histories.
When an accurate history is not obtainable and a poison causing
delayed toxicity (i.e., a toxic time-bomb) or irreversible damage is
suspected, blood and urine should be sent for appropriate toxicologic screening and quantitative analysis. During poison absorption
and distribution, blood levels may be greater than those in tissue
and may not correlate with toxicity. However, high blood levels of
agents whose metabolites are more toxic than the parent compound
(acetaminophen, ethylene glycol, or methanol) may indicate the
need for additional interventions (antidotes, dialysis). Most patients
who remain asymptomatic or who become asymptomatic 6 h after
ingestion are unlikely to develop subsequent toxicity and can be
discharged safely. Longer observation will be necessary for patients
who have ingested toxic time-bombs.
During the toxic phase—the interval between the onset of poisoning and its peak effects—management is based primarily on
clinical and laboratory findings. Effects after an overdose usually
begin sooner, peak later, and last longer than they do after a therapeutic dose. A drug’s published pharmacokinetic profile in standard
references such as the Physician’s Desk Reference (PDR) is usually
different from its toxicokinetic profile in overdose. Resuscitation
and stabilization are the first priority. Symptomatic patients should
have an IV line placed and should undergo oxygen saturation determination, cardiac monitoring, and continuous observation. Baseline laboratory, ECG, and x-ray evaluation may also be appropriate.
Intravenous glucose (unless the serum level is documented to be
normal), naloxone, and thiamine should be considered in patients
with altered mental status, particularly those with coma or seizures.
Decontamination should also be considered, but it is less likely to be
effective during this phase than during the pretoxic phase.
TABLE 459-3 Fundamentals of Poisoning Management
Supportive Care
Airway protection Treatment of seizures
Oxygenation/ventilation Correction of temperature
abnormalities
Treatment of arrhythmias Correction of metabolic derangements
Hemodynamic support Prevention of secondary complications
Prevention of Further Poison Absorption
Gastrointestinal decontamination Decontamination of other sites
Gastric lavage Eye decontamination
Activated charcoal Skin decontamination
Whole-bowel irrigation Body cavity evacuation
Dilution
Endoscopic/surgical removal
Enhancement of Poison Elimination
Multiple-dose activated charcoal
administration
Alteration of urinary pH
Chelation
Hyperbaric oxygenation
Extracorporeal removal
Hemodialysis
Hemoperfusion
Hemofiltration
Plasmapheresis
Exchange transfusion
Administration of Antidotes
Neutralization by antibodies Metabolic antagonism
Neutralization by chemical binding Physiologic antagonism
Prevention of Reexposure
Adult education Notification of regulatory agencies
Child-proofing Psychiatric referral
3587Poisoning and Drug Overdose CHAPTER 459
Measures that enhance poison elimination may shorten the
duration and severity of the toxic phase. However, they are not
without risk, which must be weighed against the potential benefit.
Diagnostic certainty (usually via laboratory confirmation) is generally a prerequisite. Intestinal (gut) dialysis with repetitive doses of
activated charcoal (see “Multiple-Dose Activated Charcoal,” later)
can enhance the elimination of selected poisons such as theophylline or carbamazepine. Urinary alkalinization may enhance the
elimination of salicylates and a few other poisons. Chelation therapy can enhance the elimination of selected metals. Extracorporeal
elimination methods are effective for many poisons, but their
expense and risk make their use reasonable only in patients who
would otherwise have an unfavorable outcome.
During the resolution phase of poisoning, supportive care and
monitoring should continue until clinical, laboratory, and ECG
abnormalities have resolved. Since chemicals are eliminated sooner
from the blood than from tissues, blood levels are usually lower
than tissue levels during this phase and again may not correlate with
toxicity. This discrepancy applies particularly when extracorporeal
elimination procedures are used. Redistribution from tissues may
cause a rebound increase in the blood level after termination of
these procedures (e.g., lithium). When a metabolite is responsible
for toxic effects, continued treatment may be necessary in the
absence of clinical toxicity or abnormal laboratory studies.
SUPPORTIVE CARE
The goal of supportive therapy is to maintain physiologic homeostasis until detoxification is accomplished and to prevent and treat
secondary complications such as aspiration, bedsores, cerebral and
pulmonary edema, pneumonia, rhabdomyolysis, renal failure, sepsis, thromboembolic disease, coagulopathy, and generalized organ
dysfunction due to hypoxemia or shock.
Admission to an intensive care unit is indicated for the following: patients with severe poisoning (coma, respiratory depression,
hypotension, cardiac conduction abnormalities, cardiac arrhythmias, hypothermia or hyperthermia, seizures); those needing close
monitoring, antidotes, or enhanced elimination therapy; those
showing progressive clinical deterioration; and those with significant underlying medical problems. Patients with mild to moderate
toxicity can be managed on a general medical service, on an intermediate care unit, or in an emergency department observation area,
depending on the anticipated duration and level of monitoring
needed (intermittent clinical observation vs continuous clinical,
cardiac, and respiratory monitoring). Patients who have attempted
suicide require continuous observation and measures to prevent
self-injury until they are no longer suicidal.
Respiratory Care Endotracheal intubation for protection against
the aspiration of gastrointestinal contents is of paramount importance in patients with CNS depression or seizures as this complication can increase morbidity and mortality rates. Mechanical
ventilation may be necessary for patients with respiratory depression or hypoxemia and for facilitation of therapeutic sedation or
paralysis of patients in order to prevent or treat hyperthermia, acidosis, and rhabdomyolysis associated with neuromuscular hyperactivity. Since clinical assessment of respiratory function can be
inaccurate, the need for oxygenation and ventilation is best determined by continuous pulse oximetry or arterial blood-gas analysis.
The gag reflex is not a reliable indicator of the need for intubation.
A patient with CNS depression may maintain airway patency while
being stimulated but not if left alone. Drug-induced pulmonary
edema is usually noncardiac rather than cardiac in origin, although
profound CNS depression and cardiac conduction abnormalities
suggest the latter. Measurement of pulmonary artery pressure may
be necessary to establish the cause and direct appropriate therapy.
Extracorporeal measures (membrane oxygenation, extracorporeal
membrane oxygenation [ECMO], venoarterial perfusion, cardiopulmonary bypass) and partial liquid (perfluorocarbon) ventilation
may be appropriate for severe but reversible respiratory failure. In
the last decade, ECMO has been increasingly used for critically ill
poisoned patients where standard resuscitative therapy or antidotes
have not been helpful, but further research is still needed to determine the right toxicologic indications for this treatment strategy.
Cardiovascular Therapy Maintenance of normal tissue perfusion
is critical for complete recovery to occur once the offending agent
has been eliminated. Focused bedside echocardiography or measurement of central venous pressure may help prioritize therapeutic
strategies. If hypotension is unresponsive to volume expansion and
appropriate goal-directed antidotal therapy, treatment with norepinephrine, epinephrine, or high-dose dopamine may be necessary.
Intraaortic balloon pump counterpulsation and venoarterial or
cardiopulmonary perfusion techniques should be considered for
severe but reversible cardiac failure. For patients with a return of
spontaneous circulation after resuscitative treatment for cardiopulmonary arrest secondary to poisoning, therapeutic hypothermia
should be used according to protocol. Bradyarrhythmias associated with hypotension generally should be treated as described in
Chaps. 244 and 245. Glucagon, calcium, and high-dose insulin
with dextrose may be effective in beta blocker and calcium channel
blocker poisoning. Antibody therapy may be indicated for cardiac
glycoside poisoning.
Supraventricular tachycardia associated with hypertension and
CNS excitation is almost always due to agents that cause generalized
physiologic excitation (Table 459–1). Most cases are mild or moderate in severity and require only observation or nonspecific sedation
with a benzodiazepine. In severe cases or those associated with
hemodynamic instability, chest pain, or ECG evidence of ischemia,
specific therapy is indicated. When the etiology is sympathetic
hyperactivity, treatment with a benzodiazepine should be prioritized. Further treatment with a combined alpha and beta blocker
(labetalol), a calcium channel blocker (verapamil or diltiazem),
or a combination of a beta blocker and a vasodilator (esmolol
and nitroprusside) may be considered for cases refractory to high
doses of benzodiazepines only when adequate sedation has been
achieved but cardiac conduction or blood pressure abnormalities
persist. Treatment with an α-adrenergic antagonist (phentolamine)
alone may sometimes be appropriate. If the cause is anticholinergic
poisoning, physostigmine alone can be effective. Supraventricular
tachycardia without hypertension is generally secondary to vasodilation or hypovolemia and responds to fluid administration.
For ventricular tachyarrhythmias due to tricyclic antidepressants
and other membrane-active agents (Table 459-1), sodium bicarbonate is indicated, whereas class IA, IC, and III antiarrhythmic
agents are contraindicated because of similar electrophysiologic
effects. Although lidocaine and phenytoin are historically safe for
ventricular tachyarrhythmias of any etiology, sodium bicarbonate
should be considered first for any ventricular arrhythmia suspected
to have a toxicologic etiology. Intravenous lipid emulsion therapy
has shown benefit for treatment of arrhythmias and hemodynamic
instability from various membrane-active agents. Beta blockers can
be hazardous if the arrhythmia is due to sympathetic hyperactivity.
Magnesium sulfate and overdrive pacing (by isoproterenol or a
pacemaker) may be useful in patients with torsades des pointes and
prolonged QT intervals. Magnesium and anti-digoxin antibodies
should be considered in patients with severe cardiac glycoside poisoning. Invasive (esophageal or intracardiac) ECG recording may
be necessary to determine the origin (ventricular or supraventricular) of wide-complex tachycardias (Chap. 246). If the patient is
hemodynamically stable, however, it is reasonable to simply observe
the patient rather than to administer another potentially proarrhythmic agent. Arrhythmias may be resistant to drug therapy until
underlying acid-base, electrolyte, oxygenation, and temperature
derangements are corrected.
Central Nervous System Therapies Neuromuscular hyperactivity and seizures can lead to hyperthermia, lactic acidosis,
and rhabdomyolysis and should be treated aggressively. Seizures
caused by excessive stimulation of catecholamine receptors (sympathomimetic or hallucinogen poisoning and drug withdrawal)
3588 PART 14 Poisoning, Drug Overdose, and Envenomation
or decreased activity of GABA (isoniazid poisoning) or glycine
(strychnine poisoning) receptors are best treated with agents that
enhance GABA activity, such as benzodiazepine or barbiturates.
Since benzodiazepines and barbiturates act by slightly different
mechanisms (the former increases the frequency via allosteric modulation at the receptor and the latter directly increases the duration
of chloride channel opening in response to GABA), therapy with
both may be effective when neither is effective alone. Seizures
caused by isoniazid, which inhibits the synthesis of GABA at several
steps by interfering with the cofactor pyridoxine (vitamin B6
), may
require high doses of supplemental pyridoxine. Seizures resulting
from membrane destabilization (beta blocker or cyclic antidepressant poisoning) require GABA enhancers (benzodiazepines first,
barbiturates second). Phenytoin is contraindicated in toxicologic
seizures: Animal and human data demonstrate worse outcomes
after phenytoin loading, especially in theophylline overdose. For
poisons with central dopaminergic effects (methamphetamine,
phencyclidine) manifested by psychotic behavior, a dopamine
receptor antagonist, such as haloperidol or ziprasidone, may be
useful. In anticholinergic and cyanide poisoning, specific antidotal
therapy may be necessary. The treatment of seizures secondary to
cerebral ischemia or edema or to metabolic abnormalities should
include correction of the underlying cause. Neuromuscular paralysis is indicated in refractory cases. Electroencephalographic monitoring and continuing treatment of seizures are necessary to prevent
permanent neurologic damage. Serotonergic receptor overstimulation in serotonin syndrome may be treated with cyproheptadine.
Other Measures Temperature extremes, metabolic abnormalities,
hepatic and renal dysfunction, and secondary complications should
be treated by standard therapies.
PREVENTION OF POISON ABSORPTION
Gastrointestinal Decontamination Whether or not to perform gastrointestinal decontamination and which procedure to use depends
on the time since ingestion; the existing and predicted toxicity of
the ingestant; the availability, efficacy, and contraindications of the
procedure; and the nature, severity, and risk of complications. The
efficacy of all decontamination procedures decreases with time, and
data are insufficient to support or exclude a beneficial effect when
they are used >1 h after ingestion. The average time from ingestion
to presentation for treatment is >1 h for children and >3 h for adults.
Most patients will recover from poisoning uneventfully with good
supportive care alone, but complications of gastrointestinal decontamination, particularly aspiration, can prolong this process. Hence,
gastrointestinal decontamination should be performed selectively,
not routinely, in the management of overdose patients. It is clearly
unnecessary when predicted toxicity is minimal or the time of
expected maximal toxicity has passed without significant effect.
Activated charcoal has comparable or greater efficacy; has fewer
contraindications and complications; and is less aversive and invasive than ipecac or gastric lavage. Thus, it is the preferred method
of gastrointestinal decontamination in most situations. Activated
charcoal suspension (in water) is given orally via a cup, straw, or
small-bore nasogastric tube. The generally recommended dose is
1 g/kg body weight because of its dosing convenience, although in
vitro and in vivo studies have demonstrated that charcoal adsorbs
≥90% of most substances when given in an amount equal to
10 times the weight of the substance. Palatability may be increased
by adding a sweetener (sorbitol) or a flavoring agent (cherry, chocolate, or cola syrup) to the suspension. Charcoal adsorbs ingested
poisons within the gut lumen, allowing the charcoal-toxin complex
to be evacuated with stool. Charged (ionized) chemicals such as
mineral acids, alkalis, and highly dissociated salts of cyanide, fluoride, iron, lithium, and other inorganic compounds are not well
adsorbed by charcoal. In studies with animals and human volunteers, charcoal decreases the absorption of ingestants by an average
of 73% when given within 5 min of ingestant administration, 51%
when given at 30 min, and 36% when given at 60 min. For this
reason, charcoal given before hospital arrival by prehospital emergency medical services (EMS) increases the potential clinical benefit. Side effects of charcoal include nausea, vomiting, and diarrhea
or constipation. Charcoal may also prevent the absorption of orally
administered therapeutic agents, so the timing and the dose administered need to be adjusted. Complications include mechanical
obstruction of the airway, aspiration, vomiting, and bowel obstruction and infarction caused by inspissated charcoal. Charcoal is not
recommended for patients who have ingested corrosives because it
obscures endoscopy.
Gastric lavage should be considered for life-threatening poisons
that cannot be treated effectively with other decontamination,
elimination, or antidotal therapies (e.g., colchicine). Gastric lavage
is performed by sequentially administering and aspirating ~5 mL
of fluid per kilogram of body weight through a no. 40 French orogastric tube (no. 28 French tube for children). Except in infants, for
whom normal saline is recommended, tap water is acceptable. The
patient should be placed in Trendelenburg and left lateral decubitus
positions to prevent aspiration (even if an endotracheal tube is
in place). Lavage decreases ingestant absorption by an average of
52% if performed within 5 min of ingestion administration, 26% if
performed at 30 min, and 16% if performed at 60 min. Significant
amounts of ingested drug are recovered from <10% of patients.
Aspiration is a common complication (occurring in up to 10% of
patients), especially when lavage is performed improperly. Serious
complications (esophageal and gastric perforation, tube misplacement in the trachea) occur in ~1% of patients. For this reason, the
physician should personally insert the lavage tube and confirm its
placement, and the patient must be cooperative during the procedure. Gastric lavage is contraindicated in corrosive or petroleum
distillate ingestions because of the respective risks of gastroesophageal perforation and aspiration pneumonitis. It is also contraindicated in patients with a compromised unprotected airway and those
at risk for hemorrhage or perforation due to esophageal or gastric
pathology or recent surgery. Finally, gastric lavage is absolutely
contraindicated in combative patients or those who refuse, as most
published complications involve patient resistance to the procedure.
Syrup of ipecac, an emetogenic agent that was once the substance
most commonly used for decontamination, no longer has a role in
poisoning management. Even the American Academy of Pediatrics—
traditionally the strongest proponent of ipecac—issued a policy
statement in 2003 recommending that ipecac should no longer be
used in poisoning treatment. Chronic ipecac use (by patients with
anorexia nervosa or bulimia) has been reported to cause electrolyte
and fluid abnormalities, cardiac toxicity, and myopathy.
Whole-bowel irrigation is performed by administering a bowelcleansing solution containing electrolytes and polyethylene glycol
(Golytely, Colyte) orally or by gastric tube at a rate of 2 L/h (0.5 L/h
in children) until rectal effluent is clear. The patient must be in a
sitting position. Although data are limited, whole-bowel irrigation
appears to be as effective as other decontamination procedures
in volunteer studies. It is most appropriate for those who have
ingested foreign bodies, packets of illicit drugs, and agents that are
poorly adsorbed by charcoal (e.g., heavy metals). This procedure is
contraindicated in patients with bowel obstruction, ileus, hemodynamic instability, and compromised unprotected airways.
Cathartics are salts (disodium phosphate, magnesium citrate
and sulfate, sodium sulfate) or saccharides (mannitol, sorbitol) that
historically have been given with activated charcoal to promote the
rectal evacuation of gastrointestinal contents. However, no animal,
volunteer, or clinical data have ever demonstrated any decontamination benefit from cathartics. Abdominal cramps, nausea, and
occasional vomiting are side effects. Complications of repeated dosing include severe electrolyte disturbances and excessive diarrhea.
Cathartics are contraindicated in patients who have ingested corrosives and in those with preexisting diarrhea. Magnesium-containing
cathartics should not be used in patients with renal failure.
Dilution (i.e., drinking water, another clear liquid, or milk at a
volume of 5 mL/kg of body weight) is recommended only after the
3589Poisoning and Drug Overdose CHAPTER 459
ingestion of corrosives (acids, alkali). It may increase the dissolution
rate (and hence absorption) of capsules, tablets, and other solid
ingestants and should not be used in these circumstances.
Endoscopic or surgical removal of poisons may be useful in rare
situations, such as ingestion of a potentially toxic foreign body that
fails to transit the gastrointestinal tract, a potentially lethal amount
of a heavy metal (arsenic, iron, mercury, thallium), or agents that
have coalesced into gastric concretions or bezoars (heavy metals,
lithium, salicylates, sustained-release preparations). Patients who
become toxic from cocaine due to its leakage from ingested drug
packets require immediate surgical intervention.
Decontamination of Other Sites Immediate, copious flushing
with water, saline, or another available clear, drinkable liquid is the
initial treatment for topical exposures (exceptions include alkali
metals, calcium oxide, phosphorus). Saline is preferred for eye
irrigation. A triple wash (water, soap, water) may be best for dermal
decontamination. Inhalational exposures should be treated initially
with fresh air or supplemental oxygen. The removal of liquids from
body cavities such as the vagina or rectum is best accomplished by
irrigation. Solids (drug packets, pills) should be removed manually,
preferably under direct visualization.
ENHANCEMENT OF POISON ELIMINATION
Although the elimination of most poisons can be accelerated by
therapeutic interventions, the pharmacokinetic efficacy (removal
of drug at a rate greater than that accomplished by intrinsic elimination) and clinical benefit (shortened duration of toxicity or
improved outcome) of such interventions are often more theoretical
than proven. Accordingly, the decision to use such measures should
be based on the actual or predicted toxicity and the potential efficacy, cost, and risks of therapy.
Multiple-Dose Activated Charcoal Repetitive oral dosing with
charcoal can enhance the elimination of previously absorbed substances by binding them within the gut as they are excreted in the
bile, are secreted by gastrointestinal cells, or passively diffuse into
the gut lumen (reverse absorption or enterocapillary exsorption).
Doses of 0.5–1 g/kg of body weight every 2–4 h, adjusted downward
to avoid regurgitation in patients with decreased gastrointestinal
motility, are generally recommended. Pharmacokinetic efficacy
approaches that of hemodialysis for some agents (e.g., phenobarbital, theophylline). Multiple-dose therapy should be considered only
for selected agents (theophylline, phenobarbital, carbamazepine,
dapsone, quinine). Complications include intestinal obstruction,
pseudo-obstruction, and nonocclusive intestinal infarction in
patients with decreased gut motility. Because of electrolyte and fluid
shifts, sorbitol and other cathartics are absolutely contraindicated
when multiple doses of activated charcoal are administered.
Urinary Alkalinization Ion trapping via alteration of urine pH
may prevent the renal reabsorption of poisons that undergo excretion by glomerular filtration and active tubular secretion. Since
membranes are more permeable to nonionized molecules than to
their ionized counterparts, acidic (low-pKa
) poisons are ionized and
trapped in alkaline urine, whereas basic ones become ionized and
trapped in acid urine. Urinary alkalinization (producing a urine pH
≥7.5 and a urine output of 3–6 mL/kg of body weight per hour by
the addition of sodium bicarbonate to an IV solution) enhances the
excretion of chlorophenoxyacetic acid herbicides, chlorpropamide,
diflunisal, fluoride, methotrexate, phenobarbital, sulfonamides,
and salicylates. Contraindications include congestive heart failure,
renal failure, and cerebral edema. Acid-base, fluid, and electrolyte
parameters should be monitored carefully. Although acid diuresis
may make theoretical sense for some overdoses (amphetamines), it
is never indicated and is potentially harmful.
Extracorporeal Removal Hemodialysis, charcoal or resin hemoperfusion, hemofiltration, plasmapheresis, and exchange transfusion are capable of removing any toxin from the bloodstream.
Agents most amenable to enhanced elimination by dialysis have
low molecular mass (<500 Da), high water solubility, low protein
binding, small volumes of distribution (<1 L/kg of body weight),
prolonged elimination (long half-life), and high dialysis clearance
relative to total-body clearance. Molecular weight, water solubility,
and protein binding do not limit the efficacy of the other forms of
extracorporeal removal.
Dialysis should be considered in cases of severe poisoning due to
carbamazepine, ethylene glycol, isopropyl alcohol, lithium, methanol, theophylline, salicylates, and valproate. Although hemoperfusion may be more effective in removing some of these poisons, it
does not correct associated acid-base and electrolyte abnormalities,
and most hospitals no longer have hemoperfusion cartridges readily
available. Fortunately, recent advances in hemodialysis technology
make it as effective as hemoperfusion for removing poisons such as
caffeine, carbamazepine, and theophylline. Both techniques require
central venous access and systemic anticoagulation and may result
in transient hypotension. Hemoperfusion may also cause hemolysis, hypocalcemia, and thrombocytopenia. Peritoneal dialysis and
exchange transfusion are less effective but may be used when other
procedures are unavailable, contraindicated, or technically difficult
(e.g., in infants). Exchange transfusion may be indicated in the
treatment of severe arsine- or sodium chlorate–induced hemolysis,
methemoglobinemia, and sulfhemoglobinemia. Although hemofiltration can enhance elimination of aminoglycosides, vancomycin,
and metal-chelate complexes, the roles of hemofiltration and plasmapheresis in the treatment of poisoning are not yet defined.
Candidates for extracorporeal removal therapies include patients
with severe toxicity whose condition deteriorates despite aggressive
supportive therapy; those with potentially prolonged, irreversible,
or fatal toxicity; those with dangerous blood levels of toxins; those
who lack the capacity for self-detoxification because of liver or renal
failure; and those with a serious underlying illness or complication
that will adversely affect recovery.
Other Techniques The elimination of heavy metals can be
enhanced by chelation, and the removal of carbon monoxide can
be accelerated by hyperbaric oxygenation.
ADMINISTRATION OF ANTIDOTES
Antidotes counteract the effects of poisons by neutralizing them
(e.g., antibody-antigen reactions, chelation, chemical binding) or
by antagonizing their physiologic effects (e.g., activation of opposing nervous system activity, provision of a competitive metabolic
or receptor substrate). Poisons or conditions with specific antidotes include acetaminophen, anticholinergic agents, anticoagulants, benzodiazepines, beta blockers, calcium channel blockers,
carbon monoxide, cardiac glycosides, cholinergic agents, cyanide,
drug-induced dystonic reactions, ethylene glycol, fluoride, heavy
metals, hypoglycemic agents, isoniazid, membrane-active agents,
methemoglobinemia, opioids, sympathomimetics, and a variety of
envenomations. Intravenous lipid emulsion has been shown to be
a successful antidote for poisoning from various anesthetics and
membrane-active agents (e.g., cyclic antidepressants), but the exact
mechanism of benefit is still under investigation. Antidotes can significantly reduce morbidity and mortality rates but are potentially
toxic if used for inappropriate reasons. Since their safe use requires
correct identification of a specific poisoning or syndrome, details of
antidotal therapy are discussed with the conditions for which they
are indicated (Table 459-4).
PREVENTION OF REEXPOSURE
Poisoning is a preventable illness. Unfortunately, some adults and
children are poison-prone, and recurrences are common. Unintentional polypharmacy poisoning has become especially common
among adults with developmental delays, among the growing population of geriatric patients who are prescribed a large number of
medications, and among adolescents and young adults experimenting with pharmaceuticals for recreational euphoria. Adults with
unintentional exposures should be instructed regarding the safe use
of medications and chemicals (according to labeling instructions).
Confused patients may need assistance with the administration of
3590 PART 14 Poisoning, Drug Overdose, and Envenomation
TABLE 459-4 Pathophysiologic Features and Treatment of Specific Toxic Syndromes and Poisonings
PHYSIOLOGIC
CONDITION, CAUSES EXAMPLES MECHANISM OF ACTION CLINICAL FEATURES SPECIFIC TREATMENTS
Stimulated
Sympatheticsa
Sympathomimetics α1
-Adrenergic agonists
(decongestants):
phenylephrine,
phenylpropanolamine
β2
-Adrenergic agonists
(bronchodilators):
albuterol, terbutaline
Nonspecific adrenergic
agonists: amphetamines,
cocaine, ephedrine
Stimulation of central and
peripheral sympathetic receptors
directly or indirectly (by promoting
release or inhibiting reuptake of
norepinephrine and sometimes
dopamine)
Physiologic stimulation (Table
459-2). Reflex bradycardia
can occur with selective α1
agonists; β agonists can cause
hypotension and hypokalemia.
Phentolamine, a nonselective α1
-
adrenergic receptor antagonist,
for severe hypertension due to
α1
-adrenergic agonists; propranolol,
a nonselective β blocker, for
hypotension and tachycardia due
to β2
agonists; either labetalol,
a β blocker with α-blocking
activity, or phentolamine with
esmolol, metoprolol, or another
cardioselective β blocker for
hypertension with tachycardia due
to nonselective agents (β blockers,
if used alone, can exacerbate
hypertension and vasospasm
due to unopposed α stimulation.);
benzodiazepines; propofol
Ergot alkaloids Ergotamine, methysergide,
bromocriptine, pergolide
Stimulation and inhibition of
serotonergic and α-adrenergic
receptors; stimulation of dopamine
receptors
Physiologic stimulation (Table
459-2); formication; vasospasm
with limb (isolated or
generalized), myocardial, and
cerebral ischemia progressing
to gangrene or infarction.
Hypotension, bradycardia, and
involuntary movements can
also occur.
Nitroprusside or nitroglycerine for
severe vasospasm; prazosin (an
α1
blocker), captopril, nifedipine,
and cyproheptadine (a serotonin
receptor antagonist) for mild-tomoderate limb ischemia; dopamine
receptor antagonists (antipsychotics)
for hallucinations and movement
disorders
Methylxanthines Caffeine, theophylline Inhibition of adenosine synthesis
and adenosine receptor
antagonism; stimulation of
epinephrine and norepinephrine
release; inhibition of
phosphodiesterase resulting in
increased intracellular cyclic
adenosine and guanosine
monophosphate
Physiologic stimulation
(Table 459-2); pronounced
gastrointestinal symptoms and
β agonist effects (see above).
Toxicity occurs at lower drug
levels in chronic poisoning than
in acute poisoning.
Propranolol, a nonselective β
blocker, or esmolol for tachycardia
with hypotension; any β blocker
for supraventricular or ventricular
tachycardia without hypotension;
elimination enhanced by multipledose charcoal, hemoperfusion,
and hemodialysis. Indications for
hemoperfusion or hemodialysis
include unstable vital signs, seizures,
and a theophylline level of 80–100 μg/
mL after an acute overdose and
40–60 μg/mL with chronic exposure.
Monoamine oxidase
inhibitors
Phenelzine,
tranylcypromine,
selegiline
Inhibition of monoamine oxidase
resulting in impaired metabolism
of endogenous catecholamines
and exogenous sympathomimetic
agents
Delayed or slowly progressive
physiologic stimulation
(Table 459-2); terminal
hypotension and bradycardia in
severe cases
Short-acting agents (e.g.,
nitroprusside, esmolol) for severe
hypertension and tachycardia;
direct-acting sympathomimetics (e.g.,
norepinephrine, epinephrine) for
hypotension and bradycardia
Anticholinergics
Antihistamines Diphenhydramine,
doxylamine, pyrilamine
Inhibition of central and
postganglionic parasympathetic
muscarinic cholinergic receptors.
At high doses, amantadine,
diphenhydramine, orphenadrine,
phenothiazines, and tricyclic
antidepressants have additional
nonanticholinergic activity
(see below).
Physiologic stimulation
(Table 459-2); dry skin
and mucous membranes,
decreased bowel sounds,
flushing, and urinary retention;
myoclonus and picking activity.
Central effects may occur
without significant autonomic
dysfunction.
Physostigmine, an
acetylcholinesterase inhibitor (see
below), for delirium, hallucinations,
and neuromuscular hyperactivity.
Contraindications include asthma and
non-anticholinergic cardiovascular
toxicity (e.g., cardiac conduction
abnormalities, hypotension, and
ventricular arrhythmias).
Antipsychotics Chlorpromazine,
olanzapine, quetiapine,
thioridazine
Inhibition of α-adrenergic,
dopaminergic, histaminergic,
muscarinic, and serotonergic
receptors. Some agents also inhibit
sodium, potassium, and calcium
channels.
Physiologic depression (Table
459-2), miosis, anticholinergic
effects (see above),
extrapyramidal reactions (see
below), tachycardia
Sodium bicarbonate for ventricular
tachydysrhythmias associated with
QRS prolongation; magnesium,
isoproterenol, and overdrive pacing
for torsades des pointes. Avoid class
IA, IC, and III antiarrhythmics.
Belladonna alkaloids Atropine, hyoscyamine,
scopolamine
Inhibition of central and
postganglionic parasympathetic
muscarinic cholinergic receptors
Physiologic stimulation
(Table 459-2); dry skin
and mucous membranes,
decreased bowel sounds,
flushing, and urinary retention;
myoclonus and picking activity.
Central effects may occur
without significant autonomic
dysfunction.
Physostigmine, an
acetylcholinesterase inhibitor (see
below), for delirium, hallucinations,
and neuromuscular hyperactivity.
Contraindications include asthma and
non-anticholinergic cardiovascular
toxicity (e.g., cardiac conduction
abnormalities, hypotension, and
ventricular arrhythmias).
(Continued)
3591Poisoning and Drug Overdose CHAPTER 459
TABLE 459-4 Pathophysiologic Features and Treatment of Specific Toxic Syndromes and Poisonings
PHYSIOLOGIC
CONDITION, CAUSES EXAMPLES MECHANISM OF ACTION CLINICAL FEATURES SPECIFIC TREATMENTS
Cyclic antidepressants Amitriptyline, doxepin,
imipramine
Inhibition of α-adrenergic,
dopaminergic, GABA-ergic,
histaminergic, muscarinic, and
serotonergic receptors; inhibition of
sodium channels (see membraneactive agents); inhibition of
norepinephrine and serotonin
reuptake
Physiologic depression (Table
459-2), seizures, tachycardia,
cardiac conduction delays
(increased PR, QRS, JT, and
QT intervals; terminal QRS
right-axis deviation) with
aberrancy and ventricular
tachydysrhythmias;
anticholinergic toxidrome (see
above)
Hypertonic sodium bicarbonate (or
hypertonic saline) for ventricular
tachydysrhythmias associated with
QRS prolongation. Use of phenytoin
is controversial. Avoid class IA, IC,
and III antiarrhythmics. IV emulsion
therapy may be beneficial in some
cases.
Mushrooms and plants Amanita muscaria and
A. pantherina, henbane,
jimson weed, nightshade
Inhibition of central and
postganglionic parasympathetic
muscarinic cholinergic receptors
Physiologic stimulation (Table
459-2); dry skin and mucous
membranes, decreased bowel
sounds, flushing, and urinary
retention; myoclonus and
picking activity. Central effects
may occur without significant
autonomic dysfunction.
Physostigmine, an
acetylcholinesterase inhibitor (see
below), for delirium, hallucinations,
and neuromuscular hyperactivity.
Contraindications include asthma and
nonanticholinergic cardiovascular
toxicity (e.g., cardiac conduction
abnormalities, hypotension, and
ventricular arrhythmias).
Depressed
Sympatholytics
α2
-Adrenergic agonists Clonidine, guanabenz,
tetrahydrozoline and
other imidazoline
decongestants, tizanidine
and other imidazoline
muscle relaxants
Stimulation of α2
-adrenergic
receptors leading to inhibition of
CNS sympathetic outflow. Activity
at nonadrenergic imidazoline
binding sites also contributes to
CNS effects.
Physiologic depression (Table
459-2), miosis. Transient initial
hypertension may be seen.
Dopamine and norepinephrine
for hypotension; atropine for
symptomatic bradycardia; naloxone
for CNS depression (inconsistently
effective)
Antipsychotics Chlorpromazine,
clozapine, haloperidol,
risperidone, thioridazine
Inhibition of α-adrenergic,
dopaminergic, histaminergic,
muscarinic, and serotonergic
receptors. Some agents also inhibit
sodium, potassium, and calcium
channels.
Physiologic depression
(Table 459-2), miosis,
anticholinergic effects (see
above), extrapyramidal
reactions (see below),
tachycardia. Cardiac
conduction delays (increased
PR, QRS, JT, and QT
intervals) with ventricular
tachydysrhythmias, including
torsades des pointes, can
sometimes develop.
Sodium bicarbonate for ventricular
tachydysrhythmias associated with
QRS prolongation; magnesium,
isoproterenol, and overdrive pacing
for torsades des pointes. Avoid class
IA, IC, and III antiarrhythmics.
β-Adrenergic blockers Cardioselective (β1
)
blockers: atenolol,
esmolol, metoprolol
Nonselective (β1
and
β2
) blockers: nadolol,
propranolol, timolol
Partial β agonists:
acebutolol, pindolol
α1
Antagonists: carvedilol,
labetalol
Membrane-active agents:
acebutolol, propranolol,
sotalol
Inhibition of β-adrenergic receptors
(class II antiarrhythmic effect).
Some agents have activity at
additional receptors or have
membrane effects (see below).
Physiologic depression
(Table 459-2), atrioventricular
block, hypoglycemia,
hyperkalemia, seizures.
Partial agonists can cause
hypertension and tachycardia.
Sotalol can cause increased
QT interval and ventricular
tachydysrhythmias. Onset may
be delayed after sotalol and
sustained-release formulation
overdose.
Glucagon for hypotension and
symptomatic bradycardia. Atropine,
isoproterenol, dopamine, dobutamine,
epinephrine, and norepinephrine may
sometimes be effective. High-dose
insulin (with glucose and potassium
to maintain euglycemia and
normokalemia), electrical pacing, and
mechanical cardiovascular support
for refractory cases.
Calcium channel
blockers
Diltiazem, nifedipine and
other dihydropyridine
derivatives, verapamil
Inhibition of slow (type L)
cardiovascular calcium channels
(class IV antiarrhythmic effect)
Physiologic depression
(Table 459-2), atrioventricular
block, organ ischemia and
infarction, hyperglycemia,
seizures. Hypotension is usually
due to decreased vascular
resistance rather than to
decreased cardiac output.
Onset may be delayed for ≥12
h after overdose of sustainedrelease formulations.
Calcium and glucagon for
hypotension and symptomatic
bradycardia. Dopamine, epinephrine,
norepinephrine, atropine, and
isoproterenol are less often effective
but can be used adjunctively. Highdose insulin (with glucose and
potassium to maintain euglycemia
and normokalemia), IV lipid emulsion
therapy, electrical pacing, and
mechanical cardiovascular support
for refractory cases.
(Continued)
(Continued)
3592 PART 14 Poisoning, Drug Overdose, and Envenomation
TABLE 459-4 Pathophysiologic Features and Treatment of Specific Toxic Syndromes and Poisonings
PHYSIOLOGIC
CONDITION, CAUSES EXAMPLES MECHANISM OF ACTION CLINICAL FEATURES SPECIFIC TREATMENTS
Cardiac glycosides Digoxin, endogenous
cardioactive steroids,
foxglove and other plants,
toad skin secretions
(Bufonidae spp.)
Inhibition of cardiac Na+
, K+
-ATPase
membrane pump
Physiologic depression
(Table 459-2); gastrointestinal,
psychiatric, and visual
symptoms; atrioventricular
block with or without
concomitant supraventricular
tachyarrhythmia; ventricular
tachyarrhythmias; hyperkalemia
in acute poisoning. Toxicity
occurs at lower drug levels in
chronic poisoning than in acute
poisoning.
Digoxin-specific antibody fragments
for hemodynamically compromising
dysrhythmias, Mobitz II or thirddegree atrioventricular block,
hyperkalemia (>5.5 meq/L; in
acute poisoning only). Temporizing
measures include atropine, dopamine,
epinephrine, and external cardiac
pacing for bradydysrhythmias and
magnesium, lidocaine, or phenytoin,
for ventricular tachydysrhythmias.
Internal cardiac pacing and
cardioversion can increase
ventricular irritability and should be
reserved for refractory cases.
Cyclic antidepressants Amitriptyline, doxepin,
imipramine
Inhibition of α-adrenergic,
dopaminergic, GABA-ergic,
histaminergic, muscarinic, and
serotonergic receptors; inhibition of
sodium channels (see membraneactive agents); inhibition of
norepinephrine and serotonin
reuptake
Physiologic depression (Table
459-2), seizures, tachycardia,
cardiac conduction delays
(increased PR, QRS, JT, and QT
intervals; terminal QRS right-axis
deviation) with aberrancy and
ventricular tachydysrhythmias;
anticholinergic toxidrome (see
above)
Hypertonic sodium bicarbonate (or
hypertonic saline) for ventricular
tachydysrhythmias associated with
QRS prolongation. Use of phenytoin
is controversial. Avoid class IA, IC,
and III antiarrhythmics. IV emulsion
therapy may be beneficial in some
cases.
Cholinergics
Acetylcholinesterase
inhibitors
Muscarinic agonists
Nicotinic agonists
Carbamate insecticides
(aldicarb, carbaryl,
propoxur) and
medicinals (neostigmine,
physostigmine, tacrine);
nerve gases (sarin,
soman, tabun, VX);
organophosphate
insecticides (diazinon,
chlorpyrifos-ethyl,
malathion)
Bethanechol, mushrooms
(Boletus, Clitocybe,
Inocybe spp.), pilocarpine
Lobeline, nicotine
(tobacco)
Inhibition of acetylcholinesterase
leading to increased synaptic
acetylcholine at muscarinic and
nicotinic cholinergic receptor sites
Stimulation of CNS and
postganglionic parasympathetic
cholinergic (muscarinic) receptors
Stimulation of preganglionic
sympathetic and parasympathetic
and striated muscle (neuromuscular
junction) cholinergic (nicotine)
receptors
Physiologic depression (Table
459-2). Muscarinic signs and
symptoms: seizures, excessive
secretions (lacrimation,
salivation, bronchorrhea and
wheezing, diaphoresis), and
increased bowel and bladder
activity with nausea, vomiting,
diarrhea, abdominal cramps,
and incontinence of feces
and urine. Nicotinic signs
and symptoms: hypertension,
tachycardia, muscle cramps,
fasciculations, weakness, and
paralysis. Death is usually
due to respiratory failure.
Cholinesterase activity in
plasma and red cells is <50% of
normal in acetylcholinesterase
inhibitor poisoning.
Atropine for muscarinic signs and
symptoms; 2-PAM, a cholinesterase
reactivator, for nicotinic signs and
symptoms due to organophosphates,
nerve gases, or an unknown
anticholinesterase
Sedative-hypnoticsb
Anticonvulsants
Barbiturates
Benzodiazepines
Carbamazepine,
ethosuximide, felbamate,
gabapentin, lamotrigine,
levetiracetam,
oxcarbazepine, phenytoin,
tiagabine, topiramate,
valproate, zonisamide
Short-acting: butabarbital,
pentobarbital,
secobarbital
Long-acting:
phenobarbital, primidone
Ultrashort-acting:
estazolam, midazolam,
temazepam, triazolam
Short-acting: alprazolam,
flunitrazepam, lorazepam,
oxazepam
Long-acting:
chlordiazepoxide,
clonazepam, diazepam,
flurazepam
Pharmacologically related
agents: zaleplon, zolpidem
Potentiation of the inhibitory
effects of GABA by binding to the
neuronal GABA–A chloride channel
receptor complex and increasing
the frequency or duration of
chloride channel opening in
response to GABA stimulation.
Baclofen and, to some extent,
GHB act at the GABA–B receptor
complex. Meprobamate, its
metabolite carisoprodol, felbamate,
and orphenadrine antagonize
NDMA excitatory receptors.
Ethosuximide, valproate, and
zonisamide decrease conduction
through T-type calcium channels.
Valproate decreases GABA
degradation, and tiagabine blocks
GABA reuptake. Carbamazepine,
lamotrigine, oxcarbazepine,
phenytoin, topiramate, valproate,
and zonisamide slow the rate of
recovery of inactivated sodium
channels. Some agents also have α2
agonist, anticholinergic, and sodium
channel–blocking activity (see
above and below).
Physiologic depression (Table
459-2), nystagmus.
Delayed absorption can occur
with carbamazepine, phenytoin,
and valproate.
Myoclonus, seizures,
hypertension, and
tachyarrhythmias can occur
with baclofen, carbamazepine,
and orphenadrine.
Tachyarrhythmias can also
occur with chloral hydrate.
AGMA, hypernatremia,
hyperosmolality,
hyperammonemia, chemical
hepatitis, and hypoglycemia
can be seen in valproate
poisoning. Carbamazepine and
oxcarbazepine may produce
hyponatremia from SIADH.
Benzodiazepines, barbiturates, or
propofol for seizures.
Hemodialysis and hemoperfusion may
be indicated for severe poisoning by
some agents (see “Extracorporeal
Removal,” in text).
See above and below for treatment of
anticholinergic and sodium channel
(membrane)–blocking effects.
(Continued)
(Continued)
3593Poisoning and Drug Overdose CHAPTER 459
TABLE 459-4 Pathophysiologic Features and Treatment of Specific Toxic Syndromes and Poisonings
PHYSIOLOGIC
CONDITION, CAUSES EXAMPLES MECHANISM OF ACTION CLINICAL FEATURES SPECIFIC TREATMENTS
GABA precursors γ-Hydroxybutyrate
(sodium oxybate; GHB),
γ-butyrolactone (GBL),
1,4-butanediol
Stimulation at GABA receptor
complex increases chloride
channel opening
Physiologic depression
(Table 459-2)
Goal-directed supportive care
Muscle relaxants Baclofen, carisoprodol,
cyclobenzaprine,
etomidate, metaxalone,
methocarbamol,
orphenadrine, propofol,
tizanidine and other
imidazoline muscle
relaxants
Baclofen acts at GABA-B
receptor complex; Stimulation of
α2-adrenergic receptors inhibits
CNS sympathetic outflow. Activity at
nonadrenergic imidazoline binding
sites also contributes to CNS
effects. The others have centrallyacting and various other unknown
mechanisms of action
Physiologic depression
(Table 459-2)
Goal-directed supportive care;
benzodiazepines and barbiturates for
seizures
Other agents Chloral hydrate,
ethchlorvynol,
glutethimide,
meprobamate,
methaqualone,
methyprylon
Discordant
Asphyxiants
Cytochrome oxidase
inhibitors
Cyanide, hydrogen sulfide Inhibition of mitochondrial
cytochrome oxidase, with
consequent blockage of electron
transport and oxidative metabolism.
Carbon monoxide also binds to
hemoglobin and myoglobin and
prevents oxygen binding, transport,
and tissue uptake. (Binding to
hemoglobin shifts the oxygen
dissociation curve to the left.)
Signs and symptoms of
hypoxemia with initial
physiologic stimulation and
subsequent depression
(Table 459-2); lactic acidosis;
normal PO2
and calculated
oxygen saturation but
decreased oxygen saturation
by co-oximetry. (That measured
by pulse oximetry is falsely
elevated but is less than normal
and less than the calculated
value.) Headache and nausea
are common with carbon
monoxide. Sudden collapse
may occur with cyanide and
hydrogen sulfide exposure.
A bitter almond breath odor
may be noted with cyanide
ingestion, and hydrogen sulfide
smells like rotten eggs.
High-dose oxygen; IV
hydroxocobalamin or IV sodium nitrite
and sodium thiosulfate (Lilly cyanide
antidote kit) for coma, metabolic
acidosis, and cardiovascular
dysfunction in cyanide poisoning or
victims from a fire; ECMO
Methemoglobin
inducers
Aniline derivatives,
dapsone, local
anesthetics, nitrates,
nitrites, nitrogen
oxides, nitro- and
nitrosohydrocarbons,
phenazopyridine,
primaquine-type
antimalarials,
sulfonamides
Oxidation of hemoglobin iron
from ferrous (Fe2+) to ferric (Fe3+)
state prevents oxygen binding,
transport, and tissue uptake.
(Methemoglobinemia shifts oxygen
dissociation curve to the left.)
Oxidation of hemoglobin protein
causes hemoglobin precipitation
and hemolytic anemia (manifesting
as Heinz bodies and “bite cells” on
peripheral-blood smear).
Signs and symptoms of
hypoxemia with initial
physiologic stimulation and
subsequent depression (Table
459-2), gray-brown cyanosis
unresponsive to oxygen at
methemoglobin fractions
>15–20%, headache, lactic
acidosis (at methemoglobin
fractions >45%), normal PO2
and
calculated oxygen saturation
but decreased oxygen
saturation and increased
methemoglobin fraction by
co-oximetry (Oxygen saturation
by pulse oximetry may be
falsely increased or decreased
but is less than normal and less
than the calculated value.)
High-dose oxygen; IV methylene blue
for methemoglobin fraction >30%,
symptomatic hypoxemia, or ischemia
(contraindicated in G6PD deficiency);
exchange transfusion and hyperbaric
oxygen for severe or refractory cases
(Continued)
(Continued)
3594 PART 14 Poisoning, Drug Overdose, and Envenomation
TABLE 459-4 Pathophysiologic Features and Treatment of Specific Toxic Syndromes and Poisonings
PHYSIOLOGIC
CONDITION, CAUSES EXAMPLES MECHANISM OF ACTION CLINICAL FEATURES SPECIFIC TREATMENTS
AGMA inducers Ethylene glycol Ethylene glycol causes CNS
depression and increased serum
osmolality. Metabolites (primarily
glycolic acid) cause AGMA, CNS
depression, and renal failure.
Precipitation of oxalic acid
metabolite as calcium salt in tissues
and urine results in hypocalcemia,
tissue edema, and crystalluria.
Initial ethanol-like intoxication,
nausea, vomiting, increased
osmolar gap, calcium oxalate
crystalluria; delayed AGMA,
back pain, renal failure; coma,
seizures, hypotension, ARDS in
severe cases
Sodium bicarbonate to correct
acidemia; thiamine, folinic acid,
magnesium, and high-dose pyridoxine
to facilitate metabolism; ethanol or
fomepizole for AGMA, crystalluria
or renal dysfunction, ethylene
glycol level >3 mmol/L (20 mg/dL),
and ethanol-like intoxication or
increased osmolal gap if level not
readily obtainable; hemodialysis for
persistent AGMA, lack of clinical
improvement, and renal dysfunction;
hemodialysis also useful for
enhancing ethylene glycol elimination
and shortening duration of treatment
when ethylene glycol level is
>8 mmol/L (50 mg/dL).
Iron Hydration of ferric (Fe3+) ion
generates H+
. Non-transferrinbound iron catalyzes formation
of free radicals that cause
mitochondrial injury, lipid
peroxidation, increased capillary
permeability, vasodilation, and
organ toxicity.
Initial nausea, vomiting,
abdominal pain, diarrhea;
AGMA, cardiovascular and
CNS depression, hepatitis,
coagulopathy, and seizures
in severe cases. Radiopaque
iron tablets may be seen on
abdominal x-ray.
Whole-bowel irrigation for large
ingestions; endoscopy and
gastrostomy if clinical toxicity
and large number of tablets are
still visible on x-ray; IV hydration;
sodium bicarbonate for acidemia; IV
deferoxamine for systemic toxicity,
iron level >90 μmol/L (500 μg/dL)
Methanol Methanol causes ethanol-like CNS
depression and increased serum
osmolality. Formic acid metabolite
causes AGMA and retinal toxicity.
Initial ethanol-like intoxication,
nausea, vomiting, increased
osmolar gap; delayed AGMA,
visual (clouding, spots,
blindness) and retinal (edema,
hyperemia) abnormalities;
coma, seizures, cardiovascular
depression in severe cases;
possible pancreatitis
Gastric aspiration for recent
ingestion; sodium bicarbonate to
correct acidemia; high-dose folinic
acid or folate to facilitate metabolism;
ethanol or fomepizole for AGMA,
visual symptoms, methanol level
>6 mmol/L (20 mg/dL), and ethanollike intoxication or increased osmolal
gap if level not readily obtainable;
hemodialysis for persistent AGMA,
lack of clinical improvement, and
renal dysfunction; hemodialysis
also useful for enhancing methanol
elimination and shortening duration of
treatment when methanol level is
>15 mmol/L (50 mg/dL)
Salicylate Increased sensitivity of CNS
respiratory center to changes in and
stimulates respiration. Uncoupling
of oxidative phosphorylation,
inhibition of Krebs cycle enzymes,
and stimulation of carbohydrate
and lipid metabolism generate
unmeasured endogenous anions
and cause AGMA.
Initial nausea, vomiting,
hyperventilation, alkalemia,
alkaluria; subsequent alkalemia
with both respiratory alkalosis
and AGMA and paradoxical
aciduria; late acidemia
with CNS and respiratory
depression; cerebral and
pulmonary edema in severe
cases. Hypoglycemia,
hypocalcemia, hypokalemia,
and seizures can occur.
IV hydration and supplemental
glucose; sodium bicarbonate
to correct acidemia; urinary
alkalinization for systemic toxicity;
hemodialysis for coma, cerebral
edema, seizures, pulmonary edema,
renal failure, progressive acid-base
disturbances or clinical toxicity,
salicylate level >7 mmol/L (100 mg/dL)
following acute overdose
CNS syndromes
Extrapyramidal
reactions
Antipsychotics (see
above), some cyclic
antidepressants and
antihistamines
Decreased CNS dopaminergic
activity with relative excess of
cholinergic activity
Akathisia, dystonia,
parkinsonism
Oral or parenteral anticholinergic
agent such as benztropine or
diphenhydramine
Isoniazid Interference with activation and
supply of pyridoxal-5-phosphate,
a cofactor for glutamic acid
decarboxylase, which converts
glutamic acid to GABA, results in
decreased levels of this inhibitory
CNS neurotransmitter; complexation
with and depletion of pyridoxine
itself; inhibition of nicotine adenine
dinucleotide–dependent lactate and
hydroxybutyrate dehydrogenases,
resulting in substrate accumulation
Nausea, vomiting, agitation,
confusion; coma, respiratory
depression, seizures, lactic and
ketoacidosis in severe cases
High-dose IV pyridoxine (vitamin B6
)
for agitation, confusion, coma, and
seizures; diazepam or barbiturates
for seizures
(Continued)
(Continued)
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