globus pallidus
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Transcript globus pallidus
Neurotoxicology
By: Laurence Poliquin-Lasnier
R4 Neurology
Outline
General principles
Terrestrial biotoxins
Metal intoxications
Organic chemicals intoxications
Marine Neurotoxins
General Principles
Peripheral neuropathy of the distal axonopathy type is the most common
presentation of North American neurotoxic disease
Detailed history is important to establish causative agent
Virtually all neurotoxic disease improves or stabilizes following withdrawal
from exposure
Progression of illness for years following removal strongly suggests the
condition is not due to an exogenous chemical
Laboratory data are available for heavy metals and drugs of abuse, but not for
most industrial or environmental agents and electrodiagnostic studies are nonspecific
Age and preexisting conditions (eg.: hereditary neuropathy) can increase
vulnerability to neurotoxic agents
Eg.: a person with Charcot-Marie-Tooth disease given vinca alkaloid tx may develop
an unusually severe neuropathy
Vulnerability of
peripheral nervous
system motor unit and
subcellular structures
Terrestrial biotoxins
1. Bacterial
2. Clostridial
3. Envenomation
4. Botanical
1-Bacterial toxin: Diphteria
Diphtheria is an acute, contagious disease caused by the grampositive bacillus Corynebacterium diphtheriae
There are two forms of symptomatic infection (respiratory and
cutaneous) and an asymptomatic carrier state
The respiratory form of diphtheria causes the characteristic
pseudomembranous pharyngitis
Other common complications of severe infection include myocarditis,
neuritis, and less often nephritis
C. diphtheriae solely lives in the mucous membrane and skin of
humans and infects via airborne respiratory droplets, direct contact
with respiratory secretions of symptomatic individuals, or infected
skin lesions
Asymptomatic carriers are an important mode of transmission
What is the most common severe complication of C. diphteria?
Diphteria
Acute demyelinating polyneuropathy >most common severe complication
Diphtheritic neuropathy is an uncommon
disease in Western Europe and the
United States due to vaccination
Large epidemic from 1990 to 1995 was
reported in the former Soviet Union
Fatality rate 2-3%
Diphteria
15% incidence of neurologic complications was reported in adults
Correlation between the severity of the diphtheritic polyneuropathy and the
severity of the diphtheria infection
Latency in development of diphtheritic polyneuropathy varies from 18 to 46
days from the initial infection (mean 30 days)
Approximately 2/3 of patients who developed a diphtheritic polyneuropathy
had a preceding serious diphtheria infection with both cardiac and renal
impairment
Neurologic manifestations of diphtheria are biphasic
Early bulbar disturbance (wks 3 to 5) with cranial neuropathies (ocular and lower CN
may be affected)
Late motor weakness in the trunk and extremities (wks 5 to 8)
Improvement in cranial nerves occurs with ongoing motor disturbance in trunk
and extremities
Diphteria
Weakness in the limbs can be both proximal and distal with
associated atrophy in severe cases
Paralysis of the diaphragm and respiratory failure can occur
Sensory disturbances in all modalities with paraesthesias of
distal extremities and often a sensory ataxia
Hypotonia, hyporeflexia, and downgoing plantar responses
Significant abnormalities of parasympathetic and
sympathetic function are often present and more common
with severe cases
Diphteria
Pathogenesis: paranodal
demyelination and
segmental demyelination
both at ventral and dorsal
spinal roots and peripheral
nerve
Diphteria
Large DDx
Diagnosis: Isolation of C. diphtheriae on culture with
toxigenic testing with nasopharyngeal swab from the
patient and his/her contacts
C. diphtheriae requires special culture median containing
tellurite
Elek test is performed to determine if the bacillus
produces toxin and is an important test in the diagnostic
process
Measurement of serum antibodies to diphtheria toxin may
also help assess the probability of diphtheria
PCR available for confirmation
NCS: demyelinating
Diphteria
Treatment:
Antibiotic therapy in combination with antitoxin
administration within 48 hours of diagnosis to decrease
the chances of developing diphtheritic polyneuropathy
Antitoxin does not neutralize toxin that is already bound
to tissues -> delaying its administration is associated
with an increase in mortality risk
Antibiotics to eradicate and avoid transmission
Case #1
57-year-old farmer was admitted to the hospital with a 1week history of right lower extremity muscular rigidity that
over a period of a week started to spread to his axial
muscles including the neck, back, and abdominal muscles
He reported stepping on a nail in the barn 2 weeks prior to
the onset of symptoms and still had an open festering
wound at the puncture site
He then developed laryngospasms that led to respiratory
compromise requiring intubation
His sensorium remained clear
Diagnosis?
2- Bacterial toxin: Clostridial->
Tetanus
Clostridium tetani
Anaerobic, gram positive rod
Metabolizes in anaerobic conditions and reproduces via
spores that can survive in aerobic conditions
The spores are the common mode of transmission
The bacterium survives in soil and in the intestines and
feces of animals, from which the spore invades the body
through seemingly insignificant wounds and subsequently
multiplies
Tetanus
Early manifestations of generalized tetanus include rigidity of the masseter muscles (trismus aka lockjaw)
and of facial muscles with a distinct straightening of the upper lip causing a grimacing posture to the face
(risus sardonicus)
Frequent localized stiffness near the site of the penetrating wound followed by rigidity of the axial muscles
involving the neck, back muscles (opisthotonus), and abdomen
With progression, extremities become stiff with relative sparing of the distal muscles
Spasms can be significant enough to break long bones of the extremities
Paroxysmal reflex spasms can occur in severe cases, generally in response to voluntary movements or to
external and internal stimuli
In severe cases, muscles of deglutition may also go into trismus, causing dysphagia and dysarthria ->
laryngospasms can lead to respiratory compromise and asphyxia
Over a period of approximately 2 wks, the severity of symptoms can worsen, and by 4 weeks recovery
usually begins
A hypersympathetic state may be a manifestation of more severe cases with fluctuations of BP and HR
Profuse sweating, high fever, and hypersalivation are also common signs of autonomic instability
Tetanus
Neonatal tetanus usually occurs in the generalized form and
tends to carry a high mortality rate
The most common symptoms of neonatal tetanus are a
failure to suck and muscular twitching
Neonatal tetanus generally develops in the first 2 wks of life
in children born to mothers who have been poorly
immunized
These infants often have umbilical stump infections
In some underdeveloped countries, some practices occur in
the birthing process that put infants at risk, including the
application of clarified butter with contaminated dung fuel on
umbilical cords
Tetanus
Pathogenesis:
Tetanus is transported to the
spinal cord from the
neuromuscular junction and
then transported by
transcytosis to the inhibitory
Renshaw cell and to the
upper motor neurons
Blocks the release of glycine
and GABA from inhibitory
neurons, leading to spastic
paralysis -> no relaxation of
the antagonistic muscle
during normal contraction
Tetanus
Diagnosis: Clinical
Positive spatula test on physical: reflex spasm of the masseter muscle on
touching the posterior pharyngeal wall
Continuous, spontaneous motor unit discharges on EMG reported but not
diagnostic of tetanus
In some serious cases, elevated CSF protein and immunoglobulin levels have
been documented
C. tetani can be cultured in about 1/3 of confirmed cases from wounds
PCR assays for neurotoxin gene fragments available
The presence of serum antitoxin of 0.01 unit per mL or higher is considered
protective and makes a diagnosis of tetanus unlikely
Prognosis: related to degree of autonomic instability and type of wound/injury.
Burns, infected umbilical stumps, and compound fractures are frequently
related to a poor prognosis
Tetanus
Treatment: elimination of the source of toxin, toxin neutralization, control of
muscle rigidity and spasms, and ventilatory support
If no wound is found, careful examination for signs of parenteral drug abuse,
otitis, and careful rectal and vaginal examinations are recommended
A retained foreign body may result in continuous toxin production
Although controversial, the use of metronidazole (500 mg IV every 6 hours for
7 to 10 days) is the drug of choice
Penicillin has a central GABA antagonistic effect and can worsen spasms
Administration of human tetanus immunoglobulin is recommended before
manipulating a wound -> recommended dose is 500 units IM
Combined intrathecal (1000 units) and IM antitetanus immunoglobulin
administration gives better clinical outcomes than IM administration alone
Bacterial toxins
Another clostridial toxin -> clostridium botulinum
(covered in neuromuscular talk) with the typical
descending flaccid paralysis
Anthrax (Bacillus anthracis) -> hemorrhagic
meningoencephalitis
3-Envenomation/Snake
With the exception of the coral snake, all the venomous snakes in the United
States are pit vipers (rattlesnakes, cottonmouths, and copperheads)
The incidence of venomous snake bites in the United States is approximately
7000 to 8000 per year, but only 5-6 result in death
Confident diagnosis of a venomous snakebite requires a positive identification
of the snake and recognition of the clinical manifestations of the
envenomation
Rarely a snake will be brought in alive or dead for inspection at the clinic
Caution should be taken handling dead snakes as a bite reflex can occur even
after the death
Envenomation does not always occur with venomous
snakes (25% of all viper bites are dry)
3-Envenomation/Snake
Toxins
α-Bungarotoxin and cobrotoxin: postsynaptic blockade of
acetylcholine receptors (AChRs)
β-Bungarotoxin and crotoxin: presynaptic inhibition of acetylcholine
(ACh) release
Local pain, swelling, and erythema at site of the bite
Focal weakness or compartment syndrome
Diffuse proximal weakness resembling myasthenia gravis
Ptosis, cranial neuropathies, myokimia, dysphagia, areflexia,
fasciculations, respiratory distress
Systemic manifestations, including hypotension and shock
3-Envenomation/Snake
With pit viper envenomations, incision and suctioning at
the bite site within minutes can remove venom
Antivenin, most effective when given within 4 hrs of bite
Beware of anaphylactic reaction
3- Envenomation/Scorpion
Tityustoxin, produced by Tityus serrulatus,
causes presynaptic facilitation of ACh release
and postsynaptic activation of voltage-gated
sodium channels
Local pain and erythema at site of the bite
Excess cholinergic activity: salivation,
lacrimation, urinary incontinence, defecation,
gastroenteritis, and emesis (SLUDGE)
Local paresthesias, followed by diffuse
paresthesias (thalamic involvement) ,
fasciculations, tremors, hyperreflexia, ptosis,
nystagmus, blurred vision, dysarthria, and
dysphagia
Pandysautonomia: hypertension, hyperthermia,
hypersalivation, diaphoresis, urinary frequency,
fecal urgency
3- Envenomation/Scorpion
Treatment: supportive care
Anti-venin
With the use of Centruroides antivenin, moderate to
severe neurologic symptoms may reverse in 15 to 90
minutes
3- Envenomation/Female
black widow spider
(Latrodectus mactans)
Most important spider to cause potentially significant
morbidity
Poorly lighted area-> often sting genitalia
Toxin: α-latrotoxin, causing presynaptic facilitation of
ACh release and depletion of Ach
Erythema at site of the bite, intense pain, and
involuntary muscle spasms involving the limbs, trunk,
and diaphragm (latter causing respiratory arrest),
dysarthria, chest pain
Autonomic symptoms: hypertension, piloerection,
diaphoresis, brochospasm
Acute symptoms increase in severity during the first day
after a bite. Most symptoms generally decline after 2 to
3 days, but some mild residua may continue for several
wks
Tx: antivenin
Case #2
12-year-old girl presents to the ER with progressive gait instability, ascending weakness,
shortness of breath on exertion, slurred speech, and swallowing difficulties over 3 days
No GI or pulmonary symptoms, nor fever preceding the onset of symptoms
On examination, she was alert with some facial weakness, dysarthria, and diffuse 3-4/5
weakness worse in the legs than the arms
Reflexes were absent, and she had no sensory abnormalities
A neurologist saw the patient in the ER and thought Guillain-Barré syndrome was likely
CSF analysis and NCVs including repetitive stimulation were normal, except for lowamplitude CMAPs, making the diagnosis of Guillain-Barré syndrome unlikely
A careful examination of the patient with a comb revealed a tick at the nape of her neck.
Within hours of its removal, the patient started to get better and eventually made an
uneventful recovery within a week
Diagnosis?
3- Tick paralysis
Results from inoculation of toxin contained in the tick saliva at the
time of a blood mea
Tick paralysis is associated with over 40 species of tick worldwide,
including five species in North America; yet only four tick species
cause human disease
The tick species responsible for most cases of human tick
paralysis in the United States and Canada are Dermacentor
andersoni (the Rocky Mountain wood tick), and Dermacentor
variabilis (the American dog tick)
Other areas of the body involved include the nose, ear canals, and
genital area
The incidence is most frequent in spring and summer
3-Tick paralysis
Acute ascending paralysis over days without sensory symptoms
Unlike Lyme disease, symptoms regularly resolve after tick is removed
Symptoms usually begin 2 to 6 days after the tick becomes attached
Constitutional symptoms such as fever are lacking, but generalized fatigue is not an
uncommon initial symptom
Often mistaken for GBS-> Gait instability -> falling -> total inability to walk is a common
presentation over a couple of days and may quickly involve respiratory muscles and
cranial and bulbar muscle -> intubation
Weakness worse in the LE and ass. with hypotonia and hypo/areflexia
Isolated facial weakness has been described, although more diffuse involvement of the
cranial nerves leading to ophthalmoplegia, dysarthria, and dysphagia is more common
Reports in children of ataxia, mild encephalopathy, minor sensory disturbances
3- Tick paralysis
Pathogenesis not entirely understood but thought to block
axonal Na+ channels and to inhibit the release of ACh at
presynaptic motor nerve terminals, causing total neuromuscular
blockade
EMG/NCVs are well described and suggest axonal involvement
with evidence of denervation
CMAPs are of low amplitude and improve with the removal of
the tick as does the clinical status
Treatment: Remove the tick
Coating the tick with petroleum jelly to make it release its hold
is helpful and one should attempt to grasp the tick as close to
skin as possible and make sure to remove all of the tick's
capitulum (head)
Detection and removal of the tick usually results in rapid
improvement (hours to 1 or 2 days) in the patient's condition
Antiserum is generally neither recommended, nor necessary
4- Botanical toxin:
Amanita mushrooms
After consumption, there are initially no signs of toxicity, but a severe gastroenteritis
ensues after about 6 to 12 hrs with N/V, abdo cramping, and diarrhea
For the next 24 to 48 hrs, the patient may improve clinically, giving a sense of false hope
as during that time renal and hepatic function deteriorate
Toxicity begins upon active transport into hepatocytes where it binds to and inhibits RNA
polymerase II, leading to inhibition of protein synthesis and ultimately hepatocyte death
Hepatotoxicity and renal failure develop in the next 3 to 5 days, followed by secondary
metabolic encephalopathy
Neurologic compromise may be related to direct effects of α-amatoxin and indirect
effects of brain edema from liver failure
The key psychoactive constituents in these mushrooms are ibotenic acid, muscimol, and
muscazone
The GABA receptor agonist, muscimol, is somewhat sedating, Ibotenic acid binds to
glutamate receptors and induces an agitated delirium
Tx: supportive
Outline
General principles
Terrestrial biotoxins
Metal intoxications
Organic chemicals intoxications
Marine Neurotoxins
Metal intoxication
Arsenic
Lead
Manganese
Mercury
Industrial/environmental
toxins
A few caveats…
General
principles of
industrial and
environmental
toxins
Case #3
A 62-year-old woman was evaluated for a 3-year history of slowly
progressive, ascending, distal lower limb paresthesias. She was
on no medications and did not give a history of potential toxic
exposure. Her examination was remarkable for decreased
perception of vibration and position at the toes and a graded
decreased perception of pinprick and touch distal to the mid-shin
level. Her ankle jerks were absent. No other abnormalities were
noted on her general and systemic examination. Nerve
conductions studies revealed an axonal, symmetric, lengthdependent, predominantly sensory PN. Extensive investigations
examining various causes of neuropathy were unrewarding. A
urine heavy metal screen was, however, remarkable for a 24-hour
arsenic excretion of 862 μg (normal: less than 120 μg/24 h)
What’s your diagnosis?
Case #3
Elevation in urinary arsenic excretion is sometimes due to
the organic, nontoxic form resulting from prior seafood
ingestion
Within hours of seafood ingestion total urinary arsenic
concentration may be in the range of 100 μg/L to 10,000
μg/L
Seafood should be avoided for 3 to 4 days prior to a urine
arsenic determination
This patient admitted to seafood ingestion during and prior
to the urine collection and a repeat collection was normal
Arsenic
May be due to poisoning or man-made sources (eg.: metal
smelting, mining, abrasive blasting, pesticide manufacturing,
combustion of coal, and burning of agricultural wastes, burning of
chromated copper arsenate-treated wood in fireplaces or wood
stoves), found in tap water in Bangladesh
Arsenic is also used in the ceramic industry and manufacture of
semiconductors, light-emitting diodes, transistors, lasers, computer
microchips, and microwave circuits
Shortly after ingestion, arsenic is stored in reticuloendothelial
system, kidney and intestines and is slowly released
Slow excretion via kidney and feces
Deposited in hair within 2 wks and remains in hair for years
Arsenic
Clinical features
Acute or subacute exposure: abdo pain, nausea, vomiting,
hyperthermia, headaches, anxiety, vertigo, possibly seizure,
encephalopathy
Fatal acute poisoning: precipitous development of lethargy and coma
followed by death in few days, may be due to diffuse edema and/or
hemorrhagic encephalopathy
Low-dose chronic exposure: similar clinical features but much less
severe (abdo pain, vertigo, longstanding cognitive disturbance, persistent
headaches and development of peripheral neuropathy
Optic neuropathy: possible delayed manifestation
Metallic taste
Mee’s lines: white lines in nails, usually appear 2-3 wks after exposure
Peripheral neuropathy
Painful, distal, axonal, may mimic GBS in severe cases
Glove-stocking distribution with involvement of small and large fibers leading
to pseudoathetosis and allodynia
Distal weakness
Hypo/areflexia
Associated with exfolliative dermatitis
Arsenic
Diagnosis:
24h urine heavy metal arsenic level (may be falsely elevated
by shellfish ingestion), serum levels unreliable
Increased arsenic levels in nail clippings or pubic hair
(preferable to scalp as less chance of environmental
contamination)
Treatment
Acute: supportive (hydration, pain control, gastric lavage)
Chelation therapy with dimercaprol or its water soluble
derivative dimercaptosuccinic acid (DMSA); or penicillamine
(best if started early)
Inorganic lead
Children absorb lead more effectively than adults
Lead reaches bones, teeth, and soft tissue, and long-term storage occurs in
the skeletal system
Bone resorption causes reentry of lead into the blood stream with the potential
of causing delayed deleterious effects
Pregnancy, lactation, menopause, osteoporosis, and other events that lead to
increased bone resorption may lead to increased blood level in individuals
with substantial amount of lead stored in bone
Found in old paints, drinking water through dissolution of lead in old plumbing,
manufacture of lead-acid batteries, battery recycling plants, crushing and
smelting of lead and other metal ores, radiation shielding, blasting and
sanding of lead-coated surfaces, and soil contaminated from vehicle exhaust
and industrial emissions, ammunition, cosmetics
Inorganic lead
Children
Acute intoxicatio(90 μg/dL): acute GI illness, confusion,
lethargy, seizures, coma, and respiratory arrest with
high levels of exposure
Chronic, low-level exposure (10 μg/dL): gradual onset
of listlessness, behavioral changes, psychomotor
slowing, sleep disturbance, seizures, gait disorder
characterized by clumsiness or frank ataxia
Inorganic lead
Adults
Polyneuropathy: predominantly motor neuropathy, with
distal weakness, atrophy, and fasciculations (pain
uncommon)
Motor manifestation may be more prominent in upper
extremities: may present with bilateral wrist drop, with or
without distal lower limb weakness, often asymmetric
Motor neuropathy commonly involves radial nerve
(wristdrop is most common)
There may or may not be sensory symptoms,
predominantly paresthesias (allodynia and dysesthesias
are uncommon)
Inorganic lead
Laboratory diagnosis
Microcytic, hypochromic anemia
Basophilic stippling of red blood cells on blood smear
Renal insufficiency, azotemia
Elevated blood levels of lead
Lead interferes with hemoglobin synthesis by inhibiting the enzymes δaminolevulinic acid dehydratase and ferrochelatase and results in
elevated free erythrocyte protoporphyrin (FEP) which is more accurate
than serum lead levels for chronic toxicity but because of poor
sensitivity, serum lead level is still the preferred screening method
Treatment: chelation with DMSA, intravenous calcium disodiumEDTA, or penicillamine
Manganese
Exposure
Primary source of exposure (occupational): miners, ferromanganese
smelting plant workers, workers in manganese ore-crushing plants,
welders, and those involved in the manufacture of dry batteries
Patients receiving total parenteral nutrition containing manganese
Pathology: neuronal loss and gliosis affecting the globus pallidus and
subthalamic nucleus; uncommon involvement of substantia nigra
Main source of disposal is biliary excretion: patients with biliary atresia or
chronic liver disease are prone to develop manganese toxicity (may explain
high T1 signal in pallidum observed in chronic liver disease)
Mechanism: oxidative stress generated through mitochondrial perturbation,
NMDA-mediated excitotoxicity, and disruption in iron metabolism
Manganese
Clinical features
Onset of symptoms may occur early (1-2 months after
exposure) or may be delayed (about 20 years after
exposure)
Headaches, neuropsychiatric manifestations (memory
disturbance, hallucinations, aggressive behavior, apathy,
irritability, social withdrawal, personality changes, and
psychosis, referred to as “manganese madness”)
Extrapyramidal symptoms: parkinsonism
Hypophonic and monotonous speech
Absence of typical parkinsonian rest tremor, but there may be a
fine, low-amplitude, high-frequency tremor
Gait: retropulsion, propulsion, often tendency to walk on toes
with elbows flexed and erect posture
Manganese
Symmetric abnormally increased signal in the globus pallidus (A) and
substantia nigra (B) (may be transient)
The typical finding is really the increased pallidal signal
Manganese
Diagnosis:
Manganese can be detected in blood for days to weeks
after exposure ceases
Manganese levels in urine and feces may be used as a
marker for exposure within the previous few hours
Brain MRI: high T1 signal in the globus pallidus (also
striatum and midbrain) bilaterally because of manganese
accumulation
Treatment:
Levodopa: partial to no benefit
Chelation with EDTA: improvement in some patients
Mercury
Inorganic Mercury
Acute intoxication: acute colitis, vomiting, renal failure,
stomatitis, little cognitive impairment except for irritability and
delirium with acute poisoning
Chronic, low-grade toxicity: tremor, peripheral neuropathy
Personality changes, anxiety, but little cognitive impairment
Peripheral neuropathy: sensorimotor axonopathy,
associated with sensory loss, sensory ataxia, pain,
paresthesias, distal weakness, atrophy
Organic Mercury
Methylmercury: better penetrance of blood-brain barrier
Predilection for dorsal root ganglia, calcarine cortex,
and cerebellar granular layer (may also affect parietal
cortex)
Organic Mercury
Clinical features
Classic triad: gingivitis, tremor, and a neuropsychiatric illness
Cerebellar and sensory ataxia
Peripheral neuropathy
Cortical blindness from involvement of the calcarine cortex
Sensory disturbance due to involvement of dosal root ganglia
and sensory cortex
Deafness, dysarthria
Choreoathetosis
Motor neuron syndrome resembling ALS, with both LMN
features (atrophy and fasciculations) and UMN features
(hyperreflexia)
Cognitive impairment (“mad as a hatter”): short-term memory
loss, depression, hallucinations, other features of psychosis
Organic Mercury
Diagnosis
Because of the distribution of mercury throughout the body,
blood mercury levels are not reliable indicators of excessive
mercury burdens
Blood mercury levels are recommended for acute intoxications
(as elevations in blood levels will precede elevations in urine
levels) and for suspected organic poisoning
Urinary mercury concentrations correlate well with exposure to
elemental or inorganic mercury but poor correlation with clinical
severity
Treatment:
Chelation with penicillamine or DMSA
Check fish consumption
Outline
General principles
Terrestrial biotoxins
Metal intoxications
Organic chemicals intoxications
Marine Neurotoxins
Organic chemicals
intoxication
Acrylamide
Hexacarbon solvents
Carbon disulfide
Carbon monoxide
Toluene
Trichloroethylene
Methanol
Organophosphate
Acrylamide
Monomeric acrylamide (not polyacrylamide) is neurotoxic
Found in ore processing, wastewater management, gel
chromatography and in the production of polyacrylamide
Acute intoxication with severely high exposure: seizures,
encephalopathy
Chronic, moderately high exposure: gradual onset of
encephalopathy and peripheral neuropathy
Chronic, low-grade exposure: peripheral neuropathy
Acrylamide
Features of peripheral neuropathy
Predominantly axonal, distal neuropathy
Preceded by skin irritation and peeling
Neurotoxicity may occur in abnormalities of axonal (retrograde)
transport; accumulation of neurofilaments and axonal loss are
evident in sural nerve biopsy specimens
Predominantly sensory neuropathy, involving both small and
large fibers
Reduced proprioceptive and vibratory sensation, sensory
ataxia, hyporeflexia, numbness, paresthesias, incoordination
Motor involvement (distal weakness) may be present with
repetitive, high-grade exposure
Hexacarbon solvents (n-hexane and
methyl n-butyl ketone)
Both converted to 2,5-hexanediol, which is toxic to peripheral nerve
axons and affects axonal transport (hence, giant multifocal axonal
enlargements from accumulation of neurofilaments)
Used as paint, varnish, and glue (exposure may occur in person
sniffing glue)
Acute exposure: euphoria, hallucinations, headaches
(encephalopathy does not occur)
Progressive sensorimotor peripheral neuropathy with slowed
conduction velocities on electrodiagnostic testing, may look like
GBS if severe
Despite cessation of exposure, continued progression may occur
for wks (coasting) prior to arrest and significant subsequent
improvement
Carbon disulfide
Used in manufacturing rayon and cellophane
Primary route of intoxication: inhalation (or ingestion)
Acute inhalation of large amounts of the compound can produce
encephalopathy (varying severity)
Sensorimotor peripheral neuropathy with chronic exposure:
predominantly sensory involvement, with paresthesias and numbness
and some motor involvement
Cranial nerve involvement with vestibular, auditory, and ocular
symptoms has also been observed
Long-term exposure could also possibly cause: minor affective or
cognitive disorder, pyramidal or extrapyramidal symptoms
(parkinsonism), optic neuropathy
Diagnosis: urine metabolite 2-thiothiazolidine-4-carboxylic acid
Carbon monoxide
Pure form: odorless, colorless gas
Produced by combustion of carbon-based fuels
Mechanism of action:
Binds to hemoglobin with greater affinity than oxygen
(forming carboxyhemoglobin), competes with binding of
oxygen to hemoglobin
Prevents oxygenation of tissues
Severity of clinical presentation depends on
concentration of the gas in the exposed environment
and duration of exposure
Carbon monoxide
Clinical features of acute intoxication may range from headaches, nausea,
dizziness to confusion, encephalopathy, pyramidal and extrapyramidal
symptoms, seizures, coma, death
Survivors of acute intoxication who have partial or complete recovery may suffer
from delayed deterioration and recurrence of the aforementioned symptoms;
some may progress to persistent vegetative state
The classic cherry-red discoloration of the skin and cyanosis are rarely seen
Pathology of acute or subacute stage: diffuse cerebral edema, scattered
petechial hemorrhages in white matter and more prominent hemorrhagic foci in
the globus pallidus bilaterally
Pathology of chronic stage: necrosis and cavitation of the globus pallidus,
confluent foci of necrosis in subcortical white matter
Carbon monoxide
CO poisoning = MRI lesions involving globus pallidus and cerebral deep WM
A) Symmetric high signal intensity lesions in bilateral globus pallidi
B) MRI in same pt as in A reveals high signal lesions in bilateral substantia nigra (dotted
arrow) in addition to bilateral pallidal lesions
C) MRI obtained 2 months after exposure shows confluent high signal lesions in the
bilateral periventricular deep white matter
Toluene
Used as solvent in paint, varnishes, thinners, glues, dyes;
used to synthesize benzene
Acute intoxication: encephalopathy with euphoria,
incoordination and ataxia, confusion, headache
Chronic use: euphoria, disihnibition, memory and attentional
deficits, tremor, cerebellar symptoms, optic neuropathy and
other cranial neuropathies
Exposure to high concentrations may lead to bone marrow
suppression
Diagnosis: hippuric acid (urine metabolite)
Trichloroethylene
Industrial solvent
Typical presentation with high-level exposure: cranial
neuropathies, especially trigeminal neuropathy
Trigeminal neuropathy: typically facial numbness, followed
by weakness of muscles of mastication
There may also be ptosis, weakness of muscles of facial
expression, abnormalities of extraocular movements
Other nonspecific symptoms: headaches, dizziness, fatigue,
insomnia
Methanol
Causes necrosis of optic nerves and putamina bilaterally
Acute intoxication
Presentation often delayed for several hours until methanol is
metabolized to formaldehyde and formic acid
Headache, dizziness, nausea, blurred vision
Permanent visual loss may occur
Parkinsonism
Severe effects: encephalopathy, seizures, cardiopulmonary
failure, coma, death
Pathology: likely caused by formate metabolites, hypoxemia, and
metabolic acidosis
4-Methyl-1H-pyrazole (fomepizole) may be used to treat patients
>12 years: acts as effective inhibitor of alcohol dehydrogenase
Methanol
Abnormal signal in bilateral putamen
Organophosphates
Mainly used in insecticides but also in fuel additives,
hydraulic fluids, and lubricants
Acts as ACEI
Absorbed through GI or respiratory tract or skin
Organophosphate
*In 20% of pts
*May occur without the other
phases
Outline
General principles
Terrestrial biotoxins
Metal intoxications
Organic chemicals intoxications
Marine Neurotoxins
Marine neurotoxins
Ciguatera fish poisoning
Paralytic shellfish poisoning
Neurotoxic shellfish poisoning
Amnestic shellfish poisoning
Pufferfish poisoning
Case #4
A 48-year-old woman vacationing in Jamaica for 1 month beginning in June ate local fish
daily. After 3 weeks, she and her father both developed nausea and emesis within a few
hours of eating a large, cooked barracuda
That afternoon, she began having fatigue and pruritus without rash, involving chest,
arms, and thighs. Sensation to pinprick and temperature were grossly intact by selfexamination (patient is a physician)
By the next morning, she was experiencing burning sensations in her hands and feet
bilaterally. Standing barefoot on cool floor tiles was perceived as burning pain. The
burning sensations in her hands increased with holding them under cool running water.
Drinking cold beverages caused burning sensations of her mouth and tongue
By the fifth day, the pruritus, burning dysesthesias, and paradoxical perceptions of
temperature had resolved, although her fatigue persisted, somewhat worse than usual
(past history of multiple sclerosis)
Neurologic examination after she returned home 3 weeks later was without significant
change from prior examinations (baseline generalized hyperreflexia due to multiple
sclerosis). Cerebral MRI showed no actively enhancing plaques. A few more white matter
hyperintensities were noted as interval change from her last MRI obtained 3 years before
Should you be worried? Is this MS exacerbation or intoxication?
Case #4
Typical case of ciguatera poisoning
Barracuda are reef predators
Release of CTX by the microorganisms on the reef is more likely to occur in
the warmer summer months
The onset of GI symptoms in both the patient and her father implicates the
shared fish ingestion as the source of the gGI symptoms
The principal initial differential diagnoses would be scombroid toxicity (spoiled
fish) or a relapse of her MS
The occurrence of pruritus without rash distinguishes ciguatera from
scombroid toxicity
The emergence of sensory symptoms the next day, with paradoxical thermal
perceptions, is clinically confirmatory of an ingested fish toxin such as CTX
and distinguishes her sensory symptoms from a demyelinative etiology
Ciguatera fish poisoning
Most common nonbacterial form of food poisoning
related to seafood ingestion in the United States,
Canada, and Europe
Caused by ciguatera toxins produced by dinoflagellates
in different species of reef fish
Ciguatoxins: increase sodium permeability via
tetrodotoxin-sensitive voltage-gated sodium
channels in nerves and muscles, causing membrane
depolarization
Maitotoxin: increases calcium permeability of
voltage-gated calcium channels
Ciguatera fish poisoning
Clinical symptoms at onset: abdo pain and cramps,
hypersalivation, nausea, vomiting, diarrhea
Neurologic manifestations typically follow: dysesthesias of
extremities, spreading paresthesias (including circumoral),
pruritis (either generalized or on palms and soles)
Other: inverted sensory phenomenon (e.g., cold objects feel
warm), sensation of having loose teeth, headache, vertigo,
dizziness, dry mouth, metallic taste
Cardiovascular manifestations: hypotension, bradycardia,
hypertension, tachycardia, arrhythmias, heart block, pulmonary
edema, congestive heart failure
Most symptoms remit in 1 week after exposure, but certain
symptoms may persist for years after original exposure
Paralytic shellfish poisoning
Caused by saxitoxins and related compounds from dinoflagellates
found in certain shellfish
Toxin blocks voltage-dependent Na+ channels in nerve and
muscle
Abrupt onset (within 30-60 min after ingestion) of symptoms:
paresthesias of face, tongue, perioral areas, and lips; vertigo;
dysarthria; ophthalmoplegia; pupillary abnormalities; ataxia
Weakness does not occur in every patient (despite name): when
present, may involve the limbs, cranial musculature, swallowing,
and respiratory muscles
Lack of GI illness at onset: toxin has some anticholinergic activity
and may act to slow gastric emptying; this, together with absence
of emesis, may enhance absorption of the toxin
Neurotoxic shellfish poisoning
Caused by brevetoxins, polyether neurotoxin produced by
the marine dinoflagellate Karenia brevis and found in
shellfish
Brevetoxins
Potent lipid-soluble neurotoxins that bind to sodium channels
on nerve and muscle cell membranes
Produce excessive influx of sodium ions across mem- branes,
causing cellular dysfunction or death
Similar to, but less severe than, ciguatera
Onset of symptoms: minutes to several hours after ingestion
of contaminated food
Neurotoxic shellfish poisoning
Illness begins with GI symptoms: nausea, vomiting,
diarrhea, abdo pain and cramping, rectal burning
Neurologic manifestations occur concurrently with GI
illness:
Circumoral paresthesias progressing to involve pharynx,
torso, and extremities
Muscle weakness; myalgias; tremor; dysphagia;
mydriasis
Inverted temperature sensory phenomenon (as with
ciguatera fish poisoning)
Diagnosis: ELISA assay
Amnestic shellfish poisoning
Caused by domoic acid: glutamate receptor agonist, excitatory
neurotoxin acting on various CNS glutamate receptors, especially
those of hippocampus
Domoic acid: found in shellfish, including certain species of mussel
Initial GI symptoms, usually within first 24 hours after ingestion:
nausea, vomiting, abdominal cramps, diarrhea
Neurologic symptoms within 48 hours after ingestion: seizures,
hemiparesis, ophthalmoplegia, neuropathy, altered mentation,
coma
Memory impairment: anterograde and, less common but more
severe, retrograde
Gradual improvement over 3 months
Pufferfish poisoning
Most cases associated with consumption of pufferfish from waters of Indo-Pacific ocean
regions
Due to tetrodotoxins in various fish, including puffer fish; block voltage-gated Na+
channels
First symptom of intoxication: perioral paresthesias, appearing 20 minutes to 3 hours
after consuming contaminated food
Paresthesias spread to face and limbs
Other symptoms: headaches, sensation of floating, epigastric pain, nausea/vomiting,
diarrhea
Following these symptoms: paralysis
May be respiratory distress, dysarthria, dyspnea, convulsions, altered mentation, and
death within 4 to 6 hours
Coma and seizures may occur, High mortality rate
Death may be due to cardiac arrhythmias or respiratory paralysis; patients may remain
completely alert and lucid until death
Conclusion
General principles
Peripheral neuropathy is the most common presentation of
North American neurotoxic disease
Detailed history is important to establish causative agent
Virtually all neurotoxic disease improves or stabilizes following
withdrawal from exposure
Terrestrial biotoxins
Diphteria -> GBS like, anti-toxin + antibx
Tetanus -> spasms, trismus, anti-toxin before you wash the
wound, think about umbilical stumps in children as a source
Envenomation -> don’t play with vipers, scorpions or spiders
Tick paralysis -> GBS like
Conclusion
Metal intoxications
Manganese = increased T1
signal in the globus pallidus
Organic chemicals intoxications
Most organic chemicals are
solvents that cause
encephalopathy
CO poisoning = increased T2 in
globus pallidus and cerebral
deep WM
Methanol = increased T2 signal
in putamen, visual loss
Marine Neurotoxins
Often cause unusual
paresthesias and may lead to
paralysis
References
Neurotoxicology continuum
Mayo clinic board review