CCP 222 Toxicology ☠️

Question 1

GOLDMARK (anion gap mnemonic)

a new mnemonic recommended to replace MUDPILES for causes of anion-gap metabolic acidosis

Answer 1

G - Glycols (ethylene glycol, propylene glycol)
O - Oxoproline (acetaminophen ingestion)
L - L Lactate
D - D Lactate (short bowel, propylene glycol)
M - Methanol
A - ASA
R - Renal failure
K - Ketoacidosis (DKA, starvation, alcoholism)

Question 2

causes of NAGMA

💵💵💵💵 MONEY SLIDE 💵💵💵💵

Answer 2

1. GI (diarrhea, pancreatic fistula)
2. Renal (RTA I, II, IV)
3. Too much N/S (hyperchloremic)

Question 3

causes of AGMA (KULT)

💵💵💵💵 MONEY SLIDE 💵💵💵💵

Answer 3

1. Ketones (starvation, DKA, alcoholism)
2. Uraemia
3. Lactate (L and D lactate)
4. Toxins (ASA, methanol, ethylene glycol, toluene)

Question 4

At what point do we intubate profound metabolic acidosis?

What indicates that someone with a metabolic acidosis is “failing”

💵💵💵💵 MONEY SLIDE 💵💵💵💵

Answer 4

When they start to develop a superimposed respiratory acidosis

Question 5

Steps to preparing a bicarb infusion

🔥🔥🔥MEGA PEARL🔥🔥🔥

Answer 5

1. Draw out 30cc of D5W from a 1L bag
2. Put 3 amps of NaHCO3- in to replace it
3. Standard infusion rate = 250mL/hr

this shit HAS to be in D5W. if you use 0.9% Saline or LR you will create a HYPERTONIC SOLUTION because the Na+ content will be too high. you will fuck up your patient

Question 6

key physical findings when differentiating a toxic exposure (characterizing a toxidrome)

Answer 6

1. odors
2. Pupillary findings
3. Neuromuscular abnormalities
4. Mental status alterations
5. Skin findings
6. Temperature alterations
7. Blood pressure and heart rate alterations
8. Respiratory disturbances

Question 7

what is covered on a “urine drug screen”

Answer 7

1. Amphetamines
2. Cocaine
3. Marijuana
4. Opiates
5. Phencyclidine (PCP)

Question 8

the guiding principle of medical toxicology

Answer 8

“treat the patient, not the poison”

Supportive care is key

Question 9

Delirium tremens clinical findings

Answer 9

1. Delirium
2. agitation
3. tachycardia
4. hypertension
5. fever
6. diaphoresis

Question 10

Delirium tremens time of onset from last drink

Answer 10

48 to 96 hours

Question 11

Alcohol withdrawal seizures time of onset from last drink (different from full blown DT’s)

Answer 11

6 to 48 hours

Question 12

fomepizole MOA

Answer 12

1. Fomepizole prevents the formation of toxic alcohol metabolites via inhibition of alcohol dehydrogenase (primary enzyme involved in alcohol metabolism)
2. toxic alcohols themselves aren’t toxic, it’s their metabolites/breakdown products

Question 13

primary treatment for toxic alcohol poisoning

Answer 13

1. Inhibition of alcohol dehydrogenase through either fomepizole or ethanol
2. this prevents the development of toxic acid metabolites

Question 14

How to set up a Bicarb infusion for profound metabolic acidosis

Answer 14

1. mix sodium bicarbonate 8.4% 3 ampules (150 mEq) in 1L of D5W
2. infuse at 250 mL/hour

Question 15

primary toxic metabolite of methanol

Answer 15

1. formate (derived from formic acid)

Question 16

primary toxic metabolites of ethylene glycol (there’s three… 💎💎💎)

Answer 16

1. glycolate
2. glyoxylate
3. oxalate

Question 17

harmful manifestations of methanol poisoning

Answer 17

1. blindness due to direct toxicity at the optic nerves

2. profound anion gap metabolic acidosis

Question 18

major manifestations of Ethylene glycol poisoning

Answer 18

1. acute kidney injury due to deposition of calcium oxalate crystals within the renal tubules
2. profound anion gap metabolic acidosis

EHYLENE GLYCOL = OXALATE CRYSTALS = AKI (because the crystal plug up your GU system)

Question 19

most common source of ethylene glycol (for ingestion)

Answer 19

1. automotive antifreeze

this is oftentimes going to be a suicide attempt in teens/adults. kids are prone to accidental ingestion

Question 20

most common sources of methanol (for ingestion)

Answer 20

1. windshield washer fluid
2. automotive antifreeze
3. “moonshine” (impure home made alcohol)

classic case is people making home made hooch, their hooch ends up impure, and they get methanol toxic. this is the classic stereotype of the blind Appalachian hillbilly

Question 21

classic “mixed picture” acid-base disturbance seen in Salicylate toxicity

Answer 21

1. respiratory alkalosis (crosses blood brain barrier and stimulates tachypnea. it is NOT a compensatory tachypnea to the metabolic acidosis)
2. metabolic acidosis.
3. finally respiratory acidosis (when they start to get pooched and their ventilatory effort begins to fail)

Question 22

Treatment goals for salicylate toxicity

Answer 22

“Alkalinize and dialyze”

Question 23

key findings of a poisoning history

Answer 23

1. time, route, and quantity of exposure
2. coingestants
3. onset of symptoms

Question 24

key exam findings in salicylate toxicity

Answer 24

1. Vitals: tachycardia, tachypnea/hyperpnea, hyperthermia
2. Gastrointestinal (GI): nausea, vomiting, and abdominal pain
3. CNS: tinnitus/hearing dysfunction, coma/seizures
4. Pulmonary: non-cardiogenic pulmonary edema, acute respiratory distress syndrome
5. Dermatologic: diaphoresis

Question 25

pathophysiology of salicylate toxicity

Answer 25

1. At a physiologic serum pH, salicylic acid exists in an ionized state as a weak acid
2. in toxicity (acidic environment), salicylic acid is converted to an un-ionized (highly permeable) state
3. ATP production becomes limited secondary to Krebs cycle interference.
4. Energy is released in the form of heat as a result of uncoupling oxidative phosphorylation
5. Renal hemodynamics are ultimately impaired, and anion gap metabolic acidosis ensues

Question 26

key pearls for tubing a salicylate toxicity patient

💵💵💵💵 MONEY SLIDE 💵💵💵💵

Answer 26

1. Don’t do it!
2. Hold off until your hand is forced (deteriorating mental status, acute lung injury, agitation)
3. If intubating maintain or exceed minute ventilation requirements
4. pursue aggressive bag-valve mask procedures (delayed sequence intubation if possible)
5. ensure adequate fluid loading and hydration prior to induction. these patients are usually dry! (also consider administering 1x amp D50 IV immediately before sedation to treat unrecognized neuroglycopenia, a sinister complication of salicylate toxicity)
6. use amps of bicarb peri intubation (administer 2 mEq/kg IV bolus sodium bicarbonate)
7. RSI with most experienced intubator and get the tube in quick
8. adjust vent settings to maximize minute ventilation (e.g. 8-10 cc/kg breaths, high RR)

Question 27

rescue therapy for acetaminophen toxicity

Answer 27

N-acetylcysteine (NAC)

Question 28

N-acetyl-p-aminophenol (acetaminophen) abbreviation

Answer 28

APAP

Question 29

toxic dose range for acetaminophen

Answer 29

1. > 150 mg/kg or >10g in adults and adolescents

2. >200-250 mg/kg in infants and toddlers

Question 30

Stage I of acetaminophen toxicity

Answer 30

quiescent phase…

2-24 hr post ingestion. usually asymptomatic. if symptoms present, usually GI-related (N/V, abdominal tenderness)

liver labs (AST/ALT) and coags (PT/INR) are typically normal, may become mildly elevated

Question 31

Stage II of acetaminophen toxicity

Answer 31

1-2 days post ingestion, minimal symptoms. may develop RUQ pain

elevated AST/ALT, bilirubin, INR

Question 32

Stage III of acetaminophen toxicity

Answer 32

72-96 hours post ingestion, Maximal stage of hepatotoxicity!

elevated AST/ALT, Abnormal LFT’s (rising PT/INR)

this is the full meal deal. full blown hepatic failure. this is the stage where these guys get super fucked up

Question 33

Stage IV of acetaminophen toxicity

Answer 33

> 5 days post ingestion. progression to MODS/Death.

resolution of hepatotoxicity in survivors

Question 34

what is the clinical utility of activated charcoal (AC) in toxic ingestion?

Answer 34

1. Patients may benefit from the administration of activated charcoal (AC) in a single dose of 1 g/kg (maximum dose 50 g)
2. Typically only works if given within one to two hours of ingestion

Question 35

key clinical features of solvents, anesthetics, or sedatives (SAS) Toxidrome

Answer 35

1. CNS depression
2. decreased LOC (progressing to coma in some cases)
3. hypoventilation
4. ataxia (difficulty balancing and walking)
5. hypothermia

Question 36

key clinical features of anticholinergic toxidrome

💵💵💵💵 MONEY SLIDE 💵💵💵💵

Answer 36

1. dilated pupils (mydriasis) “blind as a bat”
2. decreased sweating (anhidrosis) “dry as a bone”
3. hyperthermia “hot as hell”
4. delirium “mad as a hatter”
5. flushed skin “red as a beet”
6. decreased UO and decreased bowel sounds (urinary retention and constipation)
7. tachycardia

Question 37

key clinical features of cholinergic toxidrome

💵💵💵💵 MONEY SLIDE 💵💵💵💵

Answer 37

“DUMBBELLS”

1. Diarrhea
2. Urination
3. Miosis
4. Bradycardia (increased parasympathetic response)
5. Bronchoconstriction
6. Excitation (myoclonic twitches/seizures)
7. Lacrimation (parasympathetic stimulation of lacrimal glands)
8. Lethargy
9. Salivation (parasympathetic stimulation of salivary glands)

Question 38

key clinical features of opioid toxidrome

Answer 38

1. pinpoint pupils (miosis)
2. central nervous system depression
3. respiratory depression
4. hypothermia
5. hypoactive bowel sounds

Question 39

key clinical features of Sympathomimetic Toxidrome

Answer 39

1. tachycardia
2. tachypnea
3. hypertension
4. anxiety/agitation/delirium/hallucinations
5. hyperthermia with diaphoresis
6. dilated pupils (mydriasis)
7. seizures

Question 40

pathophysiology of cardiac toxicity associated with cocaine use

Answer 40

1. Cocaine is an ester anesthetic that acts via sodium channel blockade
2. leads to QRS widening and slowed conduction on ECG

Question 41

key clinical differences between Acute sympathomimetic and anticholinergic toxidromes

Answer 41

1. sympathomimetic and anticholinergic toxidromes have similar features of febrile agitated delirium with tachycardia and hypertension
2. Major difference: Diaphoresis with sympathomimetics and dry skin with anticholinergics
3. Minor differences: Reactive pupils with sympathomimetics and minimally reactive pupils with urinary retention in anticholinergics

Question 42

mechanism of digoxin

Answer 42

1. Cardiac glycosides inhibit sodium-potassium-ATPase
2. levels of intracellular Na+ and extracellular K+ increase
3. The increase in intracellular Na+ eventually results in an increase in intracellular Ca++, increasing cardiac contractility
4. Digoxin increases vagal tone and shortens the refractory period of the myocardium
5. This leads to bradycardia and increased automaticity

Question 43

drug class of digoxin

Answer 43

cardiac glycoside

Question 44

primary treatment modality for digoxin toxicity

Answer 44

1. digoxin-specific antibody fragments (digoxin-Fab)

2. also known as “Digi-bind”

Question 45

primary means of death in digoxin toxicity

Answer 45

1. cardiac manifestations of toxicity
2. brady-tachydysrhythmias
3. hyperkalemia
4. cariogenic shock

Question 46

most common ECG finding indicating digoxin toxicity

Answer 46

1. new onset PVC’s in the setting of a patient taking digoxin

Question 47

signs of chronic/long term digoxin toxicity

Answer 47

1. fatigue
2. malaise
3. nausea
4. dizziness
5. visual disturbances such as xanthopsia (yellow haloes)
6. chromatopsia (color vision disturbances)
7. scotomas (area of partial alteration in the field of vision)
8. reduced visual acuity

Question 48

common clinical syndrome seen in BB + CCB overdose

Answer 48

1. refractory hypotension
2. bradydysrhythmias (conduction blocks)
3. cardiogenic shock
4. death

Question 49

primary clinical distinction between CCB OD and BB OD

Answer 49

1. Hyperglycemia is common with CCB overdose (CCB block voltage gated Ca++ channels in pancreatic beta cells that are necessary for insulin release)
2. hypoglycemia is common with BB overdose (BBs interfere with glycogenolysis and gluconeogenesis)

Question 50

CCB mechanism

Answer 50

1. CCBs block voltage-gated Ca++ channels responsible for excitation of the myocardium and smooth and skeletal muscle

Question 51

Beta blocker mechanism

Answer 51

1. BBs inhibit epinephrine and norepinephrine adrenergic stimulation on beta receptors
2. beta receptors are found on the heart, smooth muscles, arteries, airways, kidneys, and other tissues.

Question 52

CCB toxicity pathophysiology

Answer 52

1. Antagonism of the Ca++ channels decreases Ca++ influx, resulting in impaired muscle contraction.
2. Ca++ channel antagonists impair insulin release, resulting in intracellular hypoglycemia (extracellular hyperglycaemia) rendering the cells less efficient at energy production

Question 53

beta blocker toxicity pathophysiology

Answer 53

1. BBs antagonize beta receptors
2. in beta receptor blockade cAMP production is reduced
3. this inhibition results in a decrease in cardiac inotropy and chronotropy
4. Antagonism of non-cardiac beta receptors impairs gluconeogenesis and glycogenolysis, resulting in hypoglycaemia

Question 54

what is the mechanism behind high-dose insulin therapy in BB and CCB overdose?

💵💵💵💵 MONEY SLIDE 💵💵💵💵

Answer 54

1. high-dose insulin improves hemodynamic parameters because of direct inotropic effects independent of cAMP
2. also has anti-inflammatory effects, and antioxidant effects

Question 55

which antidepressants have the highest rate of mortality

Answer 55

1. Tricyclic antidepressants (TCA’s)
2. monoamine oxidase inhibitors (MAOI’s)
3. dopamine and norepinephrine reuptake inhibitor’s (DNRI)

Question 56

characteristic findings in TCA overdose

Answer 56

Think “neuro-cardiac”

1. CNS depression
2. seizures
3. hypotension
4. dysrhythmias

Question 57

characteristic findings in MAOI overdose

Answer 57

Think “adrenergic crisis”

1. adrenergic storm
2. coma
3. complete cardiovascular collapse

Question 58

characteristic findings in bupropion (wellbutrin) DNRI overdose

Answer 58

think “stimulant toxidrome”

1. tachycardia
2. tremor
3. agitation/hallucination
4. delayed onset seizures

Question 59

define Serotonin syndrome

Answer 59

1. potentially life-threatening condition associated with increased serotonergic activity in the central nervous system (CNS)
2. presents with the clinical triad of autonomic instability, altered mental status, and neuromuscular findings (eg, hyperreflexia, clonus)
3. must be in the context of exposure to a serotonergic agent

Question 60

explain the cardio toxicity of TCA overdose

Answer 60

1. QRS complex widening occurs due to fast Na+ channel inactivation by ionized TCA binding to the Na+ channel
2. Sinus tach occurs due to anticholinergic effects and increased norepinephrine
3. QTc prolongation occurs secondary to QRS widening
4. Hypotension occurs due to impaired cardiac conduction and peripheral alpha 1 blockade.

Question 61

explain CNS toxicity in TCA overdose

Answer 61

1. Agitation and delirium occur due to antimuscarinic and antihistaminic effects.
2. Seizures occur d/t increased norepinephrine, Na+ channel blockade, and GABA inhibition

Question 62

first-line treatment for cyanide poisoning

Answer 62

1. Hydroxocobalamin
2. 5 g IV over 30 min (may repeat dose × 1)
3. Forms cyanocobalamin (vitamin B12)

Question 63

pathophysiology of cyanide toxicity

Answer 63

1. Inhibition of cytochrome c oxidase within the electron transport chain halts ATP formation
2. this results in the accumulation of H+ and profound acidemia

Question 64

diagnosing cyanide toxicity

Answer 64

1. Diagnosis is clinical
2. history of occupational or environmental exposure
3. presence of rapidly progressive cardiovascular collapse
4. presence of profound lactatemia
5. “Cherry-red” skin color is unreliable. may be a late or postmortem finding

Question 65

clinical manifestations of cyanide toxicity

Answer 65

1. Central nervous system: headache, agitation, confusion, seizures, coma
2. Cardiovascular: tachy-brady dysrhythmias, hypotension, cardiovascular collapse
3. Pulmonary: tachypnea, followed by bradypnea
4. Gastrointestinal: nausea,vomiting, abdominal pain
5. metabolic: Serum lactate >8-10 mmol/L is highly sensitive for cyanide toxicity
6. Severe anion gap acidosis is anticipated in cyanide toxicity (hyperlactatemia)

Question 66

median toxic dose (TD50) definition

Answer 66

1. the dose required to produce a defined toxic effect in 50% of subjects

Question 67

median lethal dose (LD50) definition

Answer 67

1. the dose required to kill 50% of subjects

Question 68

median effective dose (ED50) definition

Answer 68

1. the dose at which 50% of individuals exhibit the specified effect
2. the dose of a drug that produces, on average, a specified all-or-none response in 50% of a test population

Question 69

therapeutic index definition

Answer 69

1. the ratio of the TD50 to the ED50

2. a parameter which reflects the selectivity of a drug to elicit a desired effect rather than toxicity.

Question 70

therapeutic window definition

Answer 70

1. the range between the minimum toxic dose and the minimum therapeutic dose
2. the range of doses over which the drug is effective for most of the population and the toxicity is acceptable.

Question 71

key history features for EtOH usage/withdrawal

Answer 71

1. time of last drink
2. quantity
3. daily allotment
4. co-ingestants
5. onset of symptoms

Question 72

Signs and symptoms of mild ethanol withdrawal

Answer 72

1. Tremor
2. anxiety
3. insomnia
4. sweating
5. anorexia

Question 73

Signs and symptoms of moderate ethanol withdrawal

Answer 73

1. Autonomic instability (increased heart rate, blood pressure, temperature)
2. visual/tactile/auditory hallucinations

Question 74

Signs and symptoms of severe ethanol withdrawal

Answer 74

1. Severe autonomic instability
2. extreme agitation
3. altered sensorium
4. extreme tremors/seizures (delirium tremens)

Question 75

classic triad of wernicke encephalopathy

Answer 75

1. mental status changes
2. ophthalmoplegia
3. ataxic gait

Question 76

define Wernicke encephalopathy

Answer 76

1. acute brain disorder that results from thiamine deficiency
2. Thiamine is a cofactor for several key enzymes important in energy metabolism
3. thiamine deficiency initiates neuronal injury by inhibiting metabolism in brain regions with high metabolic requirements
4. Thiamine deficiency in alcoholics results from a combo of decreased PO intake, reduced GI absorption, decreased hepatic storage, and impaired utilization

Question 77

define Korsakoff syndrome

Answer 77

1. a late neuropsychiatric manifestation of Wernicke encephalopathy (WE)
2. characterized by profound anterograde and retrograde amnesia
3. most frequently in alcohol abusers after an episode of WE
4. most patients with KS show typical WE lesions
5. 80 percent of alcohol abusers recovering from classic WE exhibit amnesia of KS

Question 78

Z-drugs

Answer 78

1. Zolpidem, zopiclone, and zaleplon

2. structurally unrelated to benzodiazepines but bind to the benzodiazepine site on the GABA-A receptor

Question 79

describe flumazenil

Answer 79

1. GABA-A receptor antagonist
2. rapid onset of action and a high affinity for the benzodiazepine binding site on the GABA-A receptor
3. will not reverse the effects of other sedative-hypnotics such as barbiturates or other sedatives such as ethanol

Question 80

“2 salt and a sticky BUN”

this is for CALCULATED serum osmolarity

💵💵💵💵 MONEY SLIDE 💵💵💵💵

Answer 80

Calculated Serum osmolarity = “2 salt and a sticky BUN”

Calculated osmolarity = (2 x Na) + Glucose + BUN + (1.25 x ETOH)

Question 81

What is the normal osmolar gap?

💵💵💵💵 MONEY SLIDE 💵💵💵💵

Answer 81

Osmolar Gap = Measured Serum Osmolality - Calculated Serum osmolarity (Og = Om - Oc)

normal osmolar gap is arbitrarily set at 10. But can range from -15 to 10 in population

Question 82

define osmolar gap

Answer 82

the difference between measured serum osmolality and calculated serum osmolality

Question 83

define an osmole

Answer 83

1. an osmole is the amount of a substance that yields the number of particles that would depress the freezing point of the solvent by 1.86K (such as volatile alcohols)
2. a good way of thinking about this is with antifreeze. antifreeze is usually ethylene glycol (an alcohol) which has a very low freezing point (approx -40 Celsius)

Question 84

most common toxicological causes of an elevated osmolar gap

Answer 84

1. methanol
2. ethylene glycol
3. isopropanol (Isopropyl alcohol)
4. ethanol

Question 85

name the three types of cholinergic receptors

Answer 85

1. central
2. muscarinic
3. nicotinic

Question 86

effects of Excess acetylcholine at muscarinic receptors

Answer 86

1. symptoms increased secretions
2. bronchoconstriction
3. bradycardia
4. vomiting
5. abdominal cramping

Question 87

effects of Excess acetylcholine at nicotinic receptors

Answer 87

1. muscle fasciculations or paralysis d/t activation of the neuromuscular junction

Question 88

CNS effects of excess acetylcholine

Answer 88

1. headache
2. drowsiness
3. confusion
4. dizziness

Question 89

three main methods of GI decontamination in toxic ingestion

Answer 89

1. Gastric lavage
2. Activated charcoal
3. Whole-bowel irrigation

Question 90

MOA for organophosphate toxicity

Answer 90

1. blocks the action of Ach esterase at the neuromuscular junction.
2. Ach acts on nicotinic and muscarinic receptors

Question 91

muscarinic effects of organophosphate poisoning

💵💵💵💵 MONEY SLIDE 💵💵💵💵

Answer 91

1. Muscarinic receptors in heart, eye, lung, GI, skin and sweat glands
2. Bradycardia/hypotension
3. Miosis
4. Bronchorrhea / Bronchospasm
5. Hyperperistalsis (SLUDGE)
6. Sweating
7. Vasodilation

Question 92

nicotinic effects of organophosphate poisoning

💵💵💵💵 MONEY SLIDE 💵💵💵💵

Answer 92

1. fasciculations, flaccid paralysis

2. tachycardia, hypertension

Question 93

dializable drugs

Answer 93

I - Isopropanol (Isopropyl alcohol) 
S - salicylate
T - theophyline 
U - urea 
M - metformin/methanol
B - barbiturates 
L - lithium
E - ethylene glycol
D - dabigatran

Question 94

The Rumack-Matthew nomogram (acetaminophen tox)

💵💵💵💵 MONEY SLIDE 💵💵💵💵

Answer 94

determines toxic 4 hour level + Calculates NAC dosing for acetaminophen overdose

MUST HAVE:

1. Acute, single ingestions (where entire ingestion occurs within an 8-hour period).
2. A known time of ingestion.
3. Immediate release formulation.
4. Absence of formulations or coingestants that alter absorption and bowel motility (e.g. anticholinergics, opioids).

Notes:

1. An acetaminophen concentration obtained prior to 4 hours post-ingestion cannot be plotted on the Rumack-Matthew nomogram, and only confirms acetaminophen exposure, not toxicity
2. Get an accurate time of ingestion: the Rumack-Matthew nomogram is entirely dependent on knowing time of ingestion.
3. Start NAC treatment within 8 hours post-ingestion to ↓ the risk of hepatotoxicity (AST or ALT > 1000 IU/L).
4. In patients presenting 8-24 hours post-ingestion, start NAC while awaiting the acetaminophen concentration; once this is resulted, NAC can be continued or discontinued depending on the level.

Question 95

describe the classic “mixed picture” acid-base disturbance seen in Salicylate toxicity

Answer 95

respiratory alkalosis followed by metabolic acidosis.

Question 96

pathophysiology of salicylate toxicity

Answer 96

Salicylates uncouple oxidative phosphorylation, impair ATP synthesis, and promote lipolysis

1. At a physiologic serum pH, salicylic acid exists in an ionized state as a weak acid; in toxicity (acidic environment), it is converted to an un-ionized (highly permeable) state
2. ATP production is limited secondary to Krebs cycle interference
3. Energy is released in the form of heat d/t uncoupling oxidative phosphorylation
4. Renal hemodynamics are ultimately impaired, and AGMA ensues

Question 97

physical exam findings seen in salicylate toxicity

Answer 97

Vitals: tachycardia, tachypnea/hyperpnea, hyperthermia (late, severe toxicity)
GI: nausea, vomiting, and abdominal pain
CNS: tinnitus/hearing dysfunction, coma/seizures (late, severe toxicity)
Pulmonary: non-cardiogenic pulmonary edema, ARDS
Dermatologic: diaphoresis

Question 98

treatment pathway for salicylate toxicity

Answer 98

1. Support ABCs, prevent further organ toxicity by encouraging salicylate elimination
2. Alkalinize the serum/urine (1-2 mEq/kg sodium bicarb. IV bolus followed by sodium bicarb. infusion (3 amps into 1L D5W) @ 1.5-2 X maintenance rate) goal serum pH ~7.5; goal urine pH >7.5
3. Salicylate overdose + IV sodium bicarbonate therapy = potential hypokalemia. Avoid hypokalemia because it prevents alkalization of the urine, prolonged elimination of salicylate (goal K+ 4.0 to 4.5 mEq/L)
4. Monitor Ca++ levels (ionized/total); IV NaHCO3– can cause hypocalcemia
5. Consider glucose supplementation if altered mental status (Serum glucose may be normal but CNS levels may be low d/t effects of salicylates)
6. CCP transport for emergent hemodialysis

Question 99

classic ABG findings in salicylate toxicity

Answer 99

1. Primary respiratory alkalosis followed by a mixed acid-base disorder (respiratory alkalosis and metabolic acidosis).
2. The metabolism of salicylates causes an increase in the anion gap. Salicylate is the primary unmeasured anion; however, lactic acid is also produced from anaerobic metabolism, which contributes to the anion gap.
3. Many chemistry analyzers report a false elevation of chloride in the setting of salicylate toxicity, which can skew the anion gap

Question 100

pathophysiologic pathway of methanol metabolism in the body

Answer 100

1. Methanol is metabolized in the liver to formaldehyde by alcohol dehydrogenase.
2. The formaldehyde is then metabolized by aldehyde dehydrogenase to formic acid.
3. The formic acid inhibits cytochrome-C in the mitochondria, shifting the cell to anaerobic glycolysis → lactic acid accumulation

Question 101

M in the MUDPILES mnemonic

Answer 101

Methanol ingestion

elevated anion gap metabolic acidosis (formic acid buildup and lactic acid buildup)

Question 102

pathophysiologic pathway of Ethylene glycol metabolism in the body

Answer 102

1. Ethylene glycol is metabolized in the liver to glycoaldehyde by alcohol dehydrogenase.
2. Glycoaldehyde is converted to glycolic acid by aldehyde dehydrogenase, which is then converted to glyoxylic acid, then to oxalic acid.
3. oxalic acid combines with serum calcium to form the classic calcium oxalate crystals found in the urine of patients who have consumed ethylene glycol

Question 103

E in the MUDPILES mnemonic

Answer 103

Ethylene glycol ingestion

elevated anion gap metabolic acidosis

Question 104

most commonly ingested toxic alcohol

Answer 104

Isopropanol (Isopropyl alcohol)

Question 105

most common sources of Isopropanol (Isopropyl alcohol)

Answer 105

solvents, disinfectants, mouthwashes, lotions, rubbing alcohol, hand sanitizers

Question 106

pathophysiologic pathway of Isopropanol (Isopropyl alcohol) metabolism in the body

Answer 106

1. hepatically metabolized by alcohol dehydrogenase to acetone.
2. The acetone does not undergo further metabolism, and no acid byproducts are formed.
3. This means that isopropanol is the only toxic alcohol that does not cause an elevated anion gap acidosis

Question 107

define and describe Osmolar gap

Answer 107

1. difference between the Measured Serum Osmolality minus the Calculated Serum Osmolarity
2. equate to the amount of particles present in the serum that are not accounted for by the calculated Osmolarity formula

Calculated Serum osmolarity = “2 salt and a sticky BUN”
Calculated osmolarity = (2 x Na) + Glucose + BUN + (1.25 x ETOH)

Osmolar Gap = Measured Serum Osmolality - Calculated Serum osmolarity (Og = Om - Oc)

normal osmolar gap is arbitrarily set at 10. But can range from -15 to 10 in population

Question 108

the only substances that consistently increase the serum Osm gap

Answer 108

ethanol, methanol, ethylene glycol, isopropyl alcohol, acetone, mannitol, and glycerol

Question 109

toxic end product of methanol metabolism

Answer 109

formic acid

Question 110

toxic end products of ethylene glycol metabolism

Answer 110

glycolic and oxalic acid

Question 111

what is the distinguishing feature which differentiates TOXIC alcohol poisoning from ethanol toxicity

Answer 111

elevated osmolar gap

Question 112

specific manifestations of ethylene glycol toxicity

Answer 112

1. significant renal failure d/t oxalate crystal deposition in the kidneys and glycolic acid, which is directly nephrotoxic
2. hypocalcemia and tetany can result d/t oxalate binding to calcium.

Question 113

specific manifestations of methanol toxicity

Answer 113

MeOH toxicity classically causes visual disturbances (“snowfield” vision) due to formic acid-induced optic neuropathy

Question 114

specific manifestations of Isopropanol toxicity

Answer 114

causes ketosis without acidosis (no lactic acid formed!)

Usually benign clinical course but can occasionally cause hemorrhagic gastritis.

Fomepizole and HD not usually indicated

Question 115

specific manifestations of Propylene glycol toxicity

Answer 115

often due to IV medication preparations containing this alcohol (e.g., diazepam, lorazepam, esmolol, nitroglycerin, phenobarbital, phenytoin)

can result in severe lactic acidosis.

Question 116

MOA of fomepizole

Answer 116

1. competitively inhibits alcohol dehydrogenase, which is involved in the metabolism of all alcohols, including ethanol.
2. It is given to prevent the buildup of toxic metabolites from ethylene glycol (glycolic acid, glyoxylic acid, and oxalic acid) and methanol (formic acid) whose deposition in tissues can cause irreparable damage

Question 117

discuss the role for vitamin supplementation in toxic alcohol poisoning

Answer 117

1. Give folic or folinic acid to patients with Methanol toxicity to divert metabolism away from formic acid to carbon dioxide and water.
2. Give folic acid, pyridoxine, and thiamine to patients with ethylene glycol toxicity to divert metabolism to nontoxic metabolites

Question 118

in what clinical picture should one suspect toxic alcohol poisoning

Answer 118

unexplained elevated anion gap metabolic acidosis and elevated osmolar gap

Question 119

Goals of management in toxic alcohol poisoning

Answer 119

1. Block the toxic metabolites with fomepizole or ethanol
2. Correct pH to 7.2 with bicarb
3. Eliminate toxic metabolites with dialysis (especially methanol)

Question 120

describe an approach to intubation for toxic alcohol patient (hint: severe metabolic acidosis)

Answer 120

Consider DSI with ketamine and beware of the acidosis; match the pre-intubation respiratory rate with post intubation respiratory rate and consider bicarbonate boluses to avoid worsening acidosis and cardiovascular collapse

Question 121

Indications for fomepizole or ethanol in toxic alcohol poisoning

Answer 121

1. Known ingestion of methanol, ethylene glycol or diethylene glycol without access to rapid serum osmolality
2. AG metabolic acidosis or elevated osmolar gap plus strong suspicion of ingestion
3. Serum methanol >8 mmol/L
4. Serum ethylene glycol >3.2 mmol/L
5. Suspicion of toxic alcohol ingestion with evidence of end organ damage (ocular, renal)

Question 122

Lab clues for toxic alcohol poisoning

Answer 122

1. AG metabolic acidosis (caused by toxic alcohol +/- elevated lactate and renal failure)
2. High osmolality +/- osmolar gap (note that osmolality decreases with time)
3. Low ethanol level in intoxicated patient
4. Hypocalcemia with prolonged QT

Question 123

when/how is The Rumack-Matthew nomogram used to determine the risk of APAP-induced hepatoxicity ?

Answer 123

Use after a single acute ingestion only (not for chronic or repeated ingestions) to determine if treatment is req’d

the nomogram starts at 4 hours post-ingestion

Obtain serum APAP level at 4 hours post ingestion: If the APAP plots above the treatment line, or “150-line”, treat with NAC

Question 124

MOA for NAC in acetaminophen toxicity

Answer 124

1. The non-toxic route of APAP metabolism gets saturated in overdoses, which leads to the formation of the toxic metabolite NAPQI.
2. N-acetylcysteine acts as a glutathione precursor and substitute to aid the conversion of N-acetyl-p-benzoquinoneimine to non-toxic metabolites.
3. NAC helps replenish glutathione stores to conjugate the toxic metabolite, and assists with other routes of liver metabolism as well

Question 125

4 stages of acetaminophen toxicity

Answer 125

Stage 1 (0.5-24 hrs): mild nausea, emesis, weakness
Stage 2 (24-72 hrs): hepatotoxicity +/- nephrotoxicity => RUQ abdominal pain
Stage 3 (72-96 hrs): hepatotoxicity peaks => nausea, vomiting, jaundice, coagulopathy
Stage 4 (4 days -2 wks): recovery or decompensation resulting in death

Question 126

sources of salicylate overdose OTHER than aspirin

Answer 126

oil of wintergreen (methyl salicylate)
BenGay (topical methyl salicylate)
PeptoBismol (bismuth subsalicylate)

Question 127

discuss the approach to sodium bicarb in TCA toxicity

Answer 127

1. Sodium bicarbonate is the primary treatment for QRS widening, arrhythmias, or hypotension associated with TCA overdoses.
2. administering sodium bicarbonate for QRS > 100-120 ms is appropriate
3. Bicarbonate is administered at 1-2 meq/kg IVP. This dose may be repeated q5 minutes, until the QRS interval narrows and the hypotension resolves.
4. After 3 rounds of bicarb, start a bicarbonate drip (3 amps in 1L D5W) at a rate of 250 cc/hr. continued 12-24 hours after the EKG has normalized