Lysergic acid diethylamide toxicity: Difference between revisions

Revision as of 20:15, 12 January 2021

Background

Also known as d-lysergic acid diethylamide and LSD

Mechanism

Similar to chemical properties of serotonin
- 5-HT2 agonists, mediating excitatory neurotransmitter release.^[1]
LSD also binds to dopaminergic receptors, contributing to its psychogenic affects.^[2]

Pharmacology

Known as one of the most potent psychoactive drug, doses of minimum of 25μg. Doses of 1 to 1.5 μg/kg produce psychedelic effects, with the “optimum” dosage for a typical fully unfolded LSD reaction is estimated to be in the range of 100–200 μg.
Route of administration can be PO (most common), IM, or IV.^[3]
- PO: Usual Dose 100-250μg, Onset 30-45mins, Peak effect 1-2.5hrs, Total duration 9-12hrs
- IM: Usual Dose 100-250μg, Onset 15-20mins, Peak effect 1hr, Total duration 9-10hrs
- IV: Usual Dose 40-180μg, Onset 3-5mins, Peak effect 1hr, Total duration 9-10hrs
Tolerance to LSD-25 builds up over consistent use and cross-tolerance has been demonstrated between LSD, mescaline and psilocybin.^[4]

Clinical Features

Effects begin around 20-40 minutes after injection
Euphoria
Dizziness
Visual and auditory hallucinations
Effects taper off after about 6-8 hours and are usually completely gone after a nights sleep."

"Good Trips" are much like what is described as above, with seemingly normal or usual objects and experiences appearing new and changed to something breath-taking.

"Bad Trips" include experiences of paranoia, acute panic reactions, and agitation, usually stemming from the users prior mood to ingesting LSD. This, along with the user's altered perception of their environment, can lead to the user being subjected to dangers resulting in serious injury, disability, or death.

Differential Diagnosis

Hallucinations

Serotonin-Like Agents

Lysergic acid diethylamide (LSD)
Psilocybin ("magic mushrooms")
N,N-Dimethyltryptamine (DMT)
5-methoxy- dimethyltryptamine (5-MeO-DMT)
25C-NBOMe

Enactogens

Designer amphetamines
Bath salts
Ecstasy (MDMA)
Mescaline (peyote)
Synthetic cannabinoids

Dissociative Agents

Phencyclidine (PCP)
Ketamine
Dextromethorphan
Nitrous oxide

Plant-based Hallucinogenics

Marijuana
Salvia
Absinthe
Isoxazole Mushrooms
Hawaiian baby woodrose (Argyreia nervosa)
Hawaiian woodrose (Merremia tuberosa)
Morning glory (Ipomoea violacea)
Olili- uqui (Rivea corymbosa)

Organic causes

Delirium
Intracranial mass to occipital or temporal lobes
Encephalitis, limbic encephalitis, anti-NMDA receptor encephalitis
Migraine
Seizure
Hypocalcemia/Hypercalcemia
Rift valley fever
Rabies
Syphilis
Vitamin B7 deficiency
Pellagra
Dementia
- Parkinson's Disease

Other Toxicologic Causes

Alcohol withdrawal
Anticholinergic Toxicity
Tricyclic (TCA) Toxicity
Synthetic cannabinoids
Inhalant abuse
Nitrogen narcosis
GHB withdrawal
Hydrocarbon toxicity
Heavy metal toxicity
Multiple medications: montelukast, doxapram, hyoscyamine, tizanidine, peramivir, amantadine, rimantadine, bromocriptine, methylergonovine, benztropine, doxepin, voriconazole, acyclovir, valacyclovir, ganciclovir, cimetidine, penicillin G Procaine, clarithromycin, metoclopramide
Inhalant abuse

Psychiatric Causes ^[5]

Schizophrenia, schizoaffective disorder, schizophreniform disorder
Depression with psychotic features
Bipolar disorder
Charles Bonnet Syndrome (in the visually impaired)

Serotonin-Like Agents

LSD
Psilocybin and psilocin dimethyltryptamine (DMT) and 5-methoxy- dimethyltryptamine (5-MeO-DMT)
Naturally occurring plants like :Hawaiian baby woodrose (Argyreia nervosa), Hawaiian woodrose (Merremia tuberosa), morning glory (Ipomoea violacea), and olili- uqui (Rivea corymbosa)

Enactogens

Designer amphetamines - Bath Salts, Ecstasy (MDMA)
Mescaline (Peyote)

Dissociative Agents

PCP
Ketamine
Dextromethorphan

Plant-based Hallucinogenics

Marijuana
Salvia
Absinthe
Isoxazole Mushrooms

Psychiatric Illnesses

Schizophrenia
Schizo-affective disorder
Dementia
Delirium

Evaluation

Usually clinical, based on history and presentation

Most blood and urine tests are restricted to research and unavailable for clinical usage

Research Tests

Found in blood specimens (6–12 hours) and urine (2–4 days) after usage
Metabolite (2-oxo-3-hydroxy-LSD) present in urine for a longer time than LSD itself.^[6]

Management

Assess for signs of trauma or exposure
Assure patient and staff safety
Agitation:
- Ativan 1-2mg IV, titrate to effect
- Haloperidol 5-10mg IV, titrate to effect (use as 2nd line agent as may lower seizure threshold)

Consider co-ingestions, hypoglycemia, and risk for rhabdomyolysis^[7]

Disposition

Simple LSD ingestion can be safely discharged after a period of observation, once patient has returned to sober baseline and has a safe disposition plan (~4-6 hours)
Symptoms lasting longer than 8-12hrs can be managed in an observation unit or admitted
- Further work-up and admission is indicated for persistent psychosis or altered mental status,

External Links

References

↑ Ly, B. "Hallucinogens", Rosen's Emergency Medicine: Concepts and Clinical Practice. 7th Ed. Pgs 2010-2012
↑ Marona-Lewicka D, Thisted RA, Nichols DE (2005). "Distinct temporal phases in the behavioral pharmacology of LSD: Dopamine D2 receptor-mediated effects in the rat and implications for psychosis". Psychopharmacology 180 (3): 427–435.
↑ Passie, T. "The Pharmacology of Lysergic Acid Diethylamide: A Review". CNS Neuroscience & Therapeutics, Volume 14, Issue 4, pages 295–314, Winter 2008
↑ Passie, T. "The Pharmacology of Lysergic Acid Diethylamide: A Review". CNS Neuroscience & Therapeutics, Volume 14, Issue 4, pages 295–314, Winter 2008
↑ Visual Hallucinations: Differential Diagnosis and Treatment. PMID PMC2660156
↑ Passie, T. "The Pharmacology of Lysergic Acid Diethylamide: A Review". CNS Neuroscience & Therapeutics, Volume 14, Issue 4, pages 295–314, Winter 2008
↑ Glaspy, J. "Drugs of Abuse". Emergency Medicine Manual, 6th Ed. Chapt 103, Pgs 502-504.

Authors:

[1] Ly, B. "Hallucinogens", Rosen's Emergency Medicine: Concepts and Clinical Practice. 7th Ed. Pgs 2010-2012

[2] Marona-Lewicka D, Thisted RA, Nichols DE (2005). "Distinct temporal phases in the behavioral pharmacology of LSD: Dopamine D2 receptor-mediated effects in the rat and implications for psychosis". Psychopharmacology 180 (3): 427–435.

[3] Passie, T. "The Pharmacology of Lysergic Acid Diethylamide: A Review". CNS Neuroscience & Therapeutics, Volume 14, Issue 4, pages 295–314, Winter 2008

[4] Passie, T. "The Pharmacology of Lysergic Acid Diethylamide: A Review". CNS Neuroscience & Therapeutics, Volume 14, Issue 4, pages 295–314, Winter 2008

[5] Visual Hallucinations: Differential Diagnosis and Treatment. PMID PMC2660156

[6] Passie, T. "The Pharmacology of Lysergic Acid Diethylamide: A Review". CNS Neuroscience & Therapeutics, Volume 14, Issue 4, pages 295–314, Winter 2008

[7] Glaspy, J. "Drugs of Abuse". Emergency Medicine Manual, 6th Ed. Chapt 103, Pgs 502-504.

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@@ Line 16: / Line 16: @@
 ==Clinical Features==
-The acute ingestion of LSD is described as:
+*Effects begin around 20-40 minutes after injection
-"The initial effects begin 20-40 minutes  with a sense of euphoria and dizziness...LSD is best described as a drug that strikes down barriers. The person who uses LSD is likely to feel detached  from his/her ego, and can cross between states of consciousness.  The user's perceptions are altered, causing visual and auditory hallucinations.  One may notice that the walls of room are "breathing" or that motionless curtains appear to be moving.  Senses appear to mix:  a user might see music, taste colors, or hear visual stimuli.  The LSD experience is often difficult to describe by  users -- words lose meaning and are often insufficient in describing the effects of the drug; thoughts may seem unclear.  Effects taper off after about 6-8 hours and are usually completely gone after  a nights sleep."<ref>https://www.erowid.org/chemicals/lsd/lsd_effects1.shtml</ref>
+*Euphoria
+*Dizziness
+*Visual and auditory [[hallucinations]]
+*Effects taper off after about 6-8 hours and are usually completely gone after  a nights sleep."
 "Good Trips" are much like what is described as above, with seemingly normal or usual objects and experiences appearing new and changed to something breath-taking.