Psychedelic Substances: The Little Book of

PSYCHEDELIC
THE LITTLE BOOK OF
SUBSTANCES
PSYCHEDELIC.SUPPORT
PSILOCYBIN
4-PHOSPHORYLOXY-N,N-DIMETHYLTRYPTAMINE
Psilocybin is a naturally occurring tryptamine alkaloid found in upwards of 200
species of fungi. When consumed, the body rapidly metabolizes psilocybin to
psilocin which activates serotonin 2A (5-HT2A) receptors and profoundly changes
consciousness for 3-6 hours. Psilocybin is a classical psychedelic characterized by
visual distortions, heightened bodily sensations, colorful visions, altered auditory
perceptions, synthesia, strong emotions, hallucinations, and spatial and cognitive
shifts in relation to space and time.
BRAND NAME: none

CHEMICAL NAME:
4-phosphoryloxy-N,N-dimethyltryptamine
DRUG CLASSIFICATION: classic
psychedelic
DRUG TYPE: psilocybin (synthetic),
psilocybin-containing fungi
LEGAL STATUS: illegal in most
countries
CONTROLLED SUBSTANCE (USA):

Schedule I
CLINICAL TRIAL SPONSORS

Usona Institute
COMPASS Pathways
Heffter Institute
Beckley Foundation
University investigator-initiated studies
Many new companies

PSILOCYBIN
CLINICAL & THERAPEUTICS
Synthetic psilocybin is under investigation in clinical trials in the United States and
Europe for several health conditions. The FDA granted Breakthrough Therapy
designations for psilocybin therapy for both treatment-resistant depression and
major depressive disorder. A Breakthrough Therapy designation can quicken
regulatory approval timelines for novel therapeutics that show better performance
than available medications for life-threatening conditions. Psilocybin clinical trials
are ongoing with FDA marketing approval possible in 2024 or later.
POSITIVE EFFECTS NEGATIVE EFFECTS

Visual distortions Panic attacks, anxiety, or confusion
Vivid imagery with eyes open or Paranoia
closed Dysphoria
Auditory and visual hallucinations Irrational and reckless behavior
Sensory synthesia Impaired concentration and focus,
Feelings of expansiveness disordered thinking
Feelings of oneness and connection Dizziness
with others and the universe Disorientation
Heightened emotions Restlessness
Transcendence of space and time Muscle weakness
Ego dissolution Nausea or vomiting
Mystical experiences Light sensitivity
Altered cognition Pupil dilation
Introspection and insightfulness Flashbacks
PSILOCYBIN
INDICATIONS UNDER STUDY In most countries of the world,
FOR PSILOCYBIN possession and use of psilocybin
mushrooms are illegal. However,
psilocybin retreats are operating

Major depressive disorder
legally in a few countries such as
Treatment-resistant depression
Jamaica and the Netherlands. In
Anxiety and depression in cancer
May 2019, Denver Colorado
patients
became the first US city to
Depression in people with mild
decriminalize psilocybin
cognitive impairment or early
mushrooms followed shortly after
Alzheimer’s disease
by Oakland, Santa Cruz, Ann
Type 2 Bipolar Disorder
Arbor, Washington DC, and the
depression
state of Oregon.
Nicotine dependence
Alcohol use disorder

MECHANISMS
Substance use disorders (cocaine,
OF ACTION
opioid)
Co-occurring depression and High-affinity agonist at serotonin 2A
alcohol use disorder (5-HT2A) receptors, the primary
Cluster, migraine, and post- target for subjective effects
traumatic headache disorders Agonist at 5-HT2C, 5-HT1A, and 5-
Anorexia nervosa HT1B receptors
Obsessive compulsive disorder Modulation of serotonergic,
Demoralization in AIDS/HIV dopaminergic, and glutamatergic
survivors systems
PSILOCYBIN
The psilocybin experience can be metaphorically likened to a journey. During the journey,
the person can visit places deep within the recesses of their own mind, have out-of-body
experiences where they venture to far away universes to meet celestial beings, or even
engage in conversations with loved ones long since passed. The range of possible
experiences is infinite and dose-dependent. A person’s mental state and the environment
where psilocybin is taken affect the subjective and emotional experience.
THERAPEUTIC APPROACH DOSING IN CLINICAL TRIALS

Co-therapy team of two trained Oral (capsule)
guides/therapists deliver the Very low dose (1-9 mg psilocybin)
treatment Low dose (10-19 mg psilocybin)
1 - 4 preparatory sessions Medium dose (20-29 mg psilocybin)
1 - 4 psilocybin sessions, spaced High dose ( >30 mg psilocybin)
weeks to months apart Duration of effects 3-6 hours
Comfortable living room like setting,
participant listens to music and

SAFETY & TOLERABILITY
wears eye shades Well tolerated in individuals
Follow-up integration sessions OR screened for specific
follow-up safety/efficacy physiological and psychological
assessments health criteria
Therapeutic approaches vary widely, Increases or decreases in blood
some include motivational pressure and heart rate
enhancement therapy and various Low potential for dependence in
degrees of psychotherapy while medical and non-medical
others include psychological support settings
with very little Common adverse reactions:
preparation/integration therapy anxiety, psychological distress,
paranoid ideation, physical
discomfort, headache, nausea
PSILOCYBIN
NON-MEDICAL USES
Psilocybin-containing mushrooms have been revered in ceremonial spaces
dating back thousands of years in indigenous cultures, and are still
traditionally used by some indigenous communities in Mexico. With the
discovery of LSD, research into psychedelic compounds and their applications
in psychiatric medicine blossomed. Psilocybin was investigated for
therapeutic benefits throughout the 1960s and gained precedence in Western
cultures when it was popularized among the hippie counterculture. The 1970s
Controlled Substance Act made psilocybin a Schedule I substance where it
resides today.
COMMON STREET NAMES POPULAR

Psilocybin mushrooms or fungi SETTINGS
Magic mushrooms Home
Psychedelic mushrooms Natural environments
Caps Electronic music
Mushies festivals
Shrooms House parties
Fungus Concerts
Buttons Art festivals
Alice
COMMON
ROUTES OF
MUSHROOM
ADMINISTRATION
PREPARATIONS
Oral (dried or fresh
Teas
mushrooms)
Chocolates
Oral (synthetic psilocybin)
Crushed into a powder (edibles
Smoked
or used to fill capsules)
Lemon tek
PSILOCYBIN
NON-MEDICAL USES
COMMON PSILOCYBIN DOSES*

Microdose: 0.1 - 0.5 grams
Low dose: 0.5 - 2 grams
Moderate dose: 2 - 4 grams
High dose: >4 grams
*Potency varies across different mushroom species
PRIMARY RISKS
Misidentification of
mushrooms
Mushrooms contaminated
with molds or toxins
Physical harms caused by
changes in judgement and
dangerous behaviors
Complications with pre-
existing health conditions
Flashbacks
FACTORS
AFFECTING RISK
PROFILE
Dose
Mushroom sourcing
Pre-existing health
conditions
Set and setting
MDMA
3,4-METHYLENEDIOXYMETHAMPHETAMINE
MDMA is an amphetamine derivative classified as an entactogen or empathogen.
MDMA induces psychoactive effects of heightened emotions, openness, boundless
love, and feelings of oneness and connection to others and the universe. MDMA
stimulates the release of neurotransmitters (serotonin, dopamine, and
norepinephrine) and hormones (oxytocin, vasopressin, cortisol, and prolactin).
These neurochemicals dynamically interact to induce mind-altering effects and
increase blood pressure, body temperature, and heart rate. MDMA, also known as
Ecstacy and Molly, has been a popular party drug since the early 1980s and is
classified as a Schedule I controlled substance in the US.
BRAND NAME: none

CHEMICAL NAME: 3,4-
methylenedioxymethamphetamine
(MDMA)
DRUG CLASSIFICATION:
empathogen/entactogen
DRUG TYPE: synthetic

LEGAL STATUS: illegal world-wide
Schedule I

MAPS / MAPS PBC
MindMed
University investigator-
initiated studies
MDMA
MDMA-assisted psychotherapy is under investigation in clinical trials for treating
several mental health disorders. In a clinical setting with trained therapists, a
person undergoing MDMA treatment is first prepared for the experience in 90-
minute therapy sessions before embarking in all-day MDMA-assisted psychotherapy
sessions (2-3 sessions, spaced 1 month apart). The therapeutic process continues in
follow-up integration sessions where the person reflects on the journey, stabilizes
insights, and establishes a plan for their healing to continue outside the therapy
room.

Euphoria Panic attacks, anxiety, or confusion
Heightened awareness and sensory Nausea or vomiting
perceptions Muscle tension, tremors, shaking
Feelings of expansiveness Sweating
Feelings of oneness and connection Blurred vision
with others and the universe Teeth grinding, jaw tightness
Increased energy and alertness Moderate potential for addiction or
Empathy problematic use in non-medical
settings
INDICATIONS UNDER STUDY MECHANISMS

FOR MDMA-ASSISTED OF ACTION
PSYCHOTHERAPY
Posttraumatic stress disorder (PTSD) Binds to and reverses transporter
Anxiety related to a life-threatening proteins (SERT, NET, DAT)
illness Increase release of serotonin,
Social anxiety in autistic adults norepinephrine, and dopamine
Anorexia nervosa Increases release of hormones -
Binge eating disorder oxytocin, vasopressin, prolactin, and
Alcohol use disorder cortisol
MDMA
In 2017, the FDA granted a

THERAPEUTIC APPROACH (MAPS)
Breakthrough Therapy designation
Co-therapy team of two trained
for MDMA-assisted psychotherapy
health providers deliver the treatment
for the treatment of PTSD.
Three 90-minute preparatory sessions
Preliminary evidence showed
Three 8-hour MDMA-assisted
MDMA was a substantial
psychotherapy sessions, spaced a
improvement over available PTSD
month apart
medications (SSRIs). Clinical trials
Three integration sessions following
are now in the last phase of
each MDMA session
testing (phase 3). If significant,
MDMA could become approved
DOSING IN CLINICAL TRIALS for the treatment of PTSD by
2023.
Oral
Initial dose 75-125 mg MDMA
Supplemental dose equal to half the
initial dose (37.5 - 62.5 mg MDMA)
given two hours later
Duration of effects 6-8 hours
Well tolerated in individuals screened for specific physiological and
psychological health criteria
Increases in blood pressure, heart rate, and body temperature similar to
moderate exercise
Low potential for abuse in medically supervised administrations
Common adverse reactions (reported by >40% in phase 1 MDMA studies):
difficulty concentrating, dizziness, dry mouth, feeling cold, impaired
balance/gait, jaw clenching/tight jaw, lack of appetite, restless legs,
restlessness, and thirst
MDMA
NON-MEDICAL USES
COMMON STREET POPULAR ROUTES OF

NAMES SETTINGS ADMINISTRATION
Ecstasy Home Oral (most common)
E, X, and XTC Natural environments Snorted
Molly Nightclubs Rectal
Love drug Electronic music Injected
ADAM festivals Smoked
Beans Raves Pressed tablets, powder,
Disco biscuits Concerts capsules
House parties
Art festivals
ORAL DOSING IN
NON-MEDICAL SETTINGS
Low dose: 60-80 mg
Moderate dose: 81-130 mg

FACTORS AFFECTING
High dose: 131 - 200 mg RISK PROFILE
Very high dose: >200 mg
Dose
Frequency of dosing
PRIMARY RISKS
Contamination of drug source
Dehydration or
or polydrug/medication use
overhydration, both can
Pre-existing disease or health
cause complications when
conditions
a person has taken MDMA
Ambient temperature
Interactions of MDMA with
Activity level
other drugs or medications
Fluid intake
KETAMINE
2-(2-CHLOROPHENYL)-2-(METHYLAMINO)-CYCLOHEXANONE
Discovered in 1962 and patented in 1963, racemic ketamine is an arylcyclohexylamine
used as a rapid-acting general anesthetic agent in human and veterinary medicine.
The FDA approved ketamine in 1970 as an anesthetic drug and is now legally
prescribed off-label for a growing list of indications. Ketamine is a non-competitive
NMDA antagonist and interacts with a number of other receptor targets that
contribute to its effects.
BRAND NAME: Ketalar

CHEMICAL NAME:
2-(2-chlorophenyl)-2-(methylamino)-
cyclohexanone
DRUG CLASSIFICATION: dissociative

LEGAL STATUS: legal with a medical
prescription when clinically indicated

Schedule III

University investigator-initiated studies
Ketamine Research Foundation
Janssen
DRUG NAME/COMPANY
Ketalar / Par Sterile Products
Ketamine hydrochloride / Mylan Institutional
Ketamine hydrochloride / Hospira
Ketamine hydrochloride / West-Ward Pharms Int

KETAMINE
Beyond its primary application for anesthesia, ketamine is used as an analgesic,
anti-obsessional, and antidepressant compound, and possesses neuroprotective
and neuroplastic properties. The effects of ketamine are highly dependent on the
bioavailable dose by way of the route of administration, ranging from slight
perceptual disruptions to paralysis and full dissociation to sedation. In medical
settings, ketamine is considered relatively safe because it has less circulatory and
respiratory depression compared to other anesthetic agents. Long-term use and
high doses of ketamine are associated with greater incidence of adverse effects
and increased risk of dependence.
POSITIVE EFFECTS ACUTE NEGATIVE EFFECTS

Drowsiness
Anxiety
Dissociative (body dissociates from
Drowsiness
the mind)
Paranoid delusions
Out-of-body experiences
Dysphoria
Changes in perception, cognition,
Distorted perceptions of body and
and emotion
self
Vivid imagery, visual hallucinations
Loss of coordination
Mood enhancement
Disorientation
Ego dissolution
Confusion
Transcendence of space and time
Muscle trembles or jerks
Mystical experiences
Psychotic episodes
Experiences of death and rebirth
Accidents (falling, car, etc)
Muscle relaxation
Psychological distress
Pain relief
Loss of airway function
Feeling of awe and wonder
KETAMINE CLINICAL & THERAPEUTICS
NEGATIVE EFFECTS OF Ketamine is only FDA approved for use as
PROLONGED USE an anesthetic agent. However, the last 10
years have brought an increase in off-label

Kidney and bladder (cystitis)
prescriptions for pain management and
toxicity
mental health conditions (major depressive
Urinary tract dysfunction
disorder, OCD, suicidal ideation, and
Physical and psychological
others), meaning rigorous controlled trials to
dependence
gain FDA approval have not been
Misuse, tolerance, and addiction
conducted (except for esketamine, see next
Withdrawal syndrome
section). It's increasingly used to reduce
Flashbacks
depression symptoms and improve mood.
APPROVED INDICATIONS
Some clinicians administer ketamine to
Anesthetic compound for treat PTSD and substance use disorders,
diagnostic and surgical procedures although use for these indications is
experimental and warrants caution.

COMMON OFF-LABEL
Individuals who have substance use
INDICATIONS disorders can be more vulnerable to
Pain become ketamine dependent; those with
Major depression disorder PTSD may have traumatic memories
Mood disorders resurface. Without proper support, these
Addiction disorders* experiences can be harmful rather than
Posttraumatic stress disorder* therapeutic. Research in controlled clinical
*Experimental, caution warranted trials is necessary to establish safety
profiles, dosing, and efficacy for each
MECHANISMS OF ACTION psychiatric indication.
N-methyl-D-aspartate NMDA receptor antagonist (blocks excitatory
signalling of glutamate)
Direct and/or indirect effects at opioid, monoaminergic,
cannabinoid, nitric oxide, muscarinic, nicotinic, and sigma
receptors
Neuroprotective properties, promotes neuroplasticity
The use of ketamine for mental health DOSING*

symptoms falls into two broad Intravenous (IV)
frameworks - 0.5 mg/kg over a 40 minute infusion
pharmaceutical/biochemical and Dose for Induction of anesthesia: 1.0 -
ketamine-assisted psychotherapy (KAP). 4.5 mg/kg
Ketamine itself has physiological effects Onset of effects 45 seconds (IV)
that appear important for Intramuscular (IM)

antidepressant and other therapeutic For anxiolysis or analgesia:
effects. Some doctors will administer Low dose: 0.25 - 0.5 mg/kg
ketamine, typically through IV infusions Moderate dose: 0.5 - 1.0 mg/kg
or lozenges, to relieve psychiatric To induce psychedelic effects:
symptoms. In this framework, the drug High dose: 1.0 - 2.0 mg/kg
itself acts through neurobiological Dose for Induction of anesthesia: 6.5 -
mechanisms and the symptom relief is 13.0 mg/kg
dependent on repeated administrations Onset of effects 3 mins, Duration of
because the therapeutic effects last for effects 75 mins, sessions last 2-4 hours
days or up to two weeks. Patients are Nasal

offered minimal support and no talk 25-300 mg
therapy which may lead to a Lozenge

dependence on ketamine to achieve Transbuccal and/or sublingual
symptom reduction. Long-term use of absorption
ketamine is associated with negative 50-300 mg
side effects, namely kidney and bladder *Dosing varies depending on route of
toxicity and ketamine tolerance and administration and desired effects
dependence.
ROUTES OF ADMINISTRATION
Oral Subcutaneous
Sublingual/transbuccal Intramuscular (IM)
Intranasal Intravenous (IV)
Rectal Onset and duration of effects dependent on route
Ketamine-assisted psychotherapy (KAP) is a method where low to moderate doses of
ketamine are delivered with the intention of altering consciousness to facilitate
psychotherapy. A therapist sits and talks with a client as they experience ketamine.
Alternatively, high doses of ketamine are used to induce a non-ordinary state of
consciousness where a person experiences major shifts of perceptions in many ways
similar to classical psychedelics. Mystical-type experiences and feelings of ego
dissolution are common for high dose sessions. These effects can be extremely
negative if a person is not well prepared and supported during and afterwards.
KETAMINE-ASSISTED
PSYCHOTHERAPY
Trained therapeutic provider delivers Well tolerated in individuals
the treatment, qualified medical screened for specific
professionals prescribe ketamine off- physiological and
label psychological health criteria
Preparatory psychotherapy sessions Dose and frequency of use
Ketamine administration session with affects risk profile
psychological support and
psychotherapy during and after
Integration sessions following each
ketamine session
Either immediately after the effects of ketamine dissipate and/or in the days to weeks
to follow, a person undergoes a course of counseling or psychotherapy to examine the
experience and emotions within the framework of their personal goals. The
psychotherapeutic process aims to stabilize positive behavioral changes, consolidate
psychological material, resolve psychological issues, improve relationships, catalyze
new insights, and enhance self-awareness. While still under-researched, ketamine-
assisted psychotherapy is presumed to amplify the neurobiological properties of
ketamine by addressing underlying psychological issues and bolstering
transformational healing.
KETAMINE
NON-MEDICAL USES
Similar to other classical psychedelics, not everyone is the right fit for ketamine,
especially at higher doses. Screening for contraindicated medical and mental health
conditions is essential as is a proper setting for psychological safety. Research dating
back to the 1950s and current day psychedelic-assisted clinical trials are elucidating
how psychedelic experiences can be beneficial for therapeutic applications, and what
parameters are necessary to support a person undergoing these experiences.
WANT TO LEARN MORE ABOUT ETHICAL GUIDELINES IN

ADMINISTERING KETAMINE-ASSISTED THERAPY? CHECK OUT
KETAMINE GUIDELINES FOR CLINICIANS AND MORE FROM
KRIYA INSTITUTE.

Ketamine Nightclubs Nasal
K Discotheques Transbuccal
Special K Raves Sublingual
Kit kat House parties Intravenous
Cat tranquilizer Electronic music Intramuscular
Vitamin K festivals Rectal
Home
KETAMINE
NON-MEDICAL USES
DOSING
Dosing and effects are dependent on the route of administration. Ketamine
is administered in liquid or powder form. See clinical section for dosing
examples.
PRIMARY RISKS
Accidents
Misuse, dependence, and addiction
Pre-existing health conditions where a significant elevation of blood pressure
would be hazardous
Impaired memory and mood swings
Flashbacks
Bladder, kidney, and heart toxicity
Sexual assaults
Respiratory depression when mixed with alcohol, GHB, or opioids
*Risks of very high doses: elevated heart rate, hypertension, seizures, coma,
death, stroke, respiratory distress, asphyxiation, and psychological distress
FACTORS AFFECTING
RISK PROFILE
Pre-existing health conditions
Hypersensitivity to ketamine
Duration and frequency of use
Dose
Psychological history
History of trauma
Mixing ketamine with other substances (alcohol and GHB)
ESKETAMINE
BRAND NAME: Spravato

GENERIC NAME: S-ketamine
hydrochloride
CHEMICAL NAME: 2-(2-chlorophenyl)-2-
(methylamino)-cyclohexanone
disassociative

LEGAL STATUS: legal with a medical
prescription when clinically indicated

Schedule III
SPRAVATO (ESKETAMINE)
Spravato (esketamine)
FDA approved in 2019,
marketed by Janssen
Nasal spray
Must be used in conjunction
with specific oral
antidepressant medications
Common effects: dissociation,
sedation, sleepiness, fainting,
dizziness, spinning sensation,
anxiety, or feeling
disconnected from one’s self,
thoughts, feelings, space and
time
ESKETAMINE
APPROVED RECOMMENDED
INDICATIONS DOSING
For adults with treatment-resistant Initial dose: 56 mg
depression Induction phase (weeks 1 to 4): 56
For depressive symptoms in adults mg or 84 mg administered twice
with major depressive disorder with per week
suicidal thoughts or behaviors Maintenance phase (weeks 5 to 8):
56 mg or 84 mg administered once
TREATMENT DELIVERY weekly administered every 2 weeks
or once per week (week 9 and

Requires patient observation and
after)
monitoring by a healthcare provider
Maintenance phase (week 9 and
for 2 hours after administration
after): 56 mg or 84 mg
Only administered in certified
administered once weekly
medical offices and clinics that
administered every 2 weeks or once
have enrolled in Spravato’s program
per week depending on an
(see REMS)
individual’s response
SAFETY & TOLERABILITY ESKETAMINE CLINICAL TRIAL

Most common adverse reactions of EXCLUSIONS
Spravato plus oral antidepressant: Substance use disorder, active or
dissociation, dizziness, nausea, within the last 6 months
sedation, vertigo, hypoesthesia, Current or past psychosis
anxiety, lethargy, blood pressure Bipolar disorder
increased, vomiting, feeling drunk,
euphoric mood, and vertigo
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AYAHUASCA
N,N-DIMETHYLTRYPTAMINE (DMT)
Ayahuasca is a mixture of at least two types of plants, most commonly Psychotria viridis
and Banisteriopsis caapi, that contain N,N-dimethyltryptamine (DMT) and monoamine
oxidase inhibitors (MAOI). Originating in the Amazon basin, its use in shamanic
ceremonies for spiritual and medicinal purposes dates back centuries. The word
“ayahuasca” is Quechua and translates as “the vine or rope of the dead”. To this day,
many indigenous peoples uphold the tradition in their cultures, and it is also used
sacramentally by a number of organized religions. Interest by Western societies has
steadily increased over the last few decades because of its purported capacity to heal
intractable diseases and exert positive effects on health and wellbeing.
BRAND NAME: none

CHEMICAL NAME: N,N-dimethyltryptamine (DMT)
and harmala alkaloids [7-Methoxy-1-methyl-9H-
pyrido[3,4-b]indole (harmine); 4,9-Dihydro-7-
methoxy-1-methyl-3H-pyrido[3,4-b]indole
(harmaline); 1,2,3,4-tetrahydro-harmine
(tetrahydroharmine)]
DRUG CLASSIFICATION: psychedelic

DRUG TYPE: plant mixture
LEGAL STATUS: legal in some Central and South
American countries; illegal in the USA except for
legal religious exemption for specific churches in
the USA; decriminalized in many countries
CONTROLLED SUBSTANCE (USA): Schedule I

Sacred Medicines Public
Benefit Corporation
initiated studies
AYAHUASCA
The therapeutic potential of ayahuasca in the treatment of mood disorders,
posttraumatic stress disorder and substance use disorders, is currently under
investigation in a small number of clinical trials and surveys. The first randomized
placebo-controlled trial of ayahuasca for treatment-refractory depression
demonstrated robust and rapid antidepressant effects from a single dose of
ayahuasca when compared to placebo. Another study using data from the Global
Drug Survey suggests that the rates of alcoholism were lower in ayahuasca users
when compared to people that used LSD or mushrooms.

Vivid imagery with eyes open or Nausea or vomiting
closed Diarrhea
Purging (physical and emotional) Psychological distress
Auditory and visual hallucinations Physical discomfort
Feelings of expansiveness Impaired concentration and focus,
Feelings of oneness and connection disordered thinking
with others and the universe Dizziness
Heightened emotions Disorientation
Transcendence of space and time Muscle weakness or tension
Ego dissolution Muscle spasms
Mystical and spiritual experiences Light sensitivity
Altered cognition Pupil dilation
Introspection and insightfulness Body temperature fluctuations
Euphoria Dysphoria
Physical sensations Paranoia
Delusions
Seizures (rare)
AYAHUASCA CLINICAL & THERAPEUTICS
INDICATIONS UNDER STUDY Hearing of the potential of
FOR AYAHUASCA OR DMT ayahuasca to treat mental health
conditions, a growing number of

individuals are seeking out
Phase 1 healthy individuals (safety
ayahuasca at retreat centers in
trial for DMT)
Central and South America,
church ceremonies, and

MECHANISMS
underground community circles.
OF ACTION
Before partaking, people usually
Harmala alkaloids inhibit MAO in the follow a special diet, called a
gut allowing DMT to reach the brain ‘dieta’ in traditional practices, to
Potent partial agonist at serotonin cleanse and prepare the body for
2A (5-HT2A) receptors, the primary upcoming ayahuasca experiences.
target for subjective effects; Typically, gatherings last for a
agonist at other 5-HT subtypes weekend or up to a few weeks,
Sigma-1 receptor agonist with multiple occasions where
TAAR-1 agonist ayahuasca is consumed
Modulation of glutamatergic system
Ayahuasca induces non-ordinary states of consciousness where a person may
experience visionary states, alterations in mood and perceptions, and physical and
emotional purging. In traditional lineages, music and singing of special songs
called Icaros are predominant features of the ritual, and many who practice with
ayahuasca carry and pass down these ways of working with the medicine. The
journeyer is supported by these healing songs if physical (vomiting, diarrhea,
shaking) and emotional purging comes, or as they transverse their deepest inner
worlds. After drinking ayahuasca, it's a common practice for groups to meet the
following morning to share and process the experience with others in integration
circles. Many keep the diet in place for at least 3-7 days to solidify the effects of
the plant medicine and further reflect on the meaning and insights brought into
conscious awareness.
AYAHUASCA CLINICAL & THERAPEUTICS
Recent neuroscience research THERAPEUTIC APPROACH

suggests the active components of Supportive therapy and integration
ayahuasca can induce sessions
neuroplasticity and the generation Group administrations (planned)
of new neurons. Although this has
not been demonstrated in human

DOSING OF DMT IN
brains, these findings lend support CLINICAL TRIALS
to a neurobiological underpinning 54 mg, 69 mg, 90 mg, 115 mg (IV)
for the changes in thought patterns

DOSING OF AYAHUASCA IN
and behaviors ayahuasca drinkers
report. This isn’t to say the

CLINICAL TRIALS
psychospiritual aspects of the 0.36 mg/kg DMT (Palhano-Fontes,
experience aren’t necessary or 2017)
important, but describes how Duration of effects: 4 hours
neural pathways may adapt to SAFETY & TOLERABILITY

allow for new ways of seeing and Non-toxic
being in the world. Drug interactions can be
serious
Pharmaceutical sponsors are
Severe psychological distress
interested in taking ayahuasca
or psychotic breaks can occur
through the FDA development
path with hopeful approval. While not identical in effects to the plant-based
Developing botanical drugs is brews, a synthetic version is available and could be a
challenging, only two have ever drug studied for medical use. DMT administrations
become FDA-approved, and through routes other than oral ingestion are another
many who use ayahuasca as a method underdevelopment and could be regulated
sacrament question its place in as medicines. To mimic ayahuasca, a new trial will
modern medical practices, examine slow IV administrations of DMT to prolong
particularly if profit motives are the effects and maintain steady levels of DMT in the
predominant. ‘Pharmahuasca’ blood. Otherwise, the duration of effects is only
refers to a synthetic mixture of about 15 minutes for smoked or single injections of
DMT and harmala alkaloids. DMT.
AYAHUASCA
NON-MEDICAL USES
Indigenous peoples of the Amazon discovered ayahuasca and passed down the sacred
knowledge of these practices for many generations. Only in the 1950s did a few Westerners
really catch on to the healing properties and take interest in partaking in ayahuasca
ceremonies. Since then there has been a boom of ‘ayahuasca tourism’ where people from
all over the globe are trekking to retreat centers in Central and South America. The plants
are exported out of the jungles of the Amazon to be served at underground gatherings
across the world. This blossoming interest and resulting over harvesting of ayahuasca
threatens the sustainability of the plants and the cultures who hold plant medicines as
central tenants in their cosmologies. Conservation of the plants and their natural
ecosystems, and reciprocity to the indigenous peoples who shared their long-held wisdom
of the plants, must be paramount as psychedelics come into the focus of mainstream global
culture.
COMMON STREET POPULAR

NAMES SETTINGS
Malocas
Huasca
Yurts
Yajé
Ceremonies and
Caapi
rituals
Daime
Natural environments
Vegetal
Living rooms
Grandmother plant
Spirit molecule
ROUTES OF COMMON
ADMINISTRATION PREPARATIONS
Oral (plant brew) Banisteriopsis caapi
Oral (freeze dried capsules Psychotria viridis
of plants) Over 100 other plants
Smoked (DMT) documented
Intravenous (DMT)
Intramuscular (DMT)
AYAHUASCA
NON-MEDICAL USES
AYAHUASCA DOSES* FACTORS AFFECTING

Analysis of ayahuasca from several RISK PROFILE
sources by Callaway:
Dose
DMT concentration: between 0.16
Drug/medication interactions
mg/mL and 14.15 mg/mL (although
some samples did not contain any
Set and setting
DMT)
THH concentration: between 0.49
mg/mL and 23.80 mg/mL
Harmaline concentration: between 0.01
mg/mL and 0.9 mg/mL
Harmine concentration: between 0.45
mg/mL and 22.85 mg/mL
Doses vary across traditions between
20-200 mL
*Potency varies across brews made from
various plants
PRIMARY RISKS
Other plants added to the
mixture
Drug interactions with
contraindicated
medications
Sexual assaults
Vulnerable states;
misjudgements
Psychological distress
5-MeO-DMT
5-METHOXY-N,N-DIMETHYLTRYPTAMINE
A tryptamine derivative, 5-MeO-DMT is a very strong, fast-acting psychedelic
compound with a short duration. The effects include vision and auditory
alterations, out-of-body experiences and mystical type experiences, but unlike
other classical psychedelics the visionary effect is often eclipsed by the emotional
impact of the experience. 5-MeO-DMT has a different chemical structure and
effect profile from N,N-DMT (compound in ayahuasca), and is considered more
intense and powerful.
BRAND NAME: none

CHEMICAL NAME: 5-methoxy-N,N-
dimethyltryptamine
empathogen/entactogen
DRUG TYPE: classical psychedelic

LEGAL STATUS: illegal the US; other
countries it is unscheduled and
unregulated (i.e. Mexico)

Schedule I

GH Research Limited
Beckley PsyTech
Usona Institute
5-MeO-DMT
5-MeO-DMT can be extracted from specific plant species or from the venom of the
Incilius alvarius toad (aka, Bufo alvarius, Sonoran Desert or Colorado River toad). The
bufotoxin venom contains 5-MeO-DMT and bufotenine, both psychoactive substances.
A full dose (50 mg) of vaporized bufotoxin consists of approximately 10-15% of 5-MeO-
DMT and induces mystical type-experiences of similar intensity to high-dose psilocybin
(30 mg/70 kg). The duration of effects depends on the route of administration but for
smoked 5-MeO-DMT effects are typically felt 0-30 seconds after ingestion, peak
around 15 minutes, and dissipate 30 minutes after administration.

Euphoria Nausea or vomiting
Changes in bodily sensations Anxiety
Out of body experiences Confusion, delusion
Increased or decreased visual Pupil dilation
acuity Loss of motor control, spastic
Unity and interconnectedness movements
Perception of infinity Tremors, muscle spasms
Time distortion Respiratory depression
Catharsis Skin flushing
Ego dissolution Disorientation
Bliss Temperature regulation suppression
Spiritual experiences
Auditory distortions or
MECHANISMS OF ACTION
hallucinations
Non-selective agonist at serotonin
receptors (5-HT2A, 5-HT2C, 5-HT1A)

INDICATIONS UNDER STUDY
Bufotenine (metabolite of 5-MeO-DMT
FOR 5-MeO-DMT
and often co-occurring compound in
plants and toad) - high affinity 5-HT2A
receptor agonist
Acts at many glutamate, dopamine, and
acetylcholine receptors
5-MeO-DMT
Some suspect 5-MeO-DMT

THERAPEUTIC APPROACH (MAPS)
containing toad venom was used
Supportive therapy and integration
by ancient civilizations in
care
shamanic healing ceremonies, but
New clinical approaches under
conclusive evidence is lacking.
development
Dating back to the late 8th
century, some snuffs of South

LABORATORY DOSING American indigenous tribes were
Duration of effects 15 to 90 minutes found to contain 5-MeO-DMT. It
Inhalation (~6 to 12 mg) was first synthesized in 1936, only
IV (~0.7 to 3.1 mg) to become known to a small
Sublingual or intranasal (~10 mg) number of people in the 1970s. It's
expanding popularity over the
SAFETY & TOLERABILITY decades, and its commercial
distribution through mail orders,

Data from controlled clinical trials
prompted its placement on the
unavailable
Schedule I list of controlled
Low potential for dependence in
substances in 2011.
medical and non-medical settings
5-MeO-DMT can be easily synthesized in a laboratory, as demonstrated here by
Hamilton Morris. While some advocates argue that the constituents of bufotoxin
might have synergistic effects, the threat of over harvesting venom from toads
and the impact on local communities in the Sonoran desert is a growing concern.
Synthetic 5-MeO-DMT is an alternative that can alleviate peril of the toads and
their natural habitats. Synthetic drugs allow for much more precise dosing which
is paramount for a drug as potent as 5-MeO-DMT. Drug development sponsors
are now making a synthetic version to test for treating mental health conditions
after anecdotal reports of 5-MeO-DMT bringing relief for depression, anxiety,
substance use, and mood disorders.
5-MeO-DMT
NON-MEDICAL USES
COMMON POPULAR ROUTES OF

STREET NAMES SETTINGS ADMINISTRATION
5-MeO Home Inhalation (smoked)*
Toad medicine Natural environments IV
Sonoran toad Ceremonies Sublingual
Colorado river toad Therapeutic settings Intranasal (snorted)
venom Rectal
Bufo
God molecule
Yopo
SMOKED TOAD VENOM COMMON APPEARANCES

DOSAGE (AT LEAST 10% Dried toad venom (tan crystals)
IS 5-MEO-DMT)
*Synthetic and toad forms differ in terms
Threshold 10-20 mg
of dosing and route of administration. Toad
Moderate 20-50 mg
venom can only be administered through
Common 50-70 mg
vaporization because of other chemicals
Strong 70-100 mg
present in the venom.
PRIMARY RISKS FACTORS AFFECTING

Unknown or imprecise dosing can RISK PROFILE
lead to acute and prolonged
Dose
adverse effects
Complications with pre-existing
Set and setting
health conditions
Psychological preparation
Unskilled guides and facilitators
Psychological distress/spiritual
emergency
LSD
LYSERGIC ACID DIETHYLAMIDE
One of the most well known classical psychedelics, lysergic acid diethylamide aka
LSD, came into this world through an accidental discovery by the chemist Albert
Hoffman on April 19, 1943. He first made LSD-25 in 1938 but didn’t become aware
of the mind-shifting properties until he unknowingly absorbed a dose in the
laboratory and felt the full effects in a harrowing bicycle ride home. The profound
trip led to a quest by his employer Sandoz Laboratories to find out how this
substance could be used in clinical applications. They distributed LSD to doctors
and therapists around the world to administer to their patients and themselves in
hopes of finding a medical use.
BRAND NAME: Delysid (1950-60s)

CHEMICAL NAME: lysergic acid
diethylamide
DRUG CLASSIFICATION: classical
psychedelic

LEGAL STATUS: illegal
Schedule I

Mind Medicine
MAPS
Beckley Foundation
Investigator-initiated studies
LSD
The research lasted for a few decades and amassed reports of therapeutic value
for a wide range of mental health conditions. But by the mid-1960s, the drug had
gained popularity outside of clinical settings and became associated with the
counterculture, anti-war agenda, and hippie movement. In 1970, the Controlled
Substance Act was passed into law, placing LSD and other psychedelics in the
most restrictive class - Substance I Controlled Substances. LSD research was shut
down and the possession and use of LSD was criminalized with the highest
penalties for offenders.

Vivid imagery with eyes open or Paranoia
closed Dysphoria
Auditory and visual hallucinations Irrational and reckless behavior
Sensory synesthesia Impaired concentration and focus,
Feelings of expansiveness disordered thinking
Feelings of oneness and connection Dizziness
with others and the universe Disorientation
Heightened emotions Restlessness
Transcendence of space and time Weakness
Ego dissolution Numbness
Mystical experiences Nausea or vomiting
Altered cognition Light sensitivity
Introspection and insightfulness Pupil dilation
Flashbacks
INDICATIONS UNDER STUDY Tremors
FOR LSD Perspiration

Pain management
ADHD
Anxiety related to a life-threatening
illness

LSD
MECHANISMS Research came to a screeching
OF ACTION halt, but LSD did not disappear - it
High-affinity agonist at serotonin 2A went underground. According to a
(5-HT2A) receptor, the primary 2017 report, an estimated 10% of
target for subjective effects individuals in the US have used
Agonist at most serotonin receptors LSD in the past and 0.7% had
subtypes 5-HT1A, 5-HT2B, 5-HT2C, taken it in the last year
5-HT5A, 5-HT6; agonist at dopamine (drugabuse.org). From 2015 to
(D2) receptors 2018, LSD consumption by US
Modulation of serotonergic, adults increased 56.4%.
dopaminergic, and glutamatergic
systems
Well tolerated in individuals
THERAPEUTIC APPROACH
screened for specific
Microdose protocols (very low dose
physiological and
repeated every few days)
psychological health criteria
LSD-assisted psychotherapy
Low potential for dependence
THERAPEUTIC DOSING in medical and non-medical
settings
Oral
Very low doses: 5, 10, 20 µg Common adverse reactions in a
Typical dose: 100 µg trial: illusion, anxiety, emotional
200 µ g
distress, feeling abnormal,
Medium dose:
feeling cold
Duration of effects 6 to 12 hours
LSD is a potent substance for altering consciousness. The dosage is in micrograms ( µg) - a
tiny amount compared to most other drugs - and the duration of effects is long (anywhere
from 6 to 12 hours). Now over 50 years since it was banned, LSD is once again under study
in clinical trials. The first publication of modern-era LSD research reported significant
benefits for people coping with anxiety associated with life-threatening illnesses. Other
studies are interested in how LSD microdosing (tiny sub-perceptual, repeated doses) can
affect pain severity or ADHD symptoms.

LSD
NON-MEDICAL USES

Acid Home Oral
L Natural environments Subcutaneous
Cid Electronic music
Lucy festivals
COMMON
Dots House parties
APPEARANCES
Mellow yellow Concerts Liquid drops
Window pane Art festivals Blotter paper
Blotter Therapeutic settings Tablets (microdots) or
Orange sunshine capsules
Candy
Patch (for skin)

As with all psychedelics, the environment and
person’s psychological state can dramatically
impact the LSD experience. Not everyone is a

LSD DOSES
suitable candidate for taking LSD, particularly Microdose: 5 - 19 µg
those with a background or family history of Low dose: 20 - 75 µ g
psychotic disorders (schizophrenia, bipolar Moderate dose: 76 - 200 µg

disorder, etc). Caution and harm reduction High dose: 201 - 400 µg
practices are essential for safe use. Very high dose: >400 µ g
PRIMARY RISKS FACTORS AFFECTING

Physical harms caused by changes RISK PROFILE
in judgement and dangerous
Dose
behaviors
Set and setting
health conditions
Flashbacks

CANNABIS
Δ9-TETRAHYDROCANNABINOL (THC), CANNABIDIOL (CBD)
Cannabis is a flowering herb in the plant family Cannabaceae. The plant has been
used for medicinal and industrial purposes for thousands of years by many cultures
across the globe. It contains at least 113 naturally occurring chemical compounds
called cannabinoids. Some cannabis varieties contain a psychoactive cannabinoid
called tetrahydrocannabinol (THC) that induces a range of subjective effects
dependent on the dose. Another cannabinoid named cannabidiol (CBD) does not
cause intoxication but is used for health benefits. The flowers of Cannabis sativa
and Cannabis indica are smoked, vaporized, eaten, or topically applied for
recreational and medicinal purposes. Cannabis plants cultivated for industrial (no
THC, non-drug) use are referred to as hemp and have many uses when processed
for textiles, paper, health foods, building materials, and biodegradable plastics.
BRAND NAME: Epidiolex (cannabidiol),
Marinol (dronabinol), Syndros
(dronabinol), and Cesamet (nabilone)
CHEMICAL NAME: Δ9-

tetrahydrocannabinol (THC), cannabidiol
(CBD)
DRUG CLASSIFICATION: endocannabinoids

DRUG TYPE: THC/CBD (synthetic), cannabis plants
LEGAL STATUS: mixed in US (legal with prescription,
legal in some US states, decriminalized in some
states, US federally illegal); varies world-wide
CONTROLLED SUBSTANCE (USA): Schedule I
(THC/CBD/cannabis plants)

Pharmaceutical companies
initiated studies
CANNABIS
According to the United States federal government, cannabis remains illegal as Schedule
I Controlled Substance. However, at least 18 states and the District of Columbia have fully
legalized cannabis use and the majority of the other states have either legalized medical
cannabis use and/or decriminalized personal use.
The FDA has not approved cannabis for the treatment of any health conditions but has
approved Epidiolex (cannabidiol), a cannabis-derived drug product, and three synthetic
cannabis-related drug products - Marinol (dronabinol), Syndros (dronabinol), and
Cesamet (nabilone). The proclaimed therapeutic effects of cannabis span many
conditions but the largest amount of evidence from research supports the benefits of
cannabis for pain reduction, nausea and vomiting induced by chemotherapy, and muscle
spasticity in multiple sclerosis.

Paranoia, anxiety, panic, and
Changes in sensory perceptions
psychosis
Elevated mood
Dry mouth
Alterations in sense of time
Disorientation
Relaxation
Delusions and hallucinations (high
Euphoria
doses)
Increase in sociability
Increased heart rate
Heightened creativity
Difficulty thinking clearly
COMMON INDICATIONS FOR Altered judgement
MEDICAL CANNABIS Loss of coordination
Pain NEGATIVE EFFECTS OF

Posttraumatic stress disorder
PROLONGED USE
Epilepsy
Brain fog
Cancer and symptoms related to
Breathing problems
treatments
Dependence
Neurodegenerative diseases
Impaired memory, concentration, and
problem-solving
Fertility issues

CANNABIS
Although not backed by substantial scientific evidence, people self-medicate with
cannabis and CBD to reduce anxiety and depression symptoms, improve sleep
quality, manage stress, and mitigate PTSD symptoms. However, some research has
found that heavy use of high-potency cannabis can be associated with adverse
mental health consequences, increased risk for worsening of psychiatric symptoms
and substance use disorders, and imparied learning and memory.
MECHANISMS PREPARATIONS AND

OF ACTION APPROACHES
Whole plant preparations
THC: activation of cannabinoid CB1
Edibles
receptors
Tinctures
CBD: antagonist of GPR55
Topicals
receptors; inverse agonist of GPR3,
Cannabis-assisted psychotherapy
GPR6, and GPR12; allosteric
modulator of opioid receptors;

CANNABIS DISPENSARIES
PPAR 𝞬 agonism; inhibition of
Located in states permitting
voltage-gated cation channels;
medical or recreational cannabis
intracellular calcium release
Doctor issued medical cannabis
BRAND NAME (GENERIC) / license required in some states
PHARMACEUTICAL COMPANY Carry a variety of cannabis flowers,
Cannabis-derived drug tinctures (oils), edibles, topicals,
Epidiolex (cannabidiol) / GW and cannabis-related merchandize
Pharmaceuticals Bud tenders or medical
Synthetic cannabis-related drugs consultation available for advice
Marinol and Syndros (dronabinol) / on cannabis products.
Solvay Pharmaceuticals, PAR
Pharmaceutical Companies, Alkem Labs
Cesamet (nabilone) / Eli Lilly and
Company, Valeant Pharmaceuticals

CANNABIS CLINICAL & THERAPEUTICS
DOSING Cannabis-assisted psychotherapy
is an approach where a person

Dosing and frequency of
consumes cannabis with the
administration varies widely. Duration
intention of exploring emotions,
of effects depends on the route of
thoughts and sensations under the
administration.
guidance of a therapist. Under the
relaxing effects of cannabis, a

SAFETY & TOLERABILITY person may more easily approach
Low physiological toxicity, no and work with difficult emotions
lethal overdoses from a different self view point.
Well tolerated in individuals This technique is relatively novel
without pre-existing psychotic and encompasses other
disorders therapeutic practices such as
Challenging psychological breathing and relaxation
experiences can occur exercises. Cannabis-assisted
Adverse effects associated with psychotherapy is only available in
duration and amount of use states where cannabis is legal.

CANNABIS
NON-MEDICAL USES

Cannabis Home Inhaled (smoked)
Marijuna Outdoor environments Joints
Weed Spiritual practices Pipes
Herb Hikes Bongs
THC House parties Blunts
CBD Electronic music Inhaled (vaporized)
festivals Oral
Edibles
Drinks
Capsules
Tinctures (oils)
FACTORS AFFECTING
DOSING RISK PROFILE
Dosing and frequency of
administration varies widely. Duration
Dosage
of effects depends on the route of
Environment
administration.
Duration of use
PRIMARY RISKS
Anxiety, panic attacks, or paranoia
Memory and problem-solving impairment
Misuse, dependence, and addiction
Increased risk of psychosis or worsening of schizophrenia symptoms
in those at high genetic risk

IBOGAINE
12-METHOXYIBOGAMINE
Iboga refers to perennial rainforest shrubs in the Apocynaceae family, including
the most well known species Tabernanthe iboga. Customarily used in shamanic
healing and initiation ceremonies of Central African traditions, iboga is a plant
with roots and bark containing the psychoactive alkaloid ibogaine. People of
Gabon have practiced with iboga as a sacrament in their Bwiti religion for
hundreds of years. Through passed down knowledge accumulated over thousands
of years, providers of iboga are extensively trained to work with this plant
medicine in West African traditions.
BRAND NAME: none

CHEMICAL NAME: 12-methoxyibogamine
DRUG CLASSIFICATION: plant
mixture
DRUG TYPE: plant derived

LEGAL STATUS: illegal or restricted
in most countries; unscheduled in
Mexico and West Africa

Schedule I

initiated studies
MAPS
Sacred Medicines Public
Benefit Corporation
New pharmaceutical
companies
IBOGAINE
Ibogaine became known as a helpful tool for reducing opioid withdrawal and
craving in 1962 after Howard Lotsof accidentally discovered the anti-addictive
effects after ingesting ibogaine. It has also been shown to reverse addiction to
stimulants, alcohol, and nicotine. Preclinical research and phase 1 clinical studies
were conducted in the early 1990s to evaluate the safety of ibogaine, but the
studies were ended due to intellectual property disputes and a death associated
with ibogaine outside of medical contexts. Currently, it is not approved for the
treatment of addiction or any other medical conditions.

(HIGHER DOSES) Loss of coordination
Dream-like state Nausea
Vivid imagery with eyes closed Vomiting
Hallucinations and visual distortions Sensitivity to light and sounds
Memory recall Pupil dilation
Introspection Dizziness
Conceptual thinking Tremors
Anxiety
POSITIVE EFFECTS Delusions
(LOWER DOSES) Mania or psychosis
Increased energy Dehydration/loss of electrolytes
Stimulant effects Seizures*
Lack of appetite Irregular heartbeat
Increased blood pressure
Cardiac arrest
Death from acute heart failure or
cardiopulmonary arrest
*Related to acute alcohol or
benzodiazepine withdrawal
12-METHOXYIBOGAMINE
IBOGAINE
Observational studies and case reports show ibogaine can reduce drug craving
and withdrawal symptoms, and some individuals had sustained reductions of opioid
use 12 months after undergoing ibogaine treatment. Research in animal models
report ibogaine to reduce consumption of alcohol, stimulants, and opioids.
INDICATIONS UNDER STUDY MECHANISMS

FOR IBOGAINE OF ACTION
Alcohol use disorders Potent serotonin reuptake inhibitor
Methadone detoxification Κ -opioid receptor agonist
Opioid use disorders μ -opioid receptor agonist and
TBI partial agonist (weak)
Sigma-2 receptor agonist
Inhibits nicotinic acetylcholine
receptors and NMDA receptors
Modulates many other
neurotransmitter systems
Ibogaine clinics operate in Mexico because people can use and possess ibogaine
but it is still illegal to use it as a medicine because it is not scheduled or regulated.
Ibogaine is illegal or restricted in many countries including the USA (Schedule I
substance). With the resurgence in psychedelic research, there is renewed interest
in controlled evaluation of ibogaine. A phase 2 trial in Brazil is investigating
ibogaine for the treatment of alcohol use disorders; a phase 2 trial in Spain is
testing ibogaine for methadone detoxification. Other companies have announced
plans to conduct ibogaine research for opioid use disorders.
12-METHOXYIBOGAMINE
IBOGAINE CLINICAL & THERAPEUTICS
The ibogaine experience typically
THERAPEUTIC APPROACHES progresses through a visionary
phase (4 to 8 hours), an
Ibogaine administration under
introspection phase (8 to 20
medical supervision
hours), and finally a stimulatory
Integration and recovery support
phase (24 to 72 hours).
THERAPEUTIC DOSING OF Unlike most psychedelic
IBOGAINE HCL substances, ibogaine is associated
with serious adverse effects, and

100 mg
even death. Fatalities are usually
Ascending doses (100 to 600 mg)
attributed to other factors such as
240 mg
pre-existing medical conditions,
240 mg, 320 mg
mostly related to cardiovascular
240 mg, 320 mg, 400 mg
dysfunction, and contraindicated
medications or drugs.
SAFETY & TOLERABILITY For these reasons, medical
Individuals must be screened for screening (ECG/EKG, liver panel,
cardiovascular conditions and review of medical conditions) and
other pre-existing health discontinuation of contraindicated
conditions drugs prior to taking ibogaine is
Contraindicated medications and extremely important. Ibogaine
drugs must discontinued should never be taken alone;
Low potential for dependence in administrations should be under
medical and non-medical settings medical supervision with an
Trials ongoing - tolerability data automated external defibrillator
unavailable (AED) onsite.
12-METHOXYIBOGAMINE
IBOGAINE
NON-MEDICAL USES
Synthetic ibogaine is not widely available because the process to make it is difficult and
has yet to be optimized. Iboga plants are grown to source ibogaine. As interest in this
plant medicine grows, people must be conscientious of the impacts on the indigenous
people who traditionally use iboga and the sustainability of the plants.

Iboga Ceremonies Oral
Ibogaine Initiation rites (Bwiti, Iboga root (chewed)
Eboga Central African Ibogaine (extracted alkaloid)
Endabuse traditions)
Tabernanthe iboga Clinics
DOSES (ORAL) FOR COMMON

IBOGAINE HYDROCHLORIDE APPEARANCE
2-3 mg/kg (test dose to check for Iboga root
allergic reaction) Brown powder in capsules
6-20 mg/kg (single ‘flood dose’)
1-5 mg/kg (booster dose) PRIMARY RISKS

Dosing should never exceed 24 mg/kg Severe adverse effects or death
in 24 hours from underlying cardiac
25 mg (Microdosing) conditions

DOSES (ORAL) IBOGA ROOT BARK health conditions
5-100 grams
Interactions with other drugs or
FACTORS AFFECTING medications
RISK PROFILE Psychological distress
Dose (>12 mg/kg increase risk for cardiac abnormalities)
Contraindicated drugs and medications (including opioid drugs)
Set and setting
12-METHOXYIBOGAMINE
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PSYCHEDELIC

THE LITTLE BOOK OF

Psilocybin is a naturally occurring tryptamine alkaloid found in upwards of 200

species of fungi. When consumed, the body rapidly metabolizes psilocybin to

psilocin which activates serotonin 2A (5-HT2A) receptors and profoundly changes

consciousness for 3-6 hours. Psilocybin is a classical psychedelic characterized by

visual distortions, heightened bodily sensations, colorful visions, altered auditory

perceptions, synthesia, strong emotions, hallucinations, and spatial and cognitive

shifts in relation to space and time.

BRAND NAME: none

DRUG CLASSIFICATION: classic

DRUG TYPE: psilocybin (synthetic),

LEGAL STATUS: illegal in most

CONTROLLED SUBSTANCE (USA):

CLINICAL TRIAL SPONSORS

University investigator-initiated studies

Many new companies

designations for psilocybin therapy for both treatment-resistant depression and

major depressive disorder. A Breakthrough Therapy designation can quicken

than available medications for life-threatening conditions. Psilocybin clinical trials

are ongoing with FDA marketing approval possible in 2024 or later.

POSITIVE EFFECTS NEGATIVE EFFECTS

Vivid imagery with eyes open or Paranoia

Auditory and visual hallucinations Irrational and reckless behavior

Sensory synthesia Impaired concentration and focus,

Feelings of expansiveness disordered thinking

Feelings of oneness and connection Dizziness

with others and the universe Disorientation

Heightened emotions Restlessness

Transcendence of space and time Muscle weakness

Ego dissolution Nausea or vomiting

Mystical experiences Light sensitivity

Altered cognition Pupil dilation

Introspection and insightfulness Flashbacks

INDICATIONS UNDER STUDY In most countries of the world,

FOR PSILOCYBIN possession and use of psilocybin

mushrooms are illegal. However,

psilocybin retreats are operating

Alcohol use disorder

Co-occurring depression and High-affinity agonist at serotonin 2A

alcohol use disorder (5-HT2A) receptors, the primary

Cluster, migraine, and post- target for subjective effects

traumatic headache disorders Agonist at 5-HT2C, 5-HT1A, and 5-

Anorexia nervosa HT1B receptors

Obsessive compulsive disorder Modulation of serotonergic,

Demoralization in AIDS/HIV dopaminergic, and glutamatergic

where psilocybin is taken affect the subjective and emotional experience.

THERAPEUTIC APPROACH DOSING IN CLINICAL TRIALS

guides/therapists deliver the Very low dose (1-9 mg psilocybin)

treatment Low dose (10-19 mg psilocybin)

1 - 4 preparatory sessions Medium dose (20-29 mg psilocybin)

1 - 4 psilocybin sessions, spaced High dose ( >30 mg psilocybin)

weeks to months apart Duration of effects 3-6 hours

Comfortable living room like setting,

participant listens to music and

Follow-up integration sessions OR screened for specific

follow-up safety/efficacy physiological and psychological

assessments health criteria

Therapeutic approaches vary widely, Increases or decreases in blood

some include motivational pressure and heart rate

enhancement therapy and various Low potential for dependence in

degrees of psychotherapy while medical and non-medical