This study is being conducted to evaluate how of 30 days of intermittently microdosed psilocybin affects mood, cognition, subjective well-being and structural/functional MRI results compared to a placebo. Investigators hypothesize that compared to placebo, 30 days of intermittently microdosed psilocybin will produce observable changes in mood, cognition, subjective well-being and MRI, in the absence of psychedelic experiences.
This study is being conducted to evaluate the effects of 30 days of intermittently microdosed psilocybin in a parallel arm double-blind manner on mood, cognition, subjective well-being and structural/functional MRI compared to placebo, using validated psychological assessments and cognitive tests. Investigators hypothesize that compared to placebo, 30 days of intermittently microdosed psilocybin will produce observable changes in mood, cognition, subjective well-being and MRI, in the absence of psychedelic experiences. Demonstrating significant results in a population of healthy psychedelic non-users will establish a strong precedent for studying the effects of microdosing psychedelics in patient populations, such as those with treatment-resistant depression. Showing that microdosing minimizes risk of adverse outcomes with psychedelic treatment while maintaining beneficial effects would provide useful information relevant to clinical research in psychedelic-assisted psychotherapy. In addition to investigating claims that microdosing psychedelics may improve cognition and mood, this study also aims to test the hypothesis that these effects including those measurable at a brain level may persist beyond the course of the 30 days of the study. There are few to no studies that assessed the longevity of psychedelic effects on the majority of the above measures, so the proposed study may further establish the longer-term benefits of microdosing. The use of structural and functional magnetic resonance imaging (fMRI) will elucidate the mechanisms by which microdosing may be exerting its effects on mood and cognition. Because this is a relatively understudied area, information gleaned from this study will provide service in informing the field in general.
Study Type
INTERVENTIONAL
Allocation
RANDOMIZED
Purpose
BASIC_SCIENCE
Masking
DOUBLE
Enrollment
20
2.0mg powdered psilocybin derived from Psilocybe cubensis mushrooms, in capsules, provided three times weekly for four weeks
0mg matching capsules, provided three times weekly for four weeks
Olin Neuropsychiatry Research Center
Hartford, Connecticut, United States
The Complex Working Memory Span (CWMS) Task- fMRI measure
CWMS Task assesses immediate plus delayed recall and working memory by assessing working memory capacity by presenting a list of stimuli to be recalled while simultaneously performing a secondary task. This task uses a fully crossed design which includes both same-domain CWMS conditions (e.g. verbal storage combined with verbal processing) as well as cross-domain CWMS conditions (e.g., verbal storage combined with spatial processing). BOLD signal Infrontal lobe.
Time frame: From enrollment to end of treatment at 8 weeks.
NEO-Five-Factor-Inventory (NEO-FFI)
The NEO-FFI is a self-description questionnaire with 60 items for the measurement of the "big five": neuroticism, extraversion, openness, agreeableness, and consciousness. It uses a 5-point Likert scale ranging from "completely disagree" to "fully agree.
Time frame: From enrollment to end of treatment at 8 weeks.
Beck Depression Inventory
This scale has a total of 21 items. Each item is scored from 0-3 points, and the total score ranges from 0-63 points. The higher the score, the higher the degree of depression.
Time frame: From enrollment to end of treatment at 8 weeks.
Beck Anxiety Inventory
Beck Anxiety Inventory is a 21-item self-reported questionnaire which measures the existenceand severity of symptoms of anxiety. Each of the 21 items on BAI tool represents an anxiety symptom. A total score of 0 - 7 is interpreted as a "Minimal" level of anxiety; 8 - 15 as "Mild"; 16 - 25 as "Moderate", and 26 - 63 as "Severe".
Time frame: From enrollment to end of treatment at 8 weeks.
Harvard Flourishing Measure
12 questions, rating from 0 to 10 per question, sum score to calculate the 'flourish measure' will be used.
Time frame: From enrollment to end of treatment at 8 weeks.
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NIH Toolbox Cognitive Battery
Cognitive function will be assessed using the NIH Toolbox Cognition Battery, administered on an iPad.
Time frame: From enrollment to end of treatment at 8 weeks.
Ecological Momentary Assessments (EMAs) w/ MindLamp
Once-daily questions (EMAs) about mood and sleep will be sent via the MindLamp smartphone app.
Time frame: From enrollment to end of treatment at 8 weeks.
Switching Stroop Test
Stroop task measures response inhibition or response interference control. Participants will be shown a series of word colors that are either congruent or incongruent with the color of the word itself. The participant will be asked to respond to the color of the word and not the word itself. Responses are made with the keyboard. The incongruent condition is the more difficult condition of the two. Reaction time is recorded and a cost score is calculated, with shorter cost scores indicating better performance.
Time frame: From enrollment to end of treatment at 8 weeks.
Penn Conditional Exclusion Test
Neurocognition measure of reasoning \& problem solving in PennCNB. Scores will be transformed into z-scores. The key score will assess perseverative errors. Lowest score = 0, no max score. A higher score is correlated with worse performance, i.e. more perseverative errors.
Time frame: From enrollment to end of treatment at 8 weeks.
Flanker Inhibitory Control and Attention Test
This test is designed to evaluate an individual's ability to concentrate their attention while inhibiting automatic response tendencies that could potentially hinder goal achievement. This is the percent correct outcome from this assessment.
Time frame: From enrollment to end of treatment at 8 weeks.
Face Name Associated Memory Exam
The score ranges from 0 to 130, with a higher score indicating better speed of processing.
Time frame: From enrollment to end of treatment at 8 weeks.
9-hole pegboard dexterity test
The Nine-Hole Peg Test (9HPT) is used to measure finger dexterity in patients with various neurological diagnoses. Time to complete the test as quickly as possible
Time frame: From enrollment to end of treatment at 8 weeks.
NIH Toolbox Cognitive Battery
The Nine-Hole Peg Test (9HPT) is used to measure finger dexterity in patients with various neurological diagnoses. Time to complete the test as quickly as possible
Time frame: From enrollment to end of treatment at 8 weeks.
Neurite Orientation Dispersion and Density Imaging (NODDI)
Assessing synaptic plasticity in MRI
Time frame: From enrollment to end of treatment at 8 weeks.
Complex Working Memory Span task
Measures ability to juggle holding information (storage) and doing something with it (processing) at the same time. Percent accuracy will be reported.
Time frame: From enrollment to end of treatment at 8 weeks.
fMRI
Mean BOLD signal
Time frame: From enrollment to end of treatment at 8 weeks.