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| Name | Class |
|---|---|
| Private Philanthropic Funds | OTHER |
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The goal of this laboratory study is to establish whether and which microdoses of psilocybin are safe to administer at home to healthy participants.
Eligible participants will be given ascending doses of psilocybin trihydrate and a single, interspersed, randomized placebo on separate days in double-blind fashion. The participants will be asked to complete questionnaires and undergo safety assessments.
This study aims to enroll 20 healthy participants who will complete all study procedures. Participants will undergo a standard screening procedure. Baseline measures will be completed before the first dose. Participants will then be given ascending doses of psilocybin trihydrate (1.2 mg, 2.0 mg, 3.0 mg, and 4.2 mg) and a single, interspersed, randomized placebo on separate days in double-blind fashion at the research site. A 1 mg dose of psilocybin anhydrate is equivalent to a 1.19 mg dose of psilocybin trihydrate (used in this study). For each session, participants will be assessed with criteria for the safety of home dosing. If any dose meets criteria for at-home dosing, and a lower dose did not fail these criteria, that dose will be identified as the safe dose for the given participant. After administration of all doses of psilocybin to all participants, if a safe at-home dose was identified for all participants, that will be considered the highest safe dose for at-home administration to be used for future studies.
Visit summary:
Initial screening: Medical and psychological screening (Approx. 4 hours though portions of this may be completed remotely).
Dosing sessions: There will be 5 double-blind laboratory dosing sessions involving administration of ascending doses of psilocybin and a single, interspersed, randomized placebo dose. Baseline questionnaires will be completed on the day of the first dosing visit, and safety assessments will be administered during and at the end of each session.
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| Label | Type | Description | Intervention Names |
|---|---|---|---|
| 1.2 mg psilocybin trihydrate microdose | Experimental | Participants will receive a single microdose of 1.2 mg psilocybin trihydrate via oral capsule in the laboratory in double-blind fashion. |
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| 2.0 mg psilocybin trihydrate microdose | Experimental | Participants will receive a single microdose of 2.0 mg psilocybin trihydrate via oral capsule in the laboratory in double-blind fashion. |
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| 3.0 mg psilocybin trihydrate microdose | Experimental | Participants will receive a single microdose of 3.0 mg psilocybin trihydrate via oral capsule in the laboratory in double-blind fashion. |
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| 4.2 mg psilocybin trihydrate microdose | Experimental | Participants will receive a single microdose of 4.2 mg psilocybin trihydrate via oral capsule in the laboratory in double-blind fashion. |
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| Placebo | Placebo Comparator | Participants will receive a single placebo oral capsule in the laboratory in double-blind fashion. |
| Name | Type | Description | Arm Group Labels | Other Names |
|---|---|---|---|---|
| psilocybin trihydrate | Drug | Microdoses of psilocybin trihydrate will be administered to participants (1.2 mg, 2.0 mg, 3.0 mg, and 4.2 mg). |
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| Measure | Description | Time Frame |
|---|---|---|
| Systolic and Diastolic Blood pressure (mmHg) | Blood pressure will be measured at 60, 120, 180, and 240 minutes. A dose will be deemed safe for home dosing if participants do not have elevations in blood pressure beyond threshold values; systolic blood pressure > 150 mmHg, diastolic blood pressure > 90mmHg) at any timepoint. | Baseline, 1-4 hours post dose |
| Heart rate in beats per minute (bpm) | Heart rate will be measured at 60, 120, 180, and 240 minutes. A dose will be deemed safe for home dosing if participants do not have elevations in heart rate beyond threshold value of > 110 bpm | Baseline; 1-4 hours post dose |
| Field sobriety testing | The standardized battery of field sobriety tests includes: The Walk-and-Turn (W&T), One-Leg Stand (OLS), Horizontal Gaze Nystagmus (HGN). A dose will be deemed safe for home dosing if participants pass field sobriety testing at time of expected peak psilocybin effects. The cumulative amount of clues observed across these tasks (out of a possible 22 clues) will be reported. | Baseline; 90 minutes post dose |
| Number of participants with normal or abnormal psychological status as assessed by a psychiatric mental status exam | The Psychiatric Mental Status Exam will be a clinical interview identical to that performed by psychiatrists in daily clinical practice and will assess and document the participant's mood, affect, thought process (including the presence of formal thought disorder), paranoia, delusions, hallucinations, other perceptual alterations, speech (including rate, volume, prosody, whether or not speech is pressured), suicidal thoughts, and orientation to person, place and time. A dose will be deemed safe for home dosing if there is no evidence of abnormal psychological status on a psychiatric mental status exam performed by a blinded study psychiatrist. There is no formal scoring rubric for this outcome. A psychiatrist will use their clinical judgment to evaluate whether a participant has normal or abnormal psychological status based on a clinical interview. |
| Measure | Description | Time Frame |
|---|---|---|
| Driving Performance as assessed by The Systems Technology, Inc. Simulation (STISIM) Drive® M4000-R Console | The STISIM Drive® M4000-R Console system will be used to assess driving performance, a state-of-the-art technology that has been independently validated to reflect real-world driving conditions. Specific driving outcomes include: lateral control (i.e., SDLP), longitudinal control (i.e., standard deviation of speed (SDSP), mean speed, number of speed exceedances), total accidents (sum of number of collisions, pedestrians hit, etc.), total rule violations (sum of number of missed stop signs, illegal turns, etc.), and distance to lead vehicles. Scores range from 0 to no upper limit. Higher scores represent higher magnitude of driving impairment. |
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Inclusion Criteria:
Exclusion Criteria:
Cardiovascular screening: To qualify for the study, blood pressure at screening will be less than 130 mmHg systolic, 80 mmHg diastolic, and 90 beats per minute; mean heart rate must also be no less than 40 beats per minute. Blood pressure will be taken while subjects are at rest and have been seated or supine for at least 5 minutes.
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| Name | Role | Phone | Extension | |
|---|---|---|---|---|
| Matthew Nielsen Dick | Contact | 410-999-8066 | microdose@jh.edu |
| Name | Affiliation | Role |
|---|---|---|
| Sandeep M. Nayak, MD | Johns Hopkins University | Principal Investigator |
| Facility | Status | City | State | ZIP | Country | Contacts |
|---|---|---|---|---|---|---|
| 5510 Nathan Shock Drive | Recruiting | Baltimore | Maryland | 21224 | United States |
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This is a double-blind study. Participants will be told they will receive a range of psilocybin doses (maximum 4.2 mg) and "at least one" dose of placebo. This will control for expectancy effects on cognitive testing and questionnaires.
| Placebo | Drug | Participants will receive a capsule identical in appearance to the active drug that contains an inactive substance. |
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| 120 minutes post dose |
| Baseline; 60 minutes post dose |