A Study of Psilocybin for Major Depressive Disorder (MDD)
A Randomized, Double-Blind, Support-of-Concept Phase 2 Study of Single-Dose Psilocybin for Major Depressive Disorder (MDD)
Status
Recruiting
Start date
10/15/2019
Healthy
Accepts Healthy Volunteers
Contact
Rob Barrow, MS
608-278-7662
ClinicalTrials@usonainstitute.org
Age
21 Years
— 65 Years
Gender
All
Summary
Eighty participants, ages 21 to 65, who meet Diagnostic and Statistical Manual of Mental Disorders (DSM-5) criteria for major depressive disorder (MDD) will be stratified by study site and randomized with a 1-to-1 allocation under double-blind conditions to receive a single 25 mg oral dose of psilocybin or a single 100 mg oral dose of niacin. Niacin will serve as an active placebo.
The purpose of this study is to evaluate the potential efficacy of a single 25 mg oral dose of psilocybin for MDD compared to the active placebo in otherwise medically-healthy participants, assessed as the difference between groups in changes in depressive symptoms from Baseline to Day 8 post-dose.
Overview
Major depressive disorder (MDD) has become a health crisis of epidemic proportions in the modern world. One in six individuals in the United States will experience an episode of major depression in his or her lifetime, and it is estimated that major depression will rank second after cardiac disease as a cause of international medical morbidity by the year 2020. Depression is associated with greater disability than are most other chronic illnesses and is a risk factor for mortality. Additionally, depression predicts the later development of a number of medical conditions, including cardiac and cerebrovascular disease, hypertension, diabetes, obesity, metabolic syndrome, dementia, and cancer. Unfortunately, most patients with depression do not experience a complete resolution of symptoms with antidepressant treatment. Partial-but incomplete-response to antidepressants is associated with an increased risk of full symptomatic relapse (even when on therapy) and a worse long-term disease course. Combined with the high prevalence and significant disability associated with MDD, the fact that currently available treatments are not fully adequate highlights the tremendous need to identify novel treatment strategies.
Data suggest that psilocybin may have behavioral effects relevant to the treatment of depression and recent studies also suggest that psilocybin may possess antidepressant properties. To further assess the effects of psilocybin on MDD signs and symptoms, this trial will enroll 80 participants, ages 21 to 65, who meet criteria for MDD. Participants will be stratified by study site and randomized with a 1-to-1 allocation under double-blind conditions to receive a single 25 mg oral dose of psilocybin or a single 100 mg oral dose of niacin. Niacin will serve as an active placebo.
To enhance participant safety, a Set and Setting (SaS) protocol will be utilized similar to the protocol that has been used in all modern studies of psilocybin. The SaS protocol for this study includes: 1) a period of preparation with session Facilitators prior to dosing; 2) administration of study medications in an aesthetically pleasing room under the supervision of two Facilitators who are present throughout the session; and 3) three post-dose integration sessions during which participants are encouraged to discuss their intervention experience with the Facilitators. The SaS protocol will be identical for those randomized to psilocybin or active placebo.
The primary objective of this study is to evaluate the potential efficacy of a single 25 mg oral dose of psilocybin for MDD compared to the active placebo (niacin), assessed as the difference between groups in changes in depressive symptoms from Baseline to Day 8 post-dose.
Eligibility Criteria
Inclusion Criteria:
21 to 65 years old
Able to swallow capsules
If of childbearing potential, agree to practice an effective means of birth control throughout the duration of the study
Have an identified support person and agree to be accompanied home by that person following dosing
Have sustained moderate-severe depression symptoms at Screening and Baseline
Meet DSM-5 criteria for a diagnosis of major depressive disorder and are currently experiencing a major depressive episode of at least a 60-day duration at the time of screening
Exclusion Criteria:
Women who are pregnant or who intend to become pregnant during the study or who are currently nursing
Have any of the following cardiovascular conditions: uncontrolled hypertension, coronary artery disease, congenital long QT syndrome, cardiac hypertrophy, cardiac ischemia, congestive heart failure, myocardial infarction, tachycardia, artificial heart valve, a clinically significant screening ECG abnormality, or any other significant cardiovascular condition
Have a history of stroke or Transient Ischemic Attack (TIA)
Have moderate to severe hepatic impairment
Have epilepsy
Have insulin-dependent diabetes
Have a positive urine drug test
Nicotine dependence that would disallow an individual to be nicotine free for the 7-10 hours during the dosing period
Meet DSM-5 criteria for schizophrenia spectrum or other psychotic disorders, including major depressive disorder with psychotic features, or Bipolar I or Bipolar II Disorder
Meet DSM-5 criteria for antisocial personality disorder
Meet DSM-5 criteria for a moderate or severe alcohol or drug use disorder
Chicago, Illinois 60640 Not yet recruiting
Amber Holst
872-529-8805
aholst@greatlakesclinicaltrials.com
Baltimore, Maryland 21287 Recruiting
New York, New York 10016 Recruiting
Lauderhill, Florida 33319 Recruiting
Orbrena Wellons, MA
954-990-6326
owellons@segaltrials.com
Courtney Talbert, MS
954-990-6326
ctalbert@segaltrials.com
San Francisco, California 94110 Recruiting
Madison, Wisconsin 53706 Not yet recruiting
Bri Deyo, MPH
608-225-0718
protea.research@mailplus.wisc.edu
New Haven, Connecticut 06520 Recruiting