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Trial registered on ANZCTR

Registration number

ACTRN12623001064695

Ethics application status

Approved

Date submitted

30/08/2023

Date registered

4/10/2023

Date last updated

16/06/2024

Date data sharing statement initially provided

4/10/2023

Type of registration

Prospectively registered

Titles & IDs

Public title

Low dose psilocybin as a treatment for moderate depression

Scientific title

A Double-Blind Randomised Controlled Trial of the Efficacy of Microdosing with Psilocybin to treat Moderate Depression

Secondary ID [1]

MICRODEP01

Universal Trial Number (UTN)

Trial acronym

MICRODEP01

Linked study record

Health condition

Health condition(s) or problem(s) studied:

Major Depressive Disorder of moderate severity

Condition category

Condition code

Mental Health

Depression

Intervention/exposure

Study type

Interventional

Description of intervention(s) / exposure

The MicroDep trial will investigate a course of low dose psilocybin as a treatment for major depressive disorder of moderate severity.
The experimental drug is 4mg WP001 (psilocybin) capsules, taken orally. Participants will complete a screening and baseline visit, followed by a six week intervention. The intervention will consist of 11 doses, administered every 3-4 days. Doses will be taken on site and adherence will be confirmed by trial staff. Following the intervention participants will complete study endpoint, 1-week and 1-month followup visits. Participants will attend the trial site for all study visits. Participants will be monitored by a psychiatrist throughout the trial and may be titrated down to 2mg if they show any signs of impairment.

There will also be a neuroimaging substudy, which will recruit a maximum of 80 participants. Participants in this substudy will complete an magnetoencephalography (MEG) scan at baseline and during the first dosing visit. MEG scans are non-invasive. Participants will be asked to lie the scanner while responding to audio and visual cues via a response button.
Every third participant will be invited to take part in the neuroimaging study. If a participant declines to take part, the subsequent participant will be invited to the substudy.

Any deviation from protocol will be documented.

Intervention code [1]

Treatment: Drugs

Comparator / control treatment

Participants in the control group will be administered caffeine in identical capsules (60 mg).

Control group

Placebo

Outcomes

Primary outcome [1]

Change in the Hamilton Rating Scale for Depression (GRID-HAMD) from baseline

Timepoint [1]

Baseline and 6 weeks from baseline

Secondary outcome [1]

1. Change in GRID-HAMD from baseline to week 10

Timepoint [1]

Baseline and 1-month followup visit (week 10)

Secondary outcome [2]

2. Rates of clinical response (50% reduction on GRID-HAMD from baseline score) at week 6 (study endpoint) and week 10 (1M FollowUp)

Timepoint [2]

Study endpoint (week 6 post-baseline) & 1-month followup visit (week 10 post-baseline)

Secondary outcome [3]

3. Rates of remission (score <8 on GRID-HAMD) at week 6 (primary endpoint) and week 10 (1M FollowUp)

Timepoint [3]

Study endpoint (week 6 post-baseline) & 1-month followup visit (week 10 post-baseline)

Secondary outcome [4]

4. Proportion of participants with Severe Adverse Events or Adverse Events (e.g., headache, nausea, dizziness) associated with participation in the trial from week 1 through to week 6. Adverse events will be assessed using a study specific questionnaire.

Timepoint [4]

At conclusion of study.

Secondary outcome [5]

5. Proportion of participants with suicidality (Columbia Suicide Severity Rating Scale [CSSRS] - Brief Form scores >1) during the study

Timepoint [5]

At conclusion of study

Secondary outcome [6]

6. Proportion of participants who down-titrate dose (determined by audit of study records)

Timepoint [6]

At conclusion of study

Secondary outcome [7]

7. Proportion of participants who remain in study until study week 6 (study endpoint) and week 10 (1M FollowUp). This will be determined by audit of study records.

Timepoint [7]

At conclusion of study

Secondary outcome [8]

8. Change in Sheehan Disability Scale (SDS) from baseline to week 6 and week 10

Timepoint [8]

Baseline and study endpoint (week 6 post-baseline) & 1-month followup visit (week 10 post-baseline)

Secondary outcome [9]

9. Change in driving simulator performance from baseline to week 1 and week 5

Timepoint [9]

Baseline, visit 1B (week 1 post-baseline) and 5B (week 5 post-baseline)

Secondary outcome [10]

10. Change in cognitive function, assessed using the trailmaking test, from baseline to visits 1B, 2B, 3B, 4B, and 5B

Timepoint [10]

Baseline, visit 1B (week 1 post-baseline), 2B (week 2 post-baseline), 3B (week 3 post-baseline), 4B (week 4 post-baseline), and 5B (week 5 post-baseline)

Secondary outcome [11]

11. Change in wellbeing, assessed with the EQ-5D, from baseline to week 6 and week 10

Timepoint [11]

Baseline and study endpoint (week 6 post-baseline) & 1-month followup visit (week 10 post-baseline)

Secondary outcome [12]

12. Change in anxiety, assessed with the Depression, Anxiety, Stress Scale from baseline to week 6 and week 10

Timepoint [12]

Baseline and study endpoint (week 6 post-baseline) & 1-month followup visit (week 10 post-baseline)

Secondary outcome [13]

13. Change in alcohol misuse, assessed with the Alcohol, Smoking and Substance Involvement Test, from baseline to week 6 and week 10

Timepoint [13]

Baseline and study endpoint (week 6 post-baseline) & 1-month followup visit (week 10 post-baseline)

Secondary outcome [14]

14. Change in drug misuse, assessed with the Alcohol, Smoking and Substance Involvement Test, from baseline to week 6 and week 10

Timepoint [14]

Baseline and study endpoint (week 6 post-baseline) & 1-month followup visit (week 10 post-baseline)

Secondary outcome [15]

15. Change in tobacco misuse, assessed with the Alcohol, Smoking and Substance Involvement Test, from baseline to week 6 and week 10

Timepoint [15]

Baseline and study endpoint (week 6 post-baseline) & 1-month followup visit (week 10 post-baseline)

Secondary outcome [16]

16. Ratings of the Acceptability of Intervention Measure (AIM) at week 6

Timepoint [16]

Study endpoint (week 6 post-baseline)

Secondary outcome [17]

17. Ratings of the Intervention Appropriateness Measure (IAM) at week 6

Timepoint [17]

Study endpoint (week 6 post-baseline)

Secondary outcome [18]

18. Ratings of the Feasibility of Intervention Measure (FIM) at week 6

Timepoint [18]

Study endpoint (week 6 post-baseline)

Secondary outcome [19]

19. Change in blood-based biomarker battery (includine tryptophan metabolites, multiplex cytokine array, and enzyme-linked immunosorbent array) from baseline to week 1 and week 3 (acute biomarkers)

Timepoint [19]

Baseline, visit 1A (week 1 post-baseline), and 3B (week 3 post-baseline)

Secondary outcome [20]

20. Change in blood-based biomarker battery (includine tryptophan metabolites, multiplex cytokine array, and enzyme-linked immunosorbent array) from baseline to week 6, week 7 and week 10 (sustained biomarkers)

Timepoint [20]

Baseline, study endpoint (week 6 post-baseline), 1-week followup (week 7 post-baseline), and 1-month followup (week 10 post-baseline)

Secondary outcome [21]

21. Changes in visual long term potentitation, measured with magnetoencephlatography (MEG) from baseline to first dosing day.

Timepoint [21]

Baseline and visit 1A (week 1 post-baseline)

Secondary outcome [22]

22. Changes in resting state, measured with MEG from baseline to first dosing day.

Timepoint [22]

Baseline and visit 1A (week 1 post-baseline)

Secondary outcome [23]

23. Changes in auditory oddball performance, measured with MEG from baseline to first dosing day

Timepoint [23]

Baseline and visit 1A (week 1 post-baseline)

Eligibility

Key inclusion criteria

Participants may be included in the study if they meet all of the following inclusion criteria.
1. Age greater than or equal to 18 years at the time of screening
2. Self-reported fluency in English
3. Meets the definition of moderate depression, defined as a score of between 15 and 23 on the Hamilton Rating Scale for Depression
4. Diagnosis of major depressive disorder, as assessed by the Mini International Neuropsychiatric Interview (MINI)
5. Able to swallow WP001 or Caffeine capsules
6. Has a body weight between 50kg and 120kg, and BMI above 16.
7. Refrains from the use of any psychoactive medication not approved by the research team from baseline through Study Termination.
8. Agrees to abstain from herbal, complementary or over the counter medications with serotonergic effects including, but not limited to, St John’s Wort, S-adenosyl methionine (SAM-e), 5-hydroxytryptophan (5-HTP) and L-tryptophan.
9. Agrees to comply with contraception requirements:
a. Women of childbearing potential must have a negative urine or serum pregnancy test at screening and baseline and be non-lactating. During the study, women of childbearing potential must agree to use a highly effective method of birth control up to 7 days after the last dose.
b. Male participants must agree to use highly effective method of birth control during the participation in the study up to 7 days after the last dose.
10. Able and willing to comply with all scheduled visits, treatment plan, laboratory tests, lifestyle considerations and other study procedures
11. Agrees to study investigators communicating directly with all of their External Health Practitioners.
12. Provides a contact (relative, spouse, close friend or other Support Person) who is willing and able to be reached by the investigators in the event of a participant becoming unreachable.
13. Must agree not to operate heavy machinery, any motorised vehicle or perform tasks that might endanger oneself or others, such as those requiring fine motor control, fast response times or real-time planning for three hours following each dosing session.

Minimum age

18 Years

Maximum age

No limit

Sex

Both males and females

Can healthy volunteers participate?

Key exclusion criteria

Participants will be excluded from the study if they meet any of the following exclusion criteria:
1. Recently started new psychological therapies and/or sessions with health professionals within 30 days of consent (such as counsellor, psychotherapists). Participants with a stable regimen may be included in this study if they agree to continue with the psychological therapies and/or counselling sessions as is (frequency of the therapy and/or sessions should not change)
2. Use of antidepressant or antipsychotic medication in the prior 3 months, or plans to start new antidepressant or antipsychotic medication in the upcoming 2 months
3. Current diagnosis of psychotic disorder, bipolar disorder, personality disorder, post-traumatic stress disorder, or substance use disorders.
4. Identification of a primary mental health diagnosis apart from Major Depressive Disorder on the Mini International Neuropsychiatric Interview.
5. Any participant presenting current serious suicide risk, as determined through psychiatric interview, responses to Columbia Suicide Severity Rating Scale (C-SSRS), and clinical judgment of the investigator will be excluded. Any participant who is likely to require hospitalisation related to suicidal ideation and behaviour, in the judgment of the investigator, will not be enrolled. Any participant presenting with the following on the screening C-SSRS will be excluded:
1. Suicidal ideation score of 4 or greater within the last month of the assessment at any frequency.
2. Suicidal ideation score of 4 or greater within the last 12 months of the assessment at a frequency of once a month or more.
3. Any suicidal preparatory acts or preparatory behaviour, within the last 12 months of the assessment. Participants with non-suicidal self-injurious behaviour may be included if approved by the CI.
4. Any suicidal behaviour, including actual, aborted, or interrupted suicide attempts within lifetime.
5. Would present a serious risk to others as established through clinical interview and contact with External Health Practitioners.
6. Require ongoing concomitant therapy with a psychiatric medication for management.
6. Poorly controlled hypertension or other cardiac abnormalities.
7. History of psychosis, bipolar disorder, stroke, epilepsy, brain injury or head trauma.
8. History of serious liver (Child-Pugh B or C), kidney disease (eGFR<60ml/min).
9. First degree relative with psychotic disorder.
10. Pregnant, or trying to get pregnant, or breastfeeding
11. Use of any psychotropic drug (excluding alcohol, nicotine and caffeine) within the last 3 months from date of consent
12. Moderate to severe cannabis or alcohol use disorder in the prior 12 months
13. An illicit or prescription drug use disorder of any severity in the prior 12 months
14. Baseline 12-lead ECG that demonstrates clinically relevant abnormalities that may affect participant safety or interpretation of study results
15. Significantly abnormal laboratory blood test defined as outside the normal range and deemed clinically significant by an investigator with expertise in this field
16. Resting blood pressure exceeding 160mmHg systolic and 100mmHg diastolic
17. Currently taking part in another clinical trial involving interventions such as an investigational drug, device, or psychotherapy
18. Current evidence of, or a history of, any condition, therapy or abnormal laboratory assessment or other events that, in the opinion of the investigator, may affect safety, and/or disrupt their participation for the duration of the study

Study design

Purpose of the study

Treatment

Allocation to intervention

Randomised controlled trial

Procedure for enrolling a subject and allocating the treatment (allocation concealment procedures)

Allocation will be performed automatically by computer after eligibility is determined.

Methods used to generate the sequence in which subjects will be randomised (sequence generation)

Stratified Randomization using REDCap.
The strata being used on this trial is age (greater or lower than 35) & sex assigned at birth (male, female, intersex)

Masking / blinding

Blinded (masking used)

Who is / are masked / blinded?

The people receiving the treatment/s
The people administering the treatment/s
The people assessing the outcomes

Intervention assignment

Parallel

Other design features

Phase

Phase 2

Type of endpoint/s

Safety/efficacy

Statistical methods / analysis

Sample size and Statistical Considerations
We aim to recruit 266 participants for this study. This will allow us to detect an effect size of .4 for the primary outcome variable GRID-HAMD, with statistical power 90% and statistical significance level .05 (two-tailed). We anticipate a drop-out rate of 10%. Although the analytic approach adopted for this study uses all available data for all enrolled patients, due to the possibility of fewer EOT measurements than expected our actual recruitment target is 293.

Analysis Populations
Modified Intention-to-Treat (mITT) – is defined as all randomised participants who received at one dose of the study treatment.

Analysis of the Primary Outcome
The primary statistical analysis involves the change in the primary outcome variable (GRID-HAMD Depression scores) between the baseline visit and the end of treatment (EOT) visit (Week 6B). A contrast of study groups will be made via linear mixed models estimated via maximum likelihood. The model will include the main effects of Visit and Study group and the interaction between them. The interaction term will be statistically tested as it is a direct estimate of the difference in change with treatment between the active and placebo groups. This approach is known to be unbiased in the presence of missing values. Should the assumption of normality not be met, formal statistical inference will employ the nonparametric bootstrap.

Recruitment

Recruitment status

Recruiting

Date of first participant enrolment

Anticipated

9/10/2023

Actual

9/02/2024

Date of last participant enrolment

Anticipated

30/10/2027

Actual

Date of last data collection

Anticipated

30/01/2028

Actual

Sample size

Target

293

Accrual to date

Final

Recruitment in Australia

Recruitment state(s)

NSW

Recruitment postcode(s) [1]

2109 - Macquarie University

Funding & Sponsors

Funding source category [1]

Commercial sector/Industry

Name [1]

Woke Pharmaceuticals

Address [1]

Suite 301, 10 Bridge St,Sydney NSW 2000 Australia

Country [1]

Australia

Primary sponsor type

University

Name

Macquarie University

Address

Clinical Trials UnitLevel 3, 75 Talavera RoadMacquarie University 2109 NSW

Country

Australia

Secondary sponsor category [1]

None

Name [1]

Address [1]

Country [1]

Ethics approval

Ethics application status

Approved

Ethics committee name [1]

Macquarie University HREC

Ethics committee address [1]

Level 3, 17 Wally’s Walk Macquarie University NSW 2109

Ethics committee country [1]

Australia

Date submitted for ethics approval [1]

30/01/2023

Approval date [1]

23/02/2023

Ethics approval number [1]

520231245146817

Summary

Brief summary

MicroDep is an investigator-initiated trial evaluating the safety and efficacy of low doses of psilocybin as a treatment for depression of moderate severity. We aim to recruit 293 participants to a 6week randomised, placebo controlled trial comprising 11 dosing sessions. Participants will be assessed at baseline, at week 6, and at 1-week and 1-month followup. The primary outcome measure will be the GRID-Hamilton Depression Rating Scale. Secondary outcomes include psychological measures, neurophysiological measures, and omics-based biomarkers. There will be a neuroimaging substudy that will investigate markers of neuroplasticity in 80 participants. 
We hypothesise that low doses of psilocybin administered over a 6 week period will be superior to placebo in improving clinical outcomes in moderate depression.
If we find evidence of efficacy in the main stage, participants randomised to the placebo condition will be offered the opportunity to repeat the intervention with the active drug.

Trial website

Trial related presentations / publications

Public notes

Contacts

Principal investigator

Name

Dr Vince Polito

Address

Level 3, Room 3.81316 University AveMacquarie University, NSW 2109

Country

Australia

Phone

+61 2 98502966

Fax

[email protected]

Contact person for public queries

Name

Dr Vince Polito

Address

Clinical Trials UnitLevel 3, 75 Talavera RoadMacquarie University, NSW 2109

Country

Australia

Phone

+61 72301367

Fax

[email protected]

Contact person for scientific queries

Name

Vince Polito

Address

Level 3, Room 3.81316 University AveMacquarie University, NSW 2109

Country

Australia

Phone

+61 2 9850 2966

Fax

[email protected]

Data sharing statement

Will individual participant data (IPD) for this trial be available (including data dictionaries)?

Yes

What data in particular will be shared?

De-identified data related to registered study measures will be shared

When will data be available (start and end dates)?

Start: immediately following the publication of the long-term follow-up results
End: indefinitely

Available to whom?

Anyone who wishes to access it

Available for what types of analyses?

Any purpose

How or where can data be obtained?

Data will be shared in the Macquarie University Research Data Repository.
Data requests can also be sent to [email protected]

What supporting documents are/will be available?

No Supporting Document Provided

Results publications and other study-related documents

Documents added manually

No documents have been uploaded by study researchers.

Documents added automatically

No additional documents have been identified.

Trial Review

Documents added manually

Documents added automatically