Bristol Imperial MDMA in Alcoholism Study (BIMA)
Primary Purpose
Alcohol Use Disorder
Status
Unknown status
Phase
Phase 1
Locations
United Kingdom
Study Type
Interventional
Intervention
MDMA
Psychotherapy
Sponsored by
About this trial
This is an interventional treatment trial for Alcohol Use Disorder focused on measuring Alcohol Use Disorder
Eligibility Criteria
Inclusion Criteria
- Informed consent
- Primary diagnosis (as defined by DSM-5) of alcohol use disorder.
- Successful alcohol detoxification (no longer consuming any alcoholic substances).
- Between 18 and 65 years old.
Be able to identify in advance a supportive significant other(s):
- who could accompany the patient to study visits if required -who can be contacted by the study team in order to remind the patient about follow- up appointments or collect outcome data (such as drinking behaviour) in the event that the patient themselves cannot be contacted.
- Proficient in speaking and reading English.
- Agree to comply with requirements of protocol.
Exclusion Criteria
- Lacking capacity
- History of, or a current, primary psychotic disorder, bipolar affective disorder type 1 or personality disorder;
- Present a serious suicide risk; this will be determined using the clinical judgement of the qualified mental health professionals within the research team. They will use information from the Columbia-Suicide Severity Risk Scale (C-SSRS) which allows classification of severity of suicidal ideation and behaviour. This scale classifies severe risk as a) current suicidal ideation with intent and/or plan; b) suicidal behaviour in the last 3 months. A clinical judgement regarding the level of risk and subsequent decisions regarding eligibility and care would use a combination of the information provided by the C-SSRS, the participant's history of previous risk behaviours, any presenting mental health difficulties and environmental and clinical factors. A final decision would usually include a discussion with qualified mental health professionals within the research team.
Relevant abnormal clinical findings at screening visit judged by the investigator to render subject unsuitable for study. Including but not limited to:
- History of cardiac disease, hypertension and stroke
- History of severe liver disease, as evidenced by abnormal liver function test results, particularly reduction in albumin (normal > to 3.5 gm/dl).
- History of epilepsy;
- History of Malignant Hyperthermia (Central Core Disease);
- Regular user of Ecstasy (material represented as containing MDMA). E.g. more than five times in the last five years or at least twice in the 6 months prior to the start of the study;
- Currently taking or unwilling/unable to stop any medications inhibiting CYP 2D6, and the following medications Monoamine Oxidase Inhibitors, Ritonavir (HIV treatment), paroxetine, fluoxetine, citalopram, regular benzodiazepines or any other medications likely to interact with MDMA the opinion of the investigators, during 8 week MDMA assisted therapy only
- Regular use of/dependence on other drugs such as benzodiazepines, synthetic cannabinoids, cocaine and heroin.
For females of childbearing age/potential
- Must use an effective form of birth control for at least six days after administration of MDMA
- Must not be pregnant and/or breast-feeding, until the end of the treatment phase.
For males with partners of childbearing age/potential
- Must themselves confirm use of an effective form of birth control for at least six days after administration of MDMA and confirm their partner will also, defined in detail in protocol.
- Taken part in a study involving an investigational product in the last three months
- Patients that might face additional risks from immunosuppression (for example patients with immunological diseases, patients with active infection or history of infections within 4 weeks of MDMA administration, etc).
Sites / Locations
- Study Center: University of Bristol
Arms of the Study
Arm 1
Arm Type
Experimental
Arm Label
MDMA assisted Psychotherapy
Arm Description
All participants receive 2 sessions of MDMA-assisted psychotherapy
Outcomes
Primary Outcome Measures
Safety and tolerability as measured by adverse event
Number of patients completing 8-week course of MDMA-assisted psychotherapy.
Number of patients accepting second booster dose of MDMA during MDMA drug- assisted psychotherapy sessions.
All adverse events/reactions during the study will be tabulated, serious adverse events/ reactions will be coded according to CTCAE v4. The number of participants with treatment-related adverse events during the treatment period will be reported.
Secondary Outcome Measures
Intensity of MDMA drug effect during MDMA-assisted psychotherapy sessions
Intensity of drug effect assessed by verbal analogue scale 0 (none) 10 (most intense drug effect), participant and observer scores recorded.
Degree of psychological (subjective) distress (SUDS), participant and observer scores
Subjective Units of Distress scale (SUDS), degree of psychological (subjective) distress, rated from 0 (not at all distressed/completely relaxed) to 10 (most distressed imaginable/ panic attack). Participant and observer scores recorded.
Change in Vital signs during MDMA-assisted psychotherapy sessions: Heart Rate
The following will be measured 1 hour before dosing, at dosing, every 30 mins for 2 hours and hourly thereafter for 6 hours (extra measures taken if clinically required).
-Heart rate (bpm) Pre-dosing measures will be compared to those taken after dosing.
Change in Vital signs during MDMA-assisted psychotherapy sessions: Temperature
The following will be measured 1 hour before dosing, at dosing, every 30 mins for 2 hours and hourly thereafter for 6 hours (extra measures taken if clinically required).
-Temperature (degrees celsius) Pre-dosing measures will be compared to those taken after dosing.
Change in Vital signs during MDMA-assisted psychotherapy sessions: Systolic Blood pressure
The following will be measured 1 hour before dosing, at dosing, every 30 mins for 2 hours and hourly thereafter for 6 hours (extra measures taken if clinically required).
Blood Pressure (mmHg) Pre-dosing measures will be compared to those taken after dosing.
Change in Vital signs during MDMA-assisted psychotherapy sessions: Diastolic Blood pressure
The following will be measured 1 hour before dosing, at dosing, every 30 mins for 2 hours and hourly thereafter for 6 hours (extra measures taken if clinically required).
Blood Pressure (mmHg) Pre-dosing measures will be compared to those taken after dosing.
Subjective sleep following MDMA assisted psychotherapy
Leeds Evaluation Questionnaire, subjective, self-report measure, assessing changes in sleep quality and early morning behaviour. Visual analogue, positive end means improvement, negative ends mean decline in sleeping.
Mood rating during 7 days following MDMA assisted psychotherapy
Profile of Mood States questionnaire (POMS), a measure of mood states, 40 self-reported items, on a 5 point scale.
Acceptability of MDMA-Assisted therapy program: questionnaire
Acceptability questionnaire designed for the study, this self report measure includes visual analogue scales and free text addressing the participants acceptability of taking part in the trial.
Change in Drinking behaviour
Drinking behaviour will be assessed using the clinician administered Time Line Follow Back scale- this tool allows collection of information about alcohol and illicit drug use. Pre-detoxification (screening visit) levels will be compared to levels at the final psychotherapy visit (session 10) and follow-up visits 3, 6 and 9 months. Any illicit drug use will also be recorded using this scale and assessed similarly.
Change in Quality of Life: SF-36
The Short Form Health Survey (SF-36). Gold standard, patient reported, quality of life questionnaire. Scores at follow-up visits, compared to screening/baseline.
Change in Subjective Sleep Quality: PSQI
The Pittsburgh Sleep Quality Index. (PSQI). Sleep report questionnaire assessing the level of sleep disturbance. Scores collected at psychotherapy session 10 (final psychotherapy session), and follow-up visits compared to screening/ baseline.
Change in psychosocial functioning: Short Inventory of Problems for Alcohol (SIP)
Short Inventory of Problems for Alcohol (SIP) Scale. This is a 15-item instrument assessing the self-attributable consequences of drinking. Scores collected at psychotherapy session 10 (final psychotherapy session), and follow-up visits compared to screening/ baseline.
Change in psychosocial functioning: Generalized Anxiety Disorder 7 (GAD-7)
Generalized Anxiety Disorder 7 (GAD-7) scale. Brief self-administered questionnaire assessing anxiety. Scores collected at psychotherapy session 10 (final psychotherapy session), and follow-up visits compared to screening/ baseline.
Change in psychosocial functioning: The Patient Health Questionnaire (PHQ-9)
The Patient Health Questionnaire (PHQ-9). Brief self-administered questionnaire assessing depressive symptoms.Scores collected at psychotherapy session 10 (final psychotherapy session), and follow-up visits compared to screening/ baseline.
Change in psychosocial functioning: Interpersonal reactivity Index (IRI)
Interpersonal reactivity Index (IRI) self-administered scale assessing aspects of empathy Scores collected at psychotherapy session 10 (final psychotherapy session), and follow-up visits compared to baseline.
Change in psychosocial functioning: The self compassion scale (SCS)
The self compassion scale (SCS) self-administered scale assesses core aspects of self compassion including components of mindfulness. Scores collected at psychotherapy session 10 (final psychotherapy session), and follow-up visits compared to baseline.
The Penn Alcohol Craving Scale
The Penn Alcohol Craving Scale (PACS) will assess craving, specifically frequency, intensity and duration of thoughts about drinking.Scores collected at psychotherapy session 10 (final psychotherapy session), and follow-up visits compared to baseline.
Obsessive Compulsive Drinking Scale
Obsessive Compulsive Drinking Scale self-rated scale, used to measure obsessive and compulsive thoughts in relation to alcohol. Scores at psychotherapy session 10 (final psychotherapy session) and follow up visits will be compared to baseline
Prescribed medication use
Prescribed medication use will be collected at every face-to-face visit and number and type of medications at psychotherapy session 10 (final psychotherapy session), and follow-up visits compared to screening/baseline.
Assessment of MDMA/Ecstasy use following MDMA-assisted therapy
Participants will be asked to record any recreational MDMA use or craving to use recreational MDMA outside of the study.
Assessment of ability to collect follow-up data
Attrition at follow-up. Number of drop-outs at each visit.
Trauma History Questionnaire (THQ)
A self-report measure examining potentially traumatic experiences using a yes/no format. Administered on one occasion at the final therapy session (session 10)
Full Information
NCT ID
NCT04158778
First Posted
January 31, 2019
Last Updated
November 6, 2019
Sponsor
Imperial College London
1. Study Identification
Unique Protocol Identification Number
NCT04158778
Brief Title
Bristol Imperial MDMA in Alcoholism Study
Acronym
BIMA
Official Title
Open-Label Proof of Concept Feasibility Study to Explore the Safety, Tolerability and Potential Role of MDMA-Assisted Psychotherapy for the Treatment of Detoxified Patients With Alcohol Use Disorder
Study Type
Interventional
2. Study Status
Record Verification Date
November 2019
Overall Recruitment Status
Unknown status
Study Start Date
April 18, 2018 (Actual)
Primary Completion Date
June 12, 2020 (Anticipated)
Study Completion Date
June 12, 2020 (Anticipated)
3. Sponsor/Collaborators
Responsible Party, by Official Title
Sponsor
Name of the Sponsor
Imperial College London
4. Oversight
Studies a U.S. FDA-regulated Drug Product
No
Studies a U.S. FDA-regulated Device Product
No
Product Manufactured in and Exported from the U.S.
No
Data Monitoring Committee
No
5. Study Description
Brief Summary
The Safety, Tolerability and Role of MDMA-Assisted Psychotherapy for the treatment of detoxified patients with Alcohol Use Disorder.
Detailed Description
This is an open label within-subject feasibility study, in 20 patients with Alcohol Use Disorder who have recently undergone detoxification. All patients will receive MDMA-Assisted drug therapy. This study aims to assess if MDMA-Assisted Psychotherapy can be delivered safely and can be tolerated by patients with alcohol use disorder post-detoxification. Outcomes regarding abstinence from alcohol, quality of life and psychosocial functioning will be evaluated.
6. Conditions and Keywords
Primary Disease or Condition Being Studied in the Trial, or the Focus of the Study
Alcohol Use Disorder
Keywords
Alcohol Use Disorder
7. Study Design
Primary Purpose
Treatment
Study Phase
Phase 1
Interventional Study Model
Single Group Assignment
Model Description
Open label
Masking
None (Open Label)
Allocation
N/A
Enrollment
20 (Anticipated)
8. Arms, Groups, and Interventions
Arm Title
MDMA assisted Psychotherapy
Arm Type
Experimental
Arm Description
All participants receive 2 sessions of MDMA-assisted psychotherapy
Intervention Type
Drug
Intervention Name(s)
MDMA
Other Intervention Name(s)
3,4-methylenedioxymethamphetamine
Intervention Description
Two sessions of MDMA-assisted psychotherapy will take place (session 3 & 7) within the 10 week course of psychotherapy. An initial dose of 125mg MDMA will be followed by an optional dose of 62.5mg 2 hours later.
Intervention Type
Other
Intervention Name(s)
Psychotherapy
Intervention Description
Two sessions of MDMA-assisted psychotherapy will take place (session 3 & 7) within the 10 week course of psychotherapy.
Primary Outcome Measure Information:
Title
Safety and tolerability as measured by adverse event
Description
Number of patients completing 8-week course of MDMA-assisted psychotherapy.
Number of patients accepting second booster dose of MDMA during MDMA drug- assisted psychotherapy sessions.
All adverse events/reactions during the study will be tabulated, serious adverse events/ reactions will be coded according to CTCAE v4. The number of participants with treatment-related adverse events during the treatment period will be reported.
Time Frame
Treatment period defined as: From first attendance for a psychotherapy session (Session 1) to the last psychotherapy session (session 10, approximately 8 weeks from treatment start).
Secondary Outcome Measure Information:
Title
Intensity of MDMA drug effect during MDMA-assisted psychotherapy sessions
Description
Intensity of drug effect assessed by verbal analogue scale 0 (none) 10 (most intense drug effect), participant and observer scores recorded.
Time Frame
MDMA-assisted psychotherapy sessions, at dosing and hourly for up to 8 hours after dosing.
Title
Degree of psychological (subjective) distress (SUDS), participant and observer scores
Description
Subjective Units of Distress scale (SUDS), degree of psychological (subjective) distress, rated from 0 (not at all distressed/completely relaxed) to 10 (most distressed imaginable/ panic attack). Participant and observer scores recorded.
Time Frame
MDMA-assisted psychotherapy sessions, -1 hour before dosing, at dosing and hourly following dosing for 8 hours. P
Title
Change in Vital signs during MDMA-assisted psychotherapy sessions: Heart Rate
Description
The following will be measured 1 hour before dosing, at dosing, every 30 mins for 2 hours and hourly thereafter for 6 hours (extra measures taken if clinically required).
-Heart rate (bpm) Pre-dosing measures will be compared to those taken after dosing.
Time Frame
MDMA-assisted psychotherapy sessions: 1 hour before dosing, at dosing, every 30 mins for 2 hours and hourly thereafter for 6 hours (extra measures taken if clinically required).
Title
Change in Vital signs during MDMA-assisted psychotherapy sessions: Temperature
Description
The following will be measured 1 hour before dosing, at dosing, every 30 mins for 2 hours and hourly thereafter for 6 hours (extra measures taken if clinically required).
-Temperature (degrees celsius) Pre-dosing measures will be compared to those taken after dosing.
Time Frame
MDMA-assisted psychotherapy sessions: 1 hour before dosing, at dosing, every 30 mins for 2 hours and hourly thereafter for 6 hours (extra measures taken if clinically required).
Title
Change in Vital signs during MDMA-assisted psychotherapy sessions: Systolic Blood pressure
Description
The following will be measured 1 hour before dosing, at dosing, every 30 mins for 2 hours and hourly thereafter for 6 hours (extra measures taken if clinically required).
Blood Pressure (mmHg) Pre-dosing measures will be compared to those taken after dosing.
Time Frame
MDMA-assisted psychotherapy sessions: 1 hour before dosing, at dosing, every 30 mins for 2 hours and hourly thereafter for 6 hours (extra measures taken if clinically required).
Title
Change in Vital signs during MDMA-assisted psychotherapy sessions: Diastolic Blood pressure
Description
The following will be measured 1 hour before dosing, at dosing, every 30 mins for 2 hours and hourly thereafter for 6 hours (extra measures taken if clinically required).
Blood Pressure (mmHg) Pre-dosing measures will be compared to those taken after dosing.
Time Frame
MDMA-assisted psychotherapy sessions: 1 hour before dosing, at dosing, every 30 mins for 2 hours and hourly thereafter for 6 hours (extra measures taken if clinically required).
Title
Subjective sleep following MDMA assisted psychotherapy
Description
Leeds Evaluation Questionnaire, subjective, self-report measure, assessing changes in sleep quality and early morning behaviour. Visual analogue, positive end means improvement, negative ends mean decline in sleeping.
Time Frame
Daily for 7 days following both MDMA-assisted psychotherapy sessions (session 3 and 7).
Title
Mood rating during 7 days following MDMA assisted psychotherapy
Description
Profile of Mood States questionnaire (POMS), a measure of mood states, 40 self-reported items, on a 5 point scale.
Time Frame
Daily for 7 days following both MDMA-assisted psychotherapy sessions (session 3 and 7).
Title
Acceptability of MDMA-Assisted therapy program: questionnaire
Description
Acceptability questionnaire designed for the study, this self report measure includes visual analogue scales and free text addressing the participants acceptability of taking part in the trial.
Time Frame
2 months , completed at psychotherapy therapy sessions (1,2,3,4,5,6,7,8,9 & 10)
Title
Change in Drinking behaviour
Description
Drinking behaviour will be assessed using the clinician administered Time Line Follow Back scale- this tool allows collection of information about alcohol and illicit drug use. Pre-detoxification (screening visit) levels will be compared to levels at the final psychotherapy visit (session 10) and follow-up visits 3, 6 and 9 months. Any illicit drug use will also be recorded using this scale and assessed similarly.
Time Frame
Baseline, Screening (day 0), Completed at psychotherapy therapy sessions, 1,2,3,4,5,6,7,8,9 & 10', Follow-up 3, 6, 9 months
Title
Change in Quality of Life: SF-36
Description
The Short Form Health Survey (SF-36). Gold standard, patient reported, quality of life questionnaire. Scores at follow-up visits, compared to screening/baseline.
Time Frame
Screening (day 0), 3, 6 and 9 months
Title
Change in Subjective Sleep Quality: PSQI
Description
The Pittsburgh Sleep Quality Index. (PSQI). Sleep report questionnaire assessing the level of sleep disturbance. Scores collected at psychotherapy session 10 (final psychotherapy session), and follow-up visits compared to screening/ baseline.
Time Frame
Screening (day 0), 3, 6 and 9 months
Title
Change in psychosocial functioning: Short Inventory of Problems for Alcohol (SIP)
Description
Short Inventory of Problems for Alcohol (SIP) Scale. This is a 15-item instrument assessing the self-attributable consequences of drinking. Scores collected at psychotherapy session 10 (final psychotherapy session), and follow-up visits compared to screening/ baseline.
Time Frame
Screening (day 0), 3, 6 and 9 months
Title
Change in psychosocial functioning: Generalized Anxiety Disorder 7 (GAD-7)
Description
Generalized Anxiety Disorder 7 (GAD-7) scale. Brief self-administered questionnaire assessing anxiety. Scores collected at psychotherapy session 10 (final psychotherapy session), and follow-up visits compared to screening/ baseline.
Time Frame
Screening (day 0), 3, 6 and 9 months
Title
Change in psychosocial functioning: The Patient Health Questionnaire (PHQ-9)
Description
The Patient Health Questionnaire (PHQ-9). Brief self-administered questionnaire assessing depressive symptoms.Scores collected at psychotherapy session 10 (final psychotherapy session), and follow-up visits compared to screening/ baseline.
Time Frame
Screening (day 0), 3, 6 and 9 months
Title
Change in psychosocial functioning: Interpersonal reactivity Index (IRI)
Description
Interpersonal reactivity Index (IRI) self-administered scale assessing aspects of empathy Scores collected at psychotherapy session 10 (final psychotherapy session), and follow-up visits compared to baseline.
Time Frame
Baseline, 3, 6 and 9 months
Title
Change in psychosocial functioning: The self compassion scale (SCS)
Description
The self compassion scale (SCS) self-administered scale assesses core aspects of self compassion including components of mindfulness. Scores collected at psychotherapy session 10 (final psychotherapy session), and follow-up visits compared to baseline.
Time Frame
Baseline, psychotherapy session 10 (final psychotherapy session), follow-up visits at 3, 6 and 9 months
Title
The Penn Alcohol Craving Scale
Description
The Penn Alcohol Craving Scale (PACS) will assess craving, specifically frequency, intensity and duration of thoughts about drinking.Scores collected at psychotherapy session 10 (final psychotherapy session), and follow-up visits compared to baseline.
Time Frame
Screening (day 0), 3, 6 and 9 months
Title
Obsessive Compulsive Drinking Scale
Description
Obsessive Compulsive Drinking Scale self-rated scale, used to measure obsessive and compulsive thoughts in relation to alcohol. Scores at psychotherapy session 10 (final psychotherapy session) and follow up visits will be compared to baseline
Time Frame
Screening (day 0), 3, 6 and 9 months
Title
Prescribed medication use
Description
Prescribed medication use will be collected at every face-to-face visit and number and type of medications at psychotherapy session 10 (final psychotherapy session), and follow-up visits compared to screening/baseline.
Time Frame
Screening (day 0), 3, 6 and 9 months
Title
Assessment of MDMA/Ecstasy use following MDMA-assisted therapy
Description
Participants will be asked to record any recreational MDMA use or craving to use recreational MDMA outside of the study.
Time Frame
Screening (day 0), session 10, 3, 6 and 9 months
Title
Assessment of ability to collect follow-up data
Description
Attrition at follow-up. Number of drop-outs at each visit.
Time Frame
Follow up 3,6 and 9 months
Title
Trauma History Questionnaire (THQ)
Description
A self-report measure examining potentially traumatic experiences using a yes/no format. Administered on one occasion at the final therapy session (session 10)
Time Frame
2 month (Session 10)
10. Eligibility
Sex
All
Minimum Age & Unit of Time
18 Years
Maximum Age & Unit of Time
65 Years
Accepts Healthy Volunteers
No
Eligibility Criteria
Inclusion Criteria
Informed consent
Primary diagnosis (as defined by DSM-5) of alcohol use disorder.
Successful alcohol detoxification (no longer consuming any alcoholic substances).
Between 18 and 65 years old.
Be able to identify in advance a supportive significant other(s):
who could accompany the patient to study visits if required -who can be contacted by the study team in order to remind the patient about follow- up appointments or collect outcome data (such as drinking behaviour) in the event that the patient themselves cannot be contacted.
Proficient in speaking and reading English.
Agree to comply with requirements of protocol.
Exclusion Criteria
Lacking capacity
History of, or a current, primary psychotic disorder, bipolar affective disorder type 1 or personality disorder;
Present a serious suicide risk; this will be determined using the clinical judgement of the qualified mental health professionals within the research team. They will use information from the Columbia-Suicide Severity Risk Scale (C-SSRS) which allows classification of severity of suicidal ideation and behaviour. This scale classifies severe risk as a) current suicidal ideation with intent and/or plan; b) suicidal behaviour in the last 3 months. A clinical judgement regarding the level of risk and subsequent decisions regarding eligibility and care would use a combination of the information provided by the C-SSRS, the participant's history of previous risk behaviours, any presenting mental health difficulties and environmental and clinical factors. A final decision would usually include a discussion with qualified mental health professionals within the research team.
Relevant abnormal clinical findings at screening visit judged by the investigator to render subject unsuitable for study. Including but not limited to:
History of cardiac disease, hypertension and stroke
History of severe liver disease, as evidenced by abnormal liver function test results, particularly reduction in albumin (normal > to 3.5 gm/dl).
History of epilepsy;
History of Malignant Hyperthermia (Central Core Disease);
Regular user of Ecstasy (material represented as containing MDMA). E.g. more than five times in the last five years or at least twice in the 6 months prior to the start of the study;
Currently taking or unwilling/unable to stop any medications inhibiting CYP 2D6, and the following medications Monoamine Oxidase Inhibitors, Ritonavir (HIV treatment), paroxetine, fluoxetine, citalopram, regular benzodiazepines or any other medications likely to interact with MDMA the opinion of the investigators, during 8 week MDMA assisted therapy only
Regular use of/dependence on other drugs such as benzodiazepines, synthetic cannabinoids, cocaine and heroin.
For females of childbearing age/potential
Must use an effective form of birth control for at least six days after administration of MDMA
Must not be pregnant and/or breast-feeding, until the end of the treatment phase.
For males with partners of childbearing age/potential
Must themselves confirm use of an effective form of birth control for at least six days after administration of MDMA and confirm their partner will also, defined in detail in protocol.
Taken part in a study involving an investigational product in the last three months
Patients that might face additional risks from immunosuppression (for example patients with immunological diseases, patients with active infection or history of infections within 4 weeks of MDMA administration, etc).
Overall Study Officials:
First Name & Middle Initial & Last Name & Degree
Prof Nutt
Organizational Affiliation
Imperial College London
Official's Role
Principal Investigator
Facility Information:
Facility Name
Study Center: University of Bristol
City
Bristol
Country
United Kingdom
12. IPD Sharing Statement
Plan to Share IPD
No
Learn more about this trial
Bristol Imperial MDMA in Alcoholism Study
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