Clinical Trial Details
— Status: Not yet recruiting
Administrative data
| NCT number |
NCT05732155 |
| Other study ID # |
EMC 00077-21 |
| Secondary ID |
|
| Status |
Not yet recruiting |
| Phase |
Phase 2
|
| First received |
|
| Last updated |
|
| Start date |
June 1, 2023 |
| Est. completion date |
December 1, 2024 |
Study information
| Verified date |
February 2023 |
| Source |
HaEmek Medical Center, Israel |
| Contact |
Guy Schusheim, Dr |
| Phone |
972-4-6494138 |
| Email |
guy_sc[@]clalit.org.il |
| Is FDA regulated |
No |
| Health authority |
|
| Study type |
Interventional
|
Clinical Trial Summary
The overall objective of this study is to use standard clinical measures to explore the
safety and preliminary effectiveness of open-label MDMA-assisted therapy with a flexible dose
of methylenedioxymethamphetaminel, in participants with Post traumatic Stress Disorder and
moral injury, in individual and group treatment settings.
The overall safety objective is to assess the severity, incidence, and frequency of AEs, AEs
of Special Interest (AESIs), and Serious Adverse Events (SAEs), concomitant medication use,
suicidal ideation and behavior and vital signs .
Description:
This single-site, open-label study assesses the safety and preliminary effectiveness of
MDMA-assisted therapy in participants diagnosed with PTSD. All therapy teams have been
trained by MAPS PBC. The study will be conducted in at least 30 participants. A flexible dose
of MDMA HCl followed by a supplemental half dose unless tolerability issues emerge or a
participant declines, is administered during the Treatment Period with manualized therapy in
three open-label monthly Experimental Sessions (2 Experimental Individual Sessions, and one
Experimental Group Session). This ~18-week Treatment Period is preceded by three Preparatory
Sessions. Each Individual Experimental Session is followed by three Integrative Sessions of
non-drug psychotherapy. The Group Experimental Session is preceded by 2 Preparatory Group
Sessions and followed by 3 Group Integrative Sessions. Experimental Sessions are followed by
an overnight stay. The Primary Outcome measure, the change in PCL-5 from Baseline (Screening)
will be repeated after each Experimental Session, with the final outcome assessed at
~35-weeks post Baseline (V18).
For each participant, the study will consist of:
- Screening Period: phone screen, informed consent, eligibility assessment, and Baseline
assessments and enrollment of eligible participants
- Preparatory Period: medication tapering, Preparatory Sessions
- Treatment Period: three monthly Experimental Sessions and associated Integrative
Sessions over ~17 weeks
- Follow-up Period and Study Termination: 1 week with no study visits, followed by Primary
Outcome and Study Termination visit
After the Screening Period and Enrollment, eligible participants will begin a ~4-week
Preparatory Period. Participants will attend three, 90-minute, non-drug, Preparatory Sessions
(V1-3). Following the Preparatory Period, each participant will begin a ~17-week Treatment
Period consisting of an Individual phase and a Group phase, with 2 Individual Experimental
Sessions, and 1 Group Experimental Session. The Individual Experimental Sessions will each be
followed by three Individual Integrative Sessions, and the Group Experimental Session will be
followed by two Group Integrative Sessions. MDMA will be administered three times during the
Treatment Period (V4, V8, and V14). The Experimental Sessions will last ~8 hours. Three
90-minute Individual Integration Sessions and a PCL-5 assessment (as an exploratory measure)
will follow the first and second Individual Experimental Session (V4 and V8), each a week
apart. The first Individual Integration Session (V5) will occur the morning following V4, and
the next Individual Integration Session (V6) will occur a week later. The PCL-5 (V7) is
administered a week after V6, at the third Integration Session (V7). The same regimen will
follow Treatment 2 (V8): an Individual Integration Session (V9) will occur the morning
following V8, the next Individual Integration Session (V11) a week later, PCL-5 assessment
will take place at the same visit of the third Integration Session (V11) one week later.
Finally, the Group treatment period will begin 2-10 weeks after V11. n order to synchronize
between all individual participants, after their different dates completing V11, and to allow
their joint synchronized commencement of the group phase. To reduce this time variability to
a minimum, the Individual group members will commence their Individual treatment period
within the same week as the rest of the group. Since the study team must recruit and screen
potentially eligible participants (see Section 5.6 Recruitment Strategies), coordinate
schedules among participating staff members, and coordinate medication taper plans and
assessments there must be adequate flexibility factored into the timing of screening, initial
enrollment, and scheduling. The timing of initial enrollment for participants may be delayed
or adjusted at the sponsor-investigator's discretion. The group phase will begin with two
90-minute Preparatory Sessions (V12-V13), focused on enabling acquaintance among group
members, and discussing the individual goals of each group member. Three Integration Sessions
(V15-17), each a week apart, will follow the third Experimental Group Session (V14). V15 will
take place the morning after V14. The Primary Outcome measure will be the change in PCL-5
Score from Screening (Baseline) to V18 (Outcome), ~7 weeks after the final Experimental
Session (V14) and ~4 weeks after the final Integration Session (V17), and assessed by a rater
from the research team. V18 will also be the study termination visit.
