Clinical Trial Details
— Status: Withdrawn
Administrative data
| NCT number |
NCT04436952 |
| Other study ID # |
ENV-OCD-2020-01 |
| Secondary ID |
|
| Status |
Withdrawn |
| Phase |
N/A
|
| First received |
|
| Last updated |
|
| Start date |
July 2020 |
| Est. completion date |
July 2022 |
Study information
| Verified date |
June 2020 |
| Source |
University of Alberta |
| Contact |
n/a |
| Is FDA regulated |
No |
| Health authority |
|
| Study type |
Interventional
|
Clinical Trial Summary
Obsessive Compulsive Disorder is a highly debilitating condition with a lifetime prevalence
of 2%-3%, and a notable percentage of patients (40-60%) have a partial or no response to
medications. The present gold standard for the treatment of OCD is medications (Selective
serotonin reuptake inhibitors (SSRIs) / Clomipramine) + Exposure and Response Prevention
(ERP). There is a significant need for alternative novel methods of treatment. One of the
novel methods of treating OCD is using magnetic stimulation which has already been
successfully used in the treatment of depression. Treating OCD is difficult with regular
superficial repetitive Transcranial Magnetic Stimulation (rTMS) hence the need for coils that
targets deeper structures. Thus, we are comparing the efficacy of the two different coils
from two different manufacturers plus using ERP in combination with the different coils.
1. Deep Transcranial Magnetic Stimulation (DTMS) using BrainsWay H7 coil targets deeper
structures such as medial prefrontal cortex. The H7 coil has already shown clear
evidence in treating patients with OCD and has been approved by the FDA for clinical
use.
2. Repetitive Transcranial Magnetic Stimulation (rTMS) using MagVenture Cool D-B coil could
also target the medial prefrontal cortex. Hence it might also be equally effective as
the BrainsWay H7 coil in treating patients with OCD.
Description:
i. Purpose
a) The purpose of this study is to compare and evaluate the efficacy of repetitive
Transcranial Magnetic Stimulation (rTMS) by MagVenture and Deep Transcranial Magnetic
Stimulation (DTMS) by BrainsWay with and without the combination of active Exposure and
Response Prevention (ERP) for the treatment of patients with OCD.
ii. Hypothesis a) We hypothesize that the combination of TMS + active ERP will have a
superior efficacy in the treatment of OCD. We also hypothesize that MagVenture cool D-B80
coil will be as effective as BrainsWay H7 coil in treating patients with OCD.
iii. Justification
1. The Prospective Multicenter Randomized Double-Blind Placebo-Controlled Trial by Carmi et
al. (2019) had shown significant improvement in OCD symptoms by using the H7 coil and
provocation of OCD symptoms before and during treatment.
2. The study by Dunlop et al. (2016) has shown reduction in OCD symptom severity by using
the Cool D-B80 Coil without provocation.
3. There have been no head to head studies comparing the BrainsWay H7 coil and MagVenture
Cool D-B80 coil using provocation methods for both coils.
4. Also there have been no head to head studies comparing the gold standard treatment of
medications + active ERP with medications + active ERP + TMS and medications + TMS.
iv. Objectives
a) The aim of the study is to evaluate and compare the efficacy of DTMS treatment and the
rTMS treatment with and without the combination of active ERP in patients suffering from OCD,
in conjunction with medications approved for OCD treatment.
v. Research Method/Procedure
1. Recruit 100 patients suffering from OCD who have been treated and currently on at least
one SSRIs, SNRIs, clomipramine and at least one trial of CBT (Exposure and Response
Prevention) had an inadequate response.
2. Make a personalized provocation for each patient and using them during treatment
3. The trial will consist of 3 phases:
1. Pre-study screening and baseline assessment;
2. Treatment trial period (8 weeks); and
3. Follow-up (12 weeks).
4. Clinical severity rating scales will be taken every other week and include: (Brief
Obsessive-Compulsive Scale (BOCS), Yale-Brown Obsessive-Compulsive Scale (Y-BOCS) ,
Beck's Depression Inventory (BDI), Clinical Global Impression Severity (CGI-S) and
Clinical Global Impression Improvement (CGI-I). Safety evaluations will include adverse
event monitoring, vital signs, and cognitive changes (Mini-Mental State Exam (MMSE)).
All measures will be taken before treatment administration.
5. Pre-Study Screening and Baseline Assessment
1. Potential Patients will be given complete information describing the study
treatment and their role in the trial, and they will be encouraged to ask any
questions regarding the trial. The risks and requirements of this clinical research
trial will be explained to each potential patient. Those volunteering to take part
will read and sign the Informed Consent Form for participation in the clinical
research trial before any trial-related procedures are performed.
2. Upon obtaining the signed informed consent, inclusion and exclusion criteria will
be reviewed to verify the patient's eligibility.
3. Baseline data are defined as the data generated during the baseline visit before
the first treatment Session.
6. After the patients has been admitted into the study, they will be asked to undergo a
fMRI and then randomly organized based on age and symptom severity into the 5 different
groups.
7. Comparing 5 groups of patients with OCD 1) Group 1 - 20 patients undergoing DTMS
treatment using the H7 coil 2) Group 2 - 20 patients undergoing rTMS treatment using the
cool D-B80 coil 3) Group 3 - 20 patients undergoing DTMS treatment using the H7 coil +
ERP 4) Group 4 - 20 patients undergoing rTMS treatment using the cool D-B80 coil + ERP
5) Group 5 - 20 patients undergoing ERP only
8. Treatment Trial period
1) During the treatment phase the patients will either receive
Group 1 - medial prefrontal cortex (mPFC) DTMS 5 days a week for 8 consecutive weeks =
40 Sessions 20 Hz at 100% MT, 2 s on 20 s off intertrain interval, 50 trains, 2000
stimuli per session.
TMS will be done at active state by provocation
Group 2 - dorsomedial prefrontal cortex (DMPFC) rTMS 5 days a week for 8 consecutive
weeks = 40 sessions 10 Hz at 120% MT, 5 s on 10 s off intertrain interval, 60 trains,
First 3000 pulses to the left DMPFC then 3000 pulses to the right DMPFC. TMS will be
done at active state by provocation
Group 3 - medial prefrontal cortex (mPFC) DTMS + ERP 5 days a week for 8 consecutive
weeks = 40 sessions 20 Hz at 100% MT, 2 s on 20 s off intertrain interval, 50 trains,
2000 stimuli per session. TMS will be done at active state by provocation The ERP will
be administered for 2 hours on week 1 and week 8 and for 1 hour on Weeks 2 to 7 for a
total of 10 hours.
Group 4 - dorsomedial prefrontal cortex (DMPFC) rTMS +ERP 5 days a week for 8
consecutive weeks = 40 sessions 10 Hz at 120% MT, 5 s on 10 s off intertrain interval,
60 trains, First 3000 pulses to the left DMPFC then 3000 pulses to the right DMPFC. TMS
will be done at active state by provocation The ERP will be administered for 2 hours on
week 1 and week 8 and for 1 hour on Weeks 2 to 7 for a total of 10 hours.
Group 5 - ERP The ERP will be conducted for 2 hours on week 1 and week 8 and for 1 hour
on Weeks 2 to 7 for a total of 10 hours.
9. Prior to initiation and during each treatment of TMS, OCD symptoms will be provoked for
each patient in an individual manner to activate the relevant brain circuitry. Targeted
questions will be designed for each patient using external, internal or a combination of
provocations and the degree of provocation on a Visual Analog Scale will be recorded.
These may require adjustment as the patient improves.
10. Study evaluations will be performed every week at the beginning of the next treatment
week (from week 2), prior to the first or second (preferably second) treatment session
of that week. Procedures to be performed at the 8-week visit will also be performed in
case of Early Discontinuation of the study.
11. Follow up period 1) All patients will be followed up at week 12. vi. Plan for Data
Analysis
1. Primary Efficacy Variable
- The primary outcome measure is the BOCS and YBOCS severity rating scale. The primary
efficacy endpoint is the change in BOCS and YBOCS severity score from baseline to the
8-week visit.
2. Secondary Efficacy Variables
- Change from baseline to the 8-week visit in the Clinical Global Impression - Severity
(CGI-S) and Improvement (CGI-I) scores.
- Change from baseline to the 12-week visit in the BOCS and YBOCS severity score.
- Change from baseline to the 12-week visit in the Clinical Global Impression - Severity
(CGI-S) and Improvement (CGI-I) scores.
3. Exploratory Efficacy Variables - Change from baseline to the 8 week and 12 weeks visit
in the Beck's Depression Inventory score.
- fMRI changes before and after treatment and using fMRI to predict future response
to TMS treatment (to identify responders and non-responders)
