Plain English Summary
Background and study aims
Obsessive-compulsive disorder (OCD) is a serious mental health condition where individuals experience persistent, unwanted thoughts (obsessions) and feel compelled to perform repetitive behaviors (compulsions). These obsessions and compulsions can greatly disrupt daily life. While therapies like counseling and certain medications are successful for about half of patients, others may need alternative options like different medications or deep brain stimulation, which involves surgery and carries risks. Research is ongoing to explore new treatments, such as repetitive transcranial magnetic stimulation (rTMS), which has shown promise in treating OCD. In this study, we will investigate the effectiveness of a specific type of rTMS on reducing OCD symptoms and its impact on brain activity. To accurately assess its effectiveness, we will include a placebo stimulation in the study, where some participants will receive a simulated treatment that we do not expect to have an effect.
Who can participate?
Patients with OCD, 18 to 70 years old with no contraindications for rTMS
What does the study involve?
The participant was assigned by a computer program to one of two groups:
a) receiving active 20Hz ACDC TMS, set at 100% of their motor threshold, consisting of 40 rounds of stimulation with 50 pulses each, lasting 18 minutes, totaling 2000 pulses per session, for 1 session;
b) receiving sham ACDC TMS, where a sham coil was applied to the mPFC for 1 session.
Immediately after the stimulation, the participant underwent EEG testing while performing the Stroop task, and any side effects were assessed.
What are the possible benefits and risks of participating?
If you grant Consent, you will be contributing to the collection of data that will help decide whether TMS is an effective method in the treatment of OCD. At the same time, the conditions for which you are being treated may be improved. There is no honorarium for participating in the research.
The risks of rTMS are generally low, with the main risk being the induction of an epileptic seizure. Even this risk has so far been very rare, usually in people who are predisposed to seizures. Therefore, people who have or have had epilepsy (even a single seizure) or suspected epilepsy, or who belong to a risk group for epileptic seizures, i.e. people after a serious head injury with unconsciousness, after a stroke, with increased intracranial pressure and, according to individual assessment, with other neurological diseases affecting the brain (brain tumours, multiple sclerosis, Parkinson's disease, etc.), cannot participate in rTMS (and this project). Due to the magnetic field induction, TMS cannot be performed on persons with metallic material in the head area (vascular clips, stimulator, cochlear implants, foreign bodies, etc.) except in the mouth. If any of the conditions and situations described above apply to you, please inform the researcher who will contact you.
Where is the study run from?
National Institute of Mental Health (Czechia)
When is the study starting and how long is it expected to run for?
November 2022 to October 2023
Who is funding the study?
Charles University (Czechia)
Who is the main contact?
Dr Olga Laskov, olga.laskov@nudz.cz
Study website
https://www.nudz.cz/vyzkum/vyzkumny-program-klinicky/pracovni-skupiny/stimulacni-metody
Contact information
Type
Public, Principal Investigator
Contact name
Dr Olga Laskov
ORCID ID
http://orcid.org/0000-0002-2856-1024
Contact details
Topolova 748
Klecany
25067
Czech Republic
+420 283 088 148
olga.laskov@nudz.cz
Type
Scientific
Contact name
Dr Monika Klirova
ORCID ID
https://orcid.org/0000-0002-8092-9586
Contact details
Topolova 748
Klecany
25067
Czech Republic
+420 283 088 141
monika.klirova@nudz.cz
Additional identifiers
EudraCT/CTIS number
Nil known
IRAS number
ClinicalTrials.gov number
Nil known
Protocol/serial number
140223
Study information
Scientific title
The anterior cingulate double cone transcranial magnetic stimulation (ACDC TMS) as an instrument for the investigation of inhibitory control in patients with obsessive compulsive disorder (OCD)
Acronym
ACDC OCD
Study hypothesis
A single active ACDC TMS application in a patient population with OCD will lead to:
1. Enhancement of the inhibitory control performance as measured by the Stroop test - decrease in the interference,
2. Lower reaction times to incongruent stimuli (as previous studies showed),
3. Lower error count,
4. Decrease of the ERN, P3, and N2 amplitude in response to errors,
5. Increase of P3 and N2 latencies in response to errors,
6. Reduction of the theta amplitude in resting EEG compared to sham dTMS and
7. At the same time, we expect that the behavioral and electrophysiological changes induced by the application of active dTMS will be positively correlated with Y-BOCS rates and negatively correlated with disease duration.
Ethics approval(s)
Approved 04/11/2022, Ethics committee of the Third Faculty of Medicine, Charles University (Ruska 87, Prague, 10000, Czech Republic; +420 267102111; marek.vacha@lf3.cuni.cz), ref: GAUK140223
Study design
Randomized placebo-controlled double-blind study
Primary study design
Interventional
Secondary study design
Randomised controlled trial
Study setting(s)
Hospital, Laboratory
Study type
Other, Treatment
Patient information sheet
See outputs table
Condition
Inhibitory control in patients with obsessive compulsive disorder
Intervention
The participant was randomly (by computer program) allocated to one of the two groups: a) active 20Hz ACDC TMS, 100% of motor threshold, 40 trains, 50 pulses per train, 18 minutes duration; 2000 pulses per session; 1 session; b) sham ACDC TMS with a sham coil applied either to mPFC; 1 session. Right after the stimulation: EEG with Stroop task and side effect assessment took place.
Intervention type
Device
Pharmaceutical study type(s)
Not Applicable
Phase
Not Applicable
Drug/device/biological/vaccine name(s)
ACDC TMS was administered using a MagPro R30 stimulator with a cool D-B80 A/P coil
Primary outcome measure
Inhibitory control measured via the interference effect in the Stroop task, measured as the reaction time to incongruent minus the reaction time to congruent stimuli right after the active and sham ACDC TMS stimulation
Secondary outcome measures
Measured right after the active and sham ACDC TMS stimulation:
1. Inhibitory control measured via the reaction times change and error count in the Stroop task (as less sensitive markers)
2. Electrophysiological effect of the active and sham ACDC TMS stimulation measured using EEG
Overall study start date
04/11/2022
Overall study end date
31/10/2023
Reason abandoned (if study stopped)
Eligibility
Participant inclusion criteria
1. Male and female inpatients or outpatients from the daycare center entering six-week CBT at age 18-70 years
2. Meet DSM-V criteria for OCD as determined by Structured Clinical Interview for DSM-5 (SCID-5)
3. The mental ability to understand and sign Informed Consent Form
4. Being on a stable and adequate dose of antidepressants and/or antipsychotics (monotherapy or combination) for atleast one week prior to enrolment and if clinically appropriate to continue on an unchanged dose of medication during the trial
Participant type(s)
Patient
Age group
Adult
Lower age limit
18 Years
Upper age limit
70 Years
Sex
Both
Target number of participants
30
Total final enrolment
30
Participant exclusion criteria
1. Psychiatric comorbidity on axis I and II according to DSM V in six months before enrollment to the study
2. Personality disorder that makes participation in the trial difficult
3. History of substance dependence in the last year except nicotine
4. Contraindications of rTMS (history of epilepsy or any neurologic condition likely to increase risk of seizure, mass brain lesions, cerebrovascular accident, metal in the head, a history of major head trauma with unconsciousness longer than 5 minutes)
5. Pregnancy or breast-feeding
6. Patients with severe somatic disorders (cardiovascular disease, neoplasms, endocrinology disorders etc.)
7. Patients treated with electroconvulsive therapy less than 3 months before enrollment or suffering from neurologic disorder (e.g., epilepsy, head trauma with loss of consciousness) and patients using any treatment which can strongly affect EEG
8. Substantial suicidal risk as judged by the treating psychiatrist
9. Sensory and motor impairment precluding the participation in computer tests
Recruitment start date
01/12/2022
Recruitment end date
31/10/2023
Locations
Countries of recruitment
Czech Republic
Study participating centre
National Institute of Mental Health
Topolova 748
Klecany
25067
Czech Republic
Sponsor information
Organisation
Charles University
Sponsor details
Ovocný trh 5
Prague
116 36
Czech Republic
+420 224 491 850
info@cuni.cz
Sponsor type
University/education
Website
http://www.cuni.cz/UKENG-1.html
ROR
Funders
Funder type
University/education
Funder name
The Charles University Grant Agency (GA UK)
Alternative name(s)
Funding Body Type
Funding Body Subtype
Location
Results and Publications
Publication and dissemination plan
Team members will publish 2 papers in a peer-reviewed journal with an impact factor (e.g., Frontiers in Systems Neuroscience, Brain Research, Brain Stimulation, etc.).
Results will be also presented at national or international scientific meetings, e.g., Czech-Slovak Psychopharmacological Conference, ECNP Congress, and Brain Stimulation Conference.
Intention to publish date
01/01/2025
Individual participant data (IPD) sharing plan
The datasets generated during and/or analysed during the current study will be available upon request rom Dr. Olga Laskov olga.laskov@nudz.cz
IPD sharing plan summary
Available on request
Study outputs
Output type | Details | Date created | Date added | Peer reviewed? | Patient-facing? |
---|---|---|---|---|---|
Participant information sheet | in Czech | 17/04/2024 | No | Yes | |
Statistical Analysis Plan | 17/04/2024 | No | No |
Additional files
- 45325 PIS.pdf in Czech
- 45325 SAP.pdf