Comparing the Efficacy of fMRI-Guided vs. Standard iTBS in Treating Depression

The Royal Ottawa Mental Health Centre210 enrolled

Overview

In this triple-blind randomized controlled trial, we ask if targeting intermittent theta burst stimulation (iTBS) based on individual resting state connectivity improves treatment outcomes in major depressive disorder (MDD). For the trial, we will recruit 210 patients with major depressive disorder. Each patient will undergo a 30-40-minute MRI scan, after which they will receive a 6-week standard iTBS treatment. Participants will be randomized to receive iTBS either to the standard neuronavigated target (a technique for treatment location targeting, based on group-average connectivity) or to a personalized connectivity-guided target selected based on individual functional connectivity scans. The main outcome of this trial is response rate as determined by ≥ 50% reduction in Grid HRSD-17 scores. Secondary outcomes include remission rate, change in depression, anxiety and anhedonia symptoms, quality of life, and biological measures of heart rate variability, objective sleep measures and daily activity as a proxy of anhedonia - defined as a reduced ability to experience pleasure.

Repetitive transcranial magnetic stimulation (rTMS) is an FDA-approved and widely used focal, safe, well-tolerated, and non-invasive brain stimulation method for the treatment of depression, and has been approved in Canada. Typical clinical rTMS is delivered on the left dorsolateral prefrontal cortex (DLPFC) at a 10 Hz frequency over 30-45 minutes to induce an increase in cortical excitability, which outlasts the duration of stimulation. iTBS is a novel refinement of conventional rTMS. iTBS consists of bursts of 3 stimulations at 50 Hz at theta frequency (5 Hz). However, instead of 30 minute treatment sessions, iTBS has comparable clinical efficacy with only 3 minute treatment sessions. Currently roughly 50% of the people receiving rTMS treatment for depression respond to the treatment. One of the main goals of current research in rTMS is to find improvements in the protocol to increase the number of responders. One of the potential ways to improve rTMS is to select the target based on individual resting state functional connectivity. Within the DLPFC, there are still several possible targets for the rTMS. Functional magnetic resonance imaging (fMRI) studies have shown that therapeutic effects of rTMS are related to its effects on the subgenual anterior cingulate cortex (sgACC; Broadman area 25). Past literature has shown that in MDD the effectiveness of a target is related to its connectivity with the sgACC. A recent study showed in a retrospective sample of MDD patients that response to rTMS correlates with the distance from the personalized connectivity-guided target rather than a group average target, opening the door for individualized connectivity-guided rTMS targeting. Yet, the question whether individualized connectivity-guided rTMS targeting improves rTMS outcomes in a prospective sample has never been investigated. In this two-arm triple-blind randomized parallel assignment clinical trial we will test if 6-week treatment using individualized connectivity-guided iTBS targeting leads to better outcomes in MDD compared to conventional neuronavigated iTBS.

Interventions

repetitive Transcranial Magnetic StimulationDEVICE

Repetitive transcranial magnetic stimulation (rTMS) is a Health Canada approved treatment for major depression. Typical treatments involve 30 to 45 minutes daily sessions delivered over 4 to 6 weeks. Recent technical advances allowed the development of theta burst stimulation (TBS), a novel rTMS paradigm that reduces daily sessions to 3 to 4 minutes while maintaining the same clinical efficacy. This study will specifically be administering intermittent TBS (iTBS), which is a novel refinement of conventional rTMS and consists of bursts of 3 stimulations at 50 Hz at theta frequency (5 Hz).

Eligibility

Sex: ALLMin age: 18 Years

Medical Language ↔ Plain English

Inclusion criteria: For inclusion in the study, participants must fulfill all the following criteria: 1. voluntary and competent to consent to study, 2. Adults aged 18 years old or older, 3. can speak and read English, 4. primary and/or predominant diagnosis of major depressive episode without psychotic features in the current episode (confirmed by a Mini-International Neuropsychiatric Interview), 5. depressive symptoms have not improved after ≥ 1 adequate dose of antidepressant trial in the current depressive episode, 6. moderate symptoms in the current depressive episode as indexed by a score of at least 15 on the Grid 17-item Hamilton Rating Scale for Depression (Grid HRSD-17), 7. have been referred to rTMS treatment by their treating physician, and took a free and informed decision to follow this treatment, 8. are able to adhere to treatment schedule, 9. have stable psychotropic medications (including prescribed cannabis) or psychotherapy regimen for at least four weeks prior to entering the trial, 10. have an education-adjusted score of ≥ 24 at the Mini-Mental State Evaluation (MMSE) if they are aged ≥ 65. Exclusion criteria: Participants fulfilling any of the following criteria will be excluded from the study: 1. diagnosis of bipolar I or II disorder, based on the DSM-5 criteria 2. current or past (\< 3 months) substance (excluding caffeine or nicotine) or alcohol use disorder, as defined in DSM-5 criteria. Based on the DSM-5 criteria, mild cannabis or alcohol use disorder would be permissible in the past 3 months, moderate to severe would be an exclusion. 3. current use of illegal substances or cannabis (unless medical use, see note below), confirmed by urine drug screen 4. have a concomitant major unstable medical or neurologic illness (e.g. uncontrolled diabetes or renal dysfunction), 5. organic cause to the depressive symptoms (e.g. thyroid dysfunctions), as ruled out by the referring physician 6. acute suicidality or threat to life from self-neglect, 7. are pregnant or breastfeeding, or thinking of becoming pregnant during course of treatment (pregnancy will be assessed by a urine test), 8. have a specific contraindication for TMS (e.g., personal history of epilepsy or seizure, metallic head implant, pacemaker), 9. unwilling to maintain current antidepressant regimen, 10. are taking more than 1 mg of lorazepam per day or equivalent, 11. any other condition that, in the opinion of the investigators, would adversely affect the participant's ability to complete the study, 12. any contraindications for MRI 13. have failed a course of ECT within the current depressive episode due to the lower likelihood of response to rTMS (if they have had failed ECT in the past, this does not exclude them)

Outcomes

Primary Outcomes

Compare the efficacy of fMRI guided TMS and conventional neuronavigated TMS on clinical response.

Clinical response will be defined as a ≥ 50% reduction in the 17-Item Grid Hamilton Rating Scale for Depression (GRID-HRSD-17). The Grid HRSD is a clinician-rated instrument with seventeen items used to measure the severity of depressive episodes. Remission will be defined as a HRSD-17 score \< 8 after 6 weeks of treatment. Score scale from 0 (better outcome, no depression thus better clinical response) to 60 (worst outcome, extreme depression thus worse clinical response).

Time frame: Administered at baseline (prior to first iTBS treatment) and every 2 weeks after that for 6 weeks (week 2, week 4, and week 6).

Secondary Outcomes

Change in severity of clinician-rated depressive symptoms as measured by the Montgomery-Åsberg Depression Rating Scale (MADRS).

As a secondary measure of depressive symptoms. Score scale from 0 (better outcome, no depression) to 52 (worst outcome, extreme depression).

Time frame: Administered at screening, before the first iTBS, week 2, week 4 and after iTBS treatment (week 6).

Change in self-reported depression symptoms as measured by Beck Depression Inventory (BDI-II).

As a secondary measure of depressive symptoms. Score scale from 0 (better outcome, no depression) to 63 (worst outcome, extreme depression).

Time frame: Administered at baseline (prior to first iTBS treatment) and every week after that for 6 weeks (week 1, week 2, week 3, week 4, week 5, week 6).]

Change in self-reported anxiety symptoms as measured by Beck Anxiety Inventory (BAI)

As a secondary measure of anxiety symptoms. Score scale from 0 (better outcome, no depression) to 63 (worst outcome, extreme anxiety).

Time frame: Administered at baseline (prior to first iTBS treatment) and every week after that for 6 weeks (week 1, week 2, week 3, week 4, week 5, week 6).]

Change in self-reported suicidal thoughts symptoms as measured by Beck Scale for Suicidal Ideation (BSS).

To assess the effect of treatment on suicidal thoughts that may be improved by iTBS. Score scale from 0 (better outcome, no desire for suicide) to 38 (worst outcome, extreme desire for suicide).

Time frame: Administered at baseline (prior to first iTBS treatment) and every week after that for 6 weeks (week 1, week 2, week 3, week 4, week 5, week 6).]

Change in self-reported sleep quality as measured by Leeds Sleep Evaluation Questionnaire (LSEQ)

To assess the effect of treatment on self-report sleep that may be improved by iTBS. Score scale from 0 (better outcome, excellent sleep) to 100 (worst outcome, extremely poor sleep).

Time frame: Administered at baseline (prior to first iTBS treatment) and every week after that for 6 weeks (week 1, week 2, week 3, week 4, week 5, week 6).]

Change in self-reported sleep patterns as measured by Pittsburgh Sleep Quality Index (PSQI)

To assess the effect of treatment on self-report sleep that may be improved by iTBS. Score scale from 0 (better outcome, very high quality sleep) to 21 (worst outcome, very low quality sleep).

Time frame: Before the first iTBS and after treatment (6 weeks).

Change in quantity of sleep as measured with Empatica EmbracePlus Smartwatch

To assess the effect of treatment on objective measures of sleep patterns that may be improved by iTBS.

Time frame: Start 2 weeks before the planned start date. Continuous measurement throughout study until the 2-week follow-up visit

Change in perceived stress as measures with Perceived stress scale (PSS)

To assess the effect of treatment on self-report measures of stress that may be improved by iTBS. Score scale from 0 (better outcome, no perceived stress) to 40 (worst outcome, extreme perceived stress).

Time frame: Administered at baseline before first iTBS treatment and after treatment completion (week 6).

Change in physiological stress based on pulse rate and electrodermal activity response as measured with Empatica EmbracePlus Smartwatch

To assess the effect of treatment on objective measures of stress that may be improved by iTBS.

Time frame: Start 2 weeks before the planned start date. Continuous measurement throughout study until the 2-week follow-up visit

Change in self-reported anhedonia as measured by Snaith-Hamilton Pleasure Scale (SHAPS)

To assess the effect of treatment on self-report measures of anhedonia symptoms that may be improved by iTBS. Score scale from 0 (better outcome, no anhedonia) to 14 (worst outcome, extreme anhedonia).

Time frame: Administered at baseline (prior to first iTBS treatment) and every week after that for 6 weeks (week 1, week 2, week 3, week 4, week 5, week 6).]

Change in motion intensity (based on number of steps and total activity) as measured with Empatica EmbracePlus Smartwatch

To assess the effect of treatment on objective measures of physical activity that may be improved by iTBS.

Time frame: Start 2 weeks before the planned start date. Continuous measurement throughout study until the 2-week follow-up visit.

Change in motion heart rate variability as measured with Empatica EmbracePlus Smartwatch

To assess the effect of treatment on objective measures of heart-rate variability, which has been shown to be linked to MDD and that may be improved by iTBS.

Time frame: Start 2 weeks before the planned start date. Continuous measurement throughout study until the 2-week follow-up visit.

Change in self-reported hopelessness as measured by Beck Hopelessness Scale (BHS)

To assess the effect of treatment on self-report symptoms of hopelessness that may be improved by iTBS. Score scale from 0 (better outcome, no sense of hopelessness) to 20 (worst outcome, extreme sense of hopelessness).

Time frame: Administered at baseline (prior to first iTBS treatment) and every week after that for 6 weeks (week 1, week 2, week 3, week 4, week 5, week 6).

Change in quality of life as measured with Quality of Life Enjoyment and Satisfaction Questionnaire - Short Form (Q-LES-Q-SF)

To assess the effect of treatment on self-report measures of quality of life that may be improved by iTBS. Score scale from 0 (worse outcome, poor life satisfaction and poor life quality) to 70 (better outcome, high life satisfaction and high quality of life).

Time frame: Time Frame: Administered at baseline (prior to first iTBS treatment) and every week after that for 6 weeks (week 1, week 2, week 3, week 4, week 5, week 6).

Change in well-being as measured with Short Warwick Edinburgh Mental Well-Being Scale (SWEMWBS)

To assess the effect of treatment on self-report measures of well-being that may be improved by iTBS. Score scale from 14 (worse outcome, poor mental wellbeing) to 70 (better outcome, excellent mental well).

Time frame: Administered before the first iTBS, week 2, week 4 and after iTBS treatment (week 6).

Comparing the Efficacy of fMRI-Guided vs. Standard iTBS in Treating Depression

Overview

Conditions

Interventions

Eligibility

Locations (1)

Outcomes

Primary Outcomes

Secondary Outcomes

Central Contacts