Individualized Functional Connectivity Targeting in aiTBS for Depression (AINT)

Mass General Brigham

Status and phase

Active, not recruiting

Phase 2

Conditions

Mental Disorder

Psychiatric Disorder

Depressive Disorder, Major

Depression

Mood Disorders

Treatments

Procedure: transcranial magnetic stimulation

Study type

Interventional

Funder types

Other

Identifiers

NCT05680727

2022p001650

Details and patient eligibility

About

The goal of this clinical trial is to estimate the importance of neuroimaging in accelerated intermittent theta burst stimulation (aiTBS) for depression. Participants will receive aiTBS treatment, but they will not know if their treatment spot was found with neuroimaging or head measurements.

Full description

Techniques for modulating human brain networks are rapidly evolving. One of the most exciting new developments is accelerated intermittent theta burst stimulation (aiTBS), a transcranial magnetic stimulation (TMS) protocol that involves multiple daily treatments rather than gold standard once daily treatment. A specific accelerated iTBS protocol called Stanford Accelerated Intelligent Neuromodulation Therapy (SAINT) was cleared by the FDA in September 2022 based on two pilot studies in which patients with treatment-resistant depression rapidly and robustly improved with SAINT. Many of these patients had been depressed for decades and had not improved with conventional TMS or electroconvulsive therapy. Despite these promising results, two issues may limit SAINT scalability: 1) SAINT has only been tested at a single site in a small number of patients, 2) SAINT has never been tested without individualized resting state functional connectivity (rsfc) targeting, which is not widely available or covered by insurance. In this pilot trial, patients with treatment-resistant depression (n=40) will be randomized to one of two active treatment arms: 1) Real aiTBS with real individualized rsfc targeting, or 2) Real aiTBS with sham individualized rsfc targeting (i.e. conventional TMS targeting based on scalp landmarks). All patients will receive active stimulation, which will facilitate enrollment and reduce ethical concerns about placebo treatment in a vulnerable population when there is existing evidence of treatment efficacy. Patients and clinicians will be blind to group assignment, and blind integrity will be assessed. All patients will undergo MRI scans immediately before treatment and at one month follow up, which aligns with our clinical outcome measures.

Enrollment

40 estimated patients

Sex

All

Ages

22 to 80 years old

Volunteers

No Healthy Volunteers

Inclusion criteria

English proficiency sufficient for informed consent, questionnaires/tasks, and treatment
Primary diagnosis of major depressive disorder per Diagnostic and Statistical Manual (DSM)-V criteria (MINI International Neuropsychiatric Interview)
>20 on BDI
>20 on the MADRS 10, 11
Moderate to severe level of treatment resistance (Maudsley Staging Method)
Stable antidepressant medication regimen, or remain medication free, for 4 weeks prior to treatment and to remain on this regimen throughout the study (including all follow-up assessments after the 5-day treatment protocol).
Primary clinician responsible for psychiatric care before, during, and after the trial
Agreement to lifestyle considerations
Abstain from becoming pregnant from screening through end of treatment
Continue usual intake patterns of caffeine- or xanthine-containing products (e.g., coffee, tea, soft drinks, chocolate) throughout treatment
Abstain from alcohol for at least 24 hours before the start of each MRI and TMS session
Abstain from tobacco products during treatment day

Exclusion criteria

Active pregnancy as determined by a urine pregnancy test
Primary psychiatric diagnosis other than major depressive disorder requiring treatment other than comorbid anxiety disorder
Those who did not respond to electroconvulsive therapy (ECT) after 8 sessions
Recent (within 4 weeks) or concurrent use of rapid acting antidepressant agent (ketamine/esketamine/ECT)
History of:
Prior exposure to TMS
Neurosurgical intervention for depression
Autism spectrum disorder
Intellectual disability
Severe cognitive impairment
Significant neurological illness (e.g., dementia, Parkinson's, Huntington's, brain tumor, seizure disorder, subdural hematoma, multiple sclerosis, brain lesion)
Untreated or insufficiently treated endocrine disorder
Treatment with investigational drug or intervention during the study period
Depth-adjusted TMS treatment dose > 65% maximum stimulator output
≥ 30% change in MADRS score between screening and baseline
Anyone presenting with:
Mania or hypomania
Psychosis
Active suicidal ideation or a suicide attempt (defined by C-SSRS) within the past year
Neurological lesion
Contraindications to either TMS or MRI (e.g., metallic implants, severe insomnia > 4 hours per night with hypnotic, etc.).
Current moderate or severe substance use disorder or demonstrating signs of acute substance withdrawal
Positive urine drug screen for illicit substances
Severe borderline personality disorder
Any other condition deemed by the PI to interfere with the study or increase risk to the participant

Trial design

Primary purpose

Treatment

Allocation

Randomized

Interventional model

Parallel Assignment

Masking

Triple Blind

40 participants in 2 patient groups

real individualized resting state functional connectivity targeting

Other group

Description:

Participants in this group will receive aiTBS with neuronavigation to a treatment target identified with individualized resting state functional connectivity.

Treatment:

Procedure: transcranial magnetic stimulation

sham individualized resting state functional connectivity targeting

Other group

Description:

Participants in this group will receive aiTBS with neuronavigation to a treatment target identified with head measurements (i.e., Beam F3)

Treatment:

Procedure: transcranial magnetic stimulation