Neuromodulation in the Elderly Depressed: a Brain Im-aging Pilot Study

Universitair Ziekenhuis Brussel1 site in 1 country44 target enrollmentMay 7, 2021

ConditionsOld Age Depressive Disorder, Treatment-Resistant

Overview

Phase: Not Applicable
Intervention: Not specified
Conditions: Old Age
Sponsor: Universitair Ziekenhuis Brussel
Enrollment: 44
Locations: 1
Primary Endpoint: Clinical effect of adTMS (Changes in depression severity clinician-rated and self-report)
Status: Recruiting
Last Updated: 3 years ago

Overview Investigators Eligibility Criteria Outcomes Sites Similar Trials

Overview

Brief Summary

To evaluate safety and efficacy of an accelerated deep brain Transcranial Magnetic stimulation (adTMS) and transcutaneous direct current stimulation (tDCS) protocol in an elderly depressed patient population

Detailed Description

With a growing number of elderly persons, geriatric depression - associated with important morbidity and mortality- is becoming a significant health problem. Given the risk of polypharmacy and increased side effects, alternative non pharmaceutical treatments such as repetitive transcranial magnetic stimulation (rTMS) and transcutaneous direct current stimulation (tDCS) may offer a solution. Given our recent positive results with accelerated rTMS in the elderly depressed, we want to continue to develop non-invasive treatment stimulations. The FDA approved deep brain TMS (dTMS) technique may be a promising option, targeting the brain underneath the neocortex with potentially better response and remission rates. Therefore, in a sham-controlled randomized controled trial, we will treat 44 geriatric depressed patients with accelerated dTMS (5 sessions/day over 4 days only), and evaluate clinical efficacy and safety. One week after the last adTMS or sham treatment, all patients will have access to active treatment in a 3 week open label transcutaneous direct current stimulation (tDCS) with a home-use device. In this manner we can examine clinnical effect of tDCS in the adTMS-sham group as well as the possible maintenance effect of tDCS in the adTMS active treatment group. Because new introduced neuromodulation paradigms should be rigorously neurobiologically examined before applying them on a regular basis, this research will include multimodal brain imaging techniques to elucidate the working mechanisms of these applications in order to optimize response prediction and treatment. Gut microbes can influence human metabolism, nutrition, physiology and immune status. The "microbiota-gut-brain axis" entails a continues exchange of information between the gut and central nervous system. Several clinical and preclinical studies have emphasized the bidirectional role of microbiome disruption in depression and depression-like behavior. In the current project, we also will examine the effects of neurostimulation treatments on the gut microbiome.

Registry

clinicaltrials.gov

Start Date

May 7, 2021

End Date

July 2026

Last Updated

3 years ago

Study Type

Interventional

Study Design

Parallel

Sex

All

Investigators

Sponsor

Universitair Ziekenhuis Brussel

Responsible Party

Principal Investigator

Dieter Zeeuws

Dieter Zeeuws, MD, Head of Clinic in psychiatry

Universitair Ziekenhuis Brussel

Eligibility Criteria

Inclusion Criteria

•• In- and outpatients (age 65 year or older).
•Meeting the Diagnostic and Statistical Manual of Mental Disorders (DSM 5) criteria for unipolar depression according 17-item Hamilton depression rating scale (HDRS-17) score of 17 or more.
•Failed to respond to at least one adequate course with an antidepressant medication trial, including the current one.
•Intention to continue the current (\>6 weeks) antidepressant treatment at a stable dose dur-ing the stimulation.
•Benzodiazepines are permitted up to a maximum dose of 40 mg diazepam or equivalent. If the dosage has been recently changed, it should be stable for at least 2 weeks.
•Able to read, understand and sign the Informed Consent Form.

Exclusion Criteria

•• Psychosis (except depression with psychotic features).
•A personal history of seizures or epilepsy, a history of seizures or epilepsy in first degree relatives and the presence of any known factor that can lower the seizure threshold (sleep deprivation, substance abuse, etc.), previous head injury and the presence of metallic implants in the cephalic region (e.g., aneurysm clips, shunts, stimulators, cochlear implants, electrodes) with the exception of dental fillings. The presence of cardiac pacemakers, neurostimulators, surgical clips or other electronic equipment, comorbidity with the following neurological disorders: increased intracranial pressure, space-occupying lesion, history of stroke or transient ischemic attack, brain aneurysm and any structural brain damage with increased risk for epilepsy detected with (study related) MRI.
•Patients with cognitive disturbances or dementia (Mini Mental State) \<
•Suicide attempt within 6 months before the start of the study or present high risk of suicide per the investigator's clinical judgment and indicative response\* on the Columbia-Suicide Severity Rating Scale (C-SSRS) and 21-items Beck Scale for Suicide Ideation (BSI). \*'yes' on Item 5 (active suicidal ideation with specific plan and intent).
•Any change in the habitual psychopharmacological agents will be considered as dropout.

Outcomes

Primary Outcomes

Clinical effect of adTMS (Changes in depression severity clinician-rated and self-report)

Time Frame: screening, Day 1 (+/-3d), Day 8 (+/-3d) ,Day 15 (+/-3d) Day 36 (+/-3d)

To investigate the effect of adTMS delivered by a H1 coil to the left Dorsolateral Prefrontal Cortex (DLPFC), as an add-on treatment, on depressive symptoms in a sample of elderly patients with MDD.-measured by change in the 17 item Hamilton Depression rating Scale score. For a total score between 0 and 48, the higher the total score the more severe the depression. Response is reduction from baseline of ≥ 50% in the total score and remission is a total HAMD-17 score ≤ 7. * measured by change in the Beck-Inventory of Depression-II score. For a total score between 0 and 63, the higher the total score the more severe the depression. A score of ≤9 is the criterion for remission and BDI-II score decrease of 50% from baseline is the criterion for treatment response. * measured by change in the Geriatric Depression Scale 15 item version (GDS-15) self-rating scale score.

Secondary Outcomes

maintenance effect of tDCS 17 item Hamilton Depression rating Scale score(Day 15 (+/-3d) Day 36 (+/-3d))
Incidence of Treatment-Emergent Adverse Events assessed with the Adverse Events questionnaire(Day 8 (+/-3d) ,Day 15 (+/-3d) Day 36 (+/-3d))
effect on suicide risk as measured by change in BSI(screening, Day 1 (+/-3d), Day 8 (+/-3d) ,Day 15 (+/-3d) Day 36 (+/-3d))
Clinical effect of tDCS Beck-Inventory of Depression-II score(Day 15 (+/-3d) Day 36 (+/-3d))
possible neuroimaging biological markers for response(Day 1 (+/-3d), Day 8 (+/-3d) Day 36 (+/-3d))
maintenance effect of tDCS Beck-Inventory of Depression-II score(Day 15 (+/-3d) Day 36 (+/-3d))
effect on the gut microbiome(Day 1 (+/-3d), Day 8 (+/-3d) Day 36 (+/-3d))
Clinical effect of tDCS Geriatric Depression Scale 15 item version (GDS-15) self-rating scale score(Day 15 (+/-3d) Day 36 (+/-3d))
functional magnetic resonance imaging changes pre/post treatment in gender task as an incidental measure of emotional processing and probe of limbic function, and it's predictive value for response(Day 1 (+/-3d), Day 8 (+/-3d))
Clinical effect of tDCS 17 item Hamilton Depression rating Scale score(Day 15 (+/-3d) Day 36 (+/-3d))
effect on cognition MMSE(screening, Day 8 (+/-3d) ,Day 15 (+/-3d) Day 36 (+/-3d))
effect on suicide risk as measured by change in C-SSRS(screening, Day 1 (+/-3d), Day 8 (+/-3d) ,Day 15 (+/-3d) Day 36 (+/-3d))