Clinical Trial Details
— Status: Withdrawn
Administrative data
| NCT number |
NCT03628573 |
| Other study ID # |
H14-03368 |
| Secondary ID |
|
| Status |
Withdrawn |
| Phase |
N/A
|
| First received |
|
| Last updated |
|
| Start date |
January 2016 |
| Est. completion date |
March 1, 2018 |
Study information
| Verified date |
November 2020 |
| Source |
University of British Columbia |
| Contact |
n/a |
| Is FDA regulated |
No |
| Health authority |
|
| Study type |
Interventional
|
Clinical Trial Summary
Repetitive transcranial magnetic stimulation (rTMS) is an emerging treatment for medically
refractory major depressive disorder (MDD), and involves direct stimulation of cortical
neurons using externally applied, powerful, focused magnetic field pulses. rTMS consistently
achieves response rates of 50-55% and remission rates of 30-35% in medically refractory MDD
patients. However, the vast majority of studies have focused its use in outpatient samples.
This study will address whether accelerated rTMS (intermittent Theta Burst Stimulation
(iTBS)) can speed up the response rate and shorten length of stay in hospital for inpatients,
and which biological traits may predict response.
Description:
Major Depressive Disorder (MDD) is a highly prevalent and disabling disorder with substantial
societal cost; furthermore, the costs associated to MDD increase substantially when it
requires hospital admission. Among Neurological, Mental and Substance Use (NMS) disorders,
depression is the number one cause of disability worldwide. Considering this high increase in
prevalence, in addition to the limited efficacy of current treatments, with only 30-40% of
patients achieving remission after an initial treatment, the illness burden attributable to
NMS is projected to increase during the next decade. In Ontario alone, $12.5 billion a year
is attributed to mood disorder related costs. Unfortunately, research into the treatment and
prevention of mental illness is disproportionately low relative to the disease burden.
Approved by Health Canada for MDD in 2002, repetitive transcranial magnetic stimulation
(rTMS) is an emerging treatment for medically refractory major depressive disorder (MDD).
rTMS involves direct stimulation of cortical neurons using externally applied, powerful,
focused magnetic field pulses. Dozens of studies and several meta-analyses over the last 15
years have shown that rTMS of the dorsolateral prefrontal cortex (DLPFC) produces
statistically significant improvements in MDD, even when medications have failed. In the most
recent generation of randomized controlled trials, rTMS consistently achieves response rates
of 50-55% and remission rates of 30-35% in medically refractory MDD patients. However, the
vast majority of studies have focused on its used in outpatient samples. Furthermore, the few
studies that have investigated its used in inpatient samples have demonstrated similar
efficacy rates than medications using the conventional 10 Hz rTMS protocol. No study, has
addressed the question whether rTMS can speed up the response rate, and shorten length of
stay in hospital, nor what are the biomarkers of treatment response to rTMS in inpatient
population. Conventional rTMS protocols, as used in the major trials in the USA that secured
FDA approval in 2008, applied 3000 pulses of unpatterned, 10 Hz stimulation administered over
37.5 minutes. These protocols limit the number of patients who can be treated with a single
machine to approximately 10 per day, thus perpetuating the high cost of treatment. In
contrast, iTBS has been shown to have induce neuroplasticity, effective in MDD, and only
requires 3 minutes to administer, making it a feasible option for multiple treatments per
day, particularly in inpatient populations.
Therefore, addressing the question of biomarkers in inpatient population suffering MDD and
whether improvement can be accomplished in only 3 weeks is a critical question with very
direct impact and translation to clinical care.
HYPOTHESES:
1. Response to an index course of accelerated Left-iTBS 3 treatments per day will be
associated with associated with increased activation of frontal regions in functional
Near Infrared Spectroscopy (fNIRS) and electroencephalogram (EEG) (increase cerebral
blood flow to left DLPFC, and decrease in alpha power in left DLPFC), and decrease of
inflammatory biomarkers.
2. Depression scores on Hamilton Depression Ration Scale (HDRS)-17 will decrease by at the
end of second week of treatment, in 50% of the sample.
OBJECTIVES:
1. To investigate neurophysiological and inflammatory biomarkers in inpatients with
depression treated with accelerated rTMS.
2. To investigate the speed in reduction of symptoms to accelerated rTMS in MDD in
inpatient setting.
PROCEDURES:
The entire study will recruit a total of 50 inpatients. Patients meeting symptomatic criteria
for a depressive episode will receive Left-iTBS 3 treatments per day, 45 to 1 hour apart, for
a total of 20 consecutive days. Patients will undergo motor threshold testing to determine
the appropriate site and strength of stimulation according to standard methods then begin
treatment. Measure will also include electroencephalography (EEG), near infrared spectroscopy
(fNIRS), a blood draw, and cognitive testing, questionnaires. The treatment phase will last
20 days. Treatment will be administered daily in the morning (60 treatments total).
