Depressive Disorder Clinical Trial
Official title:
The Effect of Transcranial Direct Current Stimulation on Cognitive Side Effects of Electroconvulsive Therapy
Electroconvulsive therapy (ECT) is an effective treatment for a variety of psychiatric
disorders. However, despite continued advances in ECT technique, neurocognitive dysfunction
continues to be a frequent adverse effect. Declarative memory and less so selective memory
are often impaired after an ECT course. Immediate memory, however, is broadly preserved. It
is hypothesized that memory impairments are due to ECT induced disruptions on long term
potentiation as well as in cerebral flux and glutamatergic and cholinergic systems. Different
pharmacological agents for the treatment of ECT induced cognitive dysfunction have been
tried. Agents such as opioids, vasopressin, neuropeptides, cholinergic agents, thyroid
hormone, and stimulants have been used with equivocal results, and no controlled studies
showed clear efficacy.
Transcranial direct current stimulation (tDCS) is a non-invasive, painless brain stimulation
treatment that uses direct electrical currents to stimulate specific parts of the brain.
Electrical currents are applied constantly at low intensities (1-2 mA) over a long period,
usually in minutes (5-30 minutes), to achieve changes in cortical excitability by influencing
spontaneous neural activity. There are two types of stimulation with tDCS: anodal and
cathodal stimulation. Anodal stimulation acts to excite neuronal activity while cathodal
stimulation inhibits or reduces neuronal activity. Several studies demonstrated moderate to
strong effect sizes of tDCS in various neurocognitive and neuropsychiatric settings. Majority
of studies show positive effects of tDCS on cognitive functioning among healthy volunteers
and subjects with neurological or psychiatric conditions. Beneficial effects of online
stimulation applied over the left dorsolateral prefrontal cortex have been reported for
working memory, attention and information processing in depressed patients. To the
investigators' knowledge no studies have evaluated the potential efficacy of tDCS for the
prevention of ECT induced cognitive adverse effects.
In the current study, the investigators propose a double blind, randomized controlled trial
to test the use of tDCS as a strategy to prevent or mitigate the memory impairments
frequently associated with an ECT course.
This is a prospective, random assignment, double blind, parallel group study with an adaptive
design comparing the efficacy of tDCS performed during the course of ECT to that of sham tDCS
in patients with a major depressive episode being treated with ECT. The investigators intend
to recruit patients who are scheduled to receive an acute course of ECT. Patients who are
able and willing to provide written informed consent, and who meet study criteria when
screened, will be randomly assigned on a 1:1 ratio to receive a course of real tDCS or sham
tDCS. Subjects will receive a standard acute course of bifrontal ECT (3X/week) and depressive
symptomatology will be monitored with the Hamilton Rating Scale for Depression (HRSD-24)
before each treatment.
The primary outcome will be change in cognition from baseline to end of study. The
investigators will monitor cognitive changes before and after each ECT treatment, at the end
of the treatment course and two months after the last treatment.
Secondary outcome will be the number of treatments needed to achieve remission. Remission is
defined as two consecutive Hamilton Rating Scale for Depression (HRSD) scores <= 10, and HRSD
total score does not change > 3 points or remains < 6 at the last two consecutive treatments.
In addition, the investigators will collect data on other treatment parameters such as
seizure duration, electroencephalogram (EEG) morphology as well as hemodynamic changes.
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