Major Depression Clinical Trial
Official title:
Effects of Electroconvulsive Therapy on Monoamine Oxidase A Distribution Volume in Treatment-Resistant Depression Investigated With PET
This study aims at evaluating the effect of electroconvulsive therapy in treatment-resistant depressed patients on the major serotonin degrading enzyme in the human brain using neuroimaging methods, the monoamine oxidase A. Electroconvulsive therapy is an effective treatment option in severe cases of depression. However, the mechanisms underlying its effect remain uncertain, though variations within the serotonergic neurotransmitter system seem to be crucially involved.
In treatment-resistant depression, electroconvulsive therapy (ECT) has been shown to
effectively reduce depressive symptoms; however, the underlying neurobiological mechanisms
remain to be fully understood. Recent neuroimaging findings underline the involvement of the
serotonergic system in the mechanism of action of ECT, but studies in this context mainly
focused on serotonin receptor and the serotonin transporter. Here, the aim of the study is to
assess the effects ECT on monoamine oxidase A (MAO-A), the main serotonin degrading enzyme
which is known to be involved in antidepressant action, in humans using positron emission
tomography (PET) and the radiotracer [11C]harmine. Moreover, as the antidepressant effects of
electroconvulsive stimulations were shown to be partly mediated via changes in
neuroplasticity, a secondary aim of the present study is to assess structural alterations
caused by ECT using magnetic resonance imaging (sMRI).
Based on the literature, the investigators expect higher baseline MAO-A distribution volumes
(DVs) in depressed patients than compared to healthy subjects.Moreover, the investigators
expect overall MAO-A distribution volume (DVs) changes in the brain of depressed patients
following ECT according to the individual treatment-response. Similarly, the investigators
assume that depressed patients will exhibit structural changes of grey matter volume
following ECT.
The investigation is designed as a longitudinal mono-centre study over a duration of 36
months. 18 subjects with therapy-resistant, severe unipolar depression, aged between 18-60
years and 18 age- and sex-matched healthy subjects will be included in the study. Patients
will be recruited at the Department of Psychiatry and Psychotherapy, Medical University of
Vienna, and will be offered inpatient care. Psychotropic medication (except for drugs
directly binding MAO-A, e.g. moclobemid) of the patients is allowed if steady state has been
reached > 10 days prior to inclusion. Healthy subject will be recruited using announcements
of poster boards at the General Hospital of Vienna. Each patient will be measured three times
using a GE Advance PET scanner and the radioligand [11C]harmine. The first and second
measurements determine baseline changes in the MAO-A DVs while the third scan is used to
quantify changes induced by ECT. Healthy subjects will be measured with PET only once.
Similarly, patients will undergo three structural (T1-weighted) MRI sessions temporally
coordinated to the PET scans. Healthy subjects will be measured with MRI only once.
Each patient will be treated in 6 to 14 ECT sessions within a time interval of 2 to 5 weeks.
A brief pulse ECT machine (Thymatron System IVTM) will be used three times per week to
administer treatments either unilaterally over the right hemisphere or, if required,
bilaterally.
The MAO-A DVs will be determined using a region of interest and a whole brain voxel-wise
approach. A repeated-measures analysis of variance (ANOVA) will compare the change in the
MAO-A DVs before and after ECT (PET2-PET3) with the change between the baseline PET scans
(PET1-PET2). Secondly, MAO-A DVs from PET1 will be compared to the scans of healthy subjects
(cross-sectional part). Additionally, the correlation between treatment effects reflected in
HAM-D score and changes in MAO-A DVs will be computed. Similar statistical analyses will be
done with sMRI data.
This study would be the first to demonstrate an effect of ECT on MAO-A DVs in humans in vivo.
Given the involvement of the MAO-A in the pathophysiology of mood disorders, the present
study would be an important step towards a better understanding of antidepressant treatment
and treatment response. By comparing treatment effects and the underlying biological
mechanism, the study might help to identify biomarkers that distinguish patients who are
likely to benefit from ECT from patients who will rather be non-responders. Finally, by
investigating the role of the MAO-A DVs in ECT, its highly discussed relevance for
antidepressant action will be further elucidated and might prepare the ground for new
therapeutic strategies. Additionally, this study might contribute in substantiating potential
effects of ECT on brain structure.
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