Depression Clinical Trial
Official title:
Establishing Moderators and Biosignatures of Antidepressant Response for Clinical Care (EMBARC) for Depression
This study will examine multiple carefully selected clinical and biological markers, using both existing state-of-the-art technologies as well as pioneering, innovative approaches. The study is designed to identify moderators and mediators of treatment response for depression in order to specify a biosignature of treatment response for depression. Evaluation of the usefulness of these markers in a carefully conducted clinical trial comparing an antidepressant to placebo will assist in developing a Depression Treatment Response Index (DTRI) to help clinicians match treatments to patients with MDD, resulting in timely selection of treatments best suited for individual patients and thus approaching personalized treatment. The resulting index provides a truly novel means of synthesizing the contribution of key clinical and biological parameters in an easy to use tool for clinical care.
The current study is designed to identify biomarkers for the prediction of differential
treatment outcomes between the SSRI antidepressant sertraline (SERT) and placebo (PBO) in a
randomized trial for patients with MDD. In addition, a second stage will collect data to
explore moderators and mediators of treatment outcomes between pharmacologically distinct
active treatment arms: sertraline (SERT), a serotonergic antidepressant or bupropion (BUP), a
nonserotonergic antidepressant. To reduce biologic heterogeneity, we will only enroll
patients with early onset of DSM IV MDD (before age 30) because these criteria in probands
have been shown to be associated with increased familial loading in families. Patients will
also have recurrent MDD with 2 or more recurrences (including current episode). Additionally,
patients will be required to have a current symptom severity score of 14 or more on the Quick
Inventory of Depressive Symptomatology - Self Report (QIDS-SR), both at study screening and
at the randomization (baseline) visit. In the first stage, patients will receive an 8−week
course of treatment in one of the two study arms. As part of the Sequential Multiple
Assignment Randomized Trial (SMART) design patients that have not achieved a response at the
end of 8 weeks to their stage one treatment, defined by < 50% improvement on the Clinical
Global Improvement scale (CGI), will be switched to Stage 2 treatment (8 weeks). Patients who
have achieved satisfactory response (>= 50% improvement on the CGI) will be continued on
treatment for an additional 8 weeks.
Specific Aims
Moderator Aims (Aim 1): To identify baseline clinical, neuroimaging, neurophysiological, and
behavioral moderators of differential treatment outcome (mean symptom change and
tolerability) for sertraline (SERT, a serotonergic antidepressant) versus placebo (PBO) for
the treatment of MDD. Symptom change will be measured using the mean change from baseline in
the 17-item Hamilton Rating Scale for Depression (HRSD17). Tolerability will be measured
using the Frequency, Intensity, and Burden of Side Effects Rating (FIBSER) and the Treatment
Emergent Symptom Scale (TESS).
Mediator Aims (Aim 2): To identify early phase (week 1) changes in neuroimaging,
neurophysiological, and behavioral tasks as mediators of differential treatment outcomes
(symptom change, tolerability) to SERT and PBO.
Main Treatment Effects Aim (Aim 3): To compare the 8-week outcomes of SERT vs. PBO using
mixed model regression analysis to maximize power to discriminate treatment efficacy
differences.
Primary Outcomes:
- 17-item Hamilton Rating Scale for Depression (HRSD17)
Secondary Outcomes:
- the Frequency, Intensity, and Burden Side Effects Rating (FIBSER)
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