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Clinical Trial Summary

This study aims to better understand the mechanisms of action of antidepressants, but also the neural correlates of motivation deficits. One hundred patients with a moderate to severe major depressive episode will be enrolled in this prospective multicenter study. The objective will be to predict the therapeutic response to two first-line antidepressants on the basis of an early neurocomputational assessment of motivation. Antidepressant treatment will be administered as monotherapy after randomization between two drugs: escitalopram and vortioxetine. Patients will undergo six visits and follow-up for one year. The investigators will combine computer modeling and functional MRI to identify motivational deficits and elucidate their brain correlates before initiation, after 7 days and after 6 months of treatment. 36 healthy volunteers will also be included to allow comparison with patients with depression. They will not receive any treatment.


Clinical Trial Description

One hundred patients with a moderate to severe major depressive episode will be enrolled in this prospective multicenter study. Six visits will be scheduled within a year: - V0 (inclusion visit): verification of inclusion and exclusion criteria, information, and consent. - V1 (before randomization - baseline state): - Clinical evaluation using validated questionnaires for the severity of depression, quality of life, anhedonia, apathy, and cognitive dysfunction. - Neuro-cognitive evaluation using a battery of tests to explore motivation, emotion processing, belief construction, and their updating. Part of the tests will be performed during the functional MRI session. - Structural (anatomical) and functional MRI, ASL. - Blood samples. - Randomization and introduction of the new antidepressant will occur immediately after V1. To maximize acceptability by referring psychiatrists, dosage and co-prescriptions will be at the discretion of the psychiatrist in charge, but the assigned treatment will not be changed for 4 weeks (until V3). - V2 (7 days after the beginning of the new antidepressant - 'early response visit'): o Similar to V1. - V3 (28 days after the beginning of the new antidepressant - 'conventional response visit'): - Clinical evaluation using validated questionnaires for the severity of depression, quality of life, anhedonia, apathy, and cognitive dysfunction. - Blood samples - V4 (6 months after the beginning of the new antidepressant - 'remission visit'): - Clinical evaluation using validated questionnaires for the severity of depression, quality of life, anhedonia, apathy, and cognitive dysfunction. - Cognitive evaluation using a battery of tests to explore motivation, emotion processing, belief construction, and their updating. - Structural (anatomical) MRI, ASL - Blood samples - V5 (one year after the beginning of the new antidepressant - 'functional remission visit'): - Clinical evaluation using validated questionnaires for the severity of depression, quality of life, anhedonia, apathy, and cognitive dysfunction. 36 healthy volunteers without a history of neurologic or psychiatric disorder, matched for age, gender, and education will be included. They will perform V0-V2 (without MRI and blood sample at V2). Healthy volunteers will not receive any treatment as part of the research. ;


Study Design


Related Conditions & MeSH terms


NCT number NCT05866575
Study type Interventional
Source Centre Hospitalier St Anne
Contact Fabien Vinckier
Phone 0033683714083
Email f.vinckier@ghu-paris.fr
Status Not yet recruiting
Phase N/A
Start date June 1, 2023
Completion date December 31, 2026

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