Clinical validation of a combinatorial PharmAcogeNomic approach in major Depressive disorder: an Observational prospective RAndomized, participant and rater-blinded, controlled trial (PANDORA trial)

Alessandra Minelli,Chiara Cobelli,Elisabetta Maffioletti,Luisella Bocchio-Chiavetto,Giovanni Battista Tura,Chiara Magri,Edoardo Giacopuzzi,Antonio Vita,Giulia Perusi,Stefano Bignotti,Erika Vitali,Stefano Barlati,Vincenzo Dattilo,Massimo Gennarelli,Silvia Bonizzato,Vincenza Santoro,Edoardo Spina

doi:10.1186/s13063-021-05775-8

Abstract

BackgroundMajor depressive disorder (MDD) is a common, chronic, debilitating mood disorder that causes serious functional impairment and significantly decreased quality of life. Pharmacotherapy represents the first-line treatment option; however, only approximately one third of patients respond to the first treatment because of the ineffectiveness or side effects of antidepressants. Precision medicine in psychiatry might offer clinicians the possibility to tailor treatment according to the best possible evidence of efficacy and tolerability for each subject. In this context, our study aims to carry out a clinical validation of a combinatorial pharmacogenomics (PGx) test in an Italian MDD patient cohort with advocacy license independence.MethodsOur study is a prospective participant- and rater-blinded, randomized, controlled clinical observational trial enrolling 300 MDD patients who are referred to psychiatric services to receive a new antidepressant due to the failure of their current treatment and/or the onset of adverse effects. Eligible participants are randomized to the TGTG group (Treated with Genetic Test Guide) or TAU group (Treated as Usual). For all subjects, DNA is collected with a buccal brush. The primary outcome is the reduction in depressive symptomatology. The secondary outcomes involve a range of scales that assess MDD symptoms and social functioning outcomes. The assessment is performed at four timepoints: baseline and 4, 8, and 12 weeks.DiscussionThis project represents the first randomized controlled clinical trial to investigate whether a non-commercial PGx test improves outcomes in an MDD naturalistic cohort. Moreover, the identification of new genetic variants associated with non-response or side effects will improve the efficacy of the test, leading to further cost-saving.Trial registration numberClinicalTrials.gov NCT04615234. Registered on November 4, 2020.

Highlights

Major depressive disorder (MDD) is a common, chronic, debilitating mood disorder that causes serious functional impairment and significantly decreased quality of life
Minelli et al Trials (2021) 22:896. This project represents the first randomized controlled clinical trial to investigate whether a noncommercial PGx test improves outcomes in an MDD naturalistic cohort
The identification of new genetic variants associated with non-response or side effects will improve the efficacy of the test, leading to further costsaving

Summary

Introduction

Major depressive disorder (MDD) is a common, chronic, debilitating mood disorder that causes serious functional impairment and significantly decreased quality of life. The high percentage of treatment failure or incomplete remission could be a consequence of intrinsic biological and environmental heterogeneity among MDD patients [4, 5], suggesting that biomarkers of the response to ADs would be useful for clinicians to guide treatment at the individual level. In this context, pharmacogenomics (PGx) testing has the potential to reduce antidepressant discontinuation due to side effects and increase efficacy

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