Use of a gene expression signature to identify trimetazidine for repurposing to treat bipolar depression

Author:

Bortolasci Chiara C.1,Kidnapillai Srisaiyini1,Spolding Briana1,Truong Trang T. T.1ORCID,Connor Timothy1,Swinton Courtney1,Panizzutti Bruna1ORCID,Liu Zoe S. J.1,Sanigorski Andrew1,Dean Olivia M.12ORCID,Crowley Tamsyn13,Richardson Mark3,Bozaoglu Kiymet45,Vlahos Katerina4,Cowdery Stephanie1,Watmuff Brad1,Steyn Stephan F.6,Wolmarans De Wet6,Engelbrecht Barend J.6,Perry Christina2,Drummond Katherine2,Pang Terence2ORCID,Jamain Stéphane7ORCID,Gray Laura12,McGee Sean L.1,Harvey Brian H.68ORCID,Kim Jee Hyun12,Leboyer Marion7,Berk Michael129,Walder Ken1ORCID

Affiliation:

1. IMPACT The Institute for Mental and Physical Health and Clinical Translation, School of Medicine, Deakin University Geelong Australia

2. The Florey Institute of Neuroscience and Mental Health Parkville Australia

3. Bioinformatics Core Research Facility (BCRF) Deakin University Geelong Australia

4. Murdoch Children's Research Institute Parkville Victoria Australia

5. Department of Paediatrics University of Melbourne Parkville Victoria Australia

6. Centre of Excellence for Pharmaceutical Sciences, Faculty of Health Sciences North‐West University Potchefstroom South Africa

7. Univ Paris Est Créteil, INSERM, IMRB, Translational Neuropsychiatry, AP‐HP, DMU IMPACT, FHU ADAPT Fondation FondaMental Créteil France

8. SAMRC Unit on Risk and Resilience in Mental Disorders, Department of Psychiatry and Mental Health and Neuroscience Institute University of Cape Town Cape Town South Africa

9. Orygen, The National Centre of Excellence in Youth Mental Health Parkville Australia

Abstract

AbstractObjectivesThe aim of this study was to repurpose a drug for the treatment of bipolar depression.MethodsA gene expression signature representing the overall transcriptomic effects of a cocktail of drugs widely prescribed to treat bipolar disorder was generated using human neuronal‐like (NT2‐N) cells. A compound library of 960 approved, off‐patent drugs were then screened to identify those drugs that affect transcription most similar to the effects of the bipolar depression drug cocktail. For mechanistic studies, peripheral blood mononuclear cells were obtained from a healthy subject and reprogrammed into induced pluripotent stem cells, which were then differentiated into co‐cultured neurons and astrocytes. Efficacy studies were conducted in two animal models of depressive‐like behaviours (Flinders Sensitive Line rats and social isolation with chronic restraint stress rats).ResultsThe screen identified trimetazidine as a potential drug for repurposing. Trimetazidine alters metabolic processes to increase ATP production, which is thought to be deficient in bipolar depression. We showed that trimetazidine increased mitochondrial respiration in cultured human neuronal‐like cells. Transcriptomic analysis in induced pluripotent stem cell‐derived neuron/astrocyte co‐cultures suggested additional mechanisms of action via the focal adhesion and MAPK signalling pathways. In two different rodent models of depressive‐like behaviours, trimetazidine exhibited antidepressant‐like activity with reduced anhedonia and reduced immobility in the forced swim test.ConclusionCollectively our data support the repurposing of trimetazidine for the treatment of bipolar depression.

Funder

National Health and Medical Research Council

Publisher

Wiley

Subject

Biological Psychiatry,Psychiatry and Mental health

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