Multidimensional Predictors of Antidepressant Responses: Integrating Mitochondrial, Genetic, Metabolic and Environmental Factors with Clinical Outcomes

Overview

Journal Neurobiol Stress

Date 2021 Nov 24

PMID 34815985

Citations 7

Authors

Carla Nasca

Olivia Barnhill

Paolo DeAngelis

Kathleen Watson

Jue Lin

James Beasley

Sarah P Young

Alison Myoraku

Josh Dobbin

Benedetta Bigio

Bruce McEwen

Natalie Rasgon

Affiliations

Soon will be listed here.

Abstract

Major depressive disorder (MDD) is a primary psychiatric illness worldwide; there is a dearth of new mechanistic models for the development of better therapeutic strategies. Although we continue to discover individual biological factors, a major challenge is the identification of integrated, multidimensional traits underlying the complex heterogeneity of depression and treatment outcomes. Here, we set out to ascertain the emergence of the novel mitochondrial mediator of epigenetic function acetyl-L-carnitine (LAC) in relation to previously described individual predictors of antidepressant responses to the insulin-sensitizing agent pioglitazone. Herein, we report that i) subjects with MDD and shorter leukocyte telomere length (LTL) show decreased levels of LAC, increased BMI, and a history of specific types of childhood trauma; and that ii) these multidimensional factors spanning mitochondrial metabolism, cellular aging, metabolic function, and childhood trauma provide more detailed signatures to predict longitudinal changes in depression severity in response to pioglitazone than individual factors. The findings of multidimensional signatures involved in the pathophysiology of depression and their role in predicting treatment outcomes provide a starting point for the development of a mechanistic framework linking biological networks and environmental factors to clinical outcomes in pursuit of personalized medicine strategies to effectively treat MDD.

Citing Articles

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The neuropsychopharmacology of acetyl-L-carnitine (LAC): basic, translational and therapeutic implications.

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Epigenetic embedding of childhood adversity: mitochondrial metabolism and neurobiology of stress-related CNS diseases.

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Genetics and epigenetics of stress: New avenues for an old concept.

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