Acylcarnitines metabolism in depression: association with diagnostic status, depression severity and symptom profile in the NESDA cohort

Author:

milaneschi yuri1ORCID,Montanari Silvia,Jansen Rick2ORCID,Schranner Daniela,Kastenmüller Gabi,Arnold Matthias3ORCID,Janiri Delfina,Sani GabrieleORCID,Bhattacharyya Sudeepa4ORCID,Dehkordi Siamak Mahmoudian,Dunlop Boadie5ORCID,Rush Augustus,penninx brenda6ORCID,Kaddurah-Daouk Rima

Affiliation:

1. Amsterdam UMC, Vrije Universiteit/GGZ inGeest

2. Amsterdam UMC location Vrije Universiteit Amsterdam

3. Helmholtz Zentrum München

4. Arkansas State University

5. Emory University School of Medicine

6. Amsterdam UMC

Abstract

Abstract

Acylcarnitines (ACs) are involved in bioenergetics processes that may play a role in the pathophysiology of depression. Previous genomic evidence identified four ACs potentially linked to depression risk. We carried forward these ACs and tested the association of their circulating levels with Major Depressive Disorder (MDD) diagnosis, overall depression severity and specific symptom profiles. The sample from the Netherlands Study of Depression and Anxiety included participants with current (n = 1035) or remitted (n = 739) MDD and healthy controls (n = 800). Plasma levels of four ACs (short-chain: acetylcarnitine C2 and propionylcarnitine C3; medium-chain: octanoylcarnitine C8 and decanoylcarnitine C10) were measured. Overall depression severity as well as atypical/energy-related (AES), anhedonic and melancholic symptom profiles were derived from the Inventory of Depressive Symptomatology. As compared to healthy controls, subjects with current or remitted MDD presented similarly lower mean C2 levels (Cohen’s d = 0.2, p ≤ 1e-4). Higher overall depression severity was significantly associated with higher C3 levels (ß=0.06, SE = 0.02, p = 1.21e-3). No associations were found for C8 and C10. Focusing on symptom profiles, only higher AES scores were linked to lower C2 (ß=-0.05, SE = 0.02, p = 1.85e-2) and higher C3 (ß=0.08, SE = 0.02, p = 3.41e-5) levels. Results were confirmed in analyses pooling data with an additional internal replication sample from the same subjects measured at 6-year follow-up (totaling 4141 observations). Small alterations in levels of short-chain acylcarnitine levels were related to the presence and severity of depression, especially for symptoms reflecting altered energy homeostasis. Cellular metabolic dysfunctions may represent a key pathway in depression pathophysiology potentially accessible through AC metabolism.

Publisher

Springer Science and Business Media LLC

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