Publication

The neurobiology of retinoic acid in affective disorders

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Persistent URL
Last modified
  • 02/20/2025
Type of Material
Authors
    J. Douglas Bremner, Emory UniversityPeter McCaffery, University of Aberdeen
Language
  • English
Date
  • 2008-02-15
Publisher
  • Elsevier: 12 months
Publication Version
Copyright Statement
  • © 2007 Elsevier Inc. All rights reserved.
License
Final Published Version (URL)
Title of Journal or Parent Work
ISSN
  • 0278-5846
Volume
  • 32
Issue
  • 2
Start Page
  • 315
End Page
  • 331
Abstract
  • Current models of affective disorders implicate alterations in norepinephrine, serotonin, dopamine, and CRF/cortisol; however treatments targeted at these neurotransmitters or hormones have led to imperfect resolution of symptoms, suggesting that the neurobiology of affective disorders is incompletely understood. Until now retinoids have not been considered as possible contributors to affective disorders. Retinoids represent a family of compounds derived from Vitamin A that perform a large number of functions, many via the vitamin A product, retinoic acid. This signaling molecule binds to specific retinoic acid receptors in the brain which, like the glucocorticoid and thyroid hormone receptors, are part of the nuclear receptor superfamily and regulate gene transcription. Research in the field of retinoic acid in the CNS has focused on the developing brain, in part stimulated by the observation that isotretinoin (13-cis retinoic acid), an isomer of retinoic acid used in the treatment of acne, is highly teratogenic for the CNS. More recent work has suggested that retinoic acid may influence the adult brain; animal studies indicated that the administration of isotretinoin is associated with alterations in behavior as well as inhibition of neurogenesis in the hippocampus. Clinical evidence for an association between retinoids and depression includes case reports in the literature, studies of health care databases, and other sources. A preliminary PET study in human subjects showed that isotretinoin was associated with a decrease in orbitofrontal metabolism. Several studies have shown that the molecular components required for retinoic acid signaling are expressed in the adult brain ; the overlap of brain areas implicated in retinoic acid function and stress and depression suggest that retinoids could play a role in affective disorders. This report reviews the evidence in this area and describes several systems that may be targets of retinoic acid and which contribute to the pathophysiology of depression.
Author Notes
  • Correspondance: J Douglas Bremner MD, Emory University, 1256 Briarcliff Rd., Rm 308e; mailstop 1256/001/AT, Atlanta, GA 30306; Phone: (404) 712-9569; Fax: (404) 712-8442; Email: jdbremn@emory.edu.
Keywords
Research Categories
  • Psychology, Cognitive
  • Psychology, Physiological
  • Biology, Neuroscience

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