| Literature DB >> 31929189 |
Haiyin Li1, Ping Su1, Terence Ky Lai1, Anlong Jiang1, Jing Liu1, Dongxu Zhai1, Charlie Tg Campbell1, Frankie Hf Lee1, WeiDong Yong2, Suvercha Pasricha1,3, Shupeng Li1,3, Albert Hc Wong1,3,4, Kerry J Ressler5, Fang Liu1,3,4,6.
Abstract
Posttraumatic stress disorder (PTSD) can develop after exposure to severe psychological trauma, leaving patients with disabling anxiety, nightmares, and flashbacks. Current treatments are only partially effective, and development of better treatments is hampered by limited knowledge of molecular mechanisms underlying PTSD. We have discovered that the glucocorticoid receptor (GR) and FK506 binding protein 51 (FKBP51) form a protein complex that is elevated in PTSD patients compared with unaffected control subjects, subjects exposed to trauma without PTSD, and patients with major depressive disorder (MDD). The GR-FKBP51 complex is also elevated in fear-conditioned mice, an aversive learning paradigm that models some aspects of PTSD. Both PTSD patients and fear-conditioned mice had decreased GR phosphorylation, decreased nuclear GR, and lower expression of 14-3-3ε, a gene regulated by GR. We created a peptide that disrupts GR-FKBP51 binding and reverses behavioral and molecular changes induced by fear conditioning. This peptide reduces freezing time and increases GR phosphorylation, GR-FKBP52 binding, GR nuclear translocation, and 14-3-3ε expression in fear-conditioned mice. These experiments demonstrate a molecular mechanism contributing to PTSD and suggest that the GR-FKBP51 complex may be a diagnostic biomarker and a potential therapeutic target for preventing or treating PTSD.Entities:
Keywords: Neuroscience; Psychiatric diseases
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Year: 2020 PMID: 31929189 PMCID: PMC6994126 DOI: 10.1172/JCI130363
Source DB: PubMed Journal: J Clin Invest ISSN: 0021-9738 Impact factor: 14.808