| Literature DB >> 23994757 |
Sjoukje D Kuipers1, Andrea Trentani2, Eddy A van der Zee3, Johan A den Boer4.
Abstract
Growing evidence suggests neuroplasticity changes are pivotal in both the occurrence and treatment of affective disorders. Abnormal expression and/or phosphorylation of numerous plasticity-related proteins have been observed in depression, while prolonged antidepressant treatment has been associated with the attenuation of stress-mediated effects on dendritic remodeling and adult hippocampal neurogenesis in experimental animals. This study explores the neurobiological adaptations induced by chronic stress and/or long-term tianeptine treatment. Male and female rats were studied to determine the potential contributory role of sex differences on stress-induced pathology and antidepressant-mediated actions. Our results confirm chronic stress-induced HPA axis disturbance and neuroplasticity impairment in both sexes (i.e. reduced CREB phosphorylation and hippocampal BrdU labeling). Commonly ensuing neurobiological alterations were accompanied by unique sex-specific adaptations. When the antidepressant tianeptine was administered, HPA axis hyperactivity was attenuated and specific neuronal defects were ameliorated in both sexes. These findings provide novel insight into sex-related influences on the neurobiological substrates mediating chronic stress-induced actions on neuroplasticity and the mechanisms underlying tianeptine-mediated therapeutic effects.Entities:
Keywords: BrdU; CREB phosphorylation; Chronic stress; FOS expression; Sex differences; Tianeptine
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Year: 2013 PMID: 23994757 DOI: 10.1016/j.neuropharm.2013.08.018
Source DB: PubMed Journal: Neuropharmacology ISSN: 0028-3908 Impact factor: 5.250