Sex Differences in Anxiety and Depressive-Like Behaviors in Rats

Download or read book Sex Differences in Anxiety and Depressive-Like Behaviors in Rats written by Nicole Carrier and published by . This book was released on 2012 with total page pages. Available in PDF, EPUB and Kindle. Book excerpt: ABSTRACT: Anxiety and depressive disorders are the most common of all psychiatric disorders; however, current human and animal research has yet to provide a clear understanding of the neural mechanisms underlying their etiology. Demographic analyses illustrate not only the enormous prevalence and incidence of these affective disorders, but also the pervasive gender discrepancy seen worldwide in patients suffering from anxiety and depression. There are largely documented sex differences in mood disorders, where females are more than twice as likely as men to be afflicted with depression and anxiety. Overall, sexually dimorphic aspects of anxiety and depression are well documented but poorly understood, warranting additional research delving into the mechanisms behind these sex differences. Considerable sex differences occur in the incidence and prevalence of anxiety disorders where women are more anxious than men, particularly in situations where social interaction is required. In preclinical studies, the social interaction test represents a valid animal model to study sex differences in social anxiety. Indeed, female rats engage less in conspecific interactions than their male counterparts, which are behaviors indicative of higher social anxiety in female rats. Given both the high prevalence of anxiety disorders in women and the fact that little is known about the mechanisms of gender differences in anxiety, our primary aim in our first study was to investigate the neurobiological mechanisms underlying sex differences in social anxiety-like behavior in rats. We investigated the activation of several brain areas using the neuronal marker zif268 and discovered sexually dimorphic zif268 expression, increased in the male, specifically within the medial prefrontal cortex (mPFC). Through the use of zif268 antisense oligodeoxynucleotides (zif ASO), we induced a temporary downregulation of zif268 expression in the mPFC of male and female rats and found that zif268 ASO male rats show more social anxiety-like behaviors when compared with control male rats in the social interaction test. In fact, zif268 ASO males displayed social anxiety-like behaviors, which were similar to control females. Thus, downregulation of zif268 expression in the mPFC of male rats eliminated sex differences previously found in the social anxiety-like behavior tests. Interestingly, zif268 ASO in female rats had no effect on their social interaction. In our second study, we investigated the role of extracellular signal regulated kinase 2 (ERK2), an upstream regulator of zif268, in the medial prefrontal cortex (mPFC). Indeed, female rats' had lower ERK2 expression compared to male rats, and overexpression of ERK2 in the mPFC increases their social interaction to the level xii seen in their male counterparts. Our novel findings have led us to ascertain that sexually dimorphic zif268 and ERK2 expression in the mPFC are key molecular factor in mediating sex-specific anxiety-like behavior in the social interaction test. Human and animal studies suggest that testosterone may have antidepressant effects. In our third study, we sought to investigate the molecular mechanisms underlying the antidepressant effects of testosterone within the hippocampus, an area that is fundamental in the etiology of depression. The effects of testosterone replacements in gonadectomized adult male rats were investigated using the sucrose preference and forced swim tests. We explored possible effects of testosterone on hippocampal neurogenesis and gene expression of stress-related molecules. Through the use of viral vectors, we pursued the antidepressant molecular mechanism(s) of testosterone in mediating anhedonia and manipulated ERK2 expression in the dentate gyrus in gonadectomized rats with testosterone replacements. Testosterone had antidepressant effects, likely mediated by aromatization to estrogen metabolites, in the sucrose preference and forced swim tests despite having no effects on hippocampal cell proliferation or survival. We found a testosterone-dependent regulation of hippocampal ERK2 expression. Functionally, reducing ERK2 activity within the dentate gyrus induced anhedonia in gonadectomized rats receiving testosterone supplementation, whereas the overexpression of ERK2 rescued this behavior in gonadectomized rats. These results implicate a role for ERK2 signaling within the dentate gyrus area of the hippocampus as a key mediator of the antidepressant effects of testosterone. In our fourth study, we investigated the antidepressant effects and interactions between testosterone and imipramine in both male and female rats subjected to stressful conditions in order to model a depressive-like state. A chronic social isolation model was used to induce an anxiety and depressive-like behaviors in adult gonadectomized male and ovariectomized female rats receiving chronic testosterone and imipramine treatments. Their anxiety and depression-like behaviors were examined using the light-dark box, elevated plus maze, open field, sucrose preference and novelty induced hypophagia tests. In socially isolated rats, the anxiolytic and antidepressant effects of testosterone and imipramine were limited to male rats. Additionally, testosterone enhanced the neurogenic effect of imipramine on hippocampal cell proliferation in male rats. Although female rats exhibited signs of anxiety and depressive-like behaviors following social isolation, testosterone and/or imipramine administration had no anxiolytic or xiii antidepressant effects in ovariectomized females. These results suggest that testosterone and imipramine had anxiolytic and antidepressant effects in socially isolated male, but not female rats, and that testosterone enhances the effect of imipramine on cell proliferation in the hippocampus of male rats only. These studies have investigated the mechanisms underlying sex differences in the incidence and prevalence of anxiety and depressive disorders. We concentrated on the influence of gonadal hormones and several molecular targets on anxiety and depressive-like behaviors in the Sprague-Dawley rat. Overall, these studies underscore the importance of gonadal hormones in mediating sexually dimorphic behavior and gene expression within areas of the brain fundamental to anxiety and depressive disorders.