The Duration of Stress Determines Sex Specificities in the Vulnerability to Depression and in the Morphologic Remodeling of Neurons and Microglia.

Rita Gaspar,Luísa Pinto,Catarina A Gomes,Filipa I Baptista,Ana João Rodrigues,Ana Verónica Domingues,Bárbara Coimbra,António F Ambrósio,Carina Soares-Cunha

doi:10.3389/fnbeh.2022.834821

Rita Gaspar, Luísa Pinto + Show 7 more

Open Access

https://doi.org/10.3389/fnbeh.2022.834821

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Abstract

Stress exposure has been shown to induce a variety of molecular and functional alterations associated with anxiety and depression. Some studies suggest that microglia, the immune cells of the brain, play a significant role in determining neuronal and behavioral responses to chronic stress and also contribute to the development of stress-related psychopathologies. However, little is known about the impact of the duration of stress exposure upon microglia and neurons morphology, particularly considering sex differences. This issue deserves particular investigation, considering that the process of morphologic remodeling of neurons and microglia is usually accompanied by functional changes with behavioral expression. Here, we examine the effects of short and long unpredictable chronic mild stress (uCMS) protocols on behavior, evaluating in parallel microglia and neurons morphology in the dorsal hippocampus (dHIP) and in the nucleus accumbens (NAc), two brain regions involved in the etiology of depression. We report that long-term uCMS induced more behavioral alterations in males, which present anxiety and depression-like phenotypes (anhedonia and helplessness behavior), while females only display anxiety-like behavior. After short-term uCMS, both sexes presented anxiety-like behavior. Microglia cells undergo a process of morphologic adaptation to short-term uCMS, dependent on sex, in the NAc: we observed a hypertrophy in males and an atrophy in females, transient effects that do not persist after long-term uCMS. In the dHIP, the morphologic adaptation of microglia is only observed in females (hypertrophy) and after the protocol of long uCMS. Interestingly, males are more vulnerable to neuronal morphological alterations in a region-specific manner: dendritic atrophy in granule neurons of the dHIP and hypertrophy in the medium spiny neurons of the NAc, both after short- or long-term uCMS. The morphology of neurons in these brain regions were not affected in females. These findings raise the possibility that, by differentially affecting neurons and microglia in dHIP and NAc, chronic stress may contribute for differences in the clinical presentation of stress-related disorders under the control of sex-specific mechanisms.

Highlights

Exposure to stress has a detrimental impact on certain brain functions, depending on the duration, type, and severity of stress
It has been reported that stress induces morphologic changes of microglia (Sugama et al, 2007), namely promoting microglial hyper-ramification in the prefrontal cortex (PFC) (Tynan et al, 2013), which supports the theory that these cells play an important role in modulating stress responses (Reus et al, 2015)
In this study we explored the effect of stress on microglia morphology in the dorsal hippocampus (dHIP) and nucleus accumbens (NAc), two key brain regions in the control of depressive-like behavior (Di Chiara et al, 1999; Nestler, 2001; Nestler and Carlezon, 2006; Bessa et al, 2013; Alves et al, 2018)

Summary

Introduction

Exposure to stress has a detrimental impact on certain brain functions, depending on the duration, type, and severity of stress. As innate immune cells of the brain, microglia play an integrative role in maintaining neuronal homeostasis (Salter and Stevens, 2017). These cells are distributed throughout the brain and function as a critical line of defense against injury and pathogenic insults (Hanisch and Kettenmann, 2007). It has been reported that stress induces morphologic changes of microglia (Sugama et al, 2007), namely promoting microglial hyper-ramification in the prefrontal cortex (PFC) (Tynan et al, 2013), which supports the theory that these cells play an important role in modulating stress responses (Reus et al, 2015). Our observations suggest that microglia remodeling upon stress are not limited to the acquisition of an amoeboid phenotype, as previously described (Sugama et al, 2007; Tynan et al, 2010; Kreisel et al, 2014), but instead may vary from different degrees of atrophy to hypertrophy

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