AI Article Synopsis
- Major depressive disorders (MDD) show sex differences, with male mice exhibiting clear links between social stress and depressive symptoms, while the relationship is less defined in females.
- Chronic stress in female mice leads to alterations in the blood-brain barrier (BBB) in mood-related brain areas, causing anxiety and depression-like behaviors when the BBB is disrupted in the prefrontal cortex.
- Analysis of endothelium cell-specific gene expression reveals pathways related to stress responses and resilience, and similar changes in BBB function and vascular biomarkers are observed in women with MDD, suggesting BBB dysfunction may influence stress responses in females.
Article Abstract
Prevalence, symptoms, and treatment of depression suggest that major depressive disorders (MDD) present sex differences. Social stress-induced neurovascular pathology is associated with depressive symptoms in male mice; however, this association is unclear in females. Here, we report that chronic social and subchronic variable stress promotes blood-brain barrier (BBB) alterations in mood-related brain regions of female mice. Targeted disruption of the BBB in the female prefrontal cortex (PFC) induces anxiety- and depression-like behaviours. By comparing the endothelium cell-specific transcriptomic profiling of the mouse male and female PFC, we identify several pathways and genes involved in maladaptive stress responses and resilience to stress. Furthermore, we confirm that the BBB in the PFC of stressed female mice is leaky. Then, we identify circulating vascular biomarkers of chronic stress, such as soluble E-selectin. Similar changes in circulating soluble E-selectin, BBB gene expression and morphology can be found in blood serum and postmortem brain samples from women diagnosed with MDD. Altogether, we propose that BBB dysfunction plays an important role in modulating stress responses in female mice and possibly MDD.
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| http://www.ncbi.nlm.nih.gov/pmc/articles/PMC8748803 | PMC |
| http://dx.doi.org/10.1038/s41467-021-27604-x | DOI Listing |
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