Abstract
Dysregulation of innate immune responses has frequently been reported in stress-associated psychiatric disorders such as major depression. In mice, enhanced circulating cytokine levels as well as altered innate immune cell numbers have been found after stress exposure. In addition, stress-induced recruitment of peripheral monocytes to the brain has been shown to promote anxiety-like behavior. However, it is yet unclear whether specific differences in the innate immune system are associated with stress susceptibility or resilience in mice. Utilizing chronic social defeat, a model of depression and stress vulnerability, we characterized peripheral and brain-invading myeloid cells in stress-susceptible and resilient animals. In all defeated animals, we found reduced percentages of CD11c+ dendritic cells (DCs) by flow cytometry in the spleen when compared to non-defeated controls. Exclusively in susceptible mice conventional DCs of the spleen showed up-regulated expression of MHC class II and co-stimulatory CD80 molecules pointing toward an enhanced maturation phenotype of these cells. Susceptible, but not resilient animals further exhibited an increase in inflammatory Ly6Chi monocytes and higher numbers of spleen-derived CD11b+ cells that produced the proinflammatory cytokine tumor necrosis factor (TNF) upon lipopolysaccharide (LPS) stimulation. Increased percentages of peripheral CD45hi CD11b+ cells immigrated into the brain of defeated mice, regardless of resilience or susceptibility. However, cellular infiltrates in the brain of susceptible mice contained higher percentages of CC chemokine receptor 2 (CCR2+) Ly6Chi monocytes representing an inflammatory phenotype. Thus, we defined specific stress-related immune signatures involving conventional DCs and inflammatory Ly6Chi monocytes in susceptible and resilient mice. Together, our findings suggest an impact of the innate immune system in vulnerability to stress-related disorders such as major depression.
Highlights
Stressful experiences represent a major risk factor for mental illness such as major depressive disorder (MDD; Kessler et al, 2005; Krishnan and Nestler, 2008)
The aim of this study was to identify specific innate immune cell profiles induced by chronic social defeat and to elucidate whether they are associated with stress vulnerability
Based on the definition of susceptible and resilient mice, social defeat stress resulted in a markedly reduced interaction ratio in susceptible mice compared to controls (p < 0.001) and resilient mice (p < 0.001, Figure 1B)
Summary
Stressful experiences represent a major risk factor for mental illness such as major depressive disorder (MDD; Kessler et al, 2005; Krishnan and Nestler, 2008). Physiological and psychological responses to stress vary and some individuals exhibit stress resilience (Krishnan and Nestler, 2008). In addition to elevated cytokine levels, depressed patients show increased counts of neutrophils and monocytes that represent a prominent cellular source of these cytokines (Maes et al, 1992). It is an open question whether these immune changes are associated with stress vulnerability
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