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Publication : Role of Monocyte-Derived MicroRNA106b∼25 in Resilience to Social Stress.

First Author  Pfau ML Year  2019
Journal  Biol Psychiatry Volume  86
Issue  6 Pages  474-482
PubMed ID  31101319 Mgi Jnum  J:284643
Mgi Id  MGI:6385981 Doi  10.1016/j.biopsych.2019.02.023
Citation  Pfau ML, et al. (2019) Role of Monocyte-Derived MicroRNA106b approximately 25 in Resilience to Social Stress. Biol Psychiatry 86(6):474-482
abstractText  BACKGROUND: Clinical studies suggest that heightened peripheral inflammation contributes to the pathogenesis of stress-related disorders, including major depressive disorder. However, the molecular mechanisms within peripheral immune cells that mediate enhanced stress vulnerability are not well known. Because microRNAs (miRs) are important regulators of immune response, we sought to examine their role in mediating inflammatory and behavioral responses to repeated social defeat stress (RSDS), a mouse model of stress vulnerability that produces susceptible and resilient phenotypes. METHODS: We isolated Ly6c(high) monocytes via fluorescence-activated cell sorting in the blood of susceptible and resilient mice following RSDS and profiled miR expression via quantitative real-time polymerase chain reaction. Bone marrow chimeric mice were generated to confirm a causal role of the miR-106b approximately 25 cluster in bone marrow-derived leukocytes in mediating stress resilience versus susceptibility. RESULTS: We found that RSDS produces an increase in circulating Ly6c(high) inflammatory monocytes in both susceptible and resilient mice. We next investigated whether intrinsic leukocyte posttranscriptional mechanisms contribute to individual differences in stress response and the resilient phenotype. Of the miRs profiled in our panel, eight were significantly regulated by RSDS within Ly6c(high) monocytes, including miR-25-3p, a member of the miR-106b approximately 25 cluster. Selective knockout of the miR-106b approximately 25 cluster in peripheral leukocytes promoted behavioral resilience to RSDS. CONCLUSIONS: Our results identify the miR-106b approximately 25 cluster as a key regulator of stress-induced inflammation and depression that may represent a novel therapeutic target for drug development.
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