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      Microglial recruitment of IL-1β producing monocytes to brain endothelium causes stress-induced anxiety

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          Abstract

          Psychosocial stress contributes to the development of anxiety and depression. Recent clinical studies have reported increased inflammatory leukocytes in circulation of individuals with stress-related psychiatric disorders. Parallel to this, our work in mice shows that social stress causes release of inflammatory monocytes into circulation. In addition, social stress caused the development of prolonged anxiety that was dependent on inflammatory monocytes in the brain. Therefore, we hypothesize that chronic stress drives the production of inflammatory monocytes that are actively recruited to the brain by microglia, and these monocytes augment neuroinflammatory signaling and prolong anxiety. Here we show that repeated social defeat stress in mice activated threat appraisal centers in the brain that spatially coincided with microglial activation and endothelial facilitation of monocyte recruitment. Moreover, microglial depletion with a CSF1R antagonist prior to stress prevented the recruitment of monocytes to the brain and abrogated the development of anxiety. Cell-specific transcriptional profiling revealed that microglia selectively enhanced CCL2 expression, while monocytes expressed the pro-inflammatory cytokine IL-1β. Consistent with these profiles, the recruited inflammatory monocytes with stress adhered to IL-1R1 + neurovascular endothelial cells and this interaction was blocked by microglial depletion. Furthermore, disruption of IL-1β signaling by caspase-1 KO specifically within bone marrow-derived cells revealed that monocytes promoted anxiogenesis through stimulation of neurovascular IL-1R1 by IL-1β. Collectively, the development of anxiety during stress was caused by microglial recruitment of IL-1β-producing monocytes that stimulated brain endothelial IL-1R1. Thus, monocyte IL-1β production represents a novel mechanism that underlies behavioral complications associated with stress-related psychiatric disorders.

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          Microglia in the adult brain arise from Ly-6ChiCCR2+ monocytes only under defined host conditions.

          Alexander Mildner, Hauke Schmidt, Mirko Nitsche (2007)
          Microglia are crucially important myeloid cells in the CNS and constitute the first immunological barrier against pathogens and environmental insults. The factors controlling microglia recruitment from the blood remain elusive and the direct circulating microglia precursor has not yet been identified in vivo. Using a panel of bone marrow chimeric and adoptive transfer experiments, we found that circulating Ly-6C(hi)CCR2(+) monocytes were preferentially recruited to the lesioned brain and differentiated into microglia. Notably, microglia engraftment in CNS pathologies, which are not associated with overt blood-brain barrier disruption, required previous conditioning of brain (for example, by direct tissue irradiation). Our results identify Ly-6C(hi)CCR2(+) monocytes as direct precursors of microglia in the adult brain and establish the importance of local factors in the adult CNS for microglia engraftment.
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            Role of translocator protein density, a marker of neuroinflammation, in the brain during major depressive episodes.

            Elaine Setiawan, Alan Wilson, Romina Mizrahi (2015)
            The neuroinflammatory hypothesis of major depressive disorder is supported by several main findings. First, in humans and animals, activation of the immune system causes sickness behaviors that present during a major depressive episode (MDE), such as low mood, anhedonia, anorexia, and weight loss. Second, peripheral markers of inflammation are frequently reported in major depressive disorder. Third, neuroinflammatory illnesses are associated with high rates of MDEs. However, a fundamental limitation of the neuroinflammatory hypothesis is a paucity of evidence of brain inflammation during MDE. Translocator protein density measured by distribution volume (TSPO VT) is increased in activated microglia, an important aspect of neuroinflammation.
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              Targeting abnormal neural circuits in mood and anxiety disorders: from the laboratory to the clinic.

              Kerry J Ressler, Helen Mayberg (2007)
              Recent decades have witnessed tremendous advances in the neuroscience of emotion, learning and memory, and in animal models for understanding depression and anxiety. This review focuses on new rationally designed psychiatric treatments derived from preclinical human and animal studies. Nonpharmacological treatments that affect disrupted emotion circuits include vagal nerve stimulation, rapid transcranial magnetic stimulation and deep brain stimulation, all borrowed from neurological interventions that attempt to target known pathological foci. Other approaches include drugs that are given in relation to specific learning events to enhance or disrupt endogenous emotional learning processes. Imaging data suggest that common regions of brain activation are targeted with pharmacological and somatic treatments as well as with the emotional learning in psychotherapy. Although many of these approaches are experimental, the rapidly developing understanding of emotional circuit regulation is likely to provide exciting and powerful future treatments for debilitating mood and anxiety disorders.
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                Author and article information

                Journal
                Journal ID (nlm-journal-id): 9607835
                Journal ID (pubmed-jr-id): 20545
                Journal ID (nlm-ta): Mol Psychiatry
                Journal ID (iso-abbrev): Mol. Psychiatry
                Title: Molecular psychiatry
                ISSN (Print): 1359-4184
                ISSN (Electronic): 1476-5578
                Publication date Nihms-submitted: 17 March 2017
                Publication date (Electronic): 04 April 2017
                Publication date PMC-release: 05 October 2017
                Electronic Location Identifier: 10.1038/mp.2017.64
                Affiliations
                [1 ]Department of Neuroscience, The Ohio State University Wexner Medical Center
                [2 ]Division of Biosciences, The Ohio State University College of Dentistry
                [3 ]Institute for Behavioral Medicine Research, The Ohio State University College of Medicine
                Author notes
                [5 ]Corresponding authors: Jonathan Godbout, 223 IBMR Building, 460 Medical Center Drive, Columbus, OH 43210, U.S.A. Jonathan.Godbout@ 123456osumc.edu and John F. Sheridan, 120 IBMR Building, 460 Medical Center Drive, Columbus, OH 43210, U.S.A. John.Sheridan@ 123456osumc.edu
                [4]

                Current affiliation: College of Dentistry and Neuroscience Research Center, University of Costa Rica

                [*]

                Authors contributed equally to this paper

                Article
                Manuscript ID: NIHMS852761
                DOI: 10.1038/mp.2017.64
                PMC ID: 5628107
                PubMed ID: 28373688
                SO-VID: 3c6c20a6-c147-43c6-8348-1d61cf8cf852
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                Users may view, print, copy, and download text and data-mine the content in such documents, for the purposes of academic research, subject always to the full Conditions of use: http://www.nature.com/authors/editorial_policies/license.html#terms

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                Subject: Article

                ScienceOpen disciplines: Molecular medicine
                Keywords: repeated social defeat,social stress,anxiety,monocytes,endothelial cells,microglia,interleukin-1 beta
                Data availability:
                ScienceOpen disciplines: Molecular medicine
                Keywords: repeated social defeat, social stress, anxiety, monocytes, endothelial cells, microglia, interleukin-1 beta

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