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      Dual induction of TREM2 and tolerance-related transcript, Tmem176b, in amyloid transgenic mice: implications for vaccine-based therapies for Alzheimer's disease

      research-article
      Author(s): * , * , * , * , * , * , 1 , , , § , * , 2
      Publication date (Electronic):
      Journal: ASN NEURO
      Publisher: American Society for Neurochemistry
      Keywords: antigen presentation, autoimmunity, Clast1, neuroinflammation, Torid, Aβ, amyloid β peptide, CCL2, chemokine ligand 2, CFSE, carboxyfluorescein succinimidyl ester, CNS, central nervous system, DAMP, danger-associated molecular pattern, DMEM, Dulbecco's modified Eagle's medium, EAE, experimentally induced autoimmune encephalomyelitis, FBS, fetal bovine serum, GFP, green fluorescent protein, HPRT, hypoxanthine phosphoribosyl transferase, IFNγ, interferon γ, IL, interleukin, KO, knockout, LPS, lipopolysaccharide, PFA, paraformaldehyde, qPCR, quantitative PCR, Thio-S, thioflavine-S, Tmem176b, transmembrane domain protein 176b, TNF, tumour necrosis factor, TREM2, triggering receptor expressed on myeloid cells 2, WT, wild-type

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          Abstract

          Vaccine-based autoimmune (anti-amyloid) treatments are currently being examined for their therapeutic potential in Alzheimer's disease. In the present study we examined, in a transgenic model of amyloid pathology, the expression of two molecules previously implicated in decreasing the severity of autoimmune responses: TREM2 (triggering receptor expressed on myeloid cells 2) and the intracellular tolerance-associated transcript, Tmem176b (transmembrane domain protein 176b). In situ hybridization analysis revealed that both molecules were highly expressed in plaque-associated microglia, but their expression defined two different zones of plaque-associated activation. Tmem176b expression was highest in the inner zone of amyloid plaques, whereas TREM2 expression was highest in the outer zone. Induced expression of TREM2 occurred co-incident with detection of thioflavine-S-positive amyloid deposits. Transfection studies revealed that expression of TREM2 correlated negatively with motility, but correlated positively with the ability of microglia to stimulate CD4 + T-cell proliferation, TNF (tumour necrosis factor) and CCL2 (chemokine ligand 2) production, but not IFNγ (interferon γ) production. TREM2 expression also showed a positive correlation with amyloid phagocytosis in unactivated cells. However, activating cells with LPS (lipopolysaccharide), but not IFNγ, reduced the correlation between TREM2 expression and phagocytosis. Transfection of Tmem176b into both microglial and macrophage cell lines increased apoptosis. Taken together, these data suggest that, in vivo, Tmem176b + cells in closest apposition to amyloid may be the least able to clear amyloid. Conversely, the phagocytic TREM2 + microglia on the plaque outer zones are positioned to capture and present self-antigens to CNS (central nervous system)-infiltrating lymphocytes without promoting pro-inflammatory lymphocyte responses. Instead, plaque-associated TREM2 + microglia have the potential to evoke neuroprotective immune responses that may serve to support CNS function during pro-inflammatory anti-amyloid immune therapies.

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          Control of microglial neurotoxicity by the fractalkine receptor.

          Astrid E. Cardona, Erik P Pioro, Margaret E Sasse (2006)
          Microglia, the resident inflammatory cells of the CNS, are the only CNS cells that express the fractalkine receptor (CX3CR1). Using three different in vivo models, we show that CX3CR1 deficiency dysregulates microglial responses, resulting in neurotoxicity. Following peripheral lipopolysaccharide injections, Cx3cr1-/- mice showed cell-autonomous microglial neurotoxicity. In a toxic model of Parkinson disease and a transgenic model of amyotrophic lateral sclerosis, Cx3cr1-/- mice showed more extensive neuronal cell loss than Cx3cr1+ littermate controls. Augmenting CX3CR1 signaling may protect against microglial neurotoxicity, whereas CNS penetration by pharmaceutical CX3CR1 antagonists could increase neuronal vulnerability.
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            Cutting edge: TREM-2 attenuates macrophage activation.

            Isaiah Turnbull, Susan Gilfillan, Marina Cella (2006)
            The triggering receptor expressed on myeloid cells 2 (TREM-2) delivers intracellular signals through the adaptor DAP12 to regulate myeloid cell function both within and outside the immune system. The role of TREM-2 in immunity has been obscured by the failure to detect expression of the TREM-2 protein in vivo. In this study, we show that TREM-2 is expressed on macrophages infiltrating the tissues from the circulation and that alternative activation with IL-4 can induce TREM-2. TREM-2 expression is abrogated by macrophage maturation with LPS of IFN-gamma. Using TREM-2(-/-) mice, we find that TREM-2 functions to inhibit cytokine production by macrophages in response to the TLR ligands LPS, zymosan, and CpG. Furthermore, we find that TREM-2 completely accounts for the increased cytokine production previously reported by DAP12(-/-) macrophages. Taken together, these data show that TREM-2 is expressed on newly differentiated and alternatively activated macrophages and functions to restrain macrophage activation.
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              Microglia: biology and pathology.

              Manuel Graeber, Wolfgang J Streit (2010)
              The past 20 years have seen a gain in knowledge on microglia biology and microglia functions in disease that exceeds the expectations formulated when the microglia "immune network" was introduced. More than 10,000 articles have been published during this time. Important new research avenues of clinical importance have opened up such as the role of microglia in pain and in brain tumors. New controversies have also emerged such as the question of whether microglia are active or reactive players in neurodegenerative disease conditions, or whether they may be victims themselves. Premature commercial interests may be responsible for some of the confusion that currently surrounds microglia in both the Alzheimer and Parkinson's disease research fields. A critical review of the literature shows that the concept of "(micro)glial inflammation" is still open to interpretation, despite a prevailing slant towards a negative meaning. Perhaps the most exciting foreseeable development concerns research on the role of microglia in synaptic plasticity, which is expected to yield an answer to the question whether microglia are the brain's electricians. This review provides an analysis of the latest developments in the microglia field.
              Article 0 comments Cited 212 times – based on 0 reviews     Review now
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                Author and article information

                Journal
                Journal ID (nlm-ta): ASN Neuro
                Journal ID (publisher-id): ASN
                Title: ASN NEURO
                Publisher: American Society for Neurochemistry (9037 Ron Den Lane, Windermere, FL 34786 )
                ISSN (Electronic): 1759-0914
                Publication date (Electronic preprint): 14 June 2010
                Publication date (Electronic): 12 July 2010
                Publication date Collection: 2010
                Volume: 2
                Issue: 3
                Electronic Location Identifier: e00037
                Affiliations
                [1]*Division of Biomedical Sciences, University of California Riverside, 900 University Avenue, Riverside, CA 925210121, U.S.A.
                [2]†University of TbingenWilhelmstrasse 7, 72074 Tbingen, Germany
                [3]‡Novartis Institutes for BioMedical Research, Basel, CH4002, Switzerland
                [4]§Institute of Reconstructive Neurobiology, University of Bonn, SigmundFreudStr. 25, Bonn, Germany
                Author notes
                1Present address: Department of Microbiology, Oregon State University, Corvallis, OR 97331, U.S.A.
                2To whom correspondence should be addressed (email monica.carson@ 123456ucr.edu ).
                Article
                Publisher ID: e00037
                DOI: 10.1042/AN20100010
                PMC ID: 2905103
                PubMed ID: 20640189
                SO-VID: 0ca0d282-7fb7-4b73-83df-beec08e02da0
                Copyright © © 2010 The Author(s).
                License:

                This is an Open Access article distributed under the terms of the Creative Commons Attribution Non-Commercial Licence ( http://creativecommons.org/licenses/by-nc/2.5/) which permits unrestricted non-commercial use, distribution and reproduction in any medium, provided the original work is properly cited.

                History
                Date received : 14 April 2010
                Date revision received : 7 June 2010
                Date accepted : 14 June 2010
                Categories
                Subject: Research Article
                Subject: S3
                Subject: S7

                ScienceOpen disciplines: Neurosciences
                Keywords: tnf, tumour necrosis factor,cfse, carboxyfluorescein succinimidyl ester,gfp, green fluorescent protein,dmem, dulbecco's modified eagle's medium,damp, danger-associated molecular pattern,lps, lipopolysaccharide,trem2, triggering receptor expressed on myeloid cells 2,aβ, amyloid β peptide,eae, experimentally induced autoimmune encephalomyelitis,clast1,fbs, fetal bovine serum,cns, central nervous system,thio-s, thioflavine-s,pfa, paraformaldehyde,autoimmunity,tmem176b, transmembrane domain protein 176b,ccl2, chemokine ligand 2,ko, knockout,torid,wt, wild-type,neuroinflammation,ifnγ, interferon γ,antigen presentation,qpcr, quantitative pcr,il, interleukin,hprt, hypoxanthine phosphoribosyl transferase
                Data availability:
                ScienceOpen disciplines: Neurosciences
                Keywords: tnf, tumour necrosis factor, cfse, carboxyfluorescein succinimidyl ester, gfp, green fluorescent protein, dmem, dulbecco's modified eagle's medium, damp, danger-associated molecular pattern, lps, lipopolysaccharide, trem2, triggering receptor expressed on myeloid cells 2, aβ, amyloid β peptide, eae, experimentally induced autoimmune encephalomyelitis, clast1, fbs, fetal bovine serum, cns, central nervous system, thio-s, thioflavine-s, pfa, paraformaldehyde, autoimmunity, tmem176b, transmembrane domain protein 176b, ccl2, chemokine ligand 2, ko, knockout, torid, wt, wild-type, neuroinflammation, ifnγ, interferon γ, antigen presentation, qpcr, quantitative pcr, il, interleukin, hprt, hypoxanthine phosphoribosyl transferase

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