Neuroprotective intervention by interferon-γ blockade prevents CD8+ T cell-mediated dendrite and synapse loss

Kreutzfeldt, Mario; Bergthaler, Andréas; Fernandez, Marylise; Brück, Wolfgang; Steinbach, Karin; Vorm, Mariann; Coras, Roland; Blümcke, Ingmar; Bonilla, Weldy V.; Fleige, Anne; Forman, Ruth; Müller, Werner; Misgeld, Thomas; Kerschensteiner, Martin; Pinschewer, Daniel D.; Merkler, Doron

doi:10.1083/jcb.2026oia90

Cited by 26 publications

(45 citation statements)

References 44 publications

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“…However other studies have demonstrated a pathogenic impact of IFNc in demyelinating disease [134,135], while still others saw no effect of IFNc deficiency on demyelination associated with an infection [136]. Further, there are clear indications that IFNc can exacerbate neuroinflammatory disease and drive neuronal loss in other settings [137].…”

Section: Multiple Sclerosis (Ms)mentioning

confidence: 96%

Interferon gamma in autoimmunity: A complicated player on a complex stage

Lees

2015

Cytokine

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Early views of autoimmune disease cast IFNγ as a prototypic pro-inflammatory factor. It is now clear that IFNγ is capable of both pro- and anti-inflammatory activities with the functional outcome dependent on the physiological and pathological setting examined. Here, the major immune modulatory activities of IFNγ are reviewed and current evidence for the impact of IFNγ on pathology and regulation of several autoimmune diseases and disease models is summarized.

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Section: Multiple Sclerosis (Ms)mentioning

confidence: 96%

Interferon gamma in autoimmunity: A complicated player on a complex stage

Lees

2015

Cytokine

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“…It was hypothesized that these microglia played an active role in the removal of these synapses, a process termed synaptic stripping. Synaptic stripping has been observed not only after axotomy or injury, but also following infection or inflammation (Di Liberto et al 2018;Kreutzfeldt et al 2013;Trapp et al 2007;Chen et al 2014), and it involves not only excitatory perisomatic synapses (like those on lower motoneurons; Blinzinger and Kreutzberg 1968) but also inhibitory perisomatic synapses (like those in neocortex and hippocampus; Di Liberto et al 2018;Chen et al 2014). While activation of microglia following insult and inflammation may lead to synaptic stripping, it does not in all cases (Siskova et al 2009;Perry and O'Conner 2010), nor is activation a requirement for microglial to phagocytose synaptic elements.…”

Section: Loss Of Perisomatic Synapses Coincides With Microglial Enshementioning

confidence: 99%

Toxoplasmainduces stripping of perisomatic inhibitory synapses

Carrillo

Ballard

Glausen

et al. 2019

Preprint

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words)Infection and inflammation within the brain induces changes in neuronal connectivity and function. The intracellular protozoan parasite, Toxoplasma gondii, is one pathogen that infects the brain and can cause encephalitis and seizures. Persistent infection by this parasite is also associated with behavioral alterations and an increased risk for developing psychiatric illness, including schizophrenia. Current evidence from studies in humans and mouse models suggest that both seizures and schizophrenia result from a loss or dysfunction of inhibitory synapses. In line with this, we recently reported that persistent Toxoplasma gondii infection alters the distribution of glutamic acid decarboxylase 67 (GAD67), an enzyme that catalyzes GABA synthesis in inhibitory synapses. These changes could reflect a redistribution of presynaptic machinery in inhibitory neurons or a loss of inhibitory nerve terminals. To directly assess the latter possibility, we employed serial block face scanning electron microscopy (SBFSEM) and quantified inhibitory perisomatic synapses in neocortex and hippocampus following parasitic infection. Not only did persistent infection lead to a significant loss of perisomatic synapses, it induced the ensheathment of neuronal somata by phagocytic cells. Immunohistochemical, genetic, and ultrastructural analyses revealed that these phagocytic cells included reactive microglia. Finally, ultrastructural analysis identified phagocytic cells enveloping perisomatic nerve terminals, suggesting they may participate in synaptic stripping. Thus, these results suggest that microglia contribute to perisomatic inhibitory synapse loss following parasitic infection and offer a novel mechanism as to how persistent Toxoplasma gondii infection may contribute to both seizures and psychiatric illness.

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“…During LCMV meningitis, CD8 + T cells can induce a pathogenic recruitment of innate myelomonocytic cells that break down cerebral blood vessels and contribute to fatal CNS edema (Figure 1, Movie 2) [54]. CD8 + T cells can also release IFN-γ onto virally infected neurons, promoting loss of dendrites and synapses [55]. In contrast, another recent study showed that cerebral pathology does not always result from antiviral T cell activity in the infected CNS.…”

Section: Immune-mediated Control Of Cns Pathogensmentioning

confidence: 99%

Immune Surveillance of the CNS following Infection and Injury

Russo

McGavern

2015

Trends in Immunology

157

128

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The central nervous system (CNS) contains a sophisticated neural network that must be constantly surveyed in order to detect and mitigate a diverse array of challenges. The innate and adaptive immune systems actively participate in this surveillance, which is critical for the maintenance of CNS homeostasis and can facilitate the resolution of infections, degeneration, and tissue damage. Infections and sterile injuries represent two common challenges imposed on the CNS that require a prompt immune response. While the inducers of these two challenges differ in origin, the resultant responses orchestrated by the CNS share some overlapping features. Here, we review how the CNS immunologically discriminates between pathogens and sterile injuries, mobilizes an immune reaction, and, ultimately, regulates local and peripherally-derived immune cells to provide a supportive milieu for tissue repair.

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Neuroprotective intervention by interferon-γ blockade prevents CD8+ T cell-mediated dendrite and synapse loss

Cited by 26 publications

References 44 publications

Interferon gamma in autoimmunity: A complicated player on a complex stage

Interferon gamma in autoimmunity: A complicated player on a complex stage

Toxoplasmainduces stripping of perisomatic inhibitory synapses

Immune Surveillance of the CNS following Infection and Injury

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