Cytokine Signalling at the Microglial Penta-Partite Synapse

Aramideh, Jason Abbas; Vidal-Itriago, Andrés; Morsch, Marco; Graeber, Manuel B.

doi:10.3390/ijms222413186

Cited by 15 publications

(14 citation statements)

References 189 publications

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“…This effect was more apparent and prolonged in devices incubated with MCM Aβ40 compared to MCM Aβ42 . It is important to note that even the MCM Untr supernatant also reduced hmNGF release from ECB-NGF devices, indicating that NGC0211 cells are sensitive to factors released by untreated microglia, as previously shown by other reports [ 27 ]. Furthermore, we provided evidence that the activation of the HMC3 cell line with the Aβ40 peptide can contribute to a lower proliferation rate of NGC0211 cells in-vitro.…”

Section: Discussionsupporting

confidence: 78%

“…HMC3 cells treated with DMSO (0.1% final concentration) provided control for factors released by unstimulated microglia and denoted as MCM Untr . It is well known that, even under physiological conditions, microglia can release different cytokines [ 27 ]. MCM Untr itself serves as an ‘experimental control’ for additional factors, which might be released upon stimulation by activated microglia.…”

Section: Methodsmentioning

confidence: 99%

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Microglia Impairs Proliferation and Induces Senescence In-Vitro in NGF Releasing Cells Used in Encapsulated Cell Biodelivery for Alzheimer’s Disease Therapy

Mitra

Gera

Sundheimer

et al. 2022

IJMS

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There is no cure yet available for Alzheimer’s disease (AD). We recently optimized encapsulated cell biodelivery (ECB) devices releasing human mature nerve growth factor (hmNGF), termed ECB-NGF, to the basal forebrain of AD patients. The ECB-NGF delivery resulted in increased CSF cholinergic markers, improved glucose metabolism, and positive effects on cognition in AD patients. However, some ECB-NGF implants showed altered hmNGF release post-explantation. To optimize the ECB-NGF platform for future therapeutic purposes, we initiated in-vitro optimization studies by exposing ECB-NGF devices to physiological factors present within the AD brain. We report here that microglia cells can impair hmNGF release from ECB-NGF devices in-vitro, which can be reversed by transferring the devices to fresh culture medium. Further, we exposed the hmNGF secreting human ARPE-19 cell line (NGC0211) to microglia (HMC3) conditioned medium (MCM; untreated or treated with IL-1β/IFNγ/Aβ40/Aβ42), and evaluated biochemical stress markers (ROS, GSH, ΔΨm, and Alamar Blue assay), cell death indicators (Annexin-V/PI), cell proliferation (CFSE retention and Ki67) and senescence markers (SA-β-gal) in NGC0211 cells. MCMs from activated microglia reduced cell proliferation and induced cell senescence in NGC0211 cells, which otherwise resist biochemical alterations and cell death. These data indicate a critical but reversible impact of activated microglia on NGC0211 cells.

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Section: Discussionsupporting

confidence: 78%

Section: Methodsmentioning

confidence: 99%

Microglia Impairs Proliferation and Induces Senescence In-Vitro in NGF Releasing Cells Used in Encapsulated Cell Biodelivery for Alzheimer’s Disease Therapy

Mitra

Gera

Sundheimer

et al. 2022

IJMS

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“…Microglial effects upon neuronal connectivity are also not limited to the developmental stage. In the adult CNS, microglia have been shown to engulf synaptic material in both the healthy brain and in neurodegenerative conditions ( 13 , 75 – 77 ). Early ultrastructural studies described microglia-mediated displacement of synaptic terminals, suggesting that microglia actively participate in synaptic plasticity ( 78 – 80 ).…”

Section: Microglial Biologymentioning

confidence: 99%

Microglia morphophysiological diversity and its implications for the CNS

Vidal-Itriago

Radford²,

Aramideh³

et al. 2022

Front. Immunol.

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Microglia are mononuclear phagocytes of mesodermal origin that migrate to the central nervous system (CNS) during the early stages of embryonic development. After colonizing the CNS, they proliferate and remain able to self-renew throughout life, maintaining the number of microglia around 5-12% of the cells in the CNS parenchyma. They are considered to play key roles in development, homeostasis and innate immunity of the CNS. Microglia are exceptionally diverse in their morphological characteristics, actively modifying the shape of their processes and soma in response to different stimuli. This broad morphological spectrum of microglia responses is considered to be closely correlated to their diverse range of functions in health and disease. However, the morphophysiological attributes of microglia, and the structural and functional features of microglia-neuron interactions, remain largely unknown. Here, we assess the current knowledge of the diverse microglial morphologies, with a focus on the correlation between microglial shape and function. We also outline some of the current challenges, opportunities, and future directions that will help us to tackle unanswered questions about microglia, and to continue unravelling the mysteries of microglia, in all its shapes.

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“…In addition, microglia can shape synapses by direct contact with them [ 134 ]. Following synaptic injury, microglia tightly associate with dendrites and directly separate pre-synaptic and post-synaptic neurons, a process known as “synaptic stripping” [ 135 ].…”

Section: Microglial Mechanisms Of Ad Pathogenesis and Memory Impairmentmentioning

confidence: 99%

New Insights into Microglial Mechanisms of Memory Impairment in Alzheimer’s Disease

Deng

et al. 2022

Biomolecules

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Alzheimer’s disease (AD) is the most common progressive and irreversible neurodegeneration characterized by the impairment of memory and cognition. Despite years of studies, no effective treatment and prevention strategies are available yet. Identifying new AD therapeutic targets is crucial for better elucidating the pathogenesis and establishing a valid treatment of AD. Growing evidence suggests that microglia play a critical role in AD. Microglia are resident macrophages in the central nervous system (CNS), and their core properties supporting main biological functions include surveillance, phagocytosis, and the release of soluble factors. Activated microglia not only directly mediate the central immune response, but also participate in the pathological changes of AD, including amyloid-beta (Aβ) aggregation, tau protein phosphorylation, synaptic dissection, neuron loss, memory function decline, etc. Based on these recent findings, we provide a new framework to summarize the role of microglia in AD memory impairment. This evidence suggests that microglia have the potential to become new targets for AD therapy.

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Cytokine Signalling at the Microglial Penta-Partite Synapse

Cited by 15 publications

References 189 publications

Microglia Impairs Proliferation and Induces Senescence In-Vitro in NGF Releasing Cells Used in Encapsulated Cell Biodelivery for Alzheimer’s Disease Therapy

Microglia Impairs Proliferation and Induces Senescence In-Vitro in NGF Releasing Cells Used in Encapsulated Cell Biodelivery for Alzheimer’s Disease Therapy

Microglia morphophysiological diversity and its implications for the CNS

New Insights into Microglial Mechanisms of Memory Impairment in Alzheimer’s Disease

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