Siglec‐H is a microglia‐specific marker that discriminates microglia from CNS‐associated macrophages and CNS‐infiltrating monocytes

Konishi, Hiroyuki; Kobayashi, Masaaki; Kunisawa, Taikan; Imai, Kenta; Sayo, Akira; Malissen, Bernard; Crocker, Paul R.; Sato, Katsuaki; Kiyama, Hiroshi

doi:10.1002/glia.23204

Cited by 119 publications

(103 citation statements)

References 78 publications

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“…4b, c, red asterisk) [27,28,55]. Sialic acid-binding immunoglobulin-type lectin H (SiglecH), a specific microglia marker [56] that was suggested to be expressed when these cells are polarized toward the inflammatory phenotype, was also highly expressed by reactive microglia in our assay (Fig. 4c).…”

Section: Reactive Microglia and Infiltrating Macrophages Have Distincmentioning

confidence: 70%

Differential transcriptional profiles identify microglial- and macrophage-specific gene markers expressed during virus-induced neuroinflammation

DePaula-Silva

Gorbea

Doty

et al. 2019

J Neuroinflammation

102

113

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Background In the healthy central nervous system (CNS), microglia are found in a homeostatic state and peripheral macrophages are absent from the brain. Microglia play key roles in maintaining CNS homeostasis and acting as first responders to infection and inflammation, and peripheral macrophages infiltrate the CNS during neuroinflammation. Due to their distinct origins and functions, discrimination between these cell populations is essential to the comprehension of neuroinflammatory disorders. Studies comparing the gene profiles of microglia and peripheral macrophages, or macrophages in vitro-derived from bone marrow, under non-infectious conditions of the CNS, have revealed valuable microglial-specific genes. However, studies comparing gene profiles between CNS-infiltrating macrophages and microglia, when both are isolated from the CNS during viral-induced neuroinflammation, are lacking. Methods We isolated, via flow cytometry, microglia and infiltrating macrophages from the brains of Theiler’s murine encephalomyelitis virus-infected C57BL/6 J mice and used RNA-Seq, followed by validation with qPCR, to examine the differential transcriptional profiles of these cells. We utilized primary literature defining subcellular localization to determine whether or not particular proteins extracted from the transcriptional profiles were expressed at the cell surface. The surface expression and cellular specificity of triggering receptor expressed on myeloid cells 1 (TREM-1) protein were examined via flow cytometry. We also examined the immune response gene profile within the transcriptional profiles of these isolated microglia and infiltrating macrophages. Results We have identified and validated new microglial- and macrophage-specific genes, encoding cell surface proteins, expressed at the peak of neuroinflammation. TREM-1 protein was confirmed to be expressed by infiltrating macrophages, not microglia, at the peak of neuroinflammation. We also identified both unique and redundant immune functions, through examination of the immune response gene profiles, of microglia and infiltrating macrophages during neurotropic viral infection. Conclusions The differential expression of cell surface-specific genes during neuroinflammation can potentially be used to discriminate between microglia and macrophages as well as provide a resource that can be further utilized to target and manipulate specific cell responses during neuroinflammation. Electronic supplementary material The online version of this article (10.1186/s12974-019-1545-x) contains supplementary material, which is available to authorized users.

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Section: Reactive Microglia and Infiltrating Macrophages Have Distincmentioning

confidence: 70%

Differential transcriptional profiles identify microglial- and macrophage-specific gene markers expressed during virus-induced neuroinflammation

DePaula-Silva

Gorbea

Doty

et al. 2019

J Neuroinflammation

102

113

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“…For this purpose, we per-formed a synapse engulfment assay (Schafer et al, 2012) in the mossy fiber pathway to detect the volume of synaptic elements engulfed by microglia in mice, in which microglia are selectively labeled with GFP (Zhan et al, 2014) ( Figure 3A). We confirmed that no GFP(+) cell in the hippocampal CA3 was immunopositive for CCR2 (Prinz and Priller., 2010), an infiltrating cell-specific marker ( Figure S3), while GFP(+) cells were stained with an antibody for Siglec-H (Zhang et al, 2006;Konishi et al, 2017) and P2Y12R (Sasaki et al, 2003;Haynes et al, 2006;Mildner et al, 2017), which were generally used as microglia-specific markers ( Figure S3). Furthermore, GFP(+) cells expressed interleukin-1b (IL-1b), one of the typical cytokines released from microglia (Figure S3).…”

Section: Exercise In Adulthood Stimulates Microglia To Prune Synapsesmentioning

confidence: 99%

Exercise Reverses Behavioral and Synaptic Abnormalities after Maternal Inflammation

et al. 2019

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“…In addition, CSF‐1R inhibition can robustly decline the actions of nerve‐associated macrophages in the periphery (Klein et al, ). However, several studies have identified some potential markers that are exclusively expressed in microglia including Tmem119, P2RY12, Siglec‐H and Sal1, permitting distinction of resident microglia from other myeloid cells (Bennett et al, ; Butovsky et al, ; Buttgereit et al, ; Konishi et al, ). These markers, together with the Cre/loxP technology, may make it possible to deplete microglia with exquisite precision in the near future.…”

Section: Depleting Microglia In Diseases: the Friend In Need May Notmentioning

confidence: 99%

Enforced microglial depletion and repopulation as a promising strategy for the treatment of neurological disorders

Han

Zhu

Zhang

et al. 2018

Glia

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Microglia are prominent immune cells in the central nervous system (CNS) and are critical players in both neurological development and homeostasis, and in neurological diseases when dysfunctional. Our previous understanding of the phenotypes and functions of microglia has been greatly extended by a dearth of recent investigations. Distinct genetically defined subsets of microglia are now recognized to perform their own independent functions in specific conditions. The molecular profiling of single microglial cells indicates extensively heterogeneous reactions in different neurological disorders, resulting in multiple potentials for crosstalk with other kinds of CNS cells such as astrocytes and neurons. In settings of neurological diseases it could thus be prudent to establish effective cell‐based therapies by targeting entire microglial networks. Notably, activated microglial depletion through genetic targeting or pharmacological therapies within a suitable time window can stimulate replenishment of the CNS niche with new microglia. Additionally, enforced repopulation through provision of replacement cells also represents a potential means of exchanging dysfunctional with functional microglia. In each setting the newly repopulated microglia might have the potential to resolve ongoing neuroinflammation. In this review, we aim to summarize the most recent knowledge of microglia and to highlight microglial depletion and subsequent repopulation as a promising cell replacement therapy. Although glial cell replacement therapy is still in its infancy and future translational studies are still required, the approach is scientifically sound and provides new optimism for managing the neurotoxicity and neuroinflammation induced by activated microglia.

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Siglec‐H is a microglia‐specific marker that discriminates microglia from CNS‐associated macrophages and CNS‐infiltrating monocytes

Cited by 119 publications

References 78 publications

Differential transcriptional profiles identify microglial- and macrophage-specific gene markers expressed during virus-induced neuroinflammation

Differential transcriptional profiles identify microglial- and macrophage-specific gene markers expressed during virus-induced neuroinflammation

Exercise Reverses Behavioral and Synaptic Abnormalities after Maternal Inflammation

Enforced microglial depletion and repopulation as a promising strategy for the treatment of neurological disorders

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