Peripheral nerve resident macrophages are microglia-like cells with tissue-specific programming

Wang, Peter L.; Yim, Aldrin Kay-Yuen; Avey, Denis; Czepielewski, Rafael S.; Colonna, Marco; Milbrandt, Jeffrey; Randolph, Gwendalyn J.

doi:10.1101/2019.12.19.883546

Cited by 3 publications

(2 citation statements)

References 43 publications

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“…For murine zymosan-uptake studies, CD11c + enriched cells from BM and spleen were co-cultured for 2 h with 10–40 ug/mL FITC-labeled zymosan in RPMI-1640 (ThermoFisher Scientific) supplemented with 10% FCS and 1% penicillin-streptomycin. In some experiments, 20 µg/mL Dectin-1 blocking antibody (clone R1-8g7; Invivogen; [ 13 , 14 , 15 , 16 ]) was added to the culture. For human zymosan-uptake studies, human BM mononuclear cells were enriched for DCs with CD11c microbeads (Miltenyi Biotec, Leiden, The Netherlands) and co-cultured with 40 µg/mL zymosan for 2 or 16 h in RPMI-1640 (ThermoFisher Scientific, Waltham, MA, USA) supplemented with 10% FCS and 1% penicillin-streptomycin in the presence of blocking antibodies against CD11b (10 ug/mL; clone 44A; American Type Culture Collection) and CD18 (10 ug/mL; clone IB4; American Type Culture Collection) [ 17 , 18 ].…”

Section: Methodsmentioning

confidence: 99%

Bone Marrow Harbors a Unique Population of Dendritic Cells with the Potential to Boost Neutrophil Formation upon Exposure to Fungal Antigen

Goedhart

Slot

Pascutti

et al. 2021

Cells

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Apart from controlling hematopoiesis, the bone marrow (BM) also serves as a secondary lymphoid organ, as it can induce naïve T cell priming by resident dendritic cells (DC). When analyzing DCs in murine BM, we uncovered that they are localized around sinusoids, can (cross)-present antigens, become activated upon intravenous LPS-injection, and for the most part belong to the cDC2 subtype which is associated with Th2/Th17 immunity. Gene-expression profiling revealed that BM-resident DCs are enriched for several c-type lectins, including Dectin-1, which can bind beta-glucans expressed on fungi and yeast. Indeed, DCs in BM were much more efficient in phagocytosis of both yeast-derived zymosan-particles and Aspergillus conidiae than their splenic counterparts, which was highly dependent on Dectin-1. DCs in human BM could also phagocytose zymosan, which was dependent on β1-integrins. Moreover, zymosan-stimulated BM-resident DCs enhanced the differentiation of hematopoietic stem and progenitor cells towards neutrophils, while also boosting the maintenance of these progenitors. Our findings signify an important role for BM DCs as translators between infection and hematopoiesis, particularly in anti-fungal immunity. The ability of BM-resident DCs to boost neutrophil formation is relevant from a clinical perspective and contributes to our understanding of the increased susceptibility for fungal infections following BM damage.

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Section: Methodsmentioning

confidence: 99%

Bone Marrow Harbors a Unique Population of Dendritic Cells with the Potential to Boost Neutrophil Formation upon Exposure to Fungal Antigen

Goedhart

Slot

Pascutti

et al. 2021

Cells

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“…Macrophages that reside in peripheral nerve tissue are different from microglia and or nonnervous residing macrophages 13,14 and can be programmed by sensory neurons 15 . We determined whether monocytes/macrophages that infiltrate the DRG had an inflammatory ('M1') -or resolution ('M2')-like phenotype.…”

Section: Main Textmentioning

confidence: 99%

Macrophages transfer mitochondria to sensory neurons to resolve inflammatory pain

Raoof

Vlist

Willemen

et al. 2020

Preprint

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The current paradigm states that inflammatory pain passively resolves following the cessation of the inflammatory insult. Yet, in a substantial proportion of patients with inflammatory diseases, such as rheumatoid arthritis and inflammatory bowel disease, spontaneous or treatment-induced resolution of inflammation is not sufficient to resolve pain, resulting in chronic pain 1-5 . Mechanistic insight as how inflammatory pain is resolved is lacking.Here we show that macrophages actively control resolution of inflammatory pain remotely from the site of inflammation by transferring mitochondria to sensory neurons. During resolution of inflammatory pain in mice, M2-like macrophages infiltrate the dorsal root ganglia that contain the somata of sensory neurons, concurrent with the recovery of oxidative phosphorylation in sensory neurons. To resolve pain, macrophages transfer mitochondria to sensory neurons. This transfer requires expression of CD200 Receptor (CD200R) on macrophages and the noncanonical CD200R-ligand iSec1 on sensory neurons. Our data reveal a novel mechanism for active resolution of inflammatory pain and suggests a new direction for treatment of chronic pain.

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Profiling peripheral nerve macrophages reveals two macrophage subsets with distinct localization, transcriptome and response to injury

et al. 2020

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While central nervous system (CNS) microglia have been studied extensively, surprisingly little is known about macrophages populating the peripheral nervous system (PNS Macs).We performed ontogenic, transcriptomic and spatial characterization of sciatic nerve Macs (snMacs). Using multiple fate-mapping systems, we show that snMacs do not derive from the early embryonic precursors colonizing the CNS, but originate primarily from late embryonic precursors and get replaced by bone marrow-derived Macs over time. Using single-cell profiling, we identified a tissue-specific core signature of snMacs and found two spatially-separated snMacs: Relmα + Mgl1 + snMacs in the epineurium and Relmα -Mgl1-snMacs in the endoneurium. Globally, snMacs lack most core signature genes of microglia, with only the endoneurial subset expressing a restricted number of these genes. Single-cell transcriptomics revealed that in response to injury both snMacs respond differently and that the PNS, in contrast to the CNS, is permissive to prolonged engraftment of monocytederived Macs recruited upon injury.

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Peripheral nerve resident macrophages are microglia-like cells with tissue-specific programming

Cited by 3 publications

References 43 publications

Bone Marrow Harbors a Unique Population of Dendritic Cells with the Potential to Boost Neutrophil Formation upon Exposure to Fungal Antigen

Bone Marrow Harbors a Unique Population of Dendritic Cells with the Potential to Boost Neutrophil Formation upon Exposure to Fungal Antigen

Macrophages transfer mitochondria to sensory neurons to resolve inflammatory pain

Profiling peripheral nerve macrophages reveals two macrophage subsets with distinct localization, transcriptome and response to injury

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