2022
DOI: 10.3389/fimmu.2022.945485
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Microglia subtypes show substrate- and time-dependent phagocytosis preferences and phenotype plasticity

Abstract: Microglia are phagocytosis-competent CNS cells comprising a spectrum of subtypes with beneficial and/or detrimental functions in acute and chronic neurodegenerative disorders. The heterogeneity of microglia suggests differences in phagocytic activity and phenotype plasticity between microglia subtypes. To study these issues, primary murine glial cultures were cultivated in the presence of serum, different growth factors and cytokines to obtain M0-like, M1-like, and M2-like microglia as confirmed by morphology,… Show more

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Cited by 7 publications
(3 citation statements)
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References 94 publications
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“…These signatures showed a strong correlation with each other (Additional file 2 : Fig S7B). We further functionally evaluated the phagocytic capacity of freshly isolated CD11b + myeloid cells in PDOXs with different proportions of CL3 Mg-TAMs (37% PDOX P8, 26% PDOX P3, and 17% PDOX P13) and in normal brain (11% CL3 of myeloid cells) using E. coli particles labeled with fluorescent pH-sensitive dye [ 59 ]. Indeed, CD11b + cells isolated from PDOX P8 showed increased phagocytic abilities compared to CD11b + cells isolated from normal brains and PDOX P13 (Fig.…”
Section: Resultsmentioning
confidence: 99%
“…These signatures showed a strong correlation with each other (Additional file 2 : Fig S7B). We further functionally evaluated the phagocytic capacity of freshly isolated CD11b + myeloid cells in PDOXs with different proportions of CL3 Mg-TAMs (37% PDOX P8, 26% PDOX P3, and 17% PDOX P13) and in normal brain (11% CL3 of myeloid cells) using E. coli particles labeled with fluorescent pH-sensitive dye [ 59 ]. Indeed, CD11b + cells isolated from PDOX P8 showed increased phagocytic abilities compared to CD11b + cells isolated from normal brains and PDOX P13 (Fig.…”
Section: Resultsmentioning
confidence: 99%
“…Cytoskeleton proteins facilitate the engulfment and internalization of particles into a phagosome, while proteins in the endo-lysosomal compartment aid in the removal of degradation products, recycling, and antigen presentation ( Figure 3A ). In the brain, this process, mainly linked to microglia activity, participates in brain homeostasis, neural development and plasticity, synaptic connectivity, immune response, control of inflammation, and myelin repair (Galloway et al, 2019 ; Li et al, 2022 ). Several genes known to have an important role in microglial phagocytosis, especially at the cell surface, were found in the upregulated DEGs in the Acox 1 −/− genotype as compared to the WT cells ( C3, Cd200r1, Cd36, Fcgr2b, Fcgr3, Lbp, Marco, Mrc1, Tlr4 , and Trem2 ) ( Figure 3B ).…”
Section: Resultsmentioning
confidence: 99%
“…These signatures showed a strong correlation with each other (Fig S7B). We further functionally evaluated the phagocytic capacity of freshly isolated CD11b + myeloid cells in PDOXs with different proportions of CL3 Mg-TAMs (37% PDOX P8, 26% PDOX P3 and 17% PDOX P13) and in normal brain (11% CL3 of myeloid cells) using E. coli particles labeled with fluorescent pH-sensitive dye 55 . Indeed, CD11b + cells isolated from PDOX P8 showed increased phagocytic abilities compared to CD11b + cells isolated from normal brains and PDOX P13 ( , which are known to inhibit the phagocytic capacity of macrophages.…”
Section: Rare Mo and Bams Undergo Phenotypic Adaptation Toward Tam Fe...mentioning
confidence: 99%