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Single-cell transcriptomics reveals distinct inflammation-induced microglia signatures.

Carole SousaAnna GolebiewskaSuresh K PoovathingalTony KaomaYolanda Pires-AfonsoSilvia MartinaDjalil CoowarFrancisco AzuajeAlexander SkupinRudi BallingKnut BiberSimone P NiclouAlessandro Michelucci
Published in: EMBO reports (2018)
Microglia are specialized parenchymal-resident phagocytes of the central nervous system (CNS) that actively support, defend and modulate the neural environment. Dysfunctional microglial responses are thought to worsen CNS diseases; nevertheless, their impact during neuroinflammatory processes remains largely obscure. Here, using a combination of single-cell RNA sequencing and multicolour flow cytometry, we comprehensively profile microglia in the brain of lipopolysaccharide (LPS)-injected mice. By excluding the contribution of other immune CNS-resident and peripheral cells, we show that microglia isolated from LPS-injected mice display a global downregulation of their homeostatic signature together with an upregulation of inflammatory genes. Notably, we identify distinct microglial activated profiles under inflammatory conditions, which greatly differ from neurodegenerative disease-associated profiles. These results provide insights into microglial heterogeneity and establish a resource for the identification of specific phenotypes in CNS disorders, such as neuroinflammatory and neurodegenerative diseases.
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