| Literature DB >> 29399880 |
Hélène Hirbec1,2, Camille Marmai1,2, Isabelle Duroux-Richard3, Christine Roubert4, Arnaud Esclangon4, Séverine Croze5, Joël Lachuer5, Ronan Peyroutou1,2, François Rassendren1,2.
Abstract
Microglial cells have a double life as the immune cells of the brain in times of stress but have also specific physiological functions in homeostatic conditions. In pathological contexts, microglia undergo a phenotypic switch called "reaction" that promotes the initiation and the propagation of neuro-inflammation. Reaction is complex, molecularly heterogeneous and still poorly characterized, leading to the concept that microglial reactivity might be too diverse to be molecularly defined. However, it remains unknown whether reactive microglia from different pathological contexts share a common molecular signature. Using improved flow cytometry and RNAseq approaches we studied, with higher statistical power, the remodeling of microglia transcriptome in a mouse model of sepsis. Through bioinformatic comparison of our results with published datasets, we defined the microglial reactome as a set of genes discriminating reactive from homeostatic microglia. Ultimately, we identified a subset of 86 genes deregulated in both acute and neurodegenerative conditions. Our data provide a new comprehensive resource that includes functional analysis and specific molecular markers of microglial reaction which represent new tools for its unambiguous characterization.Entities:
Keywords: RNA sequencing (RNA-seq); lipopolysaccharide (LPS); microglia; neurodegenerative pathologies; transcriptome
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Year: 2018 PMID: 29399880 DOI: 10.1002/glia.23295
Source DB: PubMed Journal: Glia ISSN: 0894-1491 Impact factor: 7.452