| Literature DB >> 30471926 |
Timothy R Hammond1, Connor Dufort2, Lasse Dissing-Olesen1, Stefanie Giera3, Adam Young4, Alec Wysoker5, Alec J Walker1, Frederick Gergits2, Michael Segel4, James Nemesh5, Samuel E Marsh1, Arpiar Saunders6, Evan Macosko5, Florent Ginhoux7, Jinmiao Chen7, Robin J M Franklin4, Xianhua Piao3, Steven A McCarroll8, Beth Stevens9.
Abstract
Microglia, the resident immune cells of the brain, rapidly change states in response to their environment, but we lack molecular and functional signatures of different microglial populations. Here, we analyzed the RNA expression patterns of more than 76,000 individual microglia in mice during development, in old age, and after brain injury. Our analysis uncovered at least nine transcriptionally distinct microglial states, which expressed unique sets of genes and were localized in the brain using specific markers. The greatest microglial heterogeneity was found at young ages; however, several states-including chemokine-enriched inflammatory microglia-persisted throughout the lifespan or increased in the aged brain. Multiple reactive microglial subtypes were also found following demyelinating injury in mice, at least one of which was also found in human multiple sclerosis lesions. These distinct microglia signatures can be used to better understand microglia function and to identify and manipulate specific subpopulations in health and disease.Entities:
Keywords: activation; brain; demyelination; development; diversity; glia; heterogeneity; injury; microglia; single-cell RNA seq
Mesh:
Year: 2018 PMID: 30471926 PMCID: PMC6655561 DOI: 10.1016/j.immuni.2018.11.004
Source DB: PubMed Journal: Immunity ISSN: 1074-7613 Impact factor: 31.745