| Literature DB >> 30679343 |
Roman Sankowski1,2, Stefanie M Brendecke1, Marta Joana Costa Jordão1,3, Giuseppe Locatelli4,5, Yi-Heng Tai4,5, Tuan Leng Tay1,3,6, Eva Schramm1, Stephan Armbruster1, Nora Hagemeyer1, Olaf Groß1,7,8,9, Dominic Mai10,11, Özgün Çiçek10, Thorsten Falk7,10, Martin Kerschensteiner4,5,12, Dominic Grün13, Marco Prinz14,7,9,15.
Abstract
The innate immune cell compartment is highly diverse in the healthy central nervous system (CNS), including parenchymal and non-parenchymal macrophages. However, this complexity is increased in inflammatory settings by the recruitment of circulating myeloid cells. It is unclear which disease-specific myeloid subsets exist and what their transcriptional profiles and dynamics during CNS pathology are. Combining deep single-cell transcriptome analysis, fate mapping, in vivo imaging, clonal analysis, and transgenic mouse lines, we comprehensively characterized unappreciated myeloid subsets in several CNS compartments during neuroinflammation. During inflammation, CNS macrophage subsets undergo self-renewal, and random proliferation shifts toward clonal expansion. Last, functional studies demonstrated that endogenous CNS tissue macrophages are redundant for antigen presentation. Our results highlight myeloid cell diversity and provide insights into the brain's innate immune system.Entities:
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Year: 2019 PMID: 30679343 DOI: 10.1126/science.aat7554
Source DB: PubMed Journal: Science ISSN: 0036-8075 Impact factor: 47.728