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Publication : Tissue-resident, extravascular Ly6c(-) monocytes are critical for inflammation in the synovium.

First Author  Montgomery AB Year  2023
Journal  Cell Rep Volume  42
Issue  5 Pages  112513
PubMed ID  37204925 Mgi Jnum  J:348572
Mgi Id  MGI:7491428 Doi  10.1016/j.celrep.2023.112513
Citation  Montgomery AB, et al. (2023) Tissue-resident, extravascular Ly6c(-) monocytes are critical for inflammation in the synovium. Cell Rep 42(5):112513
abstractText  Monocytes are abundant immune cells that infiltrate inflamed organs. However, the majority of monocyte studies focus on circulating cells, rather than those in tissue. Here, we identify and characterize an intravascular synovial monocyte population resembling circulating non-classical monocytes and an extravascular tissue-resident monocyte-lineage cell (TR-MC) population distinct in surface marker and transcriptional profile from circulating monocytes, dendritic cells, and tissue macrophages that are conserved in rheumatoid arthritis (RA) patients. TR-MCs are independent of NR4A1 and CCR2, long lived, and embryonically derived. TR-MCs undergo increased proliferation and reverse diapedesis dependent on LFA1 in response to arthrogenic stimuli and are required for the development of RA-like disease. Moreover, pathways that are activated in TR-MCs at the peak of arthritis overlap with those that are downregulated in LFA1(-/-) TR-MCs. These findings show a facet of mononuclear cell biology that could be imperative to understanding tissue-resident myeloid cell function in RA.
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