| Literature DB >> 32220976 |
Basak B Ural1, Stephen T Yeung2, Payal Damani-Yokota2, Joseph C Devlin2, Maren de Vries2, Paola Vera-Licona3,4,5,6, Tasleem Samji2, Catherine M Sawai7, Geunhyo Jang8, Oriana A Perez8, Quynh Pham9, Leigh Maher9, P'ng Loke2, Meike Dittmann2, Boris Reizis8,10, Kamal M Khanna11,12.
Abstract
Tissue-resident macrophages are a diverse population of cells that perform specialized functions including sustaining tissue homeostasis and tissue surveillance. Here, we report an interstitial subset of CD169+ lung-resident macrophages that are transcriptionally and developmentally distinct from alveolar macrophages (AMs). They are primarily localized around the airways and are found in close proximity to the sympathetic nerves in the bronchovascular bundle. These nerve- and airway-associated macrophages (NAMs) are tissue resident, yolk sac derived, self-renewing, and do not require CCR2+ monocytes for development or maintenance. Unlike AMs, the development of NAMs requires CSF1 but not GM-CSF. Bulk population and single-cell transcriptome analysis indicated that NAMs are distinct from other lung-resident macrophage subsets and highly express immunoregulatory genes under steady-state and inflammatory conditions. NAMs proliferated robustly after influenza infection and activation with the TLR3 ligand poly(I:C), and in their absence, the inflammatory response was augmented, resulting in excessive production of inflammatory cytokines and innate immune cell infiltration. Overall, our study provides insights into a distinct subset of airway-associated pulmonary macrophages that function to maintain immune and tissue homeostasis.Entities:
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Year: 2020 PMID: 32220976 PMCID: PMC7717505 DOI: 10.1126/sciimmunol.aax8756
Source DB: PubMed Journal: Sci Immunol ISSN: 2470-9468