Gpnmb and Spp1 mark a conserved macrophage injury response masking fibrosis-specific programming in the lung

巨噬细胞 纤维化 脂多糖 肺纤维化 博莱霉素 炎症 生物 医学 免疫学 病理 遗传学 内科学 体外 化疗
作者
Emily M. King,Yifan Zhao,Camille M. Moore,Benjamin Steinhart,Kelsey Anderson,Brian Vestal,Peter K. Moore,Shannon A. McManus,Christopher M. Evans,Kara J. Mould,Elizabeth F. Redente,Alexandra L. McCubbrey,William J. Janssen
出处
期刊:JCI insight [American Society for Clinical Investigation]
卷期号:9 (24) 被引量:31
标识
DOI:10.1172/jci.insight.182700
摘要

Macrophages are required for healthy repair of the lungs following injury, but they are also implicated in driving dysregulated repair with fibrosis. How these 2 distinct outcomes of lung injury are mediated by different macrophage subsets is unknown. To assess this, single-cell RNA-Seq was performed on lung macrophages isolated from mice treated with LPS or bleomycin. Macrophages were categorized based on anatomic location (airspace versus interstitium), developmental origin (embryonic versus recruited monocyte derived), time after inflammatory challenge, and injury model. Analysis of the integrated dataset revealed that macrophage subset clustering was driven by macrophage origin and tissue compartment rather than injury model. Gpnmb-expressing recruited macrophages that were enriched for genes typically associated with fibrosis were present in both injury models. Analogous GPNMB-expressing macrophages were identified in datasets from both fibrotic and nonfibrotic lung disease in humans. We conclude that this subset represents a conserved response to tissue injury and is not sufficient to drive fibrosis. Beyond this conserved response, we identified that recruited macrophages failed to gain resident-like programming during fibrotic repair. Overall, fibrotic versus nonfibrotic tissue repair is dictated by dynamic shifts in macrophage subset programming and persistence of recruited macrophages.
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