期刊
JOURNAL OF EXPERIMENTAL MEDICINE
卷 215, 期 2, 页码 441-458出版社
ROCKEFELLER UNIV PRESS
DOI: 10.1084/jem.20170057
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资金
- Research Council of Norway through its Centres of Excellence funding scheme [179573]
- Southern and Eastern Norway Regional Health Authority
- Central European University European Research Council Advanced Grant SysStemCell [339431]
- Horizon - EU Framework Program Research and Innovation Programme
- European Research Council (ERC) [339431] Funding Source: European Research Council (ERC)
Macrophages (Mfs) are instrumental in maintaining immune homeostasis in the intestine, yet studies on the origin and heterogeneity of human intestinal Mfs are scarce. Here, we identified four distinct Mf subpopulations in human small intestine (SI). Assessment of their turnover in duodenal transplants revealed that all Mf subsets were completely replaced over time; Mf1 and Mf2, phenotypically similar to peripheral blood monocytes (PBMos), were largely replaced within 3 wk, whereas two subsets with features of mature Mfs, Mf3 and Mf4, exhibited significantly slower replacement. Mf3 and Mf4 localized differently in SI; Mf3 formed a dense network in mucosal lamina propria, whereas Mf4 was enriched in submucosa. Transcriptional analysis showed that all Mf subsets were markedly distinct from PBMos and dendritic cells. Compared with PBMos, Mf subpopulations showed reduced responsiveness to proinflammatory stimuli but were proficient at endocytosis of particulate and soluble material. These data provide a comprehensive analysis of human SI Mf population and suggest a precursor-progeny relationship with PBMos.
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