Fibroblastic reticular cells form reactive myeloid cell niches in human lymph nodes Journal Article


Authors: Lütge, M.; Kurz, L.; Stanossek, Y.; Meili, S.; Cheng, H. W.; De Martin, A.; Brandstadter, J.; Maillard, I.; Robinson, M. D.; Stoeckli, S. J.; Pikor, N. B.; Onder, L.; Ludewig, B.
Article Title: Fibroblastic reticular cells form reactive myeloid cell niches in human lymph nodes
Abstract: Lymph nodes play a key role in maintaining fluid balance in homeostatic and inflamed tissues and provide fibroblastic niche environments for optimal immune cell positioning and interaction. Here, we used single-cell and spatial transcriptomic analyses in combination with high-resolution imaging to molecularly define and functionally characterize niche-forming cells that control inflammation-driven remodeling in human lymph nodes. Fibroblastic reticular cells responded to inflammatory perturbation with activation and expansion of poised niche environments. Inflammation-induced adaptation of lymph node infrastructure and topography included the expansion of peptidase inhibitor 16 (PI16)–expressing reticular cell (PI16+ RC) networks that enwrap the perivenular conduit system. Interactome analyses indicated that macrophage-derived oncostatin M directs PI16+ RC activation in inflamed lymph nodes and thereby promotes immune cell aggregation in the perivenular space. In conclusion, these data demonstrate that the inflammatory remodeling of human lymph nodes results in the formation of reactive myeloid cell niches by PI16+ RCs. Copyright © 2025 The Authors, some rights reserved.
Keywords: lymph nodes; cytology; inflammation; immunology; lymph node; fibroblast; fibroblasts; bone marrow cell; myeloid cells; single cell analysis; single-cell analysis; humans; human
Journal Title: Science Immunology
Volume: 10
Issue: 107
ISSN: 2470-9468
Publisher: Amer Assoc Advancement Science  
Date Published: 2025-05-01
Start Page: eads6820
Language: English
DOI: 10.1126/sciimmunol.ads6820
PUBMED: 40315298
PROVIDER: scopus
DOI/URL:
Notes: Source: Scopus
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