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Rheumatoid arthritis
A subset of ITGA5+ synovial fibroblasts alter the inflammatory niche in RA
Nature Reviews Rheumatologyvolume 21, page1 (2025)Cite this article
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Pro-inflammatory synovial fibroblasts contribute to chronic inflammation in joints in rheumatoid arthritis (RA); however, there are currently no approved therapies that target fibroblasts in RA. Therapeutic targeting of these cells requires an in-depth understanding of fibroblast heterogeneity in disease. A study by Zheng et al. provides a single-cell and spatial atlas of synovial cells in individuals with RA and identifies a subset of activated sub-lining fibroblasts that express integrin alpha 5 (ITGA5).
ITGA5+ fibroblasts promoted the migration of naive CD4+ T cells to the joint via the CCL5–CCR4 axis and induced the differentiation of these cells to PD-1hiCXCL13+ T effector cells via TGFβ1. PD-1hiCXCL13+ T effector cells resembled a previously reported T helper cell subset that expressed CXCL13, IL-21, ICOS and MAF, and could promote B cell responses in individuals with RA. Therefore, the authors hypothesized that ITGA5+ fibroblasts might be promoting pathogenic T cell responses in the joint.
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References
Original article
Zheng, L. et al. ITGA5+ synovial fibroblasts orchestrate proinflammatory niche formation by remodelling the local immune microenvironment in rheumatoid arthritis.Ann. Rheum. Dis.https://doi.org/10.1136/ard-2024-225778 (2024)
Related article
Rao, D. et al. Pathologically expanded peripheral T helper cell subset drives B cells in rheumatoid arthritis.Nature542, 110–114 (2017)
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Nature Reviews Rheumatologyhttp://www.nature.com/nrrheum/
Holly Webster
- Holly Webster
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Correspondence toHolly Webster.
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Webster, H. A subset of ITGA5+ synovial fibroblasts alter the inflammatory niche in RA.Nat Rev Rheumatol21, 1 (2025). https://doi.org/10.1038/s41584-024-01197-3
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