AI Article Synopsis

  • * Researchers employed various techniques like flow cytometry, RNA-Seq, and qPCR to analyze OA synovial tissues, identifying specific mast cell markers and categorizing OA patients into three pathotypes based on mast cell presence.
  • * Treatment with cetirizine, an antagonist of the histamine receptor, showed promise in reducing OA severity and associated mediators, suggesting that targeting mast cell activity may improve disease outcomes.

Article Abstract

Objective: Mast cells in the osteoarthritis (OA) synovium correlate with disease severity. This study aimed to further elucidate the role of mast cells in OA by RNA-Seq analysis and pharmacological blockade of the activity of histamine, a key mast cell mediator, in murine OA.

Methods: We examined OA synovial tissues and fluids by flow cytometry, immunostaining, single-cell and bulk RNA-Seq, qPCR, and ELISA. Cetirizine, a histamine H1 receptor (HR) antagonist, was used to treat the destabilization of the medial meniscus (DMM) mouse model of OA.

Results: Flow cytometry and immunohistology analysis of OA synovial cells revealed KIT FcεRI and TPSAB1 mast cells. Single-cell RNA-Seq of OA synovial cells identified the expression of prototypical mast cell markers KIT, TPSAB1, CPA3 and HDC, as well as distinctive markers HPGD, CAVIN2, IL1RL1, PRG2, and CKLF, confirmed by bulk RNA-Seq and qPCR. A mast cell prototypical marker expression score classified 40 OA patients into three synovial pathotypes: mast cell-high, -medium, and -low. Additionally, we detected mast cell mediators including histamine, tryptase AB1, CPA3, PRG2, CAVIN2, and CKLF in OA synovial fluids. Elevated HR expression was detected in human OA synovium, and treatment of mice with the H receptor antagonist cetirizine reduced the severity and OA-related mediators in DMM.

Conclusion: Based on differential expression of prototypical and distinct mast cell markers, human OA joints can be stratified into mast cell-high, -medium, and -low synovial tissue pathotypes. Pharmacologic blockade of histamine activity holds the potential to improve OA disease outcome.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC10752578PMC
http://dx.doi.org/10.1016/j.clim.2022.109117DOI Listing

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