Surface protein and functional analyses identify CD4+CD39+ TCR αβ+ and activated TCR Vδ1+ cells with distinct pro-inflammatory functions in Crohn's Disease lesions

生物 免疫系统 T细胞受体 免疫学 炎症 流式细胞术 T细胞 克罗恩病 CD3型 CD8型 疾病 病理 医学
作者
Ján Deván,Vladimir Nosi,Julian Spagnuolo,Andrew Chancellor,Aisha Beshirova,José Pedro Loureiro,Alessandro Vacchini,Jan Hendrik Niess,Raffaele Calogero,Lucia Mori,Gennaro De Libero,Petr Hrúz
出处
期刊:Clinical and Experimental Immunology [Wiley]
标识
DOI:10.1093/cei/uxad098
摘要

Abstract Crohn’s disease (CD) is a chronic immune-mediated disorder of the gastrointestinal tract. Extensive screening studies have revealed the accumulation of immune cell subsets with unique plasticity and immunoregulatory properties in patients with CD. We performed phenotypic and functional studies on inflamed and non-inflamed bioptic tissue to investigate the presence of distinct T cells in the intestinal mucosa of CD patients. We analyzed hundreds of surface molecules expressed on cells isolated from the intestinal tissue of CD patients using anti-CD45 mAbs-based barcoding. A gene ontology enrichment analysis showed that proteins that regulate the activation of T cells were the most enriched group. We, therefore, designed T cell focused multicolour flow-cytometry panels and performed clustering analysis which revealed an accumulation of activated TEM CD4+CD39+ T cells producing IL-17 and IL-21 and increased frequency of terminally differentiated TCR Vδ1+ cells producing TNF-α and IFN-γ in inflamed tissue of CD patients. The different functional capacities of CD4+ and TCR Vδ1+ cells in CD lesions indicate their non-overlapping contribution to inflammation. The abnormally high number of terminally differentiated TCR Vδ1+ cells suggests that they are continuously activated in inflamed tissue, making them a potential target for novel therapies.

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