Gene expression of Foxp3+CD8+ Tregs induced with or without laminin a5
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https://www.ncbi.nlm.nih.gov/sra/SRP620843
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Foxp3+CD8+ regulatory T cells (CD8 Tregs) help to establish immune tolerance in models of chronic inflammation and antigen stimulation, such as graft versus host disease and chronic infections. However, the elements contributing to CD8 Treg induction remain obscure. In this study, we found that laminin a5 enhanced CD8 Treg inducation from mouse naive T cells stimulated with a combination of anit-CD3/anti-CD28/IL-2/TGFÃ. While, the suppressive ability of CD8 Tregs induced with laminin a5 was reduced by 23.8% compared to these induced without laminin a5; the cytotoxic ability of CD8 Tregs induced with laminin a5 was significant reduced (more than 64%) compared to these induced without laminin a5. Mechanistically, laminin a5 was invovled in modulating both TCR signaling and cytokine responses during induction of CD8 Tregs. Laminin a5 inihbited IFNg and TNFa expression by CD8 T cells, which further enhanced Foxp3+CD8+ Treg induction. Laminin a5-Itga6 enhanced TCR signaling by promoting activation of the LAT/Zap70/PLC?1 pathways. Overall design: sorted Foxp3-eGFP CD8+, Foxp3-eGFP CD4+ cells induced with or without laminin a5 in vitro at day 3.
创建时间:
2025-12-01



