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Role of interleukin 2 on SATB1 binding in SP CD4+ thymocytes

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NIAID Data Ecosystem2026-03-11 收录
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https://www.ncbi.nlm.nih.gov/geo/query/acc.cgi?acc=GSE116736
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Interleukine 2 (IL-2) is still one of the most interesting cytokines in T cell biology with its ability to control immune homeostasis by maintaining the functional identity of Foxp3+ regulatory T (Treg) cells and the expansion of activated conventional T (Tconv) cells. Yet, how IL-2 exactly enables Treg cells to suppress autoreactive Tconv cells and to maintain their identity is unclear. Using a mouse model in which IL-2 signaling via its high affinity receptor CD25 is selectively impaired, the “Il2ramut/mut” mouse, we report that Treg cells that only receive low IL-2 signals keep Il2ramut/mut but not WT Tconv cells “in check”, suggesting equal IL-2 signals in Treg and Tconv cells is essential to safeguard immune homeostasis. Furthermore, the comparative analysis of gene expression and epigenetic landscape of Il2ramut/mut and WT Treg cells support a model in which IL-2 "locks in” Treg cell identity and functions in vivo by controlling their genome-wide chromatin accessibility. Thymus from 6-8 weeks old aged-matched females either Il2ramut/mut (2 mice) or WT (2 mice) mice were harvested and 2x10e6 single positive (SP) CD4+ thymocytes were pre-enriched by negative selection (dynabeads), stained with fluorescent labeled antibodies against CD4 (GK1.5) and CD8α (53-6.7) and flow-sorted (Aria III) before proceeding to fixation (cross-linking), lysis, immunoprecipation against SATB1 and library preparation for sequencing.
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2019-03-21
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