IFN-I signaling in type 2 conventional dendritic cells supports TH2 and T follicular helper differentiation after allergen immunization

Greta R Webb, Kerry L Hilligan, Samuel I Old, Shiau-Choot Tang, Olivier Lamiable, F Ronchese
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Abstract

Type 2 dendritic cells (DC2s) are essential for TH2 differentiation, but the signaling pathways involved in allergen sensing, DC activation and instruction of CD4+ T cell priming remain unclear. Previous transcriptomic analyses demonstrated a type-I interferon (IFN-I) signature in skin cDC2s following immunization with non-viable larvae of Nippostrongylus brasiliensis (Nb), house dust mite (HDM), and Schistosoma egg antigen (SEA). Blocking IFN-I signaling with anti-IFNAR1 (aIFNAR1) led to reduced TH2 cytokine responses to these antigens, however, the phenotype of cytokine-producing CD4+ T cells was not further defined. Here we show that conditional loss of IFNAR1 signaling in CD11c+ DCs significantly impaired effector TH2 and TFH CD4+ T cell responses to Nb. In vivo proliferation experiments demonstrated reduced numbers of highly divided CD4+ T cells in IFNAR1deltaCD11c mice compared to IFNAR1WT, with the highly divided population comprising both TH2 and TFH. Characterization of the cDC2 compartment by flow cytometry and bulk RNAseq demonstrated lower numbers of Nb+ cDC2s in the skin-draining LN and a reduced expression of Il15 and Il15Ra in IFNAR1dletaCD11c mice compared to IFNAR1WT, while expression of costimulatory molecules including CD80, CD86, Cd40 and Pdcd1lg2 (PD-L2) was not impaired. Therefore, IFN-I conditioning of skin cDC2s is necessary for their effective priming of CD4+ T cell responses to allergens, providing evidence for a role of tissue cytokines in driving cDC2 activation in a TH2 context.
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过敏原免疫后,2 型常规树突状细胞中的 IFN-I 信号支持 TH2 和 T 滤泡辅助分化
2型树突状细胞(DC2s)对TH2分化至关重要,但过敏原感应、DC活化和CD4+ T细胞引导所涉及的信号通路仍不清楚。之前的转录组分析表明,用巴西镍梭菌(Nb)、屋尘螨(HDM)和血吸虫卵抗原(SEA)的非存活幼虫免疫皮肤cDC2后,皮肤cDC2会出现I型干扰素(IFN-I)特征。用抗 IFNAR1(aIFNAR1)阻断 IFN-I 信号导致对这些抗原的 TH2 细胞因子反应减弱,但产生细胞因子的 CD4+ T 细胞的表型尚未进一步确定。在这里,我们发现 CD11c+ DCs 中 IFNAR1 信号的有条件缺失会显著削弱效应 TH2 和 TFH CD4+ T 细胞对 Nb 的反应。体内增殖实验表明,与 IFNAR1WT 相比,IFNAR1deltaCD11c 小鼠体内高度分裂的 CD4+ T 细胞数量减少,高度分裂的细胞群包括 TH2 和 TFH。通过流式细胞术和大量 RNAseq 对 cDC2 区系进行表征后发现,与 IFNAR1WT 相比,IFNAR1dletaCD11c 小鼠皮肤引流 LN 中的 Nb+ cDC2 数量更少,Il15 和 Il15Ra 的表达也更低,而包括 CD80、CD86、Cd40 和 Pdcd1lg2 (PD-L2) 在内的共刺激分子的表达则没有受到影响。因此,IFN-I 对皮肤 cDC2 的调节是它们有效启动 CD4+ T 细胞对过敏原反应的必要条件,这为组织细胞因子在 TH2 环境中驱动 cDC2 激活的作用提供了证据。
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