Centre d'Immunologie de Marseille-Luminy, INSERM U1104, CNRS UMR7280, Aix-Marseille Université UM2, Marseille, 13288 cedex 09, France.
Institute of Molecular Medicine, Department of Neurobiology Research, University of Southern Denmark, J.B. Winsløwsvej 25, 5000, Odense C, Denmark.
Nat Commun. 2018 Mar 28;9(1):1262. doi: 10.1038/s41467-018-03619-9.
Medullary thymic epithelial cells (mTEC) purge the T cell repertoire of autoreactive thymocytes. Although dendritic cells (DC) reinforce this process by transporting innocuous peripheral self-antigens, the mechanisms that control their thymic entry remain unclear. Here we show that mTEC-CD4 thymocyte crosstalk regulates the thymus homing of SHPS-1 conventional DCs (cDC), plasmacytoid DCs (pDC) and macrophages. This homing process is controlled by lymphotoxin α (LTα), which negatively regulates CCL2, CCL8 and CCL12 chemokines in mTECs. Consequently, Ltα-deficient mice have increased expression of these chemokines that correlates with augmented classical NF-κB subunits and increased thymic recruitment of cDCs, pDCs and macrophages. This enhanced migration depends mainly on the chemokine receptor CCR2, and increases thymic clonal deletion. Altogether, this study identifies a fine-tuning mechanism of T cell repertoire selection and paves the way for therapeutic interventions to treat autoimmune disorders.
髓质胸腺上皮细胞(mTEC)清除自身反应性胸腺细胞中的 T 细胞库。尽管树突状细胞(DC)通过转运无害的外周自身抗原来增强这一过程,但控制其进入胸腺的机制仍不清楚。在这里,我们表明 mTEC-CD4 胸腺细胞相互作用调节 SHPS-1 常规 DC(cDC)、浆细胞样 DC(pDC)和巨噬细胞的胸腺归巢。这个归巢过程受淋巴毒素 α(LTα)控制,LTα 在 mTEC 中负调控趋化因子 CCL2、CCL8 和 CCL12。因此,Ltα 缺陷小鼠这些趋化因子的表达增加,与经典 NF-κB 亚基增加和 cDC、pDC 和巨噬细胞在胸腺中的募集增加相关。这种增强的迁移主要依赖于趋化因子受体 CCR2,并增加胸腺克隆性删除。总的来说,这项研究确定了 T 细胞库选择的精细调节机制,并为治疗自身免疫疾病的治疗干预铺平了道路。
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