Single-cell multiomics defines tolerogenic extrathymic Aire-expressing populations with unique homology to thymic epithelium

上皮 生物 造血 免疫学 同源(生物学) 命运图 细胞生物学 髓腔 淋巴细胞生成 干细胞 遗传学 基因 解剖 祖细胞
作者
Jiaxi Wang,Caleb A. Lareau,Jhoanne L. Bautista,Alexander R. Gupta,Katalin Sándor,Joe Germino,Yajie Yin,Matthew P. Arvedson,Gabriella C. Reeder,Nathan T. Cramer,Fang Xie,Vasilis Ntranos,Ansuman T. Satpathy,Mark S. Anderson,James M. Gardner
出处
期刊:Science immunology [American Association for the Advancement of Science (AAAS)]
卷期号:6 (65) 被引量:56
标识
DOI:10.1126/sciimmunol.abl5053
摘要

The autoimmune regulator (Aire), a well-defined transcriptional regulator in the thymus, is also found in extrathymic Aire-expressing cells (eTACs) in the secondary lymphoid organs. eTACs are hematopoietic antigen-presenting cells and inducers of immune tolerance, but their precise identity has remained unclear. Here, we use single-cell multiomics, transgenic murine models, and functional approaches to define eTACs at the transcriptional, genomic, and proteomic level. We find that eTACs consist of two similar cell types: CCR7+ Aire-expressing migratory dendritic cells (AmDCs) and an Airehi population coexpressing Aire and retinoic acid receptor–related orphan receptor γt (RORγt) that we term Janus cells (JCs). Both JCs and AmDCs have the highest transcriptional and genomic homology to CCR7+ migratory dendritic cells. eTACs, particularly JCs, have highly accessible chromatin and broad gene expression, including a range of tissue-specific antigens, as well as remarkable homology to medullary thymic epithelium and RANK-dependent Aire expression. Transgenic self-antigen expression by eTACs is sufficient to induce negative selection and prevent autoimmune diabetes. This transcriptional, genomic, and functional symmetry between eTACs (both JCs and AmDCs) and medullary thymic epithelium—the other principal Aire-expressing population and a key regulator of central tolerance—identifies a core program that may influence self-representation and tolerance across the spectrum of immune development.
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