生物
免疫系统
造血
免疫学
胎儿
T细胞
免疫耐受
免疫
细胞
干细胞
细胞生物学
骨髓
获得性免疫系统
造血干细胞
受体
电池类型
免疫受体
先天免疫系统
核糖核酸
信号转导
单细胞分析
作者
Shuai He,Chun-Ling Luo,Tao Luo,Hai-Tian Chen,Shaofeng Zhang,Jia-Xin Jiang,Xiaoyi Wang,Dong Ma,Shunying Zhao,An‐Yi Xu,Jingjing He,Zhao-Hui Ruan,Wenxin Yan,Zihao Xu,Yang Liu,Qitao Huang,Yujie Gan,Tielong Wang,Yunhua Tang,Xiaorui Liu
出处
期刊:Cell
[Cell Press]
日期:2025-10-28
卷期号:188 (25): 7291-7308.e23
被引量:5
标识
DOI:10.1016/j.cell.2025.10.003
摘要
The second trimester of pregnancy is a pivotal stage in human immune system development. Utilizing single-cell RNA sequencing and T cell receptor sequencing, we profiled 2,868,420 immune cells from 321 samples across 23 organs, including adult tissues as comparators. We identify an extrathymic CD4+ T cell subset mediating TOX2+ precursor cells' transition to mature naive CD4+ T cells. Contrary to the prevailing paradigm of fetal immune quiescence, we uncover widespread memory/activated T cells and tissue-resident memory clones shared across organs, indicating systemic immune activity beyond localized barrier defense. Cell-cell communication and functional assays indicate two tolerance mechanisms that suppress fetal T cell activation: ARG1+ neutrophils and a PTGES3/PTGER4 signaling pathway. We also find that hematopoietic stem cells (HSCs) disperse across multiple organs and show that HSCs from non-canonical hematopoietic organs differentiate into diverse immune lineages. These findings provide insights into human immune system maturation and tolerance in fetuses and adults.
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