| Literature DB >> 35761081 |
Changlu Xu1,2, Jian He3,4, Hongtao Wang1,2, Yingnan Zhang1,2, Jing Wu1,2, Lu Zhao5, Yue Li1,2, Jie Gao1,2, Guangfeng Geng1,2, Bingrui Wang1,2, Xiaoyuan Chen1,2, Zhaofeng Zheng1,2, Biao Shen1,2, Yang Zeng6, Zhijie Bai3, Hua Yang5, Shujuan Shi5, Fang Dong1,2, Shihui Ma1,2, Erlie Jiang1,2, Tao Cheng1,2, Yu Lan7, Jiaxi Zhou8,9, Bing Liu10,11,12,13, Lihong Shi14,15.
Abstract
Nonimmune cells can have immunomodulatory roles that contribute to healthy development. However, the molecular and cellular mechanisms underlying the immunomodulatory functions of erythroid cells during human ontogenesis remain elusive. Here, integrated, single-cell transcriptomic studies of erythroid cells from the human yolk sac, fetal liver, preterm umbilical cord blood (UCB), term UCB and adult bone marrow (BM) identified classical and immune subsets of erythroid precursors with divergent differentiation trajectories. Immune-erythroid cells were present from the yolk sac to the adult BM throughout human ontogenesis but failed to be generated in vitro from human embryonic stem cells. Compared with classical-erythroid precursors, these immune-erythroid cells possessed dual erythroid and immune regulatory networks, showed immunomodulatory functions and interacted more frequently with various innate and adaptive immune cells. Our findings provide important insights into the nature of immune-erythroid cells and their roles during development and diseases.Entities:
Mesh:
Year: 2022 PMID: 35761081 DOI: 10.1038/s41590-022-01245-8
Source DB: PubMed Journal: Nat Immunol ISSN: 1529-2908 Impact factor: 31.250