| Literature DB >> 31604687 |
Yang Zeng1, Chen Liu2, Yandong Gong2, Zhijie Bai2, Siyuan Hou2, Jian He2, Zhilei Bian3, Zongcheng Li1, Yanli Ni1, Jing Yan2, Tao Huang2, Hui Shi2, Chunyu Ma4, Xueying Chen5, Jinyong Wang6, Lihong Bian4, Yu Lan7, Bing Liu8, Hongbo Hu9.
Abstract
Generation of the first T lymphocytes in the human embryo involves the emergence, migration, and thymus seeding of lymphoid progenitors together with concomitant thymus organogenesis, which is the initial step to establish the entire adaptive immune system. However, the cellular and molecular programs regulating this process remain unclear. We constructed a single-cell transcriptional landscape of human early T lymphopoiesis by using cells from multiple hemogenic and hematopoietic sites spanning embryonic and fetal stages. Among heterogenous early thymic progenitors, one subtype shared common features with a subset of lymphoid progenitors in fetal liver that are known as thymus-seeding progenitors. Unbiased bioinformatics analysis identified a distinct type of pre-thymic lymphoid progenitors in the aorta-gonad-mesonephros (AGM) region. In parallel, we investigated thymic epithelial cell development and potential cell-cell interactions during thymus organogenesis. Together, our data provide insights into human early T lymphopoiesis that prospectively direct T lymphocyte regeneration, which might lead to development of clinical applications.Entities:
Keywords: T lymphopoiesis; aorta-gonad-mesonephros; early thymic progenitors; fetal liver; human; lymphoid progenitors; single-cell RNA sequencing; thymic epithelial cells; thymus-seeding progenitors
Year: 2019 PMID: 31604687 DOI: 10.1016/j.immuni.2019.09.008
Source DB: PubMed Journal: Immunity ISSN: 1074-7613 Impact factor: 31.745