| Literature DB >> 35882235 |
Gang Ren1, Binbin Lai2, Christelle Harly3, Songjoon Baek4, Yi Ding3, Mingzhu Zheng5, Yaqiang Cao6, Kairong Cui6, Yu Yang7, Jinfang Zhu8, Gordon L Hager4, Avinash Bhandoola3, Keji Zhao9.
Abstract
The differentiation of innate lymphoid cells (ILCs) from hematopoietic stem cells needs to go through several multipotent progenitor stages. However, it remains unclear whether the fates of multipotent progenitors are predefined by epigenetic states. Here, we report the identification of distinct accessible chromatin regions in all lymphoid progenitors (ALPs), EILPs, and ILC precursors (ILCPs). Single-cell MNase-seq analyses revealed that EILPs contained distinct subpopulations epigenetically primed toward either dendritic cell lineages or ILC lineages. We found that TCF-1 and GATA3 co-bound to the lineage-defining sites for ILCs (LDS-Is), whereas PU.1 binding was enriched in the LDSs for alternative dendritic cells (LDS-As). TCF-1 and GATA3 were indispensable for the epigenetic priming of LDSs at the EILP stage. Our results suggest that the multipotency of progenitor cells is defined by the existence of a heterogeneous population of cells epigenetically primed for distinct downstream lineages, which are regulated by key transcription factors. Published by Elsevier Inc.Entities:
Keywords: ChIC-seq; EILPs; GATA3; ILCPs; PU.1; TCF-1; epigenetic priming; multipotency; scMNase-seq; single-cell epigenomics
Mesh:
Year: 2022 PMID: 35882235 PMCID: PMC9393082 DOI: 10.1016/j.immuni.2022.06.019
Source DB: PubMed Journal: Immunity ISSN: 1074-7613 Impact factor: 43.474