| Literature DB >> 28003475 |
Jennifer Yang1, Yoshiaki Tanaka2, Montrell Seay1, Zhen Li3, Jiaqi Jin1, Lana Xia Garmire4, Xun Zhu4, Ashley Taylor5, Weidong Li1,6, Ghia Euskirchen7, Stephanie Halene5, Yuval Kluger8, Michael P Snyder7, In-Hyun Park2, Xinghua Pan1,9, Sherman Morton Weissman1.
Abstract
Molecular changes underlying stem cell differentiation are of fundamental interest. scRNA-seq on murine hematopoietic stem cells (HSC) and their progeny MPP1 separated the cells into 3 main clusters with distinct features: active, quiescent, and an un-characterized cluster. Induction of anemia resulted in mobilization of the quiescent to the active cluster and of the early to later stage of cell cycle, with marked increase in expression of certain transcription factors (TFs) while maintaining expression of interferon response genes. Cells with surface markers of long term HSC increased the expression of a group of TFs expressed highly in normal cycling MPP1 cells. However, at least Id1 and Hes1 were significantly activated in both HSC and MPP1 cells in anemic mice. Lineage-specific genes were differently expressed between cells, and correlated with the cell cycle stages with a specific augmentation of erythroid related genes in the G2/M phase. Most lineage specific TFs were stochastically expressed in the early precursor cells, but a few, such as Klf1, were detected only at very low levels in few precursor cells. The activation of these factors may correlate with stages of differentiation. This study reveals effects of cell cycle progression on the expression of lineage specific genes in precursor cells, and suggests that hematopoietic stress changes the balance of renewal and differentiation in these homeostatic cells.Entities:
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Year: 2017 PMID: 28003475 PMCID: PMC5388401 DOI: 10.1093/nar/gkw1214
Source DB: PubMed Journal: Nucleic Acids Res ISSN: 0305-1048 Impact factor: 16.971