Differentiation tracing identifies hematopoietic regeneration from multipotent progenitors but not stem cells

干细胞 生物 造血 祖细胞 细胞生物学 多能干细胞 细胞分化 免疫学 再生(生物学) 造血干细胞 成体干细胞 遗传学 基因
作者
Tamar Nizharadze,Katrin Busch,Ann-Kathrin Fanti,Hans-Reimer Rodewald,Thomas Höfer
出处
期刊:Cells and development [Elsevier BV]
卷期号:: 203861-203861
标识
DOI:10.1016/j.cdev.2023.203861
摘要

Hematopoietic stem cells (HSCs) and multipotent progenitors (MPPs) generate the immune system in development, and contribute to its maintenance under steady state conditions. How stem and progenitor cells respond to increased demand for mature cells upon injury is a fundamental question of stem cell biology. Several studies of murine hematopoiesis have reported increased proliferation of HSCs in situ when exposed to inflammatory stimuli, which has been taken as a proxy for increased HSC differentiation. Such surplus generation of HSC may fuel enhanced HSC differentiation or, alternatively, maintain HSC cellularity in the face of increased cell death without enhanced HSC differentiation. This key question calls for direct measurements of HSC differentiation in their natural niches in vivo. Here, we review work that quantifies native HSC differentiation by fate mapping and mathematical inference. Recent differentiation tracing studies show that HSC do not increase their differentiation rate upon a wide range of challenges, including systemic bacterial infection (sepsis), blood loss, and transient or persistent ablation of specific mature immune cells. By contrast, MPPs differentiate more rapidly in response to systemic infection to accelerate the production of myeloid cells. These new in vivo data identify MPPs as a major source of hematopoietic regeneration while HSCs might not contribute to regeneration while remaining protected.
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