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慢循环和持久的 Flt3+祖细胞有助于在天然条件下的造血。

Slow cycling and durable Flt3+ progenitors contribute to hematopoiesis under native conditions.

机构信息

Division of Experimental Hematology and Cancer Biology, Stem Cell Program, Cincinnati Children's Hospital Medical Center, Cincinnati, OH, USA.

Division of Immunobiology, Cincinnati Children's Hospital Medical Center, Cincinnati, OH, USA.

出版信息

J Exp Med. 2024 Jan 1;221(1). doi: 10.1084/jem.20231035. Epub 2023 Nov 1.

Abstract

The dynamics of the hematopoietic flux responsible for blood cell production in native conditions remains a matter of debate. Using CITE-seq analyses, we uncovered a distinct progenitor population that displays a cell cycle gene signature similar to the one found in quiescent hematopoietic stem cells. We further determined that the CD62L marker can be used to phenotypically enrich this population in the Flt3+ multipotent progenitor (MPP4) compartment. Functional in vitro and in vivo analyses validated the heterogeneity of the MPP4 compartment and established the quiescent/slow-cycling properties of the CD62L- MPP4 cells. Furthermore, studies under native conditions revealed a novel hierarchical organization of the MPP compartments in which quiescent/slow-cycling MPP4 cells sustain a prolonged hematopoietic activity at steady-state while giving rise to other lineage-biased MPP populations. Altogether, our data characterize a durable and productive quiescent/slow-cycling hematopoietic intermediary within the MPP4 compartment and highlight early paths of progenitor differentiation during unperturbed hematopoiesis.

摘要

在原生条件下,负责血细胞生成的造血通量的动态变化仍然存在争议。使用 CITE-seq 分析,我们发现了一个独特的祖细胞群体,其细胞周期基因特征与静止造血干细胞中发现的特征相似。我们进一步确定,CD62L 标记可用于表型富集 Flt3+多能祖细胞(MPP4)区室中的该群体。体外和体内功能分析验证了 MPP4 区室的异质性,并确定了 CD62L-MPP4 细胞的静止/缓慢循环特性。此外,在原生条件下的研究揭示了 MPP 区室的新的层次组织,其中静止/缓慢循环的 MPP4 细胞在稳定状态下维持长期的造血活性,同时产生其他谱系偏向的 MPP 群体。总之,我们的数据描述了 MPP4 区室中具有耐用性和生产性的静止/缓慢循环造血中间产物,并强调了在未受干扰的造血过程中祖细胞分化的早期途径。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/7222/10620607/15b646a827f6/JEM_20231035_GA.jpg

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