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Asymmetrical lymphoid and myeloid lineage commitment in multipotent hematopoietic progenitors

机译:多能造血祖细胞中的不对称淋巴和髓系谱系承诺

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摘要

The mechanism of lineage commitment from hematopoietic stem cells (HSCs) is not well understood. Although commitment to either the lymphoid or the myeloid lineage is popularly viewed as the first step of lineage restriction from HSCs, this model of hematopoietic differentiation has recently been challenged. The previous identification of multipotent progenitors (MPPs) that can produce lymphocytes and granulocyte/macrophages (GMs) but lacks erythroid differentiation ability suggests the existence of an alternative HSC differentiation program. Contribution to different hematopoietic lineages by these MPPs under physiological conditions, however, has not been carefully examined. In this study, we performed a refined characterization of MPPs by subfractionating three distinct subsets based on Flt3 and vascular cell adhesion molecule 1 expression. These MPP subsets differ in their ability to give rise to erythroid and GM lineage cells but are equally potent in lymphoid lineage differentiation in vivo. The developmental hierarchy of these MPP subsets demonstrates the sequential loss of erythroid and then GM differentiation potential during early hematopoiesis. Our results suggest that the first step of lineage commitment from HSCs is not simply a selection between the lymphoid and the myeloid lineage.
机译:对造血干细胞(HSC)沿袭承诺的机制尚不十分了解。尽管普遍认为对淋巴样或髓样谱系的承诺是HSC谱系限制的第一步,但这种造血分化模型最近受到了挑战。先前鉴定的能产生淋巴细胞和粒细胞/巨噬细胞(GM)但缺乏红系分化能力的多能祖细胞(MPP)表明存在替代的HSC分化程序。但是,尚未仔细检查这些MPP在生理条件下对不同造血谱系的贡献。在这项研究中,我们通过细分基于Flt3和血管细胞粘附分子1表达的三个不同子集,对MPP进行了精确表征。这些MPP子集产生红系和GM谱系细胞的能力不同,但在体内淋巴谱系分化方面同样有效。这些MPP子集的发育层次表明,在早期造血过程中,红系依次丢失,然后出现GM分化潜能。我们的结果表明,HSC沿袭承诺的第一步不仅仅是在淋巴和髓系之间进行选择。

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