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胎儿肝脏髓系造血通过不同的、可前瞻性分离的祖细胞亚群发生。

Fetal liver myelopoiesis occurs through distinct, prospectively isolatable progenitor subsets.

作者信息

Traver D, Miyamoto T, Christensen J, Iwasaki-Arai J, Akashi K, Weissman I L

机构信息

Department of Pathology, Stanford University School of Medicine, Stanford, CA 94305, USA.

出版信息

Blood. 2001 Aug 1;98(3):627-35. doi: 10.1182/blood.v98.3.627.

DOI:10.1182/blood.v98.3.627
PMID:11468160
Abstract

Hematopoietic fate maps in the developing mouse embryo remain imprecise. Definitive, adult-type hematopoiesis first appears in the fetal liver, then progresses to the spleen and bone marrow. Clonogenic common lymphoid progenitors and clonogenic common myeloid progenitors (CMPs) in adult mouse bone marrow that give rise to all lymphoid and myeloid lineages, respectively, have recently been identified. Here it is shown that myelopoiesis in the fetal liver similarly proceeds through a CMP equivalent. Fetal liver CMPs give rise to megakaryocyte-erythrocyte-restricted progenitors (MEPs) and granulocyte-monocyte-restricted progenitors (GMPs) that can also be prospectively isolated by cell surface phenotype. MEPs and GMPs generate mutually exclusive cell types in clonogenic colony assays and in transplantation experiments, suggesting that the lineage restriction observed within each progenitor subset is absolute under normal conditions. Purified progenitor populations were used to analyze expression profiles of various hematopoiesis-related genes. Expression patterns closely matched those of the adult counterpart populations. These results suggest that adult hematopoietic hierarchies are determined early in the development of the definitive immune system and suggest that the molecular mechanisms underlying cell fate decisions within the myeloerythroid lineages are conserved from embryo to adult. (Blood. 2001;98:627-635)

摘要

发育中的小鼠胚胎造血命运图谱仍不精确。明确的成体型造血首先出现在胎儿肝脏,然后发展至脾脏和骨髓。最近已鉴定出成年小鼠骨髓中分别产生所有淋巴系和髓系谱系的克隆性普通淋巴祖细胞和克隆性普通髓系祖细胞(CMP)。本文表明,胎儿肝脏中的髓系造血同样通过一种等效的CMP进行。胎儿肝脏CMP可产生巨核细胞 - 红细胞受限祖细胞(MEP)和粒细胞 - 单核细胞受限祖细胞(GMP),它们也可通过细胞表面表型进行前瞻性分离。在克隆集落测定和移植实验中,MEP和GMP产生相互排斥的细胞类型,这表明在正常条件下,每个祖细胞亚群内观察到的谱系限制是绝对的。纯化的祖细胞群体用于分析各种造血相关基因的表达谱。表达模式与成年对应群体的模式密切匹配。这些结果表明,成体造血层次结构在明确的免疫系统发育早期就已确定,并且表明髓红细胞谱系内细胞命运决定的分子机制从胚胎到成体是保守的。(《血液》。2001年;98:627 - 635)

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