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骨内膜龛细胞群体的分离和鉴定及其对造血干细胞的调控作用。

Isolation and characterization of endosteal niche cell populations that regulate hematopoietic stem cells.

机构信息

Department of Cell Differentiation, Keio University, Tokyo, Japan.

出版信息

Blood. 2010 Sep 2;116(9):1422-32. doi: 10.1182/blood-2009-08-239194. Epub 2010 May 14.

DOI:10.1182/blood-2009-08-239194
PMID:20472830
Abstract

The endosteal niche is critical for the maintenance of hematopoietic stem cells (HSCs). However, it consists of a heterogeneous population in terms of differentiation stage and function. In this study, we characterized endosteal cell populations and examined their ability to maintain HSCs. Bone marrow endosteal cells were subdivided into immature mesenchymal cell-enriched ALCAM(-)Sca-1(+) cells, osteoblast-enriched ALCAM(+)Sca-1(-), and ALCAM(-)Sca-1(-) cells. We found that all 3 fractions maintained long-term reconstitution (LTR) activity of HSCs in an in vitro culture. In particular, ALCAM(+)Sca-1(-) cells significantly enhanced the LTR activity of HSCs by the up-regulation of homing- and cell adhesion-related genes in HSCs. Microarray analysis showed that ALCAM(-)Sca-1(+) fraction highly expressed cytokine-related genes, whereas the ALCAM(+)Sca-1(-) fraction expressed multiple cell adhesion molecules, such as cadherins, at a greater level than the other fractions, indicating that the interaction between HSCs and osteoblasts via cell adhesion molecules enhanced the LTR activity of HSCs. Furthermore, we found an osteoblastic marker(low/-) subpopulation in ALCAM(+)Sca-1(-) fraction that expressed cytokines, such as Angpt1 and Thpo, and stem cell marker genes. Altogether, these data suggest that multiple subsets of osteoblasts and mesenchymal progenitor cells constitute the endosteal niche and regulate HSCs in adult bone marrow.

摘要

骨内膜龛对于维持造血干细胞(HSCs)至关重要。然而,它在分化阶段和功能上由异质群体组成。在这项研究中,我们对骨内膜细胞群体进行了特征描述,并研究了它们维持 HSCs 的能力。骨髓骨内膜细胞被细分为不成熟的间充质细胞富集的 ALCAM(-)Sca-1(+)细胞、成骨细胞富集的 ALCAM(+)Sca-1(-)细胞和 ALCAM(-)Sca-1(-)细胞。我们发现所有 3 个部分在体外培养中均能维持 HSCs 的长期重建(LTR)活性。特别是,ALCAM(+)Sca-1(-)细胞通过上调 HSCs 中的归巢和细胞黏附相关基因,显著增强了 HSCs 的 LTR 活性。微阵列分析表明,ALCAM(-)Sca-1(+)细胞群高度表达细胞因子相关基因,而 ALCAM(+)Sca-1(-)细胞群则以比其他细胞群更高的水平表达多种细胞黏附分子,如钙黏蛋白,表明 HSCs 和成骨细胞通过细胞黏附分子的相互作用增强了 HSCs 的 LTR 活性。此外,我们在 ALCAM(+)Sca-1(-)细胞群中发现了一个成骨细胞标记物(低/负)亚群,该亚群表达细胞因子,如 Angpt1 和 Thpo,以及干细胞标记基因。总之,这些数据表明,多个成骨细胞和间充质祖细胞亚群构成了骨内膜龛,并调节成年骨髓中的 HSCs。

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