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信号淋巴细胞激活分子家族标志物在老年小鼠和重建小鼠的造血干细胞中保守,并显著提高其纯度。

SLAM family markers are conserved among hematopoietic stem cells from old and reconstituted mice and markedly increase their purity.

作者信息

Yilmaz Omer H, Kiel Mark J, Morrison Sean J

机构信息

Howard Hughes Medical Institute, Department of Internal Medicine, Ann Arbor, MI, USA.

出版信息

Blood. 2006 Feb 1;107(3):924-30. doi: 10.1182/blood-2005-05-2140. Epub 2005 Oct 11.

Abstract

Recent advances have increased the purity of hematopoietic stem cells (HSCs) isolated from young mouse bone marrow. However, little attention has been paid to the purity of HSCs from other contexts. Although Thy-1 low Sca-1+ Lineage- c-kit+ cells from young bone marrow are highly enriched for HSCs (1 in 5 cells gives long-term multilineage reconstitution after transplantation into irradiated mice), the same population from old, reconstituted, or cytokine-mobilized mice engrafts much less efficiently (1 in 78 to 1 in 185 cells gives long-term multilineage reconstitution). To test whether we could increase the purity of HSCs isolated from these contexts, we examined the SLAM family markers CD150 and CD48. All detectable HSCs from old, reconstituted, and cyclophosphamide/G-CSF-mobilized mice were CD150+ CD48-, just as in normal young bone marrow. Thy-1 low Sca-1+ Lineage- c-kit+ cells from old, reconstituted, or mobilized mice included mainly CD48+ and/or CD150- cells that lacked reconstituting ability. CD150+ CD48- Sca-1+ Lineage- c-kit+ cells from old, reconstituted, or mobilized mice were much more highly enriched for HSCs, with 1 in 3 to 1 in 7 cells giving long-term multilineage reconstitution. SLAM family receptor expression is conserved among HSCs from diverse contexts, and HSCs from old, reconstituted, and mobilized mice engraft relatively efficiently after transplantation when contaminating cells are eliminated.

摘要

近期的进展提高了从小鼠幼龄骨髓中分离出的造血干细胞(HSC)的纯度。然而,来自其他情况的HSC纯度却很少受到关注。尽管幼龄骨髓中Thy-1低表达Sca-1+谱系阴性c-kit+细胞高度富集了HSC(移植到受辐照小鼠体内后,每5个细胞中有1个能实现长期多谱系重建),但来自老龄、已重建或经细胞因子动员的小鼠的相同细胞群体的植入效率要低得多(每78至185个细胞中有1个能实现长期多谱系重建)。为了测试我们是否能提高从这些情况中分离出的HSC的纯度,我们检测了SLAM家族标志物CD150和CD48。来自老龄、已重建和经环磷酰胺/粒细胞集落刺激因子动员的小鼠的所有可检测到的HSC都是CD150+ CD48-阴性,就像在正常幼龄骨髓中一样。来自老龄、已重建或经动员的小鼠的Thy-1低表达Sca-1+谱系阴性c-kit+细胞主要包括缺乏重建能力的CD48+和/或CD150-细胞。来自老龄、已重建或经动员的小鼠的CD150+ CD48- Sca-1+谱系阴性c-kit+细胞对HSC的富集程度要高得多,每3至7个细胞中有1个能实现长期多谱系重建。SLAM家族受体表达在来自不同情况的HSC中是保守的,并且当污染细胞被清除后,来自老龄、已重建和经动员的小鼠的HSC在移植后相对有效地植入。

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