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小鼠CD38的表达定义了一群长期重建造血干细胞。

Expression of murine CD38 defines a population of long-term reconstituting hematopoietic stem cells.

作者信息

Randall T D, Lund F E, Howard M C, Weissman I L

机构信息

Department of Pathology, Stanford Medical School, CA 94305, USA.

出版信息

Blood. 1996 May 15;87(10):4057-67.

PMID:8639761
Abstract

Using a monoclonal antibody to murine CD38, we showed that a population of adult bone marrow cells that expressed the markers Sca-1 and c-kit but lacked the lineage markers Mac-1, GR-1, B220, IgM, CD3, CD4, CD8 and CD5 could be subdivided by the expression of CD38. We showed that CD38high c-kit+ Sca-1+, linlow/-cells sorted from adult bone marrow cultured with interleukin-3 (IL-3), IL-6, and kit-L produced much larger colonies in liquid culture at a greater frequency than their CD38low/- counterparts. In addition, we found that CD36low/ - cells contained most of the day-12 colony-forming units-spleen (CFU-S) but were not long-term reconstituting cells, whereas the population that expressed higher levels of CD38 contained few, but significant, day-12 CFU-S and virtually all the long-term reconstituting stem cells. Interestingly, the CD38high Sca-1+ c-kit+ linlow/- cells isolated from day-E14.5 fetal liver were also found to be long-term reconstituting stem cells. This is in striking contrast to human hematopoietic progenitors in which the most primitive hematopoietic cells from fetal tissues lack the expression of CD38. Furthermore, because antibodies to CD38 could functionally replace antibodies to Thy-1.1 in a stem cell purification procedure, the use of anti-CD38 may be more generally applicable to the purification of hematopoietic stem cells from mouse strains that do not express the Thy-1.1 allele.

摘要

利用针对小鼠CD38的单克隆抗体,我们发现一群表达Sca-1和c-kit标志物但缺乏谱系标志物Mac-1、GR-1、B220、IgM、CD3、CD4、CD8和CD5的成年骨髓细胞可根据CD38的表达进行细分。我们发现,从用白细胞介素-3(IL-3)、IL-6和干细胞因子(kit-L)培养的成年骨髓中分选出来的CD38高表达、c-kit+、Sca-1+、lin低表达/阴性细胞,在液体培养中比其CD38低表达/阴性对应细胞产生更大菌落的频率更高。此外,我们发现CD36低表达/阴性细胞包含了大部分第12天的脾集落形成单位(CFU-S),但不是长期重建细胞,而表达较高水平CD38的细胞群中第12天的CFU-S数量很少但很显著,并且几乎包含了所有的长期重建干细胞。有趣的是,从胚胎第14.5天(E14.5)胎儿肝脏中分离出的CD38高表达、Sca-1+、c-kit+、lin低表达/阴性细胞也被发现是长期重建干细胞。这与人类造血祖细胞形成鲜明对比,在人类中,来自胎儿组织的最原始造血细胞缺乏CD38的表达。此外,由于在干细胞纯化过程中,针对CD38的抗体在功能上可以替代针对Thy-1.1的抗体,抗CD38抗体可能更普遍适用于从不表达Thy-1.1等位基因的小鼠品系中纯化造血干细胞。

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