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小鼠胎肝中造血干细胞向T、B和髓系谱系定向分化的直接证据。

Direct evidence for the commitment of hematopoietic stem cells to T, B and myeloid lineages in murine fetal liver.

作者信息

Kawamoto H, Ohmura K, Katsura Y

机构信息

Department of Immunology, Chest Disease Research Institute, Kyoto University, Japan.

出版信息

Int Immunol. 1997 Jul;9(7):1011-9. doi: 10.1093/intimm/9.7.1011.

Abstract

We established an experimental system in vitro to examine the developmental capacity of individual hematopoietic progenitors to generate T, B and myeloid (M) cells. By using this system we analyzed the process of lineage commitment of hematopoietic progenitors in murine fetal liver (FL). It is known that small numbers of B and M cells, in addition to T cells, are generated in a co-culture of hematopoietic progenitors and a deoxyguanosine-treated fetal thymus (FT) lobe. We tried to enhance the growth of B and M cells by the addition of IL-7, IL-3 and stem cell factor into the co-culture. This cytokine-supplemented FT organ culture was used to examine the developmental capacity of individual hematopoietic progenitors in FL. Single cells of lineage marker (Lin)-c-kit+Sca-1+ (Sca-1+) and Lin-c-kit+Sca-1-(Sca-1-) populations from the FL harvested at day 12 of gestation were cultured for 10 days, and the phenotypes of cells generated in each lobe were analyzed with a flow cytometer. All progenitors in the Sca-1- population were shown to be committed to generate only T, B or M cells. On the other hand, multipotent progenitors, which are capable of generating T, B and M cells, as well as unipotent progenitors committed to the T, B or M lineage were found in the Sca-1+ population. Bipotent progenitors generating M and T cells and those generating M and B cells were also found in the Sca-1+ population, which probably represent progenitors in the process of commitment. However, no bipotent progenitors generating T and B cells were detected.

摘要

我们建立了一个体外实验系统,以检测单个造血祖细胞产生T细胞、B细胞和髓系(M)细胞的发育能力。通过使用该系统,我们分析了小鼠胎肝(FL)中造血祖细胞的谱系定向过程。已知在造血祖细胞与经脱氧鸟苷处理的胎胸腺(FT)叶的共培养中,除了T细胞外,还会产生少量的B细胞和M细胞。我们试图通过在共培养中添加白细胞介素-7(IL-7)、白细胞介素-3(IL-3)和干细胞因子来促进B细胞和M细胞的生长。这种添加了细胞因子的FT器官培养用于检测FL中单个造血祖细胞的发育能力。对妊娠第12天收获的FL中谱系标记物(Lin)-c-kit+Sca-1+(Sca-1+)和Lin-c-kit+Sca-1-(Sca-1-)群体的单细胞进行10天培养,并用流式细胞仪分析每个叶中产生的细胞表型。结果显示,Sca-1-群体中的所有祖细胞仅定向产生T细胞、B细胞或M细胞。另一方面,在Sca-1+群体中发现了能够产生T细胞、B细胞和M细胞的多能祖细胞,以及定向于T、B或M谱系的单能祖细胞。在Sca-1+群体中还发现了产生M细胞和T细胞以及产生M细胞和B细胞的双能祖细胞,它们可能代表处于定向过程中的祖细胞。然而,未检测到产生T细胞和B细胞的双能祖细胞。

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