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首页> 外文期刊>The Journal of Immunology: Official Journal of the American Association of Immunologists >EBF1 is essential for B-lineage priming and establishment of a transcription factor network in common lymphoid progenitors.
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EBF1 is essential for B-lineage priming and establishment of a transcription factor network in common lymphoid progenitors.

机译:EBF1对于B谱系启动和在常见淋巴祖细胞中建立转录因子网络至关重要。

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摘要

Development of B-lymphoid cells in the bone marrow is a process under strict control of a hierarchy of transcription factors. To understand the development of a B-lymphoid-restricted functional network of transcription factors, we have investigated the cell autonomous role of the transcription factor EBF1 in early B cell development. This revealed that even though transplanted EBF1-deficient fetal liver cells were able to generate common lymphoid progenitors (CLPs) as well as B220(+)CD43(+)AA4.1(+) candidate precursor B cells, none of these populations showed signs of B lineage priming. The isolated CLPs were able to generate T lymphocytes in vitro supporting the idea that the phenotype of EBF1-deficient mice is restricted to the development of the B lineage. Furthermore, EBF deficient CLPs displayed a reduction in Ig H chain recombination as compared with their wild-type counterpart and essentially lacked transcription of B-lineage-associated genes. Among the genes displaying reduced expression in theEBF1 deficient CLPs were the transcription factors Pax5, Pou2af1 (OcaB), and FoxO1 that all appear to be direct genetic targets for EBF1 because their promoters contained functional binding sites for this factor. This leads us to suggest that EBF1 regulates a transcription factor network crucial for B lineage commitment.
机译:骨髓中B淋巴样细胞的发育是在转录因子层次严格控制下的过程。为了了解转录因子的B淋巴限制功能网络的发展,我们研究了转录因子EBF1在早期B细胞发育中的细胞自主作用。这表明即使已移植的缺乏EBF1的胎儿肝细胞能够产生常见的淋巴祖细胞(CLP)以及B220(+)CD43(+)AA4.1(+)候选前体B细胞,但这些人群均未显示出任何迹象B血统启动。分离的CLPs能够在体外产生T淋巴细胞,这支持了EBF1缺陷型小鼠的表型仅限于B谱系发育的想法。此外,与它们的野生型对应物相比,缺乏EBF的CLP表现出Ig H链重组减少,并且基本上缺乏与B谱系相关的基因的转录。在EBF1缺陷型CLP中表达降低的基因中有转录因子Pax5,Pou2af1(OcaB)和FoxO1,它们似乎都是EBF1的直接遗传靶标,因为它们的启动子均含有该因子的功能性结合位点。这使我们建议EBF1调节一个转录因子网络,对B谱系承诺至关重要。

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