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首页> 外文期刊>Nature immunology >The development of innate lymphoid cells requires TOX-dependent generation of a common innate lymphoid cell progenitor
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The development of innate lymphoid cells requires TOX-dependent generation of a common innate lymphoid cell progenitor

机译:先天淋巴细胞的发育需要普通先天淋巴细胞祖细胞的TOX依赖产生

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摘要

Diverse innate lymphoid cell (ILC) subtypes have been defined on the basis of effector function and transcription factor expression. ILCs derive from common lymphoid progenitors, although the transcriptional pathways that lead to ILC-lineage specification remain poorly characterized. Here we found that the transcriptional regulator TOX was required for the in vivo differentiation of common lymphoid progenitors into ILC lineage-restricted cells. In vitro modeling demonstrated that TOX deficiency resulted in early defects in the survival or proliferation of progenitor cells, as well as ILC differentiation at a later stage. In addition, comparative transcriptome analysis of bone marrow progenitors revealed that TOX-deficient cells failed to upregulate many genes of the ILC program, including genes that are targets of Notch, which indicated that TOX is a key determinant of early specification to the ILC lineage.
机译:基于效应子功能和转录因子表达,已经定义了多种先天性淋巴样细胞(ILC)亚型。尽管导致ILC谱系规范的转录途径仍然很差,但ILC来源于常见的淋巴样祖细胞。在这里,我们发现转录调节剂TOX是将普通淋巴祖细胞体内分化为ILC谱系限制细胞所必需的。体外建模表明,TOX缺乏会导致祖细胞存活或增殖的早期缺陷,以及后期的ILC分化。此外,对骨髓祖细胞的转录组分析表明,TOX缺陷细胞未能上调ILC程序的许多基因,包括Notch的靶基因,这表明TOX是ILC谱系早期规格的关键决定因素。

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