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首页> 外文期刊>Nature >Haematopoietic stem cells retain long-term repopulating activity and multipotency in the absence of stem-cell leukaemia SGL/tal-1 gene
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Haematopoietic stem cells retain long-term repopulating activity and multipotency in the absence of stem-cell leukaemia SGL/tal-1 gene

机译:在没有干细胞白血病SGL / tal-1基因的情况下,造血干细胞保留了长期的繁殖活性和多能性

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摘要

The production of blood cells is sustained throughout the lifetime of an individual by haematopoietic stem cells (HSCs). Specification of HSCs from mesoderm during embryonic development requires the stem cell leukaemia SCL/tal-1 gene product. Forced expression of SCL/tal-1 strongly induces blood formation in embryos, indicating that this gene has a dominant role in commitment to haematopoiesis. In the adult haematopoietic system, expression of SCL/tal-1 is enriched in HSCs and multipotent progenitors, and in erythroid and megakaryocytic lineages, consistent with roles for this factor in adult haematopoiesis. Here we assess by conditional gene targeting whether SCL/tal-1 is required continuously for the identity and function of HSCs. We find that SCL/tal-1 is dispensable for HSC engraft-ment, self-renewal and differentiation into myeloid and lym-phoid lineages; however, the proper differentiation of erythroid and megakaryocytic precursors is dependent on SCL/tal-1. Thus, SCL/tal-1 is essential for the genesis of HSCs, but its continued expression is not essential for HSC functions. These findings contrast with lineage choice mechanisms, in which the identity of haematopoietic lineages requires continuous transcription factor expression.
机译:造血干细胞(HSC)可在个体的整个生命周期中维持血细胞的生成。胚胎发育过程中中胚层的HSC规范要求干细胞白血病SCL / tal-1基因产物。 SCL / tal-1的强制表达强烈诱导胚胎中的血液形成,表明该基因在致力于造血过程中起主要作用。在成人造血系统中,SCL / tal-1的表达在HSC和多能祖细胞以及红系和巨核细胞谱系中富集,与该因子在成人造血中的作用一致。在这里,我们通过有条件的基因靶向评估HSC的身份和功能是否持续需要SCL / tal-1。我们发现SCL / tal-1对于HSC植入,自我更新和分化为髓样和淋巴-血统谱系是必不可少的。但是,红系和巨核细胞前体的适当分化取决于SCL / tal-1。因此,SCL / tal-1对于HSC的产生是必不可少的,但是其持续表达对于HSC的功能并不是必需的。这些发现与血统选择机制相反,在血统选择机制中,造血血统的身份需要连续的转录因子表达。

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