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首页> 外文期刊>Developmental biology >Zebrafish eaf1 suppresses foxo3b expression to modulate transcriptional activity of gata1 and spi1 in primitive hematopoiesis.
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Zebrafish eaf1 suppresses foxo3b expression to modulate transcriptional activity of gata1 and spi1 in primitive hematopoiesis.

机译:斑马鱼eaf1抑制foxo3b表达,以调节原始造血过程中gata1和spi1的转录活性。

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摘要

Studies implicate a potential role for EAF1 in MLL-ELL induced leukemogenesis; however the biological function of EAF1 in this process remains unknown. In this study, we show that knockdown of zebrafish eaf1 by morpholinos caused serious defects in both primitive and definitive hematopoiesis. Using microarray analysis, we identified foxo3b as a target gene suppressed by eaf1. Ectopic expression of foxo3b in embryos mimicked the phenotypes exhibited in eaf1 morphants, except that foxo3b had no effect on runx1 and c-myb expression while eaf1 morphants did not express these markers in the ventral wall of dorsal aorta. Subsequent experiments showed that a dominant negative form of Foxo3b (dn-foxo3b) partially restored primitive hematopoietic defects in eaf1 morphants, suggesting that foxo3b might serve as a key factor for mediating eaf1 function in primitive hematopoiesis. Furthermore, we observed that foxo3b inhibited the transcriptional activity of gata1 and spi1 through protein-protein interaction. Our findings not only suggest a function of eaf1 on hematopoiesis in vivo, but also reveal a novel regulatory pathway, eaf1-foxo3b-gata1/spi1, that may shed light on the role of EAF1 in MLL-ELL induced leukemogenesis.
机译:研究表明EAF1在MLL-ELL诱导的白血病发生中具有潜在作用。然而,EAF1在此过程中的生物学功能仍然未知。在这项研究中,我们表明吗啉代敲除斑马鱼eaf1导致原始和确定性造血功能严重缺陷。使用微阵列分析,我们确定了foxo3b是被eaf1抑制的靶基因。 foxo3b在胚胎中的异位表达模仿了eaf1 morphant表现出的表型,除了foxo3b对runx1和c-myb的表达没有影响,而eaf1 morphant并不在背主动脉腹壁表达这些标记。随后的实验表明,Foxo3b(dn-foxo3b)的显性负性形式部分恢复了eaf1吗啡形成者的原始造血缺陷,这表明foxo3b可能是介导eaf1在原始造血功能中发挥关键作用的因素。此外,我们观察到foxo3b通过蛋白相互作用抑制了gata1和spi1的转录活性。我们的发现不仅表明eaf1在体内具有造血功能,而且还揭示了新的调控途径eaf1-foxo3b-gata1 / spi1,这可能揭示了EAF1在MLL-ELL诱导的白血病发生中的作用。

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