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首页> 外文期刊>Blood: The Journal of the American Society of Hematology >Repression of Id2 expression by Gfi-1 is required for B-cell and myeloid development.
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Repression of Id2 expression by Gfi-1 is required for B-cell and myeloid development.

机译:B细胞和骨髓发育需要Gfi-1抑制Id2表达。

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The development of mature blood cells from hematopoietic stem cells requires coordinated activities of transcriptional networks. Transcriptional repressor growth factor independence 1 (Gfi-1) is required for the development of B cells, T cells, neutrophils, and for the maintenance of hematopoietic stem cell function. However, the mechanisms by which Gfi-1 regulates hematopoiesis and how Gfi-1 integrates into transcriptional networks remain unclear. Here, we provide evidence that Id2 is a transcriptional target of Gfi-1, and repression of Id2 by Gfi-1 is required for B-cell and myeloid development. Gfi-1 binds to 3 conserved regions in the Id2 promoter and represses Id2 promoter activity in transient reporter assays. Increased Id2 expression was observed in multipotent progenitors, myeloid progenitors, T-cell progenitors, and B-cell progenitors in Gfi-1(-/-) mice. Knockdown of Id2 expression or heterozygosity at the Id2 locus partially rescues the B-cell and myeloid development but not the T-cell development in Gfi-1(-/-) mice. These studies demonstrate a role of Id2 in mediating Gfi-1 functions in B-cell and myeloid development and provide a direct link between Gfi-1 and the B-cell transcriptional network by its ability to repress Id2 expression.
机译:从造血干细胞发育成熟的血细胞需要转录网络的协调活动。转录抑制因子生长因子独立性1(Gfi-1)是B细胞,T细胞,嗜中性粒细胞的发育以及维持造血干细胞功能所必需的。但是,尚不清楚Gfi-1调节造血作用的机制以及Gfi-1如何整合到转录网络中。在这里,我们提供证据表明Id2是Gfi-1的转录靶标,而B细胞和骨髓的发育则需要通过Gfi-1抑制Id2。 Gfi-1结合Id2启动子中的3个保守区域,并在瞬时报告基因检测中抑制Id2启动子活性。在Gfi-1(-/-)小鼠的多能祖细胞,骨髓祖细胞,T细胞祖细胞和B细胞祖细胞中观察到Id2表达增加。在Id2基因座处击倒Id2表达或杂合性可以部分拯救Gfi-1(-/-)小鼠的B细胞和骨髓发育,而不是T细胞发育。这些研究证明了Id2在介导B细胞和骨髓发育中的Gfi-1功能中的作用,并通过其抑制Id2表达的能力提供了Gfi-1和B细胞转录网络之间的直接联系。

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