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首页> 外文期刊>Blood: The Journal of the American Society of Hematology >SCL-mediated regulation of the cell-cycle regulator p21 is critical for murine megakaryopoiesis.
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SCL-mediated regulation of the cell-cycle regulator p21 is critical for murine megakaryopoiesis.

机译:SCL介导的细胞周期调控因子p21的调控对于鼠巨核细胞生成至关重要。

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Megakaryopoiesis is a complex process that involves major cellular and nuclear changes and relies on controlled coordination of cellular proliferation and differentiation. These mechanisms are orchestrated in part by transcriptional regulators. The key hematopoietic transcription factor stem cell leukemia (SCL)/TAL1 is required in early hematopoietic progenitors for specification of the megakaryocytic lineage. These early functions have, so far, prevented full investigation of its role in megakaryocyte development in loss-of-function studies. Here, we report that SCL critically controls terminal megakaryocyte maturation. In vivo deletion of Scl specifically in the megakaryocytic lineage affects all key attributes of megakaryocyte progenitors (MkPs), namely, proliferation, ploidization, cytoplasmic maturation, and platelet release. Genome-wide expression analysis reveals increased expression of the cell-cycle regulator p21 in Scl-deleted MkPs. Importantly, p21 knockdown-mediated rescue of Scl-mutant MkPs shows full restoration of cell-cycle progression and partial rescue of the nuclear and cytoplasmic maturation defects. Therefore, SCL-mediated transcriptional control of p21 is essential for terminal maturation of MkPs. Our study provides a mechanistic link between a major hematopoietic transcriptional regulator, cell-cycle progression, and megakaryocytic differentiation.
机译:巨核细胞生成是一个复杂的过程,涉及主要的细胞和核变化,并依赖于细胞增殖和分化的受控协调。这些机制部分地由转录调节子协调。在早期造血祖细胞中,关键的造血转录因子干细胞白血病(SCL)/ TAL1是巨核细胞谱系规格的必需条件。到目前为止,这些早期功能无法在功能丧失研究中全面调查其在巨核细胞发育中的作用。在这里,我们报告SCL严格控制终端巨核细胞的成熟。在巨核细胞谱系中,Scl的体内缺失会影响巨核细胞祖细胞(MkPs)的所有关键属性,即增殖,倍化,细胞质成熟和血小板释放。全基因组表达分析揭示了Scl缺失的MkPs中细胞周期调节因子p21的表达增加。重要的是,p21击倒介导的Scl突变型MkPs的拯救显示出细胞周期进程的完全恢复以及核和细胞质成熟缺陷的部分拯救。因此,SCL介导的p21转录控制对于MkP的最终成熟至关重要。我们的研究提供了主要造血转录调节因子,细胞周期进程和巨核细胞分化之间的机制联系。

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