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Dicer is selectively important for the earliest stages of erythroid development

机译:切块机对于红系发育的早期阶段具有选择性的重要性

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摘要

MicroRNAs (miRs) are involved in many aspects of normal and malignant hematopoiesis, including hematopoietic stem cell (HSC) self-renewal, proliferation, and terminal differentiation. However, a role for miRs in the generation of the earliest stages of lineage committed progenitors from HSCs has not been identified. Using Dicer inactivation, we show that the miR complex is not only essential for HSC maintenance but is specifically required for their erythroid programming and subsequent generation of committed erythroid progenitors. In bipotent pre-MegEs, loss of Dicer up-regulated transcription factors preferentially expressed in megakaryocyte progenitors (Gata2 and Zfpm1) and decreased expression of the erythroid-specific Klf1 transcription factor. These results show a specific requirement for Dicer in acquisition of erythroid lineage programming and potential in HSCs and their subsequent erythroid lineage differentiation, and in particular indicate a role for the miR complex in achieving proper balance of lineage-specific transcriptional regulators necessary for HSC multilineage potential to be maintained.
机译:MicroRNA(miRs)参与正常和恶性造血的许多方面,包括造血干细胞(HSC)自我更新,增殖和终末分化。但是,尚未确定miRs在从HSC产生世系定型祖细胞的最早阶段中的作用。使用Dicer灭活,我们显示miR复合物不仅对于HSC维持至关重要,而且对于它们的类红细胞编程和随后的定型类红细胞祖细胞的生成特别需要。在双能的前MegE中,Dicer缺失的上调转录因子优先在巨核细胞祖细胞(Gata2和Zfpm1)中表达,而红系特异性Klf1转录因子的表达降低。这些结果显示了Dicer对获得红系谱系编程和HSCs潜能及其随后的红系谱系分化的特殊要求,尤其表明了miR复合体在实现HSC多谱系潜能所必需的谱系特异性转录调节因子的适当平衡中的作用。保持。

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