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Dual role of Mpl receptor during the establishment of definitive hematopoiesis.

机译:Mpl受体在确定性造血过程中的双重作用。

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Cytokine signaling pathways are important in promoting hematopoietic stem cell (HSC) self-renewal, proliferation and differentiation. Mpl receptor and its ligand, TPO, have been shown to play an essential role in the early steps of adult hematopoiesis. We previously demonstrated that the cytoplasmic domain of Mpl promotes hematopoietic commitment of embryonic stem cells in vitro, and postulated that Mpl could be important in the establishment of definitive hematopoiesis. To answer this question, we investigated the temporal expression of Mpl during mouse development by in situ hybridization. We found Mpl expression in the HSCs clusters emerging in the AGM region, and in the fetal liver (FL) as early as E10.5. Using Mpl(-/-) mice, the functional relevance of Mpl expression was tested by comparing the hematopoietic progenitor (HP) content, long-term hematopoietic reconstitution (LTR) abilities and HSC content of control and Mpl(-/-) embryos at different times of development. In the AGM, we observed delayed production of HSCs endowed with normal LTR but presenting a self-renewal defect. During FL development, we detected a decrease in HP and HSC potential associated with a defect in amplification and self-renewal/survival of the lin(-) AA4.1(+) Sca1(+) population of HSCs. These results underline the dual role of Mpl in the generation and expansion of HSCs during establishment of definitive hematopoiesis.
机译:细胞因子信号通路在促进造血干细胞(HSC)自我更新,增殖和分化中很重要。 Mpl受体及其配体TPO已显示在成人造血的早期步骤中起着至关重要的作用。我们以前证明了Mpl的胞质域在体外促进了胚胎干细胞的造血作用,并假设Mpl在确定的造血功能的建立中可能很重要。为了回答这个问题,我们通过原位杂交研究了小鼠发育过程中Mpl的瞬时表达。我们发现Mpl在早于E10.5的AGM地区和胎儿肝脏(FL)中出现的HSC簇中表达。使用Mpl(-/-)小鼠,通过比较对照组和Mpl(-/-)胚胎的造血祖细胞(HP)含量,长期造血重建(LTR)能力和HSC含量,测试了Mpl表达的功能相关性。发展的不同时期。在年度股东大会上,我们观察到了具有正常LTR却导致自我更新缺陷的HSC的延迟生产。在FL的发展过程中,我们检测到与HSCs lin(-)AA4.1(+)Sca1(+)人群的扩增和自我更新/生存缺陷相关的HP和HSC电位下降。这些结果强调了在确定的造血过程中,Mpl在HSC的产生和扩展中的双重作用。

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