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首页> 外文期刊>Blood: The Journal of the American Society of Hematology >Identification of key regulatory pathways of myeloid differentiation using an mESC-based karyotypically normal cell model
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Identification of key regulatory pathways of myeloid differentiation using an mESC-based karyotypically normal cell model

机译:使用基于mESC的核型正常细胞模型鉴​​定髓系分化的关键调控途径

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Understanding the process of myeloid differentiation offers important insights into both normal and abnormal developmental processes but is limited by the dearth of experimental models. Here we show that myeloid progenitors can be derived from embryonic stem cells, immortalized, and applied to the study of the mechanisms underlying myeloid differentiation. The embryonic stem cell-derived myeloid progenitors, when immortalized with estrogen-regulated Hoxb8 protein, demonstrate normal karyotyping, are genetically tractable, and can be differentiated into functional neutrophils. Using this model, we identified mammalian target of rapamycin complex 1 as a critical regulator of myeloid differentiation. Together, our studies led to a convenient, karyotypically normal, and genetically manipulatable cellular system, which can be used to shed new light on the mechanisms for myeloid differentiation. (Blood. 2012;120(24):4712-4719)
机译:了解骨髓分化的过程提供了正常和异常发育过程的重要见解,但受到缺乏实验模型的限制。在这里,我们显示髓样祖细胞可以源自胚胎干细胞,永生化,并用于研究髓样分化的潜在机制。胚胎干细胞来源的骨髓祖细胞,当被雌激素调节的Hoxb8蛋白永生化时,表现出正常的核型,可遗传遗传,并且可以分化为功能性中性粒细胞。使用此模型,我们确定了雷帕霉素复合物1的哺乳动物靶标是髓样分化的关键调节剂。在一起,我们的研究导致了一个方便,核型正常和遗传可操纵的细胞系统,可用于阐明骨髓分化的机制。 (血液.2012; 120(24):4712-4719)

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