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A small molecule primes embryonic stem cells for differentiation.

机译:一个小分子引发胚胎干细胞分化。

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Embryonic stem cells (ESCs) are an attractive source of cells for disease modeling in vitro and may eventually provide access to cells/tissues for the treatment of many degenerative diseases. However, applications of ESC-derived cell types are largely hindered by the lack of highly efficient methods for lineage-specific differentiation. Using a high-content screen, we have identified a small molecule, named stauprimide, that increases the efficiency of the directed differentiation of mouse and human ESCs in synergy with defined extracellular signaling cues. Affinity-based methods revealed that stauprimide interacts with NME2 and inhibits its nuclear localization. This, in turn, leads to downregulation of c-Myc, a key regulator of the pluripotent state. Thus, our findings identify a chemical tool that primes ESCs for efficient differentiation through a mechanism that affects c-Myc expression, and this study points to an important role for NME2 in ESC self-renewal.
机译:胚胎干细胞(ESC)是用于体外疾病建模的有吸引力的细胞来源,最终可能为治疗许多退行性疾病提供接触细胞/组织的途径。然而,由于缺乏针对谱系特异性分化的高效方法,ESC衍生的细胞类型的应用受到了极大的阻碍。使用高内涵屏幕,我们已经确定了一个名为stauprimide的小分子,该分子可以与定义的细胞外信号提示协同作用,提高小鼠和人类ESC定向分化的效率。基于亲和力的方法显示,stauprimide与NME2相互作用并抑制其核定位。反过来,这导致c-Myc的下调,c-Myc是多能状态的关键调节因子。因此,我们的发现确定了一种化学工具,可以通过影响c-Myc表达的机制引发ESC进行有效分化,并且这项研究指出NME2在ESC自我更新中的重要作用。

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