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Modelling Hepatic Endoderm Development: Highly Efficient Differentiation of Human Embryonic Stem Cells to Functional Hepatic Endoderm Requires ActivinA and Wnt3a Signalling.

机译:肝内胚层发育模型:人类胚胎干细胞向功能性肝内胚层的高效分化需要ActivinA和Wnt3a信号传导。

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摘要

Human embryonic stem cells (hESCs) are a valuable source of pluripotential primary cells. However, their homogeneous cellular differentiation to specific cell types _in vitro_ has proven difficult thus far. Wnt signalling has been shown to play important roles in coordinating development and we demonstrate that Wnt3a is differentially expressed at critical stages of human liver development _in vivo_. The essential role of Wnt3a in hepatocyte differentiation from hESCs is paralleled by our _in vitro_ model, demonstrating the importance of a physiological approach to cellular differentiation. Our studies provide compelling evidence that Wnt3a signaling is important for coordinated hepato-cellular function _in vitro_ and _in vivo_. In addition, we demonstrate Wnt3a facilitates clonal plating of hESCs capable of hepatic endoderm differentiation. These studies represent an important step forward toward the use of hESC-derived hepatocytes in biomedical applications and has opened the door to high through-put metabolic analysis of human liver function.
机译:人胚胎干细胞(hESCs)是多潜能原代细胞的重要来源。然而,迄今为止,已经证明它们很难在体外分化为特定的细胞类型。已经显示出Wnt信号传导在协调发育中起重要作用,并且我们证明了Wnt3a在人体内肝脏发育的关键阶段差异表达。 Wnt3a在hESCs分化为肝细胞中的重要作用与我们的_in vitro_模型相似,表明了生理学方法对细胞分化的重要性。我们的研究提供了令人信服的证据,表明Wnt3a信号对于协调的肝细胞功能在体外和体内都很重要。此外,我们证明Wnt3a有助于能够进行肝内胚层分化的hESC的克隆培养。这些研究代表了在生物医学应用中使用hESC来源的肝细胞的重要一步,并为人类肝脏功能的高通量代谢分析打开了大门。

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