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Generation of anterior foregut endoderm from human embryonic and induced pluripotent stem cells

机译:从人类胚胎和诱导多能干细胞产生前前肠内胚层

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Directed differentiation of human embryonic stem (hES) cells and human induced pluripotent stem (hiPS) cells captures in vivo developmental pathways for specifying lineages in vitro, thus avoiding perturbation of the genome with exogenous genetic material. Thus far, derivation of endodermal lineages has focused predominantly on hepatocytes, pancreatic endocrine cells and intestinal cells(1-5). The ability to differentiate pluripotent cells into anterior foregut endoderm (AFE) derivatives would expand their utility for cell therapy and basic research to tissues important for immune function, such as the thymus; for metabolism, such as thyroid and parathyroid; and for respiratory function, such as trachea and lung. We find that dual inhibition of transforming growth factor (TGF)-beta and bone morphogenic protein (BMP) signaling after specification of definitive endoderm from pluripotent cells results in a highly enriched AFE population that is competent to be patterned along dorsoventral and anteroposterior axes. These findings provide an approach for the generation of AFE derivatives.
机译:人胚胎干(hES)细胞和人诱导的多能干(hiPS)细胞的定向分化捕获了用于在体外确定谱系的体内发育途径,从而避免了外源遗传物质对基因组的干扰。迄今为止,内胚层谱系的衍生主要集中在肝细胞,胰腺内分泌细胞和肠细胞上(1-5)。将多能细胞分化成前前肠内胚层(AFE)衍生物的能力将将其在细胞治疗和基础研究中的用途扩展到对免疫功能重要的组织(如胸腺);用于新陈代谢,例如甲状腺和甲状旁腺;并具有呼吸功能,例如气管和肺。我们发现从多能细胞的定形内胚层规范化后,转化生长因子(TGF)-β和骨形态发生蛋白(BMP)信号转导的双重抑制导致高度富集的AFE群体,能够沿背腹和前后轴构图。这些发现提供了产生AFE衍生物的方法。

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