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首页> 外文期刊>Stem Cell Reports >Small-Molecule Induction Promotes Corneal Epithelial Cell Differentiation from Human Induced Pluripotent Stem Cells
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Small-Molecule Induction Promotes Corneal Epithelial Cell Differentiation from Human Induced Pluripotent Stem Cells

机译:小分子诱导促进了来自人诱导多能干细胞的角膜上皮细胞分化

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Summary Human induced pluripotent stem cells (hiPSCs) offer unique opportunities for developing novel cell-based therapies and disease?modeling. In this study, we developed a directed differentiation method for hiPSCs toward corneal epithelial progenitor cells?capable of terminal differentiation toward mature corneal epithelial-like cells. In order to improve the efficiency and reproducibility of our method,?we replicated signaling cues active during ocular surface ectoderm development with the help of two small-molecule?inhibitors in combination with basic fibroblast growth factor (bFGF) in serum-free and feeder-free conditions. First, small-molecule induction downregulated the expression of pluripotency markers while upregulating several transcription factors essential for?normal eye development. Second, protein expression of the corneal epithelial progenitor marker p63 was greatly enhanced, with up to 95% of cells being p63 positive after 5?weeks of differentiation. Third, corneal epithelial-like cells were obtained upon further maturation.
机译:发明内容人诱导多能干细胞(HIPSCS)为发展新细胞的疗法和疾病提供独特的机会?建模。在这项研究中,我们为角膜上皮祖细胞的HIPSCS开发了一种定向的分化方法?能够朝向成熟角膜上皮样细胞分化。为了提高我们方法的效率和再现性,尤其是在两种小分子的帮助下释放在眼睛表面异影发育期间活性的信号线索,抑制剂与血清和饲养者的碱性成纤维细胞生长因子(BFGF)组合自由条件。首先,小分子诱导下调多能性标记物的表达,同时上调几种转录因子,对于常见的眼睛发育。其次,角膜上皮祖的蛋白质表达大大提高,高达95%的细胞是5?分化后的P63阳性。第三,在进一步成熟时获得角膜上皮样细胞。

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