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Prerequisite OCT4 Maintenance Potentiates the Neural Induction of Differentiating Human Embryonic Stem Cells and Induced Pluripotent Stem Cells

机译:必要的OCT4维护可增强分化人类胚胎干细胞和诱导性多能干细胞的神经诱导作用。

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摘要

Establishing an efficient differentiation procedure is prerequisite for the cell transplantation of phuipotent stem cells. Activating fibroblast growth factor (FGF) signals and inhibiting the activinodal pathway are both conserved principles to direct the neural induction (NI) of developing embryos and human embryonic stem cells (bESCs). Wnt signal and OCT4 expression are critical for the hESC pluripotency; however, their roles in cell differentiation are largely unclear. We demonstrate that in the presence of FGF2 and activin inhibitor SB431542, applying a small-molecule Wnt agonist, BIO, efficiently and rapidly steers the NI of all our tested hESCs. A human induced pluripotent stem cell (iPSC), which is refractory for efficient neural conversion by FGF2, effectively differentiated to SOX1(+) cells after the BIO/SB4315421FGF2 treatment. In addition, BIO promoted cell survival and transiently sustained OCT4 expression at the early NI stage with FGF2 and SB431542. Interestingly, at the late NI stage, the OCT4 level rapidly declined in the treated hESCs and consequently initiated the formation of neural rosettes with forebrain neuron characteristics. This study illustrates the distinct effects of Wnt activation on maintaining pluripotency and committing neural lineages at the early and late NI stages of hESCs and iPSCs, respectively.
机译:建立有效的分化程序是多能干细胞移植的前提。激活成纤维细胞生长因子(FGF)信号和抑制激活素/淋巴结通路均是指导发育中胚胎和人类胚胎干细胞(bESCs)神经诱导(NI)的保守原理。 Wnt信号和OCT4表达对于hESC多能性至关重要。然而,它们在细胞分化中的作用尚不清楚。我们证明,在存在FGF2和激活素抑制剂SB431542的情况下,应用小分子Wnt激动剂BIO可以有效且迅速地引导我们所有测试的hESC的NI。经过BIO / SB4315421FGF2处理后,人类诱导的多能干细胞(iPSC)难以通过FGF2进行有效的神经转化,有效分化为SOX1(+)细胞。另外,BIO促进了NI2早期使用FGF2和SB431542的细胞存活并短暂维持了OCT4表达。有趣的是,在NI晚期,经处理的hESC中的OCT4水平迅速下降,因此开始形成具有前脑神经元特征的神经花环。这项研究说明了Wnt激活分别对hESC和iPSC的NI早期和晚期维持多能性和提交神经谱系的显着影响。

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