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Effect of hypoxia on proliferation and neural commitment of embryonic stem cells at different stages of pluripotency

机译:缺氧对多能性不同阶段胚胎干细胞增殖和神经承诺的影响

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We have studied the effect of low oxygen levels (2% O2), or hypoxia, in the expansion and neural commitment of mouse embryonic stem (ES) cells. When ES cells were maintained in culture with leukemia inhibitory factor (LIF), cell proliferation was reduced at low oxygen levels and a simultaneous reduction in cell viability was also observed. Morphological changes and different cell cycle patterns also occurred, suggesting some early differentiation under hypoxic conditions. However, when cells were maintained in a ground state of pluripotency, by inhibition of autocrine FGF4/ERK and GSK3 signaling, hypoxia did not affect cell proliferation, and did not induce early differentiation. Nevertheless, during neural commitment, low oxygen tension exerted a positive effect on early differentiation of ES cells, resulting in a faster commitment towards neural progenitors. Overall our results demonstrate the need to specifically regulate the oxygen content, especially hypoxia, along with other culture conditions, when developing new strategies for ES cell expansion and/or controlled differentiation.
机译:我们已经研究了低氧水平(2%0 2 )的效果,或缺氧,在膨胀和小鼠胚胎干(ES)细胞的神经承诺。当ES细胞维持在培养物与白血病抑制因子(LIF),细胞增殖在低氧水平降低,并且还观察到在细胞活力同时减少。形态学变化和不同的细胞周期模式也发生,这表明在低氧条件下一些早期分化。然而,当细胞保持多能性的基态时,通过抑制自分泌FGF4 / ERK和GSK3信令,缺氧不影响细胞增殖,并且不诱导早期分化。不过,在神经承诺,低氧张力施加在ES细胞的早期分化产生积极的影响,导致对神经祖细胞更快的承诺。总的来说,我们的结果表明,需要专门规范中的氧含量,尤其是缺氧,与其他文化条件,开发ES细胞扩增和/或控制的分化新战略时一起。

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