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Effects of FGF-2 and EGF removal on the differentiation of mouse neural precursor cells

机译:FGF-2和EGF去除对小鼠神经前体细胞分化的影响

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摘要

Cell therapy for neurological disorders has advanced, and neural precursor cells (NPC) may become the ideal candidates for neural transplantation in a wide range of diseases. However, additional work has to be done to determine either the ideal culture environment for NPC expansion in vitro, without altering their plasticity, or the FGF-2 and EGF mechanisms of cell signaling in neurospheres growth, survival and differentiation. In this work we evaluated mouse neurospheres cultured with and without FGF-2 and EGF containing medium and showed that those growth factors are responsible for NPC proliferation. It is also demonstrated that endogenous production of growth factors shifts from FGF-2 to IGF-1/PDGFb upon EGF and FGF-2 withdrawal. Mouse NPC cultured in suspension showed different patterns of neuronal localization (core versus shell) for both EGF and FGF-2 withdrawal and control groups. Taken together, these results show that EGF and FGF-2 removal play an important role in NPC differentiation and may contribute to a better understanding of mechanisms of NPC differentiation. Our findings suggest that depriving NPC of growth factors prior to grafting might enhance their chance to effectively integrate into the host.
机译:用于神经系统疾病的细胞疗法已经取得了进展,神经前体细胞(NPC)可能成为在多种疾病中进行神经移植的理想人选。但是,还需要进行其他工作来确定NPC体外扩增的理想培养环境而不改变其可塑性,或者确定神经球生长,存活和分化中细胞信号的FGF-2和EGF机制。在这项工作中,我们评估了在有或没有FGF-2和EGF培养基的情况下培养的小鼠神经球,并表明这些生长因子是NPC增殖的原因。还证明了在EGF和FGF-2退出后,生长因子的内源性产生从FGF-2转移到IGF-1 / PDGFb。悬浮培养的小鼠NPC对于EGF和FGF-2戒断组和对照组均显示出不同的神经元定位模式(核心与外壳)。综上所述,这些结果表明,去除EGF和FGF-2在NPC分化中起重要作用,并且可能有助于更好地理解NPC分化的机制。我们的发现表明,在移植前剥夺NPC的生长因子可能会增加它们有效整合到宿主中的机会。

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