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Embryonic stem-derived versus somatic neural stem cells: A comparative analysis of their developmental potential and molecular phenotype

机译:胚胎干细胞与体细胞神经干细胞:发育潜力和分子表型的比较分析

摘要

Reliable procedures to induce neural commitment of totipotent undifferentiated embryonic stem (ES) cells have provided new tools for investigating the molecular mechanisms underlying cell fate choices. We extensively characterized the developmental potential of ES-induced neural cells obtained using an adaptation of the multistep induction protocol. We provided evidence that ES-derived neural proliferating cells are endowed with stem cell properties such as extensive self-renewal capacity and single-cell multipotency. In differentiating conditions, cells matured exclusively into neurons, astrocytes, and oligodendrocytes. All these features have been previously described in only somatic neural stem cells (NSCs). Therefore, we consider it more appropriate to rename our cells ES-derived NSCs. These similarities between the two NSC populations induced us to carefully compare their proliferation ability and differentiation potential. Although they were very similar in overall behavior, we scored specific differences. For instance, ES-derived NSCs proliferated at higher rate and consistently generated a higher number of neurons compared with somatic NSCs. To further investigate their relationships, we carried out a molecular analysis comparing their transcriptional profiles during proliferation. We observed a large fraction of shared expressed transcripts, including genes previously described to be critical in defining somatic NSC traits. Among the genes differently expressed, candidate genes possibly responsible for divergences between the two cell types were selected and further investigated. In particular, we showed that an enhanced MAPK (mitogen-activated protein kinase) signaling is acting in ES-induced NSCs, probably triggered by insulin-like growth factor-H. This may contribute to the high proliferation rate exhibited by these cells in culture.
机译:诱导全能未分化胚胎干(ES)细胞神经承诺的可靠程序为研究细胞命运选择的分子机制提供了新工具。我们广泛地表征了使用多步诱导方案的改编获得的ES诱导的神经细胞的发展潜力。我们提供的证据表明,源自ES的神经增殖细胞具有干细胞特性,例如广泛的自我更新能力和单细胞多能性。在分化条件下,细胞仅成熟为神经元,星形胶质细胞和少突胶质细胞。所有这些功能以前仅在体神经干细胞(NSC)中进行了描述。因此,我们认为将我们的细胞ES衍生的NSC重命名更为合适。这两个NSC种群之间的相似性促使我们仔细比较它们的增殖能力和分化潜力。尽管它们在总体行为上非常相似,但我们在具体得分上有所不同。例如,与体细胞NSC相比,ES衍生的NSC增殖速率更高,并持续产生更多数量的神经元。为了进一步研究它们之间的关系,我们进行了分子分析,比较了它们在增殖过程中的转录谱。我们观察到大部分共享的表达转录本,包括先前描述对定义体细胞NSC特性至关重要的基因。在不同表达的基因中,选择可能负责两种细胞类型差异的候选基因,并进行进一步研究。特别是,我们表明增强的MAPK(促分裂原活化蛋白激酶)信号传导在ES诱导的NSC中起作用,可能是由胰岛素样生长因子H触发的。这可能有助于这些细胞在培养中表现出高增殖速率。

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