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p53 controls genomic stability and temporal differentiation of human neural stem cells and affects neural organization in human brain organoids

机译:P53控制人神经干细胞的基因组稳定性和时间分化,并影响人脑器有机体中的神经组织

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摘要

In this study, we take advantage of human induced pluripotent stem (iPS) cell-derived neural stem cells and brain organoids to study the role of p53 during human brain development. We knocked down (KD) p53 in human neuroepithelial stem (NES) cells derived from iPS cells. Upon p53KD, NES cells rapidly show centrosome amplification and genomic instability. Furthermore, a reduced proliferation rate, downregulation of genes involved in oxidative phosphorylation (OXPHOS), and an upregulation of glycolytic capacity was apparent upon loss of p53. In addition, p53KD neural stem cells display an increased pace of differentiating into neurons and exhibit a phenotype corresponding to more mature neurons compared to control neurons. Using brain organoids, we modeled more specifically cortical neurogenesis. Here we found that p53 loss resulted in brain organoids with disorganized stem cell layer and reduced cortical progenitor cells and neurons. Similar to NES cells, neural progenitors isolated from brain organoids also show a downregulation in several OXPHOS genes. Taken together, this demonstrates an important role for p53 in controlling genomic stability of neural stem cells and regulation of neuronal differentiation, as well as maintaining structural organization and proper metabolic gene profile of neural progenitors in human brain organoids.
机译:在这项研究中,我们利用人诱导的多能干(IPS)细胞衍生的神经干细胞和脑器有机体来研究P53在人脑发育过程中的作用。我们击倒(KD)P53在衍生自IPS细胞的人神经头脑茎(NES)细胞中。在P53KD时,NES细胞迅速显示了中心体积扩增和基因组不稳定性。此外,减少氧化磷酸化(汤膦)的基因下调的增殖率降低,并且在P53损失时显而易见的糖蛋白能力的上调。此外,P53KD神经干细胞显示出与对照的分化为神经元的速度增加,与对照神经元相比表现出对应于更成熟的神经元的表型。使用脑器有机体,我们更具体地说是皮质神经发生。在这里,我们发现P53损失导致脑器有机体,具有混乱的干细胞层和减少皮质祖细胞和神经元。类似于NES细胞,从脑器子体中分离的神经祖细胞剂也显示出几种毒物基因的下调。总之,这证明了P53在控制神经干细胞的基因组稳定性以及神经元分化的调节中的重要作用,以及维持人脑器有机体中神经祖细胞的结构组织和适当代谢基因谱。

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