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Physiological Oxygen Prevents Frequent Silencing of the DLK1-DIO3 Cluster during Human Embryonic Stem Cells Culture

机译:生理氧气可防止人胚胎干细胞培养过程中DLK1-DIO3簇的频繁沉默

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摘要

Genetic and epigenetic alterations are observed in long-term culture (>30 passages) of human embryonic stem cells (hESCs); however, little information is available in early cultures. Through a large-scale gene expression analysis between initial-passage hESCs (ihESCs, <10 passages) and early-passage hESCs (ehESCs, 20-30 passages) of 12 hESC lines, we found that the DLK1-DIO3 gene cluster was normally expressed and showed normal methylation pattern in ihESC, but was frequently silenced after 20 passages. Both the DLK1-DIO3 active status in ihESCs and the inactive status in ehESCs were inheritable during differentiation. Silencing of the DLK1-DIO3 cluster did not seem to compromise the multilineage differentiation ability of hESCs, but was associated with reduced DNA damage-induced apoptosis in ehESCs and their differentiated hepatocyte-like cell derivatives, possibly through attenuation of the expression and phosphoryl-ation of p53. Furthermore, we demonstrated that 5% oxygen, instead of the commonly used 20% oxygen, is required for preserving the expression of the DLK1-DIO3 cluster. Overall, the data suggest that active expression of the DLK1-DIO3 cluster represents a new biomarker for epigenetic stability of hESCs and indicates the importance of using a proper physiological oxygen level during the derivation and culture of hESCs.
机译:在人类胚胎干细胞(hESCs)的长期培养(> 30代)中观察到了遗传和表观遗传学改变;但是,早期文化中几乎没有信息。通过对12条hESC系的初始传代hESC(ihESCs,<10传代)和早期传代hESC(ehESC,20-30传代)之间的大规模基因表达分析,我们发现DLK1-DIO3基因簇正常表达并在ihESC中显示正常的甲基化模式,但在20代后经常沉默。在分化过程中,ihESCs中的DLK1-DIO3激活状态和ehESCs中的非激活状态都是可遗传的。沉默DLK1-DIO3簇似乎并不影响hESCs的多谱系分化能力,但与ehESCs及其分化的肝细胞样细胞衍生物中DNA损伤诱导的凋亡减少有关,可能是由于表达减弱和磷酸化引起的p53。此外,我们证明保留DLK1-DIO3簇的表达需要5%的氧气,而不是通常使用的20%的氧气。总体而言,数据表明DLK1-DIO3簇的有效表达代表了hESCs表观遗传稳定性的新生物标记,并表明在hESCs的衍生和培养过程中使用适当的生理氧水平的重要性。

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