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Two Histone Variants TH2A and TH2B Enhance Human Induced Pluripotent Stem Cell Generation

机译:两个组蛋白变体TH2A和TH2B增强了人类诱导的多能干细胞的产生。

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There are two major methods of reprogramming: generation of induced pluripotent stem cells (iPSCs) by overexpressing embryonic stem cell-specific transcription factors (OCT4, SOX2, KLF4, and c-MYC) and somatic cell nuclear transfer by oocyte-specific factors. Previously, we reported oocyte-enriched histone variants TH2A, TH2B, and the histone chaperone nucleoplasmin (NPM2) enhance the reprogramming by OSKM in mice by inducing open chromatin structure. In this study, we showed that human TH2A, TH2B, and NPM2 enhance the OSKM-induced reprogramming of adult and neonatal human dermal fibroblasts and umbilical vein endothelial cells. Pluripotency of iPSCs generated by coexpressing OSKM, TH2A, TH2B, and NPM2 was shown by in vitro and in vivo differentiation assays. These iPSCs gave rise to highly differentiated teratomas compared to iPSCs induced by OSKM alone. Genome-wide analysis suggests a possibility that TH2A, TH2B, and NPM2 might regulate genes that are involved in naive stem cell stage. Thus, TH2A, TH2B, and NPM2 enhance reprogramming of human somatic cells and improve the quality of human iPSCs.
机译:重编程有两种主要方法:通过过度表达胚胎干细胞特异性转录因子(OCT4,SOX2,KLF4和c-MYC)生成诱导多能干细胞(iPSC),以及通过卵母细胞特异性因子进行体细胞核转移。以前,我们报道了富含卵母细胞的组蛋白变体TH2A,TH2B和组蛋白分子伴侣核纤溶酶(NPM2)通过诱导开放的染色质结构增强了OSKM在小鼠体内的重编程。在这项研究中,我们表明人TH2A,TH2B和NPM2增强了OSKM诱导的成人和新生儿人真皮成纤维细胞和脐静脉内皮细胞的重编程。通过体外和体内分化试验显示,共表达OSKM,TH2A,TH2B和NPM2产生的iPSC的多能性。与仅由OSKM诱导的iPSC相比,这些iPSC产生了高度分化的畸胎瘤。全基因组分析表明,TH2A,TH2B和NPM2可能调控天真干细胞阶段涉及的基因。因此,TH2A,TH2B和NPM2增强了人类体细胞的重编程并提高了人类iPSC的质量。

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