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An integrated systems biology approach identifies positive cofactor 4 as a factor that increases reprogramming efficiency

机译:集成系统生物学方法将阳性辅因子4确定为增加重编程效率的因子

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Spermatogonial stem cells (SSCs) can spontaneously dedifferentiate into embryonic stem cell (ESC)-like cells, which are designated as multipotent SSCs (mSSCs), without ectopic expression of reprogramming factors. Interestingly, SSCs express key pluripotency genes such asOct4, Sox2, Klf4 andMyc. Therefore, molecular dissection of mSSC reprogramming may provide clues about novel endogenous reprogramming or pluripotency regulatory factors. Our comparative transcriptome analysis of mSSCs and induced pluripotent stem cells (iPSCs) suggests that they have similar pluripotency states but are reprogrammed via different transcriptional pathways. We identified 53 genes as putative pluripotency regulatory factors using an integrated systems biology approach. We demonstrated a selected candidate, Positive cofactor 4 (Pc4), can enhance the efficiency of somatic cell reprogramming by promoting and maintaining transcriptional activity of the key reprograming factors. These results suggest that Pc4 has an important role in inducing spontaneous somatic cell reprogramming via up-regulation of key pluripotency genes.
机译:精原干细胞(SSCs)可以自发分化为类胚胎干细胞(ESC)类细胞,称为多能SSC(mSSCs),而无需异位表达重编程因子。有趣的是,SSC表达关键的多能性基因,例如Oct4,Sox2,Klf4和Myc。因此,mSSC重编程的分子解剖可以提供有关新型内源性重编程或多能性调节因子的线索。我们对mSSCs和诱导性多能干细胞(iPSCs)的比较转录组分析表明,它们具有相似的多能性状态,但通过不同的转录途径进行了重新编程。我们使用综合系统生物学方法鉴定了53个基因作为推定的多能性调节因子。我们证明了选定的候选者,正辅助因子4(Pc4),可以通过促进和维持关键重编程因子的转录活性来增强体细胞重编程的效率。这些结果表明,Pc4在通过关键多能性基因的上调诱导自发性体细胞重编程中具有重要作用。

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