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Embryonic stem cell-specific microRNAs contribute to pluripotency by inhibiting regulators of multiple differentiation pathways

机译:胚胎干细胞特异性microRNA通过抑制多种分化途径的调节剂来促进多能性

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The findings that microRNAs (miRNAs) are essential for early development in many species and that embryonic miRNAs can reprogram somatic cells into induced pluripotent stem cells suggest that these miRNAs act directly on transcriptional and chromatin regulators of pluripotency. To elucidate the transcription regulatory networks immediately downstream of embryonic miRNAs, we extended the motif activity response analysis approach that infers the regulatory impact of both transcription factors (TFs) and miRNAs from genome-wide expression states. Applying this approach to multiple experimental data sets generated from mouse embryonic stem cells (ESCs) that did or did not express miRNAs of the ESC-specific miR-290-295 cluster, we identified multiple TFs that are direct miRNA targets, some of which are known to be active during cell differentiation. Our results provide new insights into the transcription regulatory network downstream of ESC-specific miRNAs, indicating that these miRNAs act on cell cycle and chromatin regulators at several levels and downregulate TFs that are involved in the innate immune response.
机译:microRNA(miRNA)对于许多物种的早期发育至关重要,而胚胎miRNA可以将体细胞重编程为诱导的多能干细胞,这一发现表明这些miRNA直接作用于多能性的转录和染色质调节剂。为了阐明紧邻胚胎miRNA下游的转录调控网络,我们扩展了基序活性反应分析方法,该方法可从全基因组表达状态推断转录因子(TFs)和miRNA的调控作用。将这种方法应用于从表达或不表达ESC特异性miR-290-295簇的miRNA的小鼠胚胎干细胞(ESC)产生的多个实验数据集,我们确定了多个TF是直接miRNA靶标,其中一些是已知在细胞分化过程中是活跃的。我们的结果提供了对ESC特异性miRNA下游转录调控网络的新见解,表明这些miRNA在多个水平上作用于细胞周期和染色质调节剂,并下调与先天免疫反应有关的TF。

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