Ivey Kathryn N, Muth Alecia, Arnold Joshua, King Frank W, Yeh Ru-Fang, Fish Jason E, Hsiao Edward C, Schwartz Robert J, Conklin Bruce R, Bernstein Harold S, Srivastava Deepak
Gladstone Institute of Cardiovascular Disease, University of California, San Francisco, 1650 Owens Street, San Francisco, CA 94158, USA.
Cell Stem Cell. 2008 Mar 6;2(3):219-29. doi: 10.1016/j.stem.2008.01.016.
Cell fate decisions of pluripotent embryonic stem (ES) cells are dictated by activation and repression of lineage-specific genes. Numerous signaling and transcriptional networks progressively narrow and specify the potential of ES cells. Whether specific microRNAs help refine and limit gene expression and, thereby, could be used to manipulate ES cell differentiation has largely been unexplored. Here, we show that two serum response factor (SRF)-dependent muscle-specific microRNAs, miR-1 and miR-133, promote mesoderm formation from ES cells but have opposing functions during further differentiation into cardiac muscle progenitors. Furthermore, miR-1 and miR-133 were potent repressors of nonmuscle gene expression and cell fate during mouse and human ES cell differentiation. miR-1's effects were in part mediated by translational repression of the Notch ligand Delta-like 1 (Dll-1). Our findings indicate that muscle-specific miRNAs reinforce the silencing of nonmuscle genes during cell lineage commitment and suggest that miRNAs may have general utility in regulating cell-fate decisions from pluripotent ES cells.
多能胚胎干细胞的细胞命运决定由谱系特异性基因的激活和抑制所决定。众多信号传导和转录网络逐渐缩小并明确了胚胎干细胞的潜能。特定的微小RNA是否有助于优化和限制基因表达,进而可用于操控胚胎干细胞的分化,这在很大程度上尚未得到探索。在此,我们表明两种血清反应因子(SRF)依赖性的肌肉特异性微小RNA,即miR-1和miR-133,可促进胚胎干细胞向中胚层的形成,但在进一步分化为心肌祖细胞的过程中具有相反的功能。此外,在小鼠和人类胚胎干细胞分化过程中,miR-1和miR-133是非肌肉基因表达和细胞命运的有效抑制因子。miR-1的作用部分是通过对Notch配体Delta样1(Dll-1)的翻译抑制来介导的。我们的研究结果表明,肌肉特异性微小RNA在细胞谱系定向过程中加强了对非肌肉基因的沉默,并提示微小RNA在调控多能胚胎干细胞的细胞命运决定方面可能具有普遍用途。
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