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首页> 外文期刊>Nucleic Acids Research >Global MEF2 target gene analysis in cardiac and skeletal muscle reveals novel regulation of DUSP6 by p38MAPK-MEF2 signaling
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Global MEF2 target gene analysis in cardiac and skeletal muscle reveals novel regulation of DUSP6 by p38MAPK-MEF2 signaling

机译:心肌和骨骼肌中的全球MEF2靶基因分析揭示了p38MAPK-MEF2信号传导对DUSP6的新调节

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摘要

MEF2 plays a profound role in the regulation of transcription in cardiac and skeletal muscle lineages. To define the overlapping and unique MEF2A genomic targets, we utilized ChIP-exo analysis of cardiomyocytes and skeletal myoblasts. Of the 2783 and 1648 MEF2A binding peaks in skeletal myoblasts and cardiomyocytes, respectively, 294 common binding sites were identified. Genomic targets were compared to differentially expressed genes in RNA-seq analysis of MEF2A depleted myogenic cells, revealing two prominent genetic networks. Genes largely associated with muscle development were down-regulated by loss of MEF2A while up-regulated genes reveal a previously unrecognized function of MEF2A in suppressing growth/proliferative genes. Several up-regulated (Tprg, Mctp2, Kitl, Prrx1, Dusp6) and down-regulated (Atp1a2, Hspb7, Tmem182, Sorbs2, Lmod3) MEF2A target genes were chosen for further investigation. Interestingly, siRNA targeting of the MEF2A/D heterodimer revealed a somewhat divergent role in the regulation of Dusp6, a MAPK phosphatase, in cardiac and skeletal myogenic lineages. Furthermore, MEF2D functions as a p38MAPK-dependent repressor of Dusp6 in myoblasts. These data illustrate that MEF2 orchestrates both common and non-overlapping programs of signal-dependent gene expression in skeletal and cardiac muscle lineages.
机译:MEF2在心脏和骨骼肌谱系的转录调控中起着重要作用。为了定义重叠且独特的MEF2A基因组靶标,我们利用了心肌细胞和骨骼成肌细胞的ChIP-exo分析。在骨骼肌成肌细胞和心肌细胞的2783和1648 MEF2A结合峰中,分别鉴定出294个常见结合位点。在耗尽MEF2A的成肌细胞的RNA序列分析中,将基因组靶标与差异表达基因进行了比较,揭示了两个重要的遗传网络。由于MEF2A的缺失,与肌肉发育相关的基因被下调,而上调的基因则揭示了MEF2A在抑制生长/增殖基因方面先前未被认识的功能。选择了几个上调(Tprg,Mctp2,Kit1,Prrx1,Dusp6)和下调(Atp1a2,Hspb7,Tmem182,Sorbs2,Lmod3)的MEF2A靶基因进行进一步研究。有趣的是,靶向MEF2A / D异源二聚体的siRNA在心脏和骨骼肌成系谱系中对Dusp6(一种MAPK磷酸酶)的调控中显示出某种不同的作用。此外,MEF2D在成肌细胞中作为Dusp6的p38MAPK依赖性阻遏物起作用。这些数据说明,MEF2在骨骼肌和心肌谱系中协调信号依赖性基因表达的通用程序和非重叠程序。

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