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首页> 外文期刊>Nature Communications >Alternative splicing regulates vesicular trafficking genes in cardiomyocytes during postnatal heart development
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Alternative splicing regulates vesicular trafficking genes in cardiomyocytes during postnatal heart development

机译:出生后心脏发育过程中的可变剪接调节心肌细胞中的水泡运输基因

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During postnatal development the heart undergoes a rapid and dramatic transition to adult function through transcriptional and post-transcriptional mechanisms, including alternative splicing (AS). Here we perform deep RNA-sequencing on RNA from cardiomyocytes and cardiac fibroblasts to conduct a high-resolution analysis of transcriptome changes during postnatal mouse heart development. We reveal extensive changes in gene expression and AS that occur primarily between postnatal days 1 and 28. Cardiomyocytes and cardiac fibroblasts show reciprocal regulation of gene expression reflecting differences in proliferative capacity, cell adhesion functions and mitochondrial metabolism. We further demonstrate that AS plays a role in vesicular trafficking and membrane organization. These AS transitions are enriched among targets of two RNA-binding proteins, Celf1 and Mbnl1, which undergo developmentally regulated changes in expression. Vesicular trafficking genes affected by AS during normal development (when Celf1 is downregulated) show a reversion to neonatal splicing patterns after Celf1 re-expression in adults. Short-term Celf1 induction in adult animals results in disrupted transverse tubule organization and calcium handling. These results identify potential roles for AS in multiple aspects of postnatal heart maturation, including vesicular trafficking and intracellular membrane dynamics.RI Xia, Zheng/F-6561-2014OI Xia, Zheng/0000-0003-3364-8324
机译:在产后发育过程中,心脏会通过转录和转录后机制(包括选择性剪接(AS))迅速而急剧地转变为成年功能。在这里,我们对来自心肌细胞和心脏成纤维细胞的RNA进行深度RNA测序,以进行出生后小鼠心脏发育过程中转录组变化的高分辨率分析。我们揭示了主要在出生后第1至28天之间发生的基因表达和AS的广泛变化。心肌细胞和心脏成纤维细胞显示了基因表达的相互调节,反映了增殖能力,细胞粘附功能和线粒体代谢的差异。我们进一步证明AS在水泡运输和膜组织中发挥作用。这些AS转换丰富了两个RNA结合蛋白,Celf1和Mbnl1的靶标,它们经历了表达方面的发育调控。在正常发育过程中(当Celf1下调时)受AS影响的水泡运输基因在成人Celf1重新表达后表现出向新生儿剪接模式的回复。成年动物中的短期Celf1诱导会导致横向小管组织破坏和钙处理。这些结果确定了AS在产后心脏成熟的多个方面的潜在作用,包括水泡运输和细胞内膜动力学.RI Xia,Zheng / F-6561-2014OI Xia,Zheng / 0000-0003-3364-8324

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