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长程相互作用在骨骼肌分化过程中调节 Igf2 基因转录。

Long range interactions regulate Igf2 gene transcription during skeletal muscle differentiation.

机构信息

Department of Biochemistry and Molecular Biology, Oregon Health & Science University, Portland, Oregon 97239-3098, USA.

出版信息

J Biol Chem. 2010 Dec 10;285(50):38969-77. doi: 10.1074/jbc.M110.160986. Epub 2010 Oct 11.

Abstract

The differentiation, maintenance, and repair of skeletal muscle is controlled by interactions between genetically determined transcriptional programs regulated by myogenic transcription factors and environmental cues activated by growth factors and hormones. Signaling through the insulin-like growth factor 1 (IGF1) receptor by locally produced IGF2 defines one such pathway that is critical for normal muscle growth and for regeneration after injury. IGF2 gene and protein expression are induced as early events in muscle differentiation, but the responsible molecular mechanisms are unknown. Here we characterize a distal DNA element within the imprinted mouse Igf2-H19 locus with properties of a muscle transcriptional enhancer. We find that this region undergoes a transition to open chromatin during differentiation, whereas adjacent chromatin remains closed, and that it interacts in differentiating muscle nuclei but not in mesenchymal precursor cells with the Igf2 gene found more than 100 kb away, suggesting that chromatin looping or sliding to bring the enhancer in proximity to Igf2 promoters is also an early event in muscle differentiation. Because this element directly stimulates the transcriptional activity of an Igf2 promoter-reporter gene in differentiating myoblasts, our results indicate that we have identified a bona fide distal transcriptional enhancer that supports Igf2 gene activation in skeletal muscle cells. Because this DNA element is conserved in the human IGF2-H19 locus, our results further suggest that its muscle enhancer function also is conserved among different mammalian species.

摘要

骨骼肌肉的分化、维持和修复受遗传决定的转录程序与由生长因子和激素激活的环境线索之间的相互作用控制,这些转录程序由肌源性转录因子调节。局部产生的 IGF2 通过胰岛素样生长因子 1 (IGF1) 受体的信号转导定义了这样一条途径,该途径对于正常肌肉生长和损伤后再生至关重要。IGF2 基因和蛋白表达作为肌肉分化的早期事件被诱导,但负责的分子机制尚不清楚。在这里,我们描述了一个位于印记的小鼠 Igf2-H19 基因座内的远端 DNA 元件,该元件具有肌肉转录增强子的特性。我们发现,该区域在分化过程中向开放染色质转变,而相邻染色质保持关闭,并且在分化的肌肉核中与位于 100kb 以上的 Igf2 基因相互作用,但在间充质前体细胞中不相互作用,这表明染色质环化或滑动将增强子带到 Igf2 启动子附近也是肌肉分化的早期事件。由于该元件直接刺激分化的成肌细胞中 Igf2 启动子报告基因的转录活性,我们的结果表明,我们已经鉴定出一个真正的远端转录增强子,它支持骨骼肌细胞中 Igf2 基因的激活。由于该 DNA 元件在人类 IGF2-H19 基因座中保守,我们的结果进一步表明,其肌肉增强子功能在不同的哺乳动物物种中也保守。

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