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首页> 外文期刊>Genes and Development: a Journal Devoted to the Molecular Analysis of Gene Expression in Eukaryotes, Prokaryotes, and Viruses >PGC-1alpha regulates the neuromuscular junction program and ameliorates Duchenne muscular dystrophy.
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PGC-1alpha regulates the neuromuscular junction program and ameliorates Duchenne muscular dystrophy.

机译:PGC-1alpha调节神经肌肉接头程序并改善Duchenne肌营养不良症。

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摘要

The coactivator PGC-1alpha mediates key responses of skeletal muscle to motor nerve activity. We show here that neuregulin-stimulated phosphorylation of PGC-1alpha and GA-binding protein (GABP) allows recruitment of PGC-1alpha to the GABP complex and enhances transcription of a broad neuromuscular junction gene program. Since a subset of genes controlled by PGC-1alpha and GABP is dysregulated in Duchenne muscular dystrophy (DMD), we examined the effects of transgenic PGC-1alpha in muscle of mdx mice. These animals show improvement in parameters characteristic of DMD, including muscle histology, running performance, and plasma creatine kinase levels. Thus, control of PGC-1alpha levels in skeletal muscle could represent a novel avenue to prevent or treat DMD.
机译:辅助激活物PGC-1alpha介导骨骼肌对运动神经活动的关键反应。我们在这里显示,神经调节素刺激的PGC-1alpha和GA结合蛋白(GABP)的磷酸化允许PGC-1alpha募集到GABP复合物,并增强了广泛的神经肌肉连接基因程序的转录。由于在Duchenne肌营养不良症(DMD)中受PGC-1alpha和GABP控制的基因的一个子集失调,因此我们检查了转基因PGC-1alpha在mdx小鼠肌肉中的作用。这些动物在DMD的参数特征上有所改善,包括肌肉组织学,跑步表现和血浆肌酸激酶水平。因此,控制骨骼肌中PGC-1alpha的水平可能代表了预防或治疗DMD的新途径。

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