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首页> 外文期刊>American Journal of Physiology >MicroRNA-206 is overexpressed in the diaphragm but not the hindlimb muscle of mdx mouse.
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MicroRNA-206 is overexpressed in the diaphragm but not the hindlimb muscle of mdx mouse.

机译:MicroRNA-206在mdx小鼠的横diaphragm膜而不是后肢肌肉中过表达。

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MicroRNAs are highly conserved, noncoding RNAs involved in posttranscriptional gene silencing. MicroRNAs have been shown to be involved in a range of biological processes, including myogenesis and muscle regeneration. The objective of this study was to test the hypothesis that microRNA expression is altered in dystrophic muscle, with the greatest change occurring, of the muscles examined, in the diaphragm. The expression of the muscle-enriched microRNAs was determined in the soleus, plantaris, and diaphragm muscles of control and dystrophin-deficient (mdx) mice by semiquantitative PCR. In the soleus and plantaris, expression of the mature microRNA 133a (miR-133a) and miR-206, respectively, was decreased by approximately 25%, whereas in the diaphragm, miR-206 expression increased by 4.5-fold relative to control. The increased expression of miR-206 in the mdx diaphragm was paralleled by a 4.4-fold increase in primary miRNA-206 (pri-miRNA-206) transcript level. Expression of Myod1 was elevated 2.7-fold only in the mdx diaphragm, consistent with an earlier finding demonstrating Myod1 can activate pri-miRNA-206 transcription. Transcript levels of Drosha and Dicer, major components of microRNA biogenesis pathway, were unchanged in mdx muscle, suggesting the pathway is not altered under dystrophic conditions. Previous in vitro analysis found miR-206 was capable of repressing utrophin expression; however, under dystrophic conditions, both utrophin transcript and protein levels were significantly increased by 69% and 3.9-fold, respectively, a finding inconsistent with microRNA regulation. These results are the first to report alterations in expression of muscle-enriched microRNAs in skeletal muscle of the mdx mouse, suggesting microRNAs may have a role in the pathophysiology of muscular dystrophy.
机译:MicroRNA是高度保守的非编码RNA,参与转录后基因沉默。 MicroRNA已显示出参与一系列生物过程,包括肌发生和肌肉再生。这项研究的目的是检验以下假设:营养不良的肌肉中microRNA的表达发生了改变,而隔膜中的肌肉发生了最大的变化。通过半定量PCR确定了对照组和肌营养不良蛋白缺乏(mdx)小鼠的比目鱼,plant肌和diaphragm肌中富含肌肉的microRNA的表达。在比目鱼和plant肌中,成熟的microRNA 133a(miR-133a)和miR-206的表达分别降低了约25%,而在隔膜中,miR-206的表达相对于对照增加了4.5倍。 miR-206在mdx隔膜中表达的增加与主要miRNA-206(pri-miRNA-206)转录水平的4.4倍增加平行。 Myod1的表达仅在mdx隔膜中升高了2.7倍,这与更早的发现表明Myod1可以激活pri-miRNA-206转录相一致。 microRNA生物发生途径的主要成分Drosha和Dicer的转录水平在mdx肌肉中没有变化,表明该途径在营养不良条件下没有改变。先前的体外分析发现,miR-206能够抑制卵磷脂的表达。然而,在营养不良的条件下,促卵磷脂的转录本和蛋白质水平分别显着增加了69%和3.9倍,这与microRNA调节不一致。这些结果是第一个报告mdx小鼠骨骼肌中富含肌肉的microRNA表达变化的提示,表明microRNA可能在肌营养不良的病理生理中起作用。

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