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Protein and mIRNA profiling of radiation-induced skin injury in rats: the protective role of peroxiredoxin-6 against ionizing radiation

机译:放射线致大鼠皮肤损伤的蛋白质和mIRNA谱:peroxiredoxin-6对电离辐射的保护作用

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Radiation-induced skin injury is a serious concern during radiotherapy. However, the molecular mechanism underlying the pathogenesis of radiation-induced skin injury has not been extensively reported. Most biological functions are performed and regulated by proteins and noncoding RNAs, including microRNAs (miRNAs). The interplay between mRNA and miRNA has been implicated in disease initiation and progression. Technical advances in genomics and proteomics have enabled the exploration of the etiology of diseases and have the potential to broaden our understanding of the molecular pathogenesis of radiation-induced skin injury. In this study, we compared the protein and miRNA expression in rat skin irradiated with a 45-Gy electron beam with expression from adjacent normal tissues. We found 24 preferentially expressed proteins and 12 dysregulated miRNAs in irradiated skin. By analyzing the protein and miRNA profiles using bioinformatics tools, we identified a possible interaction between miR-214 and peroxiredoxin-6 (PRDX-6). Next, we investigated the expression of PRDX-6 and the consequences of its dysregulation. PRDX-6 is suppressed by radiation-inducible miR-214 and is involved in the pathogenesis of radiation-induced skin injury. Overexpression of PRDX-6 conferred radioresistance on cells, decreased cell apoptosis, and preserved mitochondrial integrity after radiation exposure. In addition, in vivo transfection with PRDX-6 reduced radiation-induced reactive oxygen species and the malondialdehyde concentration and ameliorated radiation-induced skin damage in rats. Our present findings illustrate the molecular changes during radiation-induced skin injury and the important role of PRDX-6 in ameliorating this damage in rats.
机译:放射线引起的皮肤损伤是放疗期间的严重问题。但是,尚未广泛报道辐射诱发的皮肤损伤的发病机理的分子机制。大多数生物学功能由蛋白质和非编码RNA(包括microRNA(miRNA))执行和调节。 mRNA和miRNA之间的相互作用已与疾病的发生和发展有关。基因组学和蛋白质组学的技术进步使人们能够探索疾病的病因,并有可能拓宽我们对放射线引起的皮肤损伤的分子发病机理的理解。在这项研究中,我们比较了用45 Gy电子束辐照的大鼠皮肤中蛋白质和miRNA的表达与邻近正常组织的表达。我们在辐照过的皮肤中发现了24种优先表达的蛋白质和12种失调的miRNA。通过使用生物信息学工具分析蛋白质和miRNA谱,我们确定了miR-214和peroxiredoxin-6(PRDX-6)之间的可能相互作用。接下来,我们研究了PRDX-6的表达及其失调的后果。 PRDX-6被放射线诱导的miR-214抑制,并参与放射线诱发的皮肤损伤的发病机理。 PRDX-6的过表达赋予细胞辐射抗性,减少细胞凋亡,并在辐射暴露后保留线粒体完整性。另外,用PRDX-6进行的体内转染可减少辐射诱导的反应性氧种类以及丙二醛浓度,并减轻辐射诱导的大鼠皮肤损伤。我们目前的发现说明了辐射引起的皮肤损伤过程中的分子变化以及PRDX-6在减轻大鼠这种损伤中的重要作用。

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