首页> 外文期刊>Mutation Research: International Journal on Mutagenesis, Chromosome Breakage and Related Subjects >Sex-specific radiation-induced microRNAome responses in the hippocampus, cerebellum and frontal cortex in a mouse model.
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Sex-specific radiation-induced microRNAome responses in the hippocampus, cerebellum and frontal cortex in a mouse model.

机译:在小鼠模型中,海马,小脑和额叶皮层中由性别特异性辐射诱导的microRNAome反应。

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Ionizing radiation is an important treatment modality, but it is also a well-known genotoxic agent capable of damaging cells and tissues. Therefore radiation treatment can cause numerous side effects in exposed tissues and organs. Radiotherapy is a part of the front-line treatment regime for brain cancer patients, but can cause severe functional and morphological changes in exposed brain tissues. However, the mechanisms of radiation-induced effects in the brain are not well understood and are under-investigated. Recent data has implicated short RNAs, especially microRNAs, as important in radiation responses, yet nothing is known about radiation-induced changes in the brain microRNAome. We analyzed the effects of X-ray irradiation on microRNA expression in the hippocampus, frontal cortex, and cerebellum of male and female mice. Here, we report tissue-, time-, and sex-specific brain radiation responses, as well as show evidence of an interplay between microRNAs and their targets. Specifically, we show that changes in the expression of the miR-29 family may be linked, at least in part, to altered expression of de novo methyltransferase DNMT3a and changed global DNA methylation levels. Further, these sex-specific epigenetic changes may be correlated to the prevalence of radiation-induced cancers in males. We identified several microRNAs that can potentially serve as biomarkers of brain radiation exposure. In summary, our study may provide an important roadmap for further analysis of microRNA expression in different brain regions of male and female mice and for detailed dissection of radiation-induced brain responses.
机译:电离辐射是一种重要的治疗方式,但它也是众所周知的能够破坏细胞和组织的遗传毒性剂。因此,放射治疗可在暴露的组织和器官中引起许多副作用。放射疗法是脑癌患者一线治疗方案的一部分,但会在裸露的脑组织中引起严重的功能和形态变化。但是,对大脑中辐射诱发作用的机制尚未完全了解,并且研究不足。最近的数据暗示短RNA,特别是microRNA在辐射反应中很重要,但关于辐射诱导的大脑microRNAome的变化一无所知。我们分析了X射线辐射对雄性和雌性小鼠海马,额叶皮层和小脑中microRNA表达的影响。在这里,我们报告了组织,时间和性别特异性的脑辐射反应,并显示了microRNA及其靶标之间相互作用的证据。具体而言,我们表明miR-29家族表达的变化可能至少部分与从头甲基转移酶DNMT3a的表达变化和全球DNA甲基化水平改变有关。此外,这些性别特异的表观遗传学变化可能与男性中辐射诱发的癌症的患病率相关。我们鉴定了几种可能作为脑辐射暴露生物标志物的microRNA。总而言之,我们的研究可能为进一步分析雄性和雌性小鼠不同大脑区域中的microRNA表达以及辐射诱导的脑反应的详细解剖提供重要的路线图。

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