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A Single Whole-Body Low Dose X-Irradiation Does Not Affect L1 B1 and IAP Repeat Element DNA Methylation Longitudinally

机译:单个全身低剂量X射线照射不会纵向影响L1B1和IAP重复元素DNA甲基化

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摘要

The low dose radioadaptive response has been shown to be protective against high doses of radiation as well as aging-induced genomic instability. We hypothesised that a single whole-body exposure of low dose radiation would induce a radioadaptive response thereby reducing or abrogating aging-related changes in repeat element DNA methylation in mice. Following sham or 10 mGy X-irradiation, serial peripheral blood sampling was performed and differences in Long Interspersed Nucleic Element 1 (L1), B1 and Intracisternal-A-Particle (IAP) repeat element methylation between samples were assessed using high resolution melt analysis of PCR amplicons. By 420 days post-irradiation, neither radiation- or aging-related changes in the methylation of peripheral blood, spleen or liver L1, B1 and IAP elements were observed. Analysis of the spleen and liver tissues of cohorts of untreated aging mice showed that the 17–19 month age group exhibited higher repeat element methylation than younger or older mice, with no overall decline in methylation detected with age. This is the first temporal analysis of the effect of low dose radiation on repeat element methylation in mouse peripheral blood and the first to examine the long term effect of this dose on repeat element methylation in a radiosensitive tissue (spleen) and a tissue fundamental to the aging process (liver). Our data indicate that the methylation of murine DNA repeat elements can fluctuate with age, but unlike human studies, do not demonstrate an overall aging-related decline. Furthermore, our results indicate that a low dose of ionising radiation does not induce detectable changes to murine repeat element DNA methylation in the tissues and at the time-points examined in this study. This radiation dose is relevant to human diagnostic radiation exposures and suggests that a dose of 10 mGy X-rays, unlike high dose radiation, does not cause significant short or long term changes to repeat element or global DNA methylation.
机译:低剂量放射适应性反应已显示出对高剂量放射以及衰老引起的基因组不稳定性的保护作用。我们假设低剂量辐射的单个全身暴露会诱导放射适应性反应,从而减少或消除小鼠中重复元素DNA甲基化的衰老相关变化。在假手术或10 mGy X射线照射后,进行了系列外周血采样,并使用高分辨熔解分析法评估了样品之间长散布的核元素1(L1),B1和脑池内A颗粒(IAP)重复元素甲基化的差异。 PCR扩增子。照射后420天,未观察到与辐射或衰老相关的外周血,脾脏或肝脏L1,B1和IAP元素甲基化的变化。对未经治疗的衰老小鼠的脾脏和肝组织的分析表明,17-19个月大的组比年轻或年长的小鼠显示出更高的重复元件甲基化,但随着年龄的增长,甲基化没有整体下降。这是低剂量辐射对小鼠外周血中重复元素甲基化影响的第一个时间分析,也是第一个检查该剂量对放射敏感性组织(脾脏)和肝癌基本组织中重复元素甲基化的长期影响的方法。老化过程(肝脏)。我们的数据表明,鼠类DNA重复元件的甲基化会随着年龄而波动,但与人类研究不同,它并未显示出与衰老有关的总体下降。此外,我们的结果表明,在本研究中检查的时间点,低剂量的电离辐射不会诱导鼠类重复元件DNA甲基化的可检测变化。该辐射剂量与人类诊断辐射的暴露有关,并且表明与高剂量辐射不同,剂量为10 mGy的X射线不会引起重复元素或总体DNA甲基化的短期或长期显着变化。

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