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在与人类相关的低剂量率下,伽马辐射对小鼠具有遗传毒性。

Gamma radiation at a human relevant low dose rate is genotoxic in mice.

机构信息

Department of Chemicals and Radiation, Norwegian Institute of Public Health, Oslo 0403, Norway.

Centre for Environmental Radioactivity (CoE CERAD), Ås 1432, Norway.

出版信息

Sci Rep. 2016 Sep 6;6:32977. doi: 10.1038/srep32977.

Abstract

Even today, 70 years after Hiroshima and accidents like in Chernobyl and Fukushima, we still have limited knowledge about the health effects of low dose rate (LDR) radiation. Despite their human relevance after occupational and accidental exposure, only few animal studies on the genotoxic effects of chronic LDR radiation have been performed. Selenium (Se) is involved in oxidative stress defence, protecting DNA and other biomolecules from reactive oxygen species (ROS). It is hypothesised that Se deficiency, as it occurs in several parts of the world, may aggravate harmful effects of ROS-inducing stressors such as ionising radiation. We performed a study in the newly established LDR-facility Figaro on the combined effects of Se deprivation and LDR γ exposure in DNA repair knockout mice (Ogg1(-/-)) and control animals (Ogg1(+/-)). Genotoxic effects were seen after continuous radiation (1.4 mGy/h) for 45 days. Chromosomal damage (micronucleus), phenotypic mutations (Pig-a gene mutation of RBC(CD24-)) and DNA lesions (single strand breaks/alkali labile sites) were significantly increased in blood cells of irradiated animals, covering three types of genotoxic activity. This study demonstrates that chronic LDR γ radiation is genotoxic in an exposure scenario realistic for humans, supporting the hypothesis that even LDR γ radiation may induce cancer.

摘要

即使在今天,广岛事件和切尔诺贝利、福岛等事故发生 70 年后,我们对于低剂量率(LDR)辐射对健康的影响仍然知之甚少。尽管在职业和意外暴露后,这些影响与人类息息相关,但只有少数关于慢性 LDR 辐射的遗传毒性影响的动物研究。硒(Se)参与氧化应激防御,保护 DNA 和其他生物分子免受活性氧(ROS)的伤害。有人假设,硒缺乏,如在世界上的一些地区发生的那样,可能会加剧 ROS 诱导的应激源(如电离辐射)的有害影响。我们在新建立的 Figaro LDR 设施中进行了一项研究,研究了 Se 缺乏和 LDR γ 暴露在 DNA 修复基因敲除小鼠(Ogg1(-/-))和对照动物(Ogg1(+/-))中的联合作用。连续辐射(1.4 mGy/h)45 天后,出现了遗传毒性效应。染色体损伤(微核)、表型突变(RBC(CD24-)的 Pig-a 基因突变)和 DNA 损伤(单链断裂/碱不稳定位点)在照射动物的血细胞中显著增加,涵盖了三种遗传毒性活性。这项研究表明,慢性 LDR γ 辐射在人类暴露场景中具有遗传毒性,支持了即使是 LDR γ 辐射也可能引发癌症的假设。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/76f6/5011728/1948e63c128d/srep32977-f1.jpg

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