首页> 外文期刊>Mutation Research: International Journal on Mutagenesis, Chromosome Breakage and Related Subjects >The effects of in utero irradiation on mutation induction and transgenerational instability in mice.
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The effects of in utero irradiation on mutation induction and transgenerational instability in mice.

机译:宫内照射对小鼠突变诱导和转基因不稳定性的影响。

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Epidemiological evidence suggests that the deleterious effects of prenatal irradiation can manifest during childhood, resulting in an increased risk of leukaemia and solid cancers after birth. However, the mechanisms underlying the long-term effects of foetal irradiation remain poorly understood. This study was designed to analyse the impact of in utero irradiation on mutation rates at expanded simple tandem repeat (ESTR) DNA loci in directly exposed mice and their first-generation (F(1)) offspring. ESTR mutation frequencies in the germline and somatic tissues of male and female mice irradiated at 12 days of gestation remained highly elevated during adulthood, which was mainly attributed to a significant increase in the frequency of singleton mutations. The prevalence of singleton mutations in directly exposed mice suggests that foetal irradiation results in genomic instability manifested both in utero and during adulthood. The frequency of ESTR mutation in the F(1) offspring of prenatally irradiated male mice was equally elevated across all tissues, which suggests that foetal exposure results in transgenerational genomic instability. In contrast, maternal in utero exposure did not affect the F(1) stability. Our data imply that the passive erasure of epigenetic marks in the maternal genome can diminish the transgenerational effects of foetal irradiation and therefore provide important clues to the still unknown mechanisms of radiation-induced genomic instability. The results of this study offer a plausible explanation for the effects of in utero irradiation on the risk of leukaemia and solid cancers after birth.
机译:流行病学证据表明,产前辐射的有害影响可能在儿童时期显现出来,导致出生后患白血病和实体癌的风险增加。但是,对胎儿辐射的长期影响的潜在机制仍知之甚少。这项研究旨在分析子宫内辐射对直接暴露小鼠及其第一代(F(1))后代中扩展的简单串联重复序列(ESTR)DNA位点突变率的影响。在成年期12天照射后,雄性和雌性小鼠的种系和体细胞组织中的ESTR突变频率在成年期仍然很高,这主要归因于单例突变频率的显着增加。在直接暴露的小鼠中单胎突变的流行表明,胎儿辐射导致子宫内和成年期均表现出基因组不稳定。在所有组织中,经产前照射的雄性小鼠的F(1)后代中ESTR突变的频率在所有组织中均升高,这表明胎儿暴露会导致跨代基因组不稳定。相反,孕妇在子宫内暴露不会影响F(1)的稳定性。我们的数据表明,母体基因组中表观遗传标记的被动消除可减少胎儿辐射的跨代效应,因此可为仍然未知的辐射诱导的基因组不稳定机制提供重要线索。这项研究的结果为子宫内辐射对出生后白血病和实体癌风险的影响提供了合理的解释。

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