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Influence of Individual Radiosensitivity on the Hormesis Phenomenon: Toward a Mechanistic Explanation Based on the Nucleoshuttling of ATM Protein

机译:单个放射敏感性对血管素的机械解释对机械解释的影响

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摘要

Hormesis is a low-dose phenomenon that has been reported to occur, to different extents, in animals, plants, and microorganisms. However, a review of the literature shows that only a few reports describe it in humans. Also, the diversity of experimental protocols and cellular models used makes deciphering the mechanisms of hormesis difficult. In humans, hormesis mostly appears in the 20 to 75 mGy dose range and in nontransformed, radioresistant cells. In a previous paper by Devic et al, a biological interpretation of the adaptive response (AR) phenomenon was proposed using our model that is based on the radiation-induced nucleoshuttling of the ATM protein (the RIANS model). Here, we showed that the 20 to 75 mGy dose range corresponds to a maximum amount of ATM monomers diffusing into the nucleus, while no DNA double-strand breaks is produced by radiation. These ATM monomers are suggested to help in recognizing and repairing spontaneous DNA breaks accumulated in cells and contribute to reductions in genomic instability and aging. The RIANS model also permitted the biological interpretation of hypersensitivity to low doses (HRS)—another low-dose phenomenon. Hence, for the first time to our knowledge, hormesis, AR, and HRS can be explained using the same unified molecular model.
机译:血液化是据报道的低剂量现象,以发生在动物,植物和微生物中的不同范围内。然而,对文献的审查表明,只有几份报告只描述了人类。而且,使用的实验方案和蜂窝模型的多样性使得破译困难的棘手机制。在人类中,Homsesis主要出现在20至75 Mgy剂量范围内和非转化的放射体细胞中。在先前的文献中,使用我们的模型提出了一种基于ATM蛋白的辐射诱导的核动物(Rian模型)的模型来提出自适应响应(AR)现象的生物学解释。在这里,我们表明,20至75 MGY剂量范围对应于扩散到细胞核中的最大ATM单体量,而没有通过辐射产生DNA双链断裂。建议这些ATM单体有助于识别和修复累积在细胞中的自发DNA断裂,并有助于减少基因组不稳定性和衰老。诉讼模型还允许对低剂量(HRS)的过敏反应的生物解释 - 其他低剂量现象。因此,首次使用相同的统一分子模型来解释我们的知识,Homeresis,AR和HRS。

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