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首页> 外文期刊>Mutation Research: International Journal on Mutagenesis, Chromosome Breakage and Related Subjects >Low-dose ionizing radiation and chromosome translocations: a review of the major considerations for human biological dosimetry.
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Low-dose ionizing radiation and chromosome translocations: a review of the major considerations for human biological dosimetry.

机译:低剂量电离辐射和染色体易位:人类生物学剂量学的主要考虑因素的综述。

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摘要

Chromosome translocations are a molecular signature of ionizing radiation exposure. Translocations persist significantly longer after exposure than other types of chromosome exchanges such as dicentrics. This persistence makes translocations the preferred aberration type for performing radiation dosimetry under conditions of protracted exposure or when exposure assessments are temporally delayed. Low doses of radiation are inherently difficult to quantify because the frequency of induced events is low and the background level of translocations among unexposed subjects can show considerable variability. Analyses of translocation frequencies can be confounded by several factors, including age of the subject, lifestyle choices such as cigarette smoking, the presence of clones of abnormal cells, and possibly genotypic variability among subjects. No significant effects of gender or race have been observed, but racial differences have not been completely ruled out. Translocation analyses may be complicated by the presence of different types of exchanges, i.e., reciprocal or non-reciprocal, and because translocations sometimes occur as a component of complex exchanges that include other forms of chromosome rearrangements. Rates of radiation exposure, ranging from acute to chronic, are known to influence the accumulation of translocations and may also affect their persistence. The influences on translocation frequencies of low-dose radiation hypersensitivity as well as the bystander effect and the adaptive response remain poorly characterized. Thus, quantifying the relationship between radiation dose and the frequency of translocations in any given subject requires attention to multiple issues. Part of the solution to understanding the in vivo dose-response relationship is to have accurate estimates of the baseline levels of translocations in healthy unexposed subjects, and some work in this area has been accomplished. Long-term cytogenetic follow-up of exposed subjects is needed to characterize translocation persistence, which is especially relevant for risk analyses. More work also needs to be done in the area of quantifying the role of known confounders. Characterizing the role of genotype will be especially important. Improvements in the ability to use translocation frequencies for low-dose biological dosimetry will require scoring very large numbers of cells per subject, which may be accomplished by developing a rapid automated image analysis system. This work would enhance our comprehension of the effects of low-dose radiation exposure and could lead to significant improvements in understanding the relationship between chromosome damage and human health.
机译:染色体易位是电离辐射暴露的分子特征。与其他类型的染色体交换(如双着丝粒)相比,暴露后易位持续的时间明显更长。这种持久性使易位型成为在长时间暴露或暴露评估时间延迟的情况下进行辐射剂量测定的首选像差类型。低剂量的辐射本来就难以量化,因为诱发事件的频率低,未暴露对象之间的易位背景水平可能显示出很大的可变性。易位频率的分析可能与多种因素混淆,包括受试者的年龄,生活方式选择(如吸烟),异常细胞克隆的存在以及受试者之间的基因型变异性。尚未观察到性别或种族的重大影响,但尚未完全排除种族差异。易位分析可能因存在不同类型的交换(即互惠或不可互惠)而变得复杂,并且因为易位有时会作为复杂交换的一部分而发生,包括其他形式的染色体重排。已知从急性到慢性的辐射暴露率会影响易位的积累,也可能影响其持久性。低剂量辐射超敏反应对易位频率的影响以及旁观者效应和适应性反应仍然很差。因此,量化任何给定受试者的辐射剂量与易位频率之间的关系都需要注意多个问题。理解体内剂量-反应关系的部分解决方案是对健康未暴露受试者的易位基线水平进行准确估计,并且已经完成了该领域的一些工作。需要对暴露的受试者进行长期的细胞遗传学随访,以表征易位持续性,这与风险分析尤其相关。在量化已知混杂因素的作用方面还需要做更多的工作。表征基因型的作用将特别重要。使用易位频率进行低剂量生物剂量测定的能力的提高将需要为每个受试者计分非常大量的细胞,这可以通过开发快速的自动化图像分析系统来实现。这项工作将增强我们对低剂量辐射暴露影响的理解,并可能导致对染色体损伤与人类健康之间关系的理解有了显着改善。

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