Genetic radiation risks: a neglected topic in the low dose debate.

Q3 Medicine
Environmental Health and Toxicology Pub Date : 2016-01-20 eCollection Date: 2016-01-01 DOI:10.5620/eht.e2016001
Inge Schmitz-Feuerhake, Christopher Busby, Sebastian Pflugbeil
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引用次数: 0

Abstract

Objectives: To investigate the accuracy and scientific validity of the current very low risk factor for hereditary diseases in humans following exposures to ionizing radiation adopted by the United Nations Scientific Committee on the Effects of Atomic Radiation and the International Commission on Radiological Protection. The value is based on experiments on mice due to reportedly absent effects in the Japanese atomic bomb (Abomb) survivors.

Methods: To review the published evidence for heritable effects after ionising radiation exposures particularly, but not restricted to, populations exposed to contamination from the Chernobyl accident and from atmospheric nuclear test fallout. To make a compilation of findings about early deaths, congenital malformations, Down's syndrome, cancer and other genetic effects observed in humans after the exposure of the parents. To also examine more closely the evidence from the Japanese A-bomb epidemiology and discuss its scientific validity.

Results: Nearly all types of hereditary defects were found at doses as low as one to 10 mSv. We discuss the clash between the current risk model and these observations on the basis of biological mechanism and assumptions about linear relationships between dose and effect in neonatal and foetal epidemiology. The evidence supports a dose response relationship which is non-linear and is either biphasic or supralinear (hogs-back) and largely either saturates or falls above 10 mSv.

Conclusions: We conclude that the current risk model for heritable effects of radiation is unsafe. The dose response relationship is non-linear with the greatest effects at the lowest doses. Using Chernobyl data we derive an excess relative risk for all malformations of 1.0 per 10 mSv cumulative dose. The safety of the Japanese A-bomb epidemiology is argued to be both scientifically and philosophically questionable owing to errors in the choice of control groups, omission of internal exposure effects and assumptions about linear dose response.

遗传辐射风险:低剂量辩论中一个被忽视的话题。
目标:调查联合国原子辐射影响问题科学委员会和国际辐射防护委员会目前采用的电离辐射照射后人类遗传性疾病极低风险系数的准确性和科学性。该数值是根据日本原子弹(原子弹爆炸)幸存者据说没有受到影响而对小鼠进行的实验得出的:审查已发表的电离辐射照射后遗传效应的证据,特别是(但不限于)切尔诺贝利事故和大气层核试验尘降物污染的人群。汇编有关父母受辐照后人类早亡、先天畸形、唐氏综合症、癌症和其他遗传影响的研究结果。同时更仔细地研究日本原子弹爆炸流行病学的证据,并讨论其科学性:结果:几乎所有类型的遗传缺陷都是在剂量低至 1 至 10 mSv 时发现的。我们根据生物机制以及新生儿和胎儿流行病学中剂量与效应之间线性关系的假设,讨论了当前风险模型与这些观察结果之间的冲突。证据表明,剂量反应关系是非线性的,要么是双相关系,要么是超线性关系(猪背关系),并且在 10 mSv 以上基本达到饱和或下降:我们的结论是,目前的辐射遗传效应风险模型是不安全的。剂量反应关系是非线性的,最低剂量的影响最大。利用切尔诺贝利的数据,我们得出所有畸形的超额相对风险为每 10 mSv 累积剂量 1.0。日本原子弹流行病学的安全性在科学和哲学上都是值得怀疑的,这是因为在选择对照组、忽略内部暴露效应和假设线性剂量反应方面存在错误。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
Environmental Health and Toxicology
Environmental Health and Toxicology Medicine-Public Health, Environmental and Occupational Health
CiteScore
2.50
自引率
0.00%
发文量
0
审稿时长
8 weeks
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