The historical foundations of cancer risk assessment and its adoption by the US EPA in the mid 1970s were based on the discovery of X-ray-induced gene mutations by Hermann J. Muller, its transformation into the linear nonthreshold (LNT) single-hit theory and the recommendations of the model by the US National Academy of Sciences, Biological Effects of Atomic/Ionizing Radiation, Genetics Panels in 1956 and 1972. This testimony summarizes substantial recent revelations which profoundly challenge the use of LNT as a default in cancer risk assessment, showing multiple significant scientific errors and incorrect interpretations, mixed with deliberate misrepresentation of the scientific record by leading ideologically motivated radiation geneticists. These novel historical and scientific findings demonstrate that the scientific foundations of the LNT single-hit model were seriously flawed and should not have been adopted for cancer risk assessment. The testimony supports the recommendation by the EPA to move away from the use of the LNT as a default in cancer risk assessment and to the formal consideration of alternative dose response models such as the threshold, hormetic and other non-linear modeling approaches.
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机译:20世纪70年代中期癌症风险评估的历史基础及其美国EPA的通过是基于通过Hermann J. Muller发现的X射线诱导的基因突变,其转化为Linear Nonthreshold(LNT)单击理论以及美国国家科学院模型的建议,1956年和1972年的原子/电离辐射,遗传板的生物学作用。该证词总结了最近的最新启示令,这些启示彻底挑战了LNT作为癌症风险评估的违约,展示了多种重要的科学错误和不正确的解释,与思想辐射的辐射遗传学家领先的科学纪录的故意歪曲。这些新颖的历史和科学调查结果表明,LNT单人灾略模型的科学基础严重缺陷,不应用于癌症风险评估。该证词支持EPA的建议将LNT推移到癌症风险评估中的默认,并正式考虑替代剂量响应模型,例如阈值,刺激和其他非线性建模方法。
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