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利用靶向和非靶向效应定量建模单一辐射束或空间辐射混合物引起的癌变。

Quantitative modeling of carcinogenesis induced by single beams or mixtures of space radiations using targeted and non-targeted effects.

机构信息

Center for Radiological Research, Columbia University Irving Medical Center, 630 West 168th St., New York, NY, 10032, USA.

Department of Mathematics, University of California, Berkeley, CA, 94720, USA.

出版信息

Sci Rep. 2021 Dec 6;11(1):23467. doi: 10.1038/s41598-021-02883-y.

Abstract

Ionizing radiations encountered by astronauts on deep space missions produce biological damage by two main mechanisms: (1) Targeted effects (TE) due to direct traversals of cells by ionizing tracks. (2) Non-targeted effects (NTE) caused by release of signals from directly hit cells. The combination of these mechanisms generates non-linear dose response shapes, which need to be modeled quantitatively to predict health risks from space exploration. Here we used a TE + NTE model to analyze data on APC mouse tumorigenesis induced by space-relevant doses of protons, He, C, O, Si or Fe ions, or γ rays. A customized weighted Negative Binomial distribution was used to describe the radiation type- and dose-dependent data variability. This approach allowed detailed quantification of dose-response shapes, NTE- and TE-related model parameters, and radiation quality metrics (relative biological effectiveness, RBE, and radiation effects ratio, RER, relative to γ rays) for each radiation type. Based on the modeled responses for each radiation type, we predicted the tumor yield for a Mars-mission-relevant mixture of these radiations, using the recently-developed incremental effect additivity (IEA) synergy theory. The proposed modeling approach can enhance current knowledge about quantification of space radiation quality effects, dose response shapes, and ultimately the health risks for astronauts.

摘要

宇航员在深空任务中遇到的电离辐射通过两种主要机制产生生物损伤

(1) 由电离轨迹直接穿过细胞引起的靶向效应 (TE)。(2) 由直接击中的细胞释放信号引起的非靶向效应 (NTE)。这些机制的结合产生了非线性剂量反应形状,需要进行定量建模以预测太空探索的健康风险。在这里,我们使用 TE+NTE 模型来分析与质子、He、C、O、Si 或 Fe 离子或 γ 射线相关的空间剂量诱导 APC 小鼠肿瘤形成的数据。使用定制的加权负二项式分布来描述辐射类型和剂量依赖性数据变异性。这种方法允许详细量化剂量反应形状、与 NTE 和 TE 相关的模型参数以及每种辐射类型的相对生物效应 (RBE) 和辐射效应比 (RER)(相对于 γ 射线)。基于每种辐射类型的建模响应,我们使用最近开发的增量效应相加 (IEA) 协同理论预测了火星任务相关混合辐射的肿瘤产量。所提出的建模方法可以增强当前关于空间辐射质量效应、剂量反应形状以及最终宇航员健康风险的量化知识。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/674b/8648899/5b5dfe1b5abe/41598_2021_2883_Fig1_HTML.jpg

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