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首页> 外文期刊>International Journal of Radiation Biology: Covering the Physical, Chemical, Biological, and Medical Effects of Ionizing and Non-ionizing Radiations >DNA DSB induced in human cells by charged particles and gamma rays: experimental results and theoretical approaches.
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DNA DSB induced in human cells by charged particles and gamma rays: experimental results and theoretical approaches.

机译:带电粒子和伽马射线在人细胞中诱导的DNA DSB:实验结果和理论方法。

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摘要

PURPOSE: To quantify the role played by radiation track structure and background fragments in modulating DNA fragmentation in human cells exposed to gamma-rays and light ions. MATERIALS AND METHODS: Human fibroblasts were exposed in vitro to different doses (in the range from 40 - 200 Gy) of (60)Co gamma-rays and 0.84 MeV protons (Linear Energy Transfer, LET, in tissue 28.5 keV/microm). The resulting DNA fragments were scored under two electrophoretic conditions, in order to optimize separation in the size ranges 0.023 - 1.0 Mbp and 1.0 - 5.7 Mbp. In parallel, DNA fragmentation was simulated both with a phenomenological approach based on the "generalized broken-stick" model, and with a mechanistic approach based on the PARTRAC (acronym of PARticle TRACk) Monte Carlo code (1.32 MeV photons were used for the simulation of (60)Co gamma-rays). RESULTS: For both gamma-rays and protons, the experimental dose response in the range 0.023 - 5.7 Mbp could be approximated as a straight line, the slope of which provided a yield of (5.3 +/- 0.4) x 10(-9) Gy(-1) bp(-1) for gamma-rays and (7.1 +/- 0.6) x 10(-9) Gy(-1) bp(-1) for protons, leading to a Relative Biological Effectiveness (RBE) of 1.3 +/- 0.2. From both theoretical analyses it appeared that, while gamma-ray data were consistent with double-strand breaks (DSB) random induction, protons at low doses showed significant deviation from randomness, implying enhanced production of small fragments in the low molecular weight part of the experimental range. The theoretical analysis of fragment production was then extended to ranges where data were not available, i.e. to fragments larger than 5.7 Mbp and smaller than 23 kbp. The main outcome was that small fragments (<23 kbp) are produced almost exclusively via non-random processes, since their number is considerably higher than that produced by a random insertion of DSB. Furthermore, for protons the number of these small fragments is a significant fraction (about 20%) of the total number of fragments; these fragments remain undetected in these experiments. Calculations for 3.3 MeV alpha particle irradiation (for which no experimental data were available) were performed to further investigate the role of fragments smaller than 23 kbp; in this case, besides the non-random character of their production, their number resulted to be at least as much as half of the total number of fragments. CONCLUSION: Comparison between experimental data and two different theoretical approaches provided further support to the hypothesis of an important role of track structure in modulating DNA damage. According to the theoretical approaches, non-randomness of fragment production was found for proton irradiation for the smaller fragments in the experimental size range and, in a significantly larger extent, for fragments of size less than 23 kbp, both for protons and alpha particles.
机译:用途:量化辐射径迹结构和背景片段在调节暴露于伽马射线和光离子的人类细胞中DNA片段化中的作用。材料与方法:将人类成纤维细胞在体外暴露于不同剂量(40-200 Gy)的(60)Coγ射线和0.84 MeV质子(线性能量转移,LET,组织中28.5 keV /微米)。在两个电泳条件下对所得的DNA片段进行评分,以优化在0.023-1.0 Mbp和1.0-5.7 Mbp大小范围内的分离。并行地,通过基于“广义破碎棒”模型的现象学方法和基于PARTRAC(PARticle TRACk的缩写)Monte Carlo代码(1.32 MeV光子)的机制方法,对DNA片段化进行了模拟。 (60)Co伽马射线)。结果:对于伽马射线和质子,在0.023-5.7 Mbp范围内的实验剂量响应可近似为一条直线,其斜率可提供(5.3 +/- 0.4)x 10(-9)的产量γ射线的Gy(-1)bp(-1)和质子的(7.1 +/- 0.6)x 10(-9)Gy(-1)bp(-1),导致相对生物有效性(RBE) 1.3 +/- 0.2。从这两个理论分析看来,尽管伽玛射线数据与双链断裂(DSB)随机诱导一致,但低剂量的质子显示出与随机性的显着偏离,这意味着小分子在低分子量部分的产生增加。实验范围。然后将片段产生的理论分析扩展到没有数据可用的范围,即扩展到大于5.7 Mbp且小于23 kbp的片段。主要结果是小片段(<23 kbp)几乎完全是通过非随机过程产生的,因为它们的数目比通过随机插入DSB产生的数目要高得多。此外,对于质子,这些小碎片的数量占碎片总数的很大一部分(约20%);这些片段在这些实验中未被发现。进行了3.3 MeVα粒子辐照的计算(尚无实验数据),以进一步研究小于23 kbp的片段的作用。在这种情况下,除了其生产具有非随机性之外,它们的数量至少是碎片总数的一半。结论:实验数据和两种不同理论方法之间的比较为轨道结构在调节DNA损伤中起重要作用的假设提供了进一步的支持。根据理论方法,发现质子辐照对于实验尺寸范围内的较小片段而言是非随机性的,对于质子和α粒子而言,对于小于23 kbp的片段而言,质子辐照的产生是非随机的。

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