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Ultra-short laser-accelerated proton pulses have similar DNA-damaging effectiveness but produce less immediate nitroxidative stress than conventional proton beams

机译:超短激光加速质子脉冲具有相似的DNA破坏效果但产生的即时氮氧化应力比常规质子束小

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摘要

Ultra-short proton pulses originating from laser-plasma accelerators can provide instantaneous dose rates at least 107-fold in excess of conventional, continuous proton beams. The impact of such extremely high proton dose rates on A549 human lung cancer cells was compared with conventionally accelerated protons and 90 keV X-rays. Between 0.2 and 2 Gy, the yield of DNA double strand breaks (foci of phosphorylated histone H2AX) was not significantly different between the two proton sources or proton irradiation and X-rays. Protein nitroxidation after 1 h judged by 3-nitrotyrosine generation was 2.5 and 5-fold higher in response to conventionally accelerated protons compared to laser-driven protons and X-rays, respectively. This difference was significant (p < 0.01) between 0.25 and 1 Gy. In conclusion, ultra-short proton pulses originating from laser-plasma accelerators have a similar DNA damaging potential as conventional proton beams, while inducing less immediate nitroxidative stress, which probably entails a distinct therapeutic potential.
机译:源自激光等离子加速器的超短质子脉冲可以提供的瞬时剂量率至少是常规连续质子束的10 7 倍。将这种极高的质子剂量率对A549人肺癌细胞的影响与常规加速质子和90 keV X射线进行了比较。在0.2和2 Gy之间,两个质子源或质子辐照和X射线之间的DNA双链断裂(磷酸化组蛋白H2AX的焦点)的产量没有显着差异。与传统的加速质子相比,由3-硝基酪氨酸的产生判断的1 h后的蛋白质硝化氧化分别是激光驱动质子和X射线的2.5和5倍。 0.25和1 Gy之间的差异非常显着(p <0.01)。总之,源自激光等离子加速器的超短质子脉冲具有与常规质子束相似的DNA破坏潜能,同时引起较少的即时氮氧化应激,这可能需要独特的治疗潜力。

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