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采用快速切换多离子束辐射的肺癌进展及对策预防。

Lung cancer progression using fast switching multiple ion beam radiation and countermeasure prevention.

机构信息

Department of Cell Biology, University of Texas Southwestern Medical Center, Dallas, TX 75390, USA.

Department of Cell Biology, University of Texas Southwestern Medical Center, Dallas, TX 75390, USA; Sevrance Biomedical Research Institute, Yonsei University College of Medicine, Seoul 03722, South Korea.

出版信息

Life Sci Space Res (Amst). 2020 Feb;24:108-115. doi: 10.1016/j.lssr.2019.07.011. Epub 2019 Aug 1.

Abstract

Most of the research in understanding space radiation-induced cancer progression and risk assessment has been performed using mono-energetic single-ion beams. However, the space radiation environment consists of a wide variety of ion species with a various range of energies. Using the fast beam switching technology developed at the NASA Space Radiation Laboratory (NSRL) at Brookhaven National Laboratory (BNL), ion species can be switched rapidly allowing investigators to use multiple ions with different energies to simulate more closely the radiation environment found in space. Here, we exposed a lung cancer susceptible mouse model (K-ras) to three sequential ion beams: Proton (H) (120 MeV/n) 20 cGy, Helium (He) (250 MeV/n) 5.0 cGy, and Silicon (Si) (300 MeV/n) 5.0 cGy with a dose rate of 0.5 cGy/min. Using three ion beams we performed whole body irradiation with a total dose of 30 cGy in two different orders: 3B-1 (H→He→Si) and 3B-2 (Si→He→H) and used 30 cGy H single-ion beam as a reference. In this study we show that whole-body irradiation with H→He→Si increases the incidence of premalignant lesions and systemic oxidative stress in mice 100 days post-irradiation more than (Si→He→H) and H only irradiation. Additionally, we observed an increase in adenomas with atypia and adenocarcinomas in H→He→Si irradiated mice but not in (Si→He→H) or H (30 cGy) only irradiated mice. When we used the H→He→Si irradiation sequence but skipped a day before exposing the mice to Si, we did not observe the increased incidence of cancer initiation and progression. We also found that a non-toxic anti-inflammatory, anti-oxidative radioprotector (CDDO-EA) reduced H→He→Si induced oxidative stress and cancer initiation almost back to baseline. Thus, exposure to H→He→Si elicits significant changes in lung cancer initiation that can be mitigated using CDDO-EA.

摘要

大多数研究理解太空辐射诱导癌症进展和风险评估都是使用单能单离子束进行的。然而,太空辐射环境由多种不同能量的离子组成。使用美国宇航局太空辐射实验室(NSRL)在布鲁克海文国家实验室(BNL)开发的快速束切换技术,研究者可以快速切换离子种类,使用不同能量的多种离子来更接近地模拟太空环境中的辐射环境。在这里,我们用三种连续的离子束照射一种肺癌易感小鼠模型(K-ras):质子(H)(120 MeV/n)20 cGy、氦(He)(250 MeV/n)5.0 cGy 和硅(Si)(300 MeV/n)5.0 cGy,剂量率为 0.5 cGy/min。我们使用三种离子束进行全身照射,总剂量为 30 cGy,两种不同的顺序:3B-1(H→He→Si)和 3B-2(Si→He→H),并使用 30 cGy H 单离子束作为参考。在这项研究中,我们发现全身照射 H→He→Si 比(Si→He→H)和 H 单离子束照射更能增加照射后 100 天小鼠的癌前病变和全身氧化应激的发生率。此外,我们观察到 H→He→Si 照射的小鼠中出现了具有非典型性的腺瘤和腺癌的数量增加,但在(Si→He→H)或 H(30 cGy)单离子束照射的小鼠中没有观察到。当我们使用 H→He→Si 照射顺序但在暴露于 Si 之前跳过一天时,我们没有观察到癌症起始和进展的发生率增加。我们还发现,一种无毒的抗炎、抗氧化辐射防护剂(CDDO-EA)可以降低 H→He→Si 诱导的氧化应激和癌症起始,使其几乎恢复到基线水平。因此,暴露于 H→He→Si 会引起肺癌起始的显著变化,而使用 CDDO-EA 可以减轻这种变化。

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