Literature DB >> 31987474

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

Krishna Luitel1, Sang Bum Kim2, Summer Barron1, James A Richardson3, Jerry W Shay4.   

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-rasLA-1) 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→HeSi) and 3B-2 (SiHe→H) and used 30 cGy H single-ion beam as a reference. In this study we show that whole-body irradiation with H→HeSi increases the incidence of premalignant lesions and systemic oxidative stress in mice 100 days post-irradiation more than (SiHe→H) and H only irradiation. Additionally, we observed an increase in adenomas with atypia and adenocarcinomas in H→HeSi irradiated mice but not in (SiHe→H) or H (30 cGy) only irradiated mice. When we used the H→HeSi 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→HeSi induced oxidative stress and cancer initiation almost back to baseline. Thus, exposure to H→HeSi elicits significant changes in lung cancer initiation that can be mitigated using CDDO-EA.
Copyright © 2019. Published by Elsevier Ltd.

Entities:  

Keywords:  CDDO-EA; GCR simulation; Ionizing radiation; Multiple Ions

Year:  2019        PMID: 31987474      PMCID: PMC6991460          DOI: 10.1016/j.lssr.2019.07.011

Source DB:  PubMed          Journal:  Life Sci Space Res (Amst)        ISSN: 2214-5524


  39 in total

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5.  High-LET Radiation Increases Tumor Progression in a K-Ras-Driven Model of Lung Adenocarcinoma.

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Journal:  Radiat Res       Date:  2017-09-27       Impact factor: 2.841

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Authors:  Francis A Cucinotta; Khiet To; Eliedonna Cacao
Journal:  Life Sci Space Res (Amst)       Date:  2017-02-01

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Authors:  Aaron A Goodarzi; Angela T Noon; Penny A Jeggo
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9.  Residential radon exposure and lung cancer in Sweden.

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10.  Use of the γ-H2AX assay to investigate DNA repair dynamics following multiple radiation exposures.

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  1 in total

1.  Heavy-Ion-Induced Lung Tumors: Dose- & LET-Dependence.

Authors:  Polly Y Chang; James Bakke; Chris J Rosen; Kathleen A Bjornstad; Jian-Hua Mao; Eleanor A Blakely
Journal:  Life (Basel)       Date:  2022-06-17
  1 in total

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