电离辐射
DNA损伤
微核试验
化学
遗传毒性
癌症研究
DNA修复
顺铂
抗氧化剂
抑制器
基因组不稳定性
毒性
生物化学
DNA
生物
遗传学
化疗
基因
辐照
物理
有机化学
核物理学
作者
Seok Won Jeong,Hwa Jin Jung,Md Mujibur Rahman,Jee Na Hwang,Young Rok Seo
标识
DOI:10.1089/jmf.2007.0719
摘要
Ionizing radiation (IR) therapy has been widely employed in the treatment of cancer. However, certain issues, including toxicity, have been raised in conjunction with IR therapy for cancer. Recently, selenomethionine (SeMet) as an antioxidant has been the subject of a great deal of attention for its chemopreventive effects. In this study, we found that DNA repair activity has been enhanced in response to SeMet against IR. In addition, our data showed that p53 functional activity was significantly reduced against IR in the cells expressing a mutant form of redox factor 1 (Ref-1) contrast with Ref-1 wild-type cells treated with SeMet, suggesting that p53 activation under the modulation of Ref-1 might play an important role in IR-treated cells in the presence of SeMet. Furthermore, IR-induced micronuclei numbers were also reduced after treatment with SeMet, strongly implicating protection by SeMet in genomic stability against IR-induced genotoxicity. From this study, we suggest that the p53-mediated protective mechanism of SeMet might provide clues for reducing side effects of IR therapy.
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