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Humans are daily exposed to background radiation and various sources of oxidative stress. My research has focused in the last 12 years on the effects of ionizing radiation on DNA, which is considered as the key target of radiation in the cell. Ionizing radiation and endogenous cellular oxidative stress can also induce closely spaced oxidatively induced DNA lesions called 'clusters' of DNA damage or locally multiply damage sites, as first introduced by John Ward. I am now interested in the repair mechanisms of clustered DNA damage, which is considered as the most difficult for the cell to repair. A main part of my research is devoted to evaluating the role of clustered DNA damage in the promotion of carcinogenesis in vitro and in vivo . Currently in my laboratory, there are two main ongoing projects. (1) Study of the role of BRCA1 and DNA-dependent protein kinase catalytic subunit repair proteins in the processing of clustered DNA damage in human cancer cells. For this project, we use several tumor cell lines, such as breast cancer cell lines MCF-7 and HCC1937 (BRCA1 deficient) and human glioblastoma cells MO59J/K; and (2) Possible use of DNA damage clusters as novel cancer biomarkers for prognostic and therapeutic applications related to modulation of oxidative stress. In this project human tumor and mice tissues are being used.
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篇名 Detection of clustered DNA lesions: Biological and clinical applications
来源期刊 世界生物化学杂志:英文版(电子版) 学科 生物学
关键词 DNA DAMAGE CLUSTERS DNA REPAIR OXIDATIVE stress Cancer Biomarkers
年,卷(期) 2011,(7) 所属期刊栏目
研究方向 页码范围 173-176
页数 4页 分类号 Q523
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DNA
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CLUSTERS
DNA
REPAIR
OXIDATIVE
stress
Cancer
Biomarkers
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世界生物化学杂志:英文版(电子版)
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1949-8454
北京市朝阳区东四环中路62号楼远洋国际中
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