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INDUCTION OF MITOCHONDRIAL DNA DELETION BY IONIZING RADIATION IN HUMAN LUNG FIBROBLAST IMR-90 CELLS  

Eom, Hyeon-Soo (Radiation Biotechnology Research Division, Korea Atomic Energy Research Institute)
Jung, U-Hee (Radiation Biotechnology Research Division, Korea Atomic Energy Research Institute)
Park, Hae-Ran (Radiation Biotechnology Research Division, Korea Atomic Energy Research Institute)
Jo, Sung-Kee (Radiation Biotechnology Research Division, Korea Atomic Energy Research Institute)
Publication Information
Journal of Radiation Protection and Research / v.34, no.2, 2009 , pp. 49-54 More about this Journal
Abstract
Mitochondrial DNA (mtDNA) deletion is a well-known marker for oxidative stress and aging and also contributes to their unfavorable effects in cultured cells and animal tissues. This study was conducted to investigate the effect of ionizing radiation (IR) on mtDNA deletion and the involvement of reactive oxygen species (ROS) in this process in human lung fibroblast (IMR-90) cells. Young IMR-90 cells at population doubling (PD) 39 were irradiated with $^{137}Cs$ $\gamma$-rays and the intracellular ROS level was determined by 2',7'-dichlorofluorescein diacetate (DCFH-DA) and mtDNA common deletion (4977bp) was detected by nested PCR. Old cells at PD 55 and $H_2O_2$-treated young cells were compared as the positive control. IR increased the intracellular ROS level and mtDNA 4977 bp deletion in IMR-90 cells dose-dependently. The increases of ROS level and mtDNA deletion were also observed in old cells and $H_2O_2$-treated young cells. To confirm the increased ROS level is essential for mtDNA deletion in irradiated cells, the effects of N-acetylcysteine (NAC) on IRinduced ROS and mtDNA deletion were examined. 5 mM NAC significantly attenuated the IR-induced ROS increase and mtDNA deletion. These results suggest that IR induces the mtDNA deletion and this process is mediated by ROS in IMR-90 cells.
Keywords
Ionizing Radiation; Mitochondrial DNA Deletion; Reactive Oxygen Species; Aging;
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