AI Article Synopsis

  • The study investigates the protective role of 8-oxoguanine glycosylase (OGG1) against radiation injury, comparing mutant KG-1 cells lacking OGG1 activity with wild-type U937 cells.
  • KG-1 displays significant radiation-induced cytotoxicities, including G2/M phase arrest, severe apoptosis, and inhibited cell growth, in contrast to the minimal effects seen in U937.
  • Findings indicate that OGG1 is crucial for cell survival during radiation damage, highlighting the toxic impact of 8-hydroxyguanine in DNA.

Article Abstract

To assess the role of 8-oxoguanine glycosylase (OGG1) in the cell defense against radiation injury, the radiation-induced cytotoxicities were compared between the mutant type KG-1 featuring a loss of OGG1 activity due to a homozygous mutation of Arg 229 Gln, and the wild type U937. While the following three obvious toxicities were displayed in KG-1, they were observed only minimally in U937. These were: a dramatic arrest at the G2/M phase indicated by a marked increase in both the number of G2/M cells and the expression of cyclin B1, cdc2, and mitotic phosphoprotein monoclonal-2 (MPM-2)-reactive proteins; a severe apoptosis shown by a marked increase in the number of cells with hypo-diploid DNA and DNA fragmentation; and as a result, a severe inhibition of cell growth and proliferation measured by the MTT test and [(3)H]-thymidine uptake assay. As expected, KG-1 exhibited a significant increase in the 8-hydroxyguanine level in DNA whereas U937 did not. However, the level of irradiation-induced lipid peroxidation was almost the same in both cell lines. All of these symptoms shown by KG-1 were observed in Molt-4 and CEM-CM3, which were also found to feature low OGG1 activity. These findings suggest that OGG1 plays an important role in cell survival from radiation-induced damage and are also indicative of the capability of 8-hydroxyguanine in DNA to induce cellular toxicities.

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Source
http://dx.doi.org/10.1016/s0891-5849(01)00793-6DOI Listing

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