Abstract

Mechanisms of Cellular and Molecular Radiosensitivity A detailed understanding of the mechanism which determine cellular radiosensitivity is necessary for the optimal use of radiation in medicine. The basic reactions caused by ionizing radiation decay very rapidly, and can damage any cellular (macro-molecules. The magnitude of the damage affecting DNA or DNA/ membrane has consistently been shown to directly affect cell survival at much later times. The chemical and/or biochemical (intra)cellular environment can be modified to favor either the repair or fixation of radiation- induced DNA damage, and a relatively simple 'competition-model', based on principles of radiation chemistry, is currently used to describe these modification. We have made detailed and quantitative test of the model, using cell survival as the assay system, and found discrepancies between predictions for the model and actual experimental results. These discrepancies could be caused by flaws or over-simplifications of the model. Alternatively, the action of the modifying chemicals could have changed the relationship between early DNA damage (occurring essentially at the same time as the radiation) and final assay (i.e. cell survival, assessed via colony formation after one week of growth). One goal of the proposed research is to continue to test the 'competition model' at the level of cell survival. Such test will include detailed measurements of the uptake and fate of aminothiol radiopretectors in mammalian cells. The affect of radioprotectors will be studied under conditions where specific mechanisms of action can be isolated (radiochemical depletion of radiosensitizers, scavenging of primary radicals, scavenging of secondary radicals, chelation of metals, inhibition of sensitizer transport and production of toxic intermediates). Other test of the model will include the effect of oxygen over a much broader rage of concentrations than has previously been possible. Special properties of nitroheterocyclic compounds will also be investigated. Effects of primary versus secondary radical scavengers will be assessed using nitrous oxide at high pressure, DMSO and formate. A second goal will be to assess DNA damage under the same conditions as the cell survival measurements. DNA damage assays will include alkaline elution and hydroxyl apatite chromatography for measuring single-strand breaks, and neutral elution for measuring double-strand breaks. The importance of crosslinks will be estimated. A third goal will be to consider more complex and realistic form of the 'competition model'.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
5R01CA049498-04
Application #
3193630
Study Section
Radiation Study Section (RAD)
Project Start
1989-05-15
Project End
1994-03-31
Budget Start
1992-04-01
Budget End
1993-03-31
Support Year
4
Fiscal Year
1992
Total Cost
Indirect Cost

  Institution

Name
University of Pennsylvania
Department
Type
Schools of Medicine
DUNS #
042250712
City
Philadelphia
State
PA
Country
United States
Zip Code
19104

  Publications

Ayene, Iraimoudi S; Koch, Cameron J; Krisch, Robert E (2007) DNA strand breakage by bivalent metal ions and ionizing radiation. Int J Radiat Biol 83:195-210
Biaglow, John E; Ayene, Iraimoudi S; Koch, Cameron J et al. (2003) Radiation response of cells during altered protein thiol redox. Radiat Res 159:484-94
Ayene, Iraimoudi S; Stamato, Thomas D; Mauldin, Stanley K et al. (2002) Mutation in the glucose-6-phosphate dehydrogenase gene leads to inactivation of Ku DNA end binding during oxidative stress. J Biol Chem 277:9929-35
Ayene, I S; Bernhard, E J; McKenna, W G et al. (2000) DNA as an important target in radiation-induced apoptosis of MYC and MYC plus RAS transfected rat embryo fibroblasts. Int J Radiat Biol 76:343-54
Biaglow, J E; Ayene, I S; Koch, C J et al. (2000) G6PD deficient cells and the bioreduction of disulfides: effects of DHEA, GSH depletion and phenylarsine oxide. Biochem Biophys Res Commun 273:846-52
Ayene, I S; Koch, C J; Tuttle, S W et al. (2000) Oxidation of cellular thiols by hydroxyethyldisulphide inhibits DNA double-strand-break rejoining in G6PD deficient mammalian cells. Int J Radiat Biol 76:1523-31
Kachur, A V; Koch, C J; Biaglow, J E (1999) Mechanism of copper-catalyzed autoxidation of cysteine. Free Radic Res 31:23-34
Horan, A D; Giandomenico, A R; Koch, C J (1999) Effect of oxygen on radiation-induced DNA damage in isolated nuclei. Radiat Res 152:144-53
Stevens, C W; Cerniglia, G J; Giandomenico, A R et al. (1998) DNA damaging agents improve stable gene transfer efficiency in mammalian cells. Radiat Oncol Investig 6:1-9
Biaglow, J E; Koch, C J; Tuttle, S W et al. (1998) The measurement of bioreductive capacity of tumor cells using methylene blue. Int J Radiat Oncol Biol Phys 42:769-73

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