Abstract

The goal of this proposal is to determine if oxidative stress contributes to heat-induced radiosensitization in human tumor cells. The hypothesis and aims were chosen on the basis of preliminary results and published work which suggests: 1) hyperthermia causes oxidative stress, and 2) mechanisms of resistance to oxidative stress also confer resistance to heat-induced radiosensitization. The hypothesis is that heat-induced increases in prooxidant production and/or reductions in cellular antioxidant capacity contribute to heat- induced radiosensitization.
The Specific Aims will: 1) determine if heat (41 degree - 43 degreeC)- induced radiosensitization correlates with increased prooxidant production in human tumor cells. 2) determine if heat (41 degree - 43 degreeC)-induced radiosensitization correlates with alterations in cellular antioxidant capacity inhuman tumor cells, 3) determine if changes in prooxidant production or antioxidant capacity similar to those produces by hyperthermia, are capable of inducing radiosensitization in human tumor cell lines in the absence of hyperthermia, and 4) develop flow cytometric methods for assessing antioxidant/prooxidant balance in human tumor cells as a tool for determining if the above observations occur in human tumors in situ. In experiments yielding positive results, the effects of heat-induced oxidative stress on DNA damage and/or DNA repair following heat and radiation will also determined also in experiments yielding positive results, causality will be determined by inhibiting increases in prooxidant production and/or inhibiting alterations in antioxidant capacity and determining the effects on heat-induced radiosensitization. The information gathered in these studies will provide a rigorous evaluation of oxidative stress in mechanisms of heat-induced radiosensitization in human tumor cells. If oxidative stress is shown to contribute to heat-induced radiosensitization, then well characterized methods of modifying oxidative stress would become available for testing as modifiers of heat-induced radiosensitization, and provide a theoretical framework for the rational design of improved treatment protocols using this combined modality.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Program Projects (P01)
Project #
5P01CA075556-05
Application #
6467387
Study Section
Project Start
2001-07-01
Project End
2003-06-30
Budget Start
Budget End
Support Year
5
Fiscal Year
2001
Total Cost
Indirect Cost

  Institution

Name
Washington University
Department
Type
DUNS #
062761671
City
Saint Louis
State
MO
Country
United States
Zip Code
63130

  Publications

Sun, Lunching; Huang, Lei; Nguyen, Phuongmai et al. (2008) DNA methyltransferase 1 and 3B activate BAG-1 expression via recruitment of CTCFL/BORIS and modulation of promoter histone methylation. Cancer Res 68:2726-35
Iliakis, George; Wu, Wenqi; Wang, Minli (2008) DNA double strand break repair inhibition as a cause of heat radiosensitization: re-evaluation considering backup pathways of NHEJ. Int J Hyperthermia 24:17-29
Laszlo, Andrei; Davidson, Teri; Harvey, Amanda et al. (2006) Alterations in heat-induced radiosensitization accompanied by nuclear structure alterations in Chinese hamster cells. Int J Hyperthermia 22:43-60
Ahmad, Iman M; Aykin-Burns, Nukhet; Sim, Julia E et al. (2005) Mitochondrial O2*- and H2O2 mediate glucose deprivation-induced stress in human cancer cells. J Biol Chem 280:4254-63
Myerson, R J; Roti Roti, J L; Moros, E G et al. (2004) Modelling heat-induced radiosensitization: clinical implications. Int J Hyperthermia 20:201-12
Gius, David; Cui, Hengmi; Bradbury, C Matthew et al. (2004) Distinct effects on gene expression of chemical and genetic manipulation of the cancer epigenome revealed by a multimodality approach. Cancer Cell 6:361-71
Iliakis, G; Krieg, T; Guan, J et al. (2004) Evidence for an S-phase checkpoint regulating DNA replication after heat shock: a review. Int J Hyperthermia 20:240-9
Vanderwaal, R P; Roti Roti, J L (2004) Heat induced 'masking' of redox sensitive component(s) of the DNA-nuclear matrix anchoring complex. Int J Hyperthermia 20:234-9
Dynlacht, J R; Xu, M; Pandita, R K et al. (2004) Effects of heat shock on the Mre11/Rad50/Nbs1 complex in irradiated or unirradiated cells. Int J Hyperthermia 20:144-56
Lin, Xiao; Zhang, Fanjie; Bradbury, C Matthew et al. (2003) 2-Deoxy-D-glucose-induced cytotoxicity and radiosensitization in tumor cells is mediated via disruptions in thiol metabolism. Cancer Res 63:3413-7

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