Abstract

The overall objective of the proposed research program is to test the hypothesis that measurable nuclear components are involved in the response- (s) of mammalian cells to therapeutic agents (ionizing radiation, hyper- thermia,,chemotherapeutic drugs, etc.). A condition sufficient to substan- tiate this hypothesis is that nuclei contain one or more measurable determinants of response to a given therapeutic modality. If this condi- tion is true, then it would follow that such measurable determinants would be candidates for potential clinically relevant predictive assays for therapeutic response. Therefore, we are proposing a series of research projects to investigate the relationships between specific nuclear (and related cytoplasmic) components and given cellular effects of certain therapeutic agents. These include nuclear determinants related to cell killing and/or damage repair following exposure to ionizing radiation or hyperthermia and determinants of cell proliferation and cell-cycle progres- sion. Emphasis is placed on ionizing radiation and hyperthermia because these modalities are used clinically and are not membrane limited. Cell proliferation is included logically because hyperthermia, ionizing radia- tion and certain chemotherapeutic agents induce cell-cycle perturbations that result in unbalanced growth, which in turn can affect the response to further treatment. In Project 1, a specific nuclear matrix protein will be studied in terms of its role in anchoring DNA loops and in radiosensitivit- y, which will provide insight into the mechanism(s) of repair and fixation of radiation damage. In Project 2, the interrelationship between the nuclear matrix and the cytoskeleton will be investigated in terms of cellular radiosensitivity. Work proposed in Project 3 will be to study the relationship between the nucleus and cytoplasm affecting the expression of lethal damage after hyperthermia. In contrast to Project 3, which will be done on tumor cells (in vitro and in vivo), Project 4 will investigate the effects of hyperthermia on a normal cell system, the macrophage system. Specifically, Project 4 will investigate the role of environmental factors in the responses of macrophages to hyperthermia. This system will allow us to find determinants for the induction of chronic thermotolerance. In Project 5, the relationship between cytoplasmic and nuclear proteins and perturbed cell-cycle transit will be studied. In this project we propose to find determinants of accelerated G1 transit resulting from unbalanced growth.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Program Projects (P01)
Project #
5P01CA051116-05
Application #
2094127
Study Section
Special Emphasis Panel (SRC (01))
Project Start
1990-04-01
Project End
1996-03-31
Budget Start
1994-04-01
Budget End
1996-03-31
Support Year
5
Fiscal Year
1994
Total Cost
Indirect Cost

  Institution

Name
Washington University
Department
Radiation-Diagnostic/Oncology
Type
Schools of Medicine
DUNS #
062761671
City
Saint Louis
State
MO
Country
United States
Zip Code
63130

  Publications

Ordoukhanian, P; Taylor, J S (2000) Caged single and double strand breaks. Bioconjug Chem 11:94-103
Roti Roti, J L; Gius, D; VanderWaal, R P et al. (2000) Changes in sub-nuclear structures and functional perturbations: implications for radiotherapy. J Cell Biochem Suppl Suppl 35:142-50
Guyton, K Z; Spitz, D R; Holbrook, N J (1996) Expression of stress response genes GADD153, c-jun, and heme oxygenase-1 in H2O2- and O2-resistant fibroblasts. Free Radic Biol Med 20:735-41
Chen, M S; Featherstone, T; Laszlo, A (1996) Amplification and altered expression of the hsc70/U14 snoRNA gene in a heat resistant Chinese hamster cell line. Cell Stress Chaperones 1:47-61
Desai, G R; Myerson, R J; Higashikubo, R et al. (1996) Carcinoma of the rectum. Possible cellular predictors of metastatic potential and response to radiation therapy. Dis Colon Rectum 39:1090-6
Malyapa, R S; Wright, W D; Taylor, Y C et al. (1996) DNA supercoiling changes and nuclear matrix-associated proteins: possible role in oncogene-mediated radioresistance. Int J Radiat Oncol Biol Phys 35:963-73
Goswami, P C; Roti Roti, J L; Hunt, C R (1996) The cell cycle-coupled expression of topoisomerase IIalpha during S phase is regulated by mRNA stability and is disrupted by heat shock or ionizing radiation. Mol Cell Biol 16:1500-8
Mackey, M A; Zhang, X F; Hunt, C R et al. (1996) Uncoupling of M-phase kinase activation from the completion of S-phase by heat shock. Cancer Res 56:1770-4
Huot, J; Houle, F; Spitz, D R et al. (1996) HSP27 phosphorylation-mediated resistance against actin fragmentation and cell death induced by oxidative stress. Cancer Res 56:273-9
Malyapa, R S; Wright, W D; Roti Roti, J L (1996) DNA supercoiling changes and nucleoid protein composition in a group of L5178Y cells of varying radiosensitivity. Radiat Res 145:239-42

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