Abstract

The overall goals of this research are to understand the mechanisms of radiation-induced injury using the new molecular biologic techniques at our disposal. Our current working hypothesis and recent research findings focus on the pulmonary sequence of events following ionizing radiation as a continuum, with no clear distinction between the pneumonitic and fibrotic phases. We propose that control of the proliferation of pulmonary fibroblasts and the synthesis and turnover of extracellular matrix components occurs through the production of specific locally generated mediators. These factors, acting through specific receptors on the cell surface, alter the rate of growth or specific gene expression of the matrix components or products that directly relate to their turnover. We intend to continue to decipher the intercellular communication between the many different cells injured, recognizing that the target has shifted from the cell per se to cellular conversation; that is the interaction between the irradiated """"""""infield"""""""" parenchymal cells of the lung (type II pneumocyte and septal fibroblast) and recruited """"""""out-of-field"""""""" inflammatory cells: macrophages, monocytes, neutrophils and, especially, the lymphocytes. We believe that the progressive elements of radiation injury may largely relate to modulation of the """"""""in-field"""""""" radiation inflammatory response through a complex cascade of cytokine release and by their chemotactic attraction for """"""""out-of-field"""""""" immune cells such as lymphocytes and monocytes. Once recruited into this disturbed microenvironment, these inflammatory cells may themselves become stimulated to produce other mediators initiating a complex """"""""cytokine cascade."""""""" It is important to recognize that in addition to influencing the rate of nature of the factors produced, radiation exposure may also directly alter the ability of a specific cell type to respond to such signals. Such alteration may occur through a change in the number or affinity of specific growth factor receptors on the target cells. To address this hypothesis we propose to examine the expression of mRNA and protein of specific growth factors and cytokines that we feel are critical components in the communication among the cells involved in the radiation response. These include TGFalpha and beta, PDGF, IL-1, TNF, IL-8/NAP and the novel chemotactic peptide MCP/MCAF, as well as measurement of receptors on populations of parenchymal cells. These will be examined in two model systems of radiation injury with which we have extensive experience, the unilung irradiated rabbit and the mouse. Both of these systems have unique advantages that we plan to exploit in the proposed experiments.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
5R01CA027791-15
Application #
2414095
Study Section
Radiation Study Section (RAD)
Program Officer
Stone, Helen B
Project Start
1980-05-01
Project End
2000-04-30
Budget Start
1997-05-01
Budget End
2000-04-30
Support Year
15
Fiscal Year
1997
Total Cost
Indirect Cost

  Institution

Name
University of Rochester
Department
Radiation-Diagnostic/Oncology
Type
Schools of Dentistry
DUNS #
208469486
City
Rochester
State
NY
Country
United States
Zip Code
14627

  Publications

Chen, Yuhchyau; Williams, Jacqueline; Ding, Ivan et al. (2002) Radiation pneumonitis and early circulatory cytokine markers. Semin Radiat Oncol 12:26-33
Chen, Y; Rubin, P; Williams, J et al. (2001) Circulating IL-6 as a predictor of radiation pneumonitis. Int J Radiat Oncol Biol Phys 49:641-8
Daly, H E; Baecher-Allan, C M; Paxhia, A T et al. (1998) Cell-specific gene expression reveals changes in epithelial cell populations after bleomycin treatment. Lab Invest 78:393-400
Johnston, C J; Stripp, B R; Piedbeouf, B et al. (1998) Inflammatory and epithelial responses in mouse strains that differ in sensitivity to hyperoxic injury. Exp Lung Res 24:189-202
Johnston, C J; Wright, T W; Rubin, P et al. (1998) Alterations in the expression of chemokine mRNA levels in fibrosis-resistant and -sensitive mice after thoracic irradiation. Exp Lung Res 24:321-37
Daly, H E; Baecher-Allan, C M; Barth, R K et al. (1997) Bleomycin induces strain-dependent alterations in the pattern of epithelial cell-specific marker expression in mouse lung. Toxicol Appl Pharmacol 142:303-10
Johnston, C J; Mango, G W; Finkelstein, J N et al. (1997) Altered pulmonary response to hyperoxia in Clara cell secretory protein deficient mice. Am J Respir Cell Mol Biol 17:147-55
Finkelstein, J N; Johnston, C; Barrett, T et al. (1997) Particulate-cell interactions and pulmonary cytokine expression. Environ Health Perspect 105 Suppl 5:1179-82
Wright, T W; Johnston, C J; Harmsen, A G et al. (1997) Analysis of cytokine mRNA profiles in the lungs of Pneumocystis carinii-infected mice. Am J Respir Cell Mol Biol 17:491-500
Johnston, C J; Piedboeuf, B; Rubin, P et al. (1996) Early and persistent alterations in the expression of interleukin-1 alpha, interleukin-1 beta and tumor necrosis factor alpha mRNA levels in fibrosis-resistant and sensitive mice after thoracic irradiation. Radiat Res 145:762-7

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