It has been proposed that telomere repeat sequences and telomere terminal transferase (telomerase) may influence mutation induction by ionizing radiation. Interstitial telomere repeat sequences are thought to be radiation-sensitive fragile sites, and telomerase has been reported to cap the ends of broken chromosomes, preventing their repair and promoting chromosome terminalization or recombination. We have been characterizing a Chinese hamster ovary cell line into which a gpt containing retroviral shuttle vector has been stably integrated. This normally stable locus in T5 cells is very sensitive to deletion mutation following ionizing radiation exposure. The gene also shows an LET response with an RBE of 3 for a particles. Analysis of the integration site has identified regions of T2AG3 telomere repeats both 3-prime and 5-prime to the gpt gene. The goal of these studies is to establish the role of telomere repeat sequences and telomerase in radiation sensitivity and genomic stability using this gpt locus as a model system. We plan to test the following hypotheses: (l) the telomere repeat sequences found at the gpt integration site were added to the vector or to the vector integration site by telomerase prior to or during integration, (2) these telomeric sequences have made the vector integration site a radiation-sensitive site, and (3) telomeres act as radiation-sensitive fragile sites by either serving as a site for further telomerase action and chromosome terminalization or by providing repeat structures to facilitate radiation-induced recombination. These studies should further our understanding of the roles that telomerase and interstitial telomere sequences play in genetic disease and help to better define the potential risks associated with environmental exposures to both low- and high-LET radiations.

Agency
National Institute of Health (NIH)
Institute
National Institute of General Medical Sciences (NIGMS)
Type
Research Project (R01)
Project #
1R01GM051827-01A1
Application #
2190565
Study Section
Radiation Study Section (RAD)
Project Start
1995-08-10
Project End
1995-10-31
Budget Start
1995-08-10
Budget End
1995-10-31
Support Year
1
Fiscal Year
1995
Total Cost
Indirect Cost
Name
University of Chicago
Department
Type
Organized Research Units
DUNS #
225410919
City
Chicago
State
IL
Country
United States
Zip Code
60637
Schwartz, J L; Jordan, R; Sun, J et al. (2000) Dose-dependent changes in the spectrum of mutations induced by ionizing radiation. Radiat Res 153:312-7
Schwartz, J L; Jordan, R; Kaufmann, W K et al. (2000) Evidence for the expression of radiation-induced potentially lethal damage being a p53-dependent process. Int J Radiat Biol 76:1037-43
Schwartz, J L; Russell, K J (1999) The effect of functional inactivation of TP53 by HPV-E6 transformation on the induction of chromosome aberrations by gamma rays in human tumor cells. Radiat Res 151:385-90
Schwartz, J L; Rasey, J; Wiens, L et al. (1999) Functional inactivation of p53 by HPV-E6 transformation is associated with a reduced expression of radiation-induced potentially lethal damage. Int J Radiat Biol 75:285-91
Schwartz, J L; Murnane, J; Weichselbaum, R R (1999) The contribution of DNA ploidy to radiation sensitivity in human tumour cell lines. Br J Cancer 79:744-7
Schwartz, J L (1998) Alterations in chromosome structure and variations in the inherent radiation sensitivity of human cells. Radiat Res 149:319-24
Schwartz, J L; Hsie, A W (1997) Genetic and cytogenetic markers of exposure to high-linear energy transfer radiation. Radiat Res 148:S87-92
Kaufmann, W K; Schwartz, J L; Hurt, J C et al. (1997) Inactivation of G2 checkpoint function and chromosomal destabilization are linked in human fibroblasts expressing human papillomavirus type 16 E6. Cell Growth Differ 8:1105-14
Schwartz, J L; Jordan, R (1997) Selective elimination of human lymphoid cells with unstable chromosome aberrations by p53-dependent apoptosis. Carcinogenesis 18:201-5