Abstract

ATM (ataxia telangiectasia mutated) heterozygosity seems to be a risk factor for cancer. Even though the penetrance seems to be low, because of the high prevalence of 1-5% in the human population, the population risk is higher than for BRCA1 and BRCA2 together. We hypothesize that the reason why only some people heterozygous for ATM develop cancer may in part be due to the fact that the human population is extremely varied with regard to additional genetic cancer predisposing or protecting factors as well as nutrition factors and that only certain gene-gene and/or gene-nutrition interactions may lead to the highest risk for cancer. Genetic instability, in particular DNA deletions are involved in the etiology of cancer. ATM deficient homozygous patients and mice show a high incidence of cancer, signs of oxidative stress and an elevated frequency of DNA deletions which we found using an in vivo pigmentation assay. This assay is based on the quantification of black spots on fur and eyes resulting from reversion of the pun mutation. This reversion occurs by deletion of 70 kb of an internal duplication within the p gene. We have also shown that ATMASRI missense mutation homozygous as well as heterozygous mice show elevated frequencies of DNA deletions. In addition, we have shown that the elevated frequency of DNA deletions in ATM homozygous disruption mutant mice is completely reverted to wildtype levels by nutritional supplementation with the radical scavenger N-acetyl cysteine (NAC). GGT deficient mice have lower levels of glutathione and show signs of oxidative stress.
In aim 1 we propose to investigate whether ATMASRI heterozygous or homozygous mice together with GGT deficiency show synergistically elevated frequencies of DNA deletions (gene-gene interactions), In aim 2 we propose to test whether ATMASRI homo and heterozygous mice nutritionally supplemented with NAC show reduced frequencies of DNA deletions and whether mice supplemented with the prooxidant BSO show an increased frequency of deletions (gene-nutrition interactions). It will be tested in the third aim whether the elevated frequency of cancer in ATMASRI homozygous mice can be reduced by chemoprevention with the antioxidant NAC (gene-nutrition interaction). Implications for human health may include that ATM patients as well as heterozygous people (1-5% of the human population) in combination with genetic or nutritional factors predisposing to a higher sensitivity to oxidative stress may show an increased risk for cancer, and that chemoprevention with antioxidants may reduce the cancer risk in such genetically predisposed people.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Environmental Health Sciences (NIEHS)
Type
Research Project (R01)
Project #
2R01ES009519-07A2
Application #
6968584
Study Section
Special Emphasis Panel (ZRG1-CDP (01))
Program Officer
Mcallister, Kimberly A
Project Start
1999-06-01
Project End
2010-05-31
Budget Start
2005-06-03
Budget End
2006-05-31
Support Year
7
Fiscal Year
2005
Total Cost
$325,972
Indirect Cost

  Institution

Name
University of California Los Angeles
Department
Pathology
Type
Schools of Medicine
DUNS #
092530369
City
Los Angeles
State
CA
Country
United States
Zip Code
90095

  Publications

Yamamoto, Mitsuko L; Maier, Irene; Dang, Angeline Tilly et al. (2013) Intestinal bacteria modify lymphoma incidence and latency by affecting systemic inflammatory state, oxidative stress, and leukocyte genotoxicity. Cancer Res 73:4222-32
Westbrook, Aya M; Wei, Bo; Braun, Jonathan et al. (2011) Intestinal inflammation induces genotoxicity to extraintestinal tissues and cell types in mice. Int J Cancer 129:1815-25
Reliene, Ramune; Yamamoto, Mitsuko L; Rao, P Nagesh et al. (2010) Genomic instability in mice is greater in Fanconi anemia caused by deficiency of Fancd2 than Fancg. Cancer Res 70:9703-10
Westbrook, Aya M; Szakmary, Akos; Schiestl, Robert H (2010) Mechanisms of intestinal inflammation and development of associated cancers: lessons learned from mouse models. Mutat Res 705:40-59
Westbrook, Aya M; Schiestl, Robert H (2010) Atm-deficient mice exhibit increased sensitivity to dextran sulfate sodium-induced colitis characterized by elevated DNA damage and persistent immune activation. Cancer Res 70:1875-84
Westbrook, Aya M; Wei, Bo; Braun, Jonathan et al. (2009) Intestinal mucosal inflammation leads to systemic genotoxicity in mice. Cancer Res 69:4827-34
Trouiller, Benedicte; Reliene, Ramune; Westbrook, Aya et al. (2009) Titanium dioxide nanoparticles induce DNA damage and genetic instability in vivo in mice. Cancer Res 69:8784-9
Westbrook, Aya M; Wei, Bo; Braun, Jonathan et al. (2009) More damaging than we think: systemic effects of intestinal inflammation. Cell Cycle 8:2482-3
Reliene, Ramune; Fleming, Sheila M; Chesselet, Marie-Francoise et al. (2008) Effects of antioxidants on cancer prevention and neuromotor performance in Atm deficient mice. Food Chem Toxicol 46:1371-7
Yamamoto, Mitsuko L; Reliene, Ramune; Oshima, Junko et al. (2008) Effects of human Werner helicase on intrachromosomal homologous recombination mediated DNA deletions in mice. Mutat Res 644:11-6

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