Abstract

The overall objective of this proposal is to develop mouse models for studying the biological function of environmentally sensitive DNA repair/cell cycle control gene variants found in the human population. The capacity for DNA repair is a major influence in the sensitivity to carcinogenic stimuli, so genetic variants must be considered in risk assessment. The concept that common variants in the population contribute to genetic risk for common diseases has triggered intense interest in identifying DNA sequence variants known as single nucleotide polymorphisms (SNPs). However, the functional significance of SNP variants in relation to environmental carcinogens is largely unknown. This proposal is designed to establish a genetically engineered mouse system as a mammalian model for human functional genomics and SNP variant-environment interactions.
The specific aims are 1) Integrate University of Washington Health Sciences resources, including genomics, transgenic technology, mouse genetics, bioinformatics, biostatistics, ecogenetics and environmental health, flow cytometry, whole mouse positron emission tomography (PET) imaging, comparative pathology, and the molecular genetics of DNA repair/cell cycle control genes, into an infrastructure for generating and characterizing SNP mutant mice. 2) Generate SNP mutant mice by gene targeting technology, and characterize and validate these mice using the integrated infrastructure resources established in Aim l. 3) Develop new mouse genomics technology including the prediction of SNP function by three- dimensional, macromolecular protein structure, and whole mouse PET imaging to detect early, environmentally induced tumorigenesis. 4) Establish an electronic database system to enhance communication of unique mouse model data and expertise to the environmental health sciences community. The development of these mouse models will mirror specific human, environmentally responsive polymorphic gene variants found in the general population, and provide a biological system for understanding the functional significance of these polymorphic variants.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Environmental Health Sciences (NIEHS)
Type
Research Project--Cooperative Agreements (U01)
Project #
5U01ES011045-03
Application #
6603306
Study Section
Special Emphasis Panel (ZES1-JPM-B (UJ))
Program Officer
Tyson, Frederick L
Project Start
2001-04-15
Project End
2006-03-31
Budget Start
2003-04-01
Budget End
2004-03-31
Support Year
3
Fiscal Year
2003
Total Cost
$1,206,544
Indirect Cost

  Institution

Name
University of Washington
Department
Veterinary Sciences
Type
Schools of Medicine
DUNS #
605799469
City
Seattle
State
WA
Country
United States
Zip Code
98195

  Publications

Treuting, Piper M; Albertson, Tina M; Preston, Bradley D (2010) Case series: acute tumor lysis syndrome in mutator mice with disseminated lymphoblastic lymphoma. Toxicol Pathol 38:476-85
Albertson, Tina M; Ogawa, Masanori; Bugni, James M et al. (2009) DNA polymerase epsilon and delta proofreading suppress discrete mutator and cancer phenotypes in mice. Proc Natl Acad Sci U S A 106:17101-4
Moore, Gina; Knoblaugh, Susan; Gollahon, Kathryn et al. (2008) Hyperinsulinemia and insulin resistance in Wrn null mice fed a diabetogenic diet. Mech Ageing Dev 129:201-6
Bailey, S Lawrence; Gurley, Kay E; Hoon-Kim, Kyung et al. (2008) Tumor suppression by p53 in the absence of Atm. Mol Cancer Res 6:1185-92
Enns, L C; Wiley, J C; Ladiges, W C (2008) Clinical relevance of transgenic mouse models for aging research. Crit Rev Eukaryot Gene Expr 18:81-91
Vermulst, Marc; Wanagat, Jonathan; Kujoth, Gregory C et al. (2008) DNA deletions and clonal mutations drive premature aging in mitochondrial mutator mice. Nat Genet 40:392-4
Gurley, Kay E; Kemp, Christopher J (2007) Ataxia-telangiectasia mutated is not required for p53 induction and apoptosis in irradiated epithelial tissues. Mol Cancer Res 5:1312-8
Vermulst, Marc; Bielas, Jason H; Kujoth, Gregory C et al. (2007) Mitochondrial point mutations do not limit the natural lifespan of mice. Nat Genet 39:540-3
Venkatesan, Ranga N; Treuting, Piper M; Fuller, Evan D et al. (2007) Mutation at the polymerase active site of mouse DNA polymerase delta increases genomic instability and accelerates tumorigenesis. Mol Cell Biol 27:7669-82
Besson, Arnaud; Gurian-West, Mark; Chen, Xueyan et al. (2006) A pathway in quiescent cells that controls p27Kip1 stability, subcellular localization, and tumor suppression. Genes Dev 20:47-64

Showing the most recent 10 out of 25 publications