Abstract

Cellular Responses to Oxidative Stress in Models of Colon Cancer Development (Overall Abstract) Humans are exposed to a multitude of chemical (e.g. pollutants and drugs) and physical (e.g. radiation) agents in the environment that induce oxidative stress in most cell types that comprise tissues and organ systems. Oxidative stress, characterized by increased levels of reactive oxygen species (ROS), can induce both aberrant signal transduction and oxidative damage to cellular macromolecules, including lipids, proteins and nucleic acids. Such oxidative changes directly contribute to a variety of deleterious biological endpoints associated with several important human diseases, including cardiovascular and neurodegenerative disorders and cancer. Several lines of evidence have revealed links among oxidative stress, inflammation and the development of colon cancer. Colorectal cancer is the third most commonly diagnosed cancer and is the second leading cause of cancer death in the United States. Currently, we have a very poor understanding of the mechanisms by which oxidative stress mediates colon tumor development. The overall theme of this program project renewal is to delineate the pathogenic contributions of two major, stress-activated cellular generators of ROS (mitochondria and Nox) and to investigate the response pathways to ROS and to ROSdamaged macromolecules which directly lead to genetic instability and other biological changes that contribute to tumor development. This program of investigation builds from information obtained during the previous support period and is comprised of four complementary, synergistic projects that will employ two powerful eukaryotic model systems (yeast and mice) in order to define important elements of the eukaryotic/mammalian oxidative stress circuitry. These systems are genetically and biochemically tractable and will also provide an important mammalian intestinal tumor model that is relevant to human colon cancer development. The great advantage of employing such model systems is that key targets and system components (a number of which were identified and analyzed during the previous period of support) can be examined within the context of a battery of isogenic yeast strains, mammalian cells, and individual animals at a level of complexity and pace not yet achievable using human tissues and cells. The information generated from such studies can subsequently be directly and quickly translated into studies utilizing human material. Dissection of these cellular damages and response pathways will lead to a clearer understanding of the role of oxidative stress in colon cancer development and will reveal novel targets for prevention and intervention.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Environmental Health Sciences (NIEHS)
Type
Research Program Projects (P01)
Project #
5P01ES011163-10
Application #
8293193
Study Section
Special Emphasis Panel (ZES1-TN-G (PD))
Program Officer
Reinlib, Leslie J
Project Start
2002-08-15
Project End
2014-06-30
Budget Start
2012-07-01
Budget End
2014-06-30
Support Year
10
Fiscal Year
2012
Total Cost
$1,293,953
Indirect Cost
$354,818

  Institution

Name
Emory University
Department
Biochemistry
Type
Schools of Medicine
DUNS #
066469933
City
Atlanta
State
GA
Country
United States
Zip Code
30322

  Publications

Morris, Lydia P; Conley, Andrew B; Degtyareva, Natalya et al. (2017) Genome-wide map of Apn1 binding sites under oxidative stress in Saccharomyces cerevisiae. Yeast 34:447-458
Limpose, Kristin L; Corbett, Anita H; Doetsch, Paul W (2017) BERing the burden of damage: Pathway crosstalk and posttranslational modification of base excision repair proteins regulate DNA damage management. DNA Repair (Amst) 56:51-64
Crouse, Gray F (2016) Non-canonical actions of mismatch repair. DNA Repair (Amst) 38:102-9
Swartzlander, Daniel B; McPherson, Annie J; Powers, Harry R et al. (2016) Identification of SUMO modification sites in the base excision repair protein, Ntg1. DNA Repair (Amst) 48:51-62
Bauer, Nicholas C; Corbett, Anita H; Doetsch, Paul W (2015) The current state of eukaryotic DNA base damage and repair. Nucleic Acids Res 43:10083-101
Flood, Carrie L; Rodriguez, Gina P; Bao, Gaobin et al. (2015) Replicative DNA polymerase ? but not ? proofreads errors in Cis and in Trans. PLoS Genet 11:e1005049
West, A Phillip; Khoury-Hanold, William; Staron, Matthew et al. (2015) Mitochondrial DNA stress primes the antiviral innate immune response. Nature 520:553-7
Bauer, Nicholas C; Doetsch, Paul W; Corbett, Anita H (2015) Mechanisms Regulating Protein Localization. Traffic 16:1039-61
Marullo, Rossella; Werner, Erica; Degtyareva, Natalya et al. (2013) Cisplatin induces a mitochondrial-ROS response that contributes to cytotoxicity depending on mitochondrial redox status and bioenergetic functions. PLoS One 8:e81162
Degtyareva, Natalya P; Heyburn, Lanier; Sterling, Joan et al. (2013) Oxidative stress-induced mutagenesis in single-strand DNA occurs primarily at cytosines and is DNA polymerase zeta-dependent only for adenines and guanines. Nucleic Acids Res 41:8995-9005

Showing the most recent 10 out of 72 publications