Abstract

The DNA damage checkpoints are cellular surveillance mechanisms that allow the cell to monitor the integrity of the genome and to signal the presence of DNA damage to the cell. These pathways play a critical role in maintaining genomic stability, and loss of checkpoint function has been implicated in the development of cancer. Genomic instability and defects in some checkpoint genes have also been linked to several syndromes that lead to premature aging, including Werner's syndrome. The long-term objective of this research is to understand the mechanism by which cells signal the presence of different forms of DNA damage to the cell cycle machinery and DNA repair proteins. The focus of this application is ATR (ATM and Rad3-related), a mammalian gene that is required for the DNA damage and replication checkpoints. The primary goal is to identify domains in ATR and other proteins that are required for ATR to sense and transduce the presence of DNA damage to the cell. The 9-1-1 complex is a heterotrimeric protein complex that may be required for ATR to signal to its downstream effectors.
The specific aims of this research are (1) to determine if the 9-1-1 complex is an upstream regulator and/or downstream effectors.
The specific aims of this research are (1) to determine if the 9-1-1 complex is an upstream regulator and/or downstream effector of ATR function (2) to identify and characterize functional domains within ATR, and (3) to purify, clone and characterize the protein that mediates the interaction of ATR with DNA. Extracts from the eggs of Xenopus laevis will be used to study the relationship between the 9-1-1 complex and ATR. Using a series of assays that we developed, the function of a specific ATR fragment that exhibits a unique nuclear localization and a dominant negative phenotype will be probed in mammalian cells. Finally, using a new assay for ATR's DNA- binding activity and a new affinity-based purification strategy, the protein that mediates the interaction of ATR with DNA will be purified, cloned and characterized. The studies will provide a better understanding of the mechanisms by which ATR signals he presence of different forms of DNA damage to the cell. Furthermore, they should provide important insights into human disease such as cancer and the complex process of human aging.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of General Medical Sciences (NIGMS)
Type
Research Project (R01)
Project #
5R01GM062193-05
Application #
7060922
Study Section
Cell Development and Function Integrated Review Group (CDF)
Program Officer
Zatz, Marion M
Project Start
2002-05-01
Project End
2007-05-17
Budget Start
2006-05-01
Budget End
2007-05-17
Support Year
5
Fiscal Year
2006
Total Cost
$269,677
Indirect Cost

  Institution

Name
Stanford University
Department
Biology
Type
Schools of Medicine
DUNS #
009214214
City
Stanford
State
CA
Country
United States
Zip Code
94305

  Publications

Cimprich, Karlene A (2007) Probing ATR activation with model DNA templates. Cell Cycle 6:2348-54
Lupardus, Patrick J; Van, Christopher; Cimprich, Karlene A (2007) Analyzing the ATR-mediated checkpoint using Xenopus egg extracts. Methods 41:222-31
Paulsen, Renee D; Cimprich, Karlene A (2007) The ATR pathway: fine-tuning the fork. DNA Repair (Amst) 6:953-66
MacDougall, Christina A; Byun, Tony S; Van, Christopher et al. (2007) The structural determinants of checkpoint activation. Genes Dev 21:898-903
Chang, Debbie J; Lupardus, Patrick J; Cimprich, Karlene A (2006) Monoubiquitination of proliferating cell nuclear antigen induced by stalled replication requires uncoupling of DNA polymerase and mini-chromosome maintenance helicase activities. J Biol Chem 281:32081-8
Lupardus, Patrick J; Cimprich, Karlene A (2006) Phosphorylation of Xenopus Rad1 and Hus1 defines a readout for ATR activation that is independent of Claspin and the Rad9 carboxy terminus. Mol Biol Cell 17:1559-69
Bomgarden, Ryan D; Lupardus, Patrick J; Soni, Deena V et al. (2006) Opposing effects of the UV lesion repair protein XPA and UV bypass polymerase eta on ATR checkpoint signaling. EMBO J 25:2605-14
Sobeck, Alexandra; Stone, Stacie; Costanzo, Vincenzo et al. (2006) Fanconi anemia proteins are required to prevent accumulation of replication-associated DNA double-strand breaks. Mol Cell Biol 26:425-37
Byun, Tony S; Pacek, Marcin; Yee, Muh-ching et al. (2005) Functional uncoupling of MCM helicase and DNA polymerase activities activates the ATR-dependent checkpoint. Genes Dev 19:1040-52
O'Connell, Matthew J; Cimprich, Karlene A (2005) G2 damage checkpoints: what is the turn-on? J Cell Sci 118:1-6

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