Abstract

The response of eukaryotes to DNA damaging agents, such as ionizing radiation, is determined by the effectiveness of a variety of DNA repair systems. Defective repair, in the form of a diminished capacity for accurate repair or through inaccurate repair processes, can lead to mutations involving genes responsible for the control of cell proliferation. Understanding the nature of these repair processes is central to the elucidation of the mechanisms through which subsequent adverse health effects such as mutations, fetal malformations, and cancers are expressed. Ionizing radiation induces various types of DNA damage in mammalian cells including DNA single-strand breaks (SSB), DNA double strand breaks (DSB), DNA-protein crosslinks, DNA-DNA interstrand crosslinks, and altered DNA bases. Although- it is obvious that human cells can repair many of these lesions, there is little detailed knowledge of the nature of the genes and the encoded enzymes that control these repair processes. ln order to understand how DNA repair modulates radiation sensitivity, oncogene expression, and recombination-related genetic diseases, radiation-specific DNA repair genes have to be isolated and characterized. During the current funding period of this project, a comprehensive strategy and all the basic grounds for the positional cloning of a human DSB repair gene XRCC5 have been established in our laboratory. Thus, the primary objective of this renewal application is to continue our efforts on the isolation and characterization of human XRCC5 gene.
The specific aims are: 1) Regional localization of human XRCC5 gene in chromosome 2 (at the megabases level); 2) Construction of a repair-proficient X-ray hybrid panel, each hybrid containing a fragment of human chromosome 2 (1-3 Mb) where the XRCC5 has been assigned ;3) Position cloning of candidate XRCC5 recombinant clones and functional analysis of these clones; 4) Molecular characterization of the cloned XRCC5 gene. We believe that this step-by- step approach utilizing advanced molecular genetic technologies will substantially facilitate the isolation of the first human radiation repair gene(s) responsible for the rejoining of ionizing radiation-induced DNA double-strand breaks.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
2R01CA050519-04
Application #
2093824
Study Section
Radiation Study Section (RAD)
Project Start
1989-07-01
Project End
1998-02-28
Budget Start
1994-03-01
Budget End
1995-02-28
Support Year
4
Fiscal Year
1994
Total Cost
Indirect Cost

  Institution

Name
Los Alamos National Lab
Department
Type
Schools of Arts and Sciences
DUNS #
City
Los Alamos
State
NM
Country
United States
Zip Code
87545

  Publications

Mori, Eiichiro; Davis, Anthony J; Hasegawa, Masatoshi et al. (2016) Lysines 3241 and 3260 of DNA-PKcs are important for genomic stability and radioresistance. Biochem Biophys Res Commun 477:235-40
Davis, Anthony J; Lee, Kyung-Jong; Chen, David J (2013) The N-terminal region of the DNA-dependent protein kinase catalytic subunit is required for its DNA double-stranded break-mediated activation. J Biol Chem 288:7037-46
Wang, Hailong; Shi, Linda Z; Wong, Catherine C L et al. (2013) The interaction of CtIP and Nbs1 connects CDK and ATM to regulate HR-mediated double-strand break repair. PLoS Genet 9:e1003277
Chung, Young Min; Park, See-Hyoung; Tsai, Wen-Bin et al. (2012) FOXO3 signalling links ATM to the p53 apoptotic pathway following DNA damage. Nat Commun 3:1000
Sun, Jingxin; Lee, Kyung-Jong; Davis, Anthony J et al. (2012) Human Ku70/80 protein blocks exonuclease 1-mediated DNA resection in the presence of human Mre11 or Mre11/Rad50 protein complex. J Biol Chem 287:4936-45
Shao, Zhengping; Davis, Anthony J; Fattah, Kazi R et al. (2012) Persistently bound Ku at DNA ends attenuates DNA end resection and homologous recombination. DNA Repair (Amst) 11:310-6
Pankotai, Tibor; Bonhomme, Celine; Chen, David et al. (2012) DNAPKcs-dependent arrest of RNA polymerase II transcription in the presence of DNA breaks. Nat Struct Mol Biol 19:276-82
Levy-Barda, Adva; Lerenthal, Yaniv; Davis, Anthony J et al. (2011) Involvement of the nuclear proteasome activator PA28? in the cellular response to DNA double-strand breaks. Cell Cycle 10:4300-10
Lee, Kyung-Jong; Lin, Yu-Fen; Chou, Han-Yi et al. (2011) Involvement of DNA-dependent protein kinase in normal cell cycle progression through mitosis. J Biol Chem 286:12796-802
Kozlov, Sergei V; Graham, Mark E; Jakob, Burkhard et al. (2011) Autophosphorylation and ATM activation: additional sites add to the complexity. J Biol Chem 286:9107-19

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