Abstract

The purpose of this proposed research is to study the molecular mechanism of cell killing by anti-cancer drugs which are known to produce protein-linked DNA breaks in vivo. Our long term goal is to understand the regulatory mechanism of cell proliferation and cell death. The proposed research focuses on the phenomenon of protein-linked DNA breaks which represents a novel type of DNA damage produced by many potent antitumor agents. Relatively little is known about the biological consequences of this particular DNA damage. Recently, there is increasing evidence that mammalian DNA topoisomerase II may be the intracellular target of these antitumor drugs and the formation of protein-linked DNA breaks may be the direct result of drug-topoisomerase or drug-topoisomerase-DNA interaction. In vitro studies have suggested that many antitumor drugs may interfere with the breakage-reunion reaction of mammalian DNA topoisomerase II by blocking the reunion of transiently broken DNA. Whether the observed in vitro reaction reflects drug action in vivo has not been fully established. Furthermore, the molecular mechanism of rapid cell killing by these antitumor drugs is still not known. In order to answer these questions, both genetic and biochemical experiments will be performed to identify mammalian DNA topoisomerase II as the cytotoxic target. Genetic analyses of drug resistant mutants will be used to identify mammalian topoisomerase II as the primary cytotoxic target of these antitumor drugs. Localization of the protein-linked DNA breaks on human chromosomes will be carried out by an indirect end labeling mapping procedure. The nucleotide sequences around the breakage sites will be determined by cloning and sequencing. DNA clones containing the strong breakage sites will be used for in vitro studies using purified HeLa topoisomerase II. Human cells treated with epipodophyllotoxin, VP-16, will be used as a model system for the analyses of the biological consequences leading to cell death.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
5R01CA039662-03
Application #
3178939
Study Section
Experimental Therapeutics Subcommittee 2 (ET)
Project Start
1985-04-01
Project End
1988-03-31
Budget Start
1987-04-01
Budget End
1988-03-31
Support Year
3
Fiscal Year
1987
Total Cost
Indirect Cost

  Institution

Name
Johns Hopkins University
Department
Type
Schools of Arts and Sciences
DUNS #
045911138
City
Baltimore
State
MD
Country
United States
Zip Code
21218

  Publications

Lin, Ren-Kuo; Ho, Chia-Wen; Liu, Leroy F et al. (2013) Topoisomerase II? deficiency enhances camptothecin-induced apoptosis. J Biol Chem 288:7182-92
Ban, Yi; Ho, Chia-Wen; Lin, Ren-Kuo et al. (2013) Activation of a novel ubiquitin-independent proteasome pathway when RNA polymerase II encounters a protein roadblock. Mol Cell Biol 33:4008-16
Chiang, Hsiao-Ling; Lin, Chi-Yu; Jan, Fan-Dan et al. (2012) A novel synthetic bipartite carrier protein for developing glycotope-based vaccines. Vaccine 30:7573-81
Su, Yee-Fun; Yang, Tsunghan; Huang, Hoting et al. (2012) Phosphorylation of Ubc9 by Cdk1 enhances SUMOylation activity. PLoS One 7:e34250
Wan, Shan; Pestka, Sidney; Jubin, Ronald G et al. (2012) Chemotherapeutics and radiation stimulate MHC class I expression through elevated interferon-beta signaling in breast cancer cells. PLoS One 7:e32542
Tsai, Yu-Chen; Pestka, Sidney; Wang, Lu-Hai et al. (2011) Interferon-? signaling contributes to Ras transformation. PLoS One 6:e24291
Lin, Ren-Kuo; Zhou, Nai; Lyu, Yi Lisa et al. (2011) Dietary isothiocyanate-induced apoptosis via thiol modification of DNA topoisomerase II?. J Biol Chem 286:33591-600
Feng, Wei; Satyanarayana, Mavurapu; Tsai, Yuan-Chin et al. (2009) 12-Substituted 2,3-dimethoxy-8,9-methylenedioxybenzo[i]phenanthridines as novel topoisomerase I-targeting antitumor agents. Bioorg Med Chem 17:2877-85
Feng, Wei; Satyanarayana, Mavurapu; Tsai, Yuan-Chin et al. (2009) Novel topoisomerase I-targeting antitumor agents synthesized from the N,N,N-trimethylammonium derivative of ARC-111, 5H-2,3-dimethoxy-8,9-methylenedioxy-5-[(2-N,N,N-trimethylammonium)ethyl]dibenzo[c,h][1,6]naphthyridin-6-one iodide. Eur J Med Chem 44:3433-8
Sharma, Lisa; Tsai, Yuan-Chin; Liu, Angela A et al. (2009) Cytotoxicity and TOP1-targeting activity of 8- and 9-amino derivatives of 5-butyl- and 5-(2-N,N-dimethylamino)ethyl-5H-dibenzo[c,h][1,6]naphthyridin-6-ones. Eur J Med Chem 44:1471-6

Showing the most recent 10 out of 97 publications