Abstract

Superoxide dismutases (SOD) are a class of essential enzymes responsible for the elimination of the toxic free radical, superoxide (O2-), and thus protect cells from oxidative stress. Inhibition of SOD impairs the ability of cells to cope with free radicals, and may provide a new strategy to kill cancer cells by mechanisms involving free radical O2- induced apoptotic cell death. However, specific SOD inhibitors with anticancer activity are not readily available for testing this new strategy. The applicant recently discovered that certain estrogen derivatives inhibited both the cellular copper/zinc-containing superoxide dismutase (CuZnSOD) and the mitochondrial manganese-containing superoxide dismutatase (MnSOD), and preferentially induced apoptosis in cancer cells but not in normal human lymphocytes. Based on these observations, the applicants propose to test the hypothesis of targeting SOD by the estrogen derivatives as a new strategy for cancer therapy. The objectives of this proposal are to investigate the biological consequences of SOD inhibition, to investigate the mechanisms by which the estrogen derivatives inhibit SOD, and to design new mechanism-based strategies to enhance the anticancer activity of the SOD-targeting compounds. Specifically, new molecular biology techniques and pharmacological/biochemical approaches will be employed to investigate the role of SOD inhibition in causing cell death by the estrogen derivatives, and to examine the free radical-mediated damage to membrane lipids, DNA, and relevant proteins such as cytochrome c. Changes in gene expression profiles associated with the estrogen derivative-induced apoptosis will be analyzed by cDNA micro-array technology. They will also use biochemical approaches to characterize the kinetics of SOD inhibition by estrogen derivatives. Laboratory investigations will be combined with computer-assisted molecular simulation technology to determine the structure-function relationship during SOD inhibition. Furthermore, the possibility of combining the SOD inhibitors with radiation and other agents such as anthracyclines that produce free radicals in cells as new strategies to enhance the anticancer activity will be tested. They anticipate that this research project will further our understanding of the mechanisms of SOD inhibition and its biological consequences, and will provide a basis both for the rational design of more potent/selective SOD inhibitors suitable for cancer therapy, and for the development of new mechanism-based strategies to enhance anticancer activity and selectivity.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
5R01CA085563-02
Application #
6489371
Study Section
Experimental Therapeutics Subcommittee 1 (ET)
Program Officer
Forry, Suzanne L
Project Start
2001-01-23
Project End
2004-12-31
Budget Start
2002-01-01
Budget End
2002-12-31
Support Year
2
Fiscal Year
2002
Total Cost
$202,500
Indirect Cost

  Institution

Name
University of Texas MD Anderson Cancer Center
Department
Internal Medicine/Medicine
Type
Other Domestic Higher Education
DUNS #
001910777
City
Houston
State
TX
Country
United States
Zip Code
77030

  Publications

Liu, P-P; Liu, J; Jiang, W-Q et al. (2016) Elimination of chronic lymphocytic leukemia cells in stromal microenvironment by targeting CPT with an antiangina drug perhexiline. Oncogene 35:5663-5673
Ogasawara, Marcia A; Liu, Jinyun; Pelicano, Helene et al. (2016) Alterations of mitochondrial biogenesis in chronic lymphocytic leukemia cells with loss of p53. Mitochondrion 31:33-39
Liu, Jinyun; Chen, Gang; Pelicano, Helene et al. (2016) Targeting p53-deficient chronic lymphocytic leukemia cells in vitro and in vivo by ROS-mediated mechanism. Oncotarget 7:71378-71389
Fiskus, Warren; Saba, Nakhle; Shen, Min et al. (2014) Auranofin induces lethal oxidative and endoplasmic reticulum stress and exerts potent preclinical activity against chronic lymphocytic leukemia. Cancer Res 74:2520-32
Liu, J; Chen, G; Feng, L et al. (2014) Loss of p53 and altered miR15-a/16-1?MCL-1 pathway in CLL: insights from TCL1-Tg:p53(-/-) mouse model and primary human leukemia cells. Leukemia 28:118-28
Liu, P-P; Liao, J; Tang, Z-J et al. (2014) Metabolic regulation of cancer cell side population by glucose through activation of the Akt pathway. Cell Death Differ 21:124-35
Pelicano, Hélène; Zhang, Wan; Liu, Jinyun et al. (2014) Mitochondrial dysfunction in some triple-negative breast cancer cell lines: role of mTOR pathway and therapeutic potential. Breast Cancer Res 16:434
Yuan, Shuqiang; Wang, Feng; Chen, Gang et al. (2013) Effective elimination of cancer stem cells by a novel drug combination strategy. Stem Cells 31:23-34
Garcia-Prieto, Celia; Riaz Ahmed, Kausar Begam; Chen, Zhao et al. (2013) Effective killing of leukemia cells by the natural product OSW-1 through disruption of cellular calcium homeostasis. J Biol Chem 288:3240-50
Trachootham, Dunyaporn; Chen, Gang; Zhang, Wan et al. (2013) Loss of p53 in stromal fibroblasts promotes epithelial cell invasion through redox-mediated ICAM1 signal. Free Radic Biol Med 58:1-13

Showing the most recent 10 out of 53 publications