Abstract

) The objective is to test whether ionizing radiation (IR) induced Ca2+ transients are critical for activation of cell cycle checkpoints; and if genetic manipulation of Ca2+ homeostasis will blunt IR-induced Ca2+ transients, short circuit IR induced cell cycle checkpoints and alter radio-sensitivity. Ca2+ homeostasis of two breast carcinoma cell lines, MCF-7 and MDA-MB-231, has been genetically manipulated by stable transfection with the B-lymphocyte Ca2+ channel, CD20, under control of an inducible promoter. An initial characterization reveals that CD20 expression increases cytosolic free [Ca2+], shortens G1 of the cell cycle, and blocks the IR-induced G1 arrest.
Three aims are proposed: (1) Continue characterization of the CD20-expressing clones to include measurements of cytosolic free [Ca2+], growth and cell cycle analysis. Representative clones and a null point assay developed to determine at what extracellular [Ca2+], the radio- biological and cell-cycle control properties of the parental and non- induced CD20 transfected cell lines are recovered in the CD20 expressing sensitive responses to IR; (2) Test whether expression of CD20 alters the IR-induced Ca2+ oscillations and the size of internal Ca2+ stores and establish the linkage between the IR-induced Ca2+ transients and cell cycle checkpoints; (3) Define Ca2+-sensitive IR-induced cell cycle checkpoints. Initially, the G1/S checkpoint of MCF7 cells will be examined since this is abrogated in CD20 Rb phosphorylation checkpoint to the Ca2+- sensitive event. Studies will focus on the synthesis, stabilities, and activities of key regulatory proteins, e.g. cyclin dependent kinases and their endogenous inhibitors, the goal being to define the most immediate, Ca2+-dependent event necessary for checkpoint activation. Based on results from Aim #1, Ca2+-sensitive S-or G2-checkpoints will be examined with the overall approach guided by the analysis of the G1/S checkpoint. Results from this experimentation may indicate possible targets for therapeutic manipulation of tumor cell radio-sensitivity.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Program Projects (P01)
Project #
5P01CA072955-04
Application #
6475010
Study Section
Project Start
2001-08-01
Project End
2003-07-31
Budget Start
1998-10-01
Budget End
1999-09-30
Support Year
4
Fiscal Year
2001
Total Cost
$184,121
Indirect Cost

  Institution

Name
Virginia Commonwealth University
Department
Type
DUNS #
City
Richmond
State
VA
Country
United States
Zip Code
23298

  Publications

Biddlestone-Thorpe, Laura; Marchi, Nicola; Guo, Kathy et al. (2012) Nanomaterial-mediated CNS delivery of diagnostic and therapeutic agents. Adv Drug Deliv Rev 64:605-13
Cardnell, Robert J G; Mikkelsen, Ross B (2011) Nitric oxide synthase inhibition enhances the antitumor effect of radiation in the treatment of squamous carcinoma xenografts. PLoS One 6:e20147
Hawkins, Amy J; Golding, Sarah E; Khalil, Ashraf et al. (2011) DNA double-strand break - induced pro-survival signaling. Radiother Oncol 101:13-7
Dever, Seth M; Golding, Sarah E; Rosenberg, Elizabeth et al. (2011) Mutations in the BRCT binding site of BRCA1 result in hyper-recombination. Aging (Albany NY) 3:515-32
Khalil, Ashraf; Morgan, Rhiannon N; Adams, Bret R et al. (2011) ATM-dependent ERK signaling via AKT in response to DNA double-strand breaks. Cell Cycle 10:481-91
Bayden, Alexander S; Yakovlev, Vasily A; Graves, Paul R et al. (2011) Factors influencing protein tyrosine nitration--structure-based predictive models. Free Radic Biol Med 50:749-62
Yakovlev, Vasily A; Rabender, Christopher S; Sankala, Heidi et al. (2010) Proteomic analysis of radiation-induced changes in rat lung: Modulation by the superoxide dismutase mimetic MnTE-2-PyP(5+). Int J Radiat Oncol Biol Phys 78:547-54
Adams, Bret R; Golding, Sarah E; Rao, Raj R et al. (2010) Dynamic dependence on ATR and ATM for double-strand break repair in human embryonic stem cells and neural descendants. PLoS One 5:e10001
Yakovlev, Vasily A; Bayden, Alexander S; Graves, Paul R et al. (2010) Nitration of the tumor suppressor protein p53 at tyrosine 327 promotes p53 oligomerization and activation. Biochemistry 49:5331-9
Akopiants, Konstantin; Zhou, Rui-Zhe; Mohapatra, Susovan et al. (2009) Requirement for XLF/Cernunnos in alignment-based gap filling by DNA polymerases lambda and mu for nonhomologous end joining in human whole-cell extracts. Nucleic Acids Res 37:4055-62

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