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Panozzo, J.; Akan, E.; Griffiths, T.D.
Argonne National Lab., IL (United States); Northern Illinois Univ., De Kalb, IL (United States). Dept. of Biological Sciences. Funding organisation: USDOE, Washington, DC (United States)1996
Argonne National Lab., IL (United States); Northern Illinois Univ., De Kalb, IL (United States). Dept. of Biological Sciences. Funding organisation: USDOE, Washington, DC (United States)1996
AbstractAbstract
[en] Previous work by many groups has documented induction of the HIV-LTR following exposure of cells to ultraviolet light and other DNA damaging agents. Our experiments set out to determine the relative activation or repression of the HIV-LTR in response to two classes of chemotherapeutic agents: Doxorubicin is a DNA-damage inducing agent, and 5-fluorouracil has an antimetabolic mode of action. Using HeLa cells stably transfected with a construct in which HIV-LTR drives expression of the chloramphenicol acetyl transferase reporter gene, we demonstrated an up to 10-fold induction following doxorubicin treatment in 24 h post-treatment. This induction was repressed by treatment with salicylic acid, suggesting a role for prostaglandin/cyclo-oxygenase pathways and/or NFKB in the inductive response. Induction by 5-fluorouracil, in contrast, was more modest (two-fold at most) though it was consistently elevated over controls
Primary Subject
Source
1996; 25 p; CONTRACT W-31109-ENG-38; Also available from OSTI as DE96007466; NTIS; US Govt. Printing Office Dep
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Report
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Country of publication
ANIMAL CELLS, ANTIBIOTICS, ANTI-INFECTIVE AGENTS, ANTIMETABOLITES, ANTINEOPLASTIC DRUGS, AZINES, DRUGS, ELECTROMAGNETIC RADIATION, HETEROCYCLIC COMPOUNDS, HYDROGEN COMPOUNDS, HYDROXY COMPOUNDS, ISOTOPE APPLICATIONS, MICROORGANISMS, ORGANIC COMPOUNDS, ORGANIC FLUORINE COMPOUNDS, ORGANIC HALOGEN COMPOUNDS, ORGANIC NITROGEN COMPOUNDS, PARASITES, PYRIMIDINES, RADIATIONS, TUMOR CELLS, URACILS, VIRUSES
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