Abstract

The long-term objectives of the proposed work are to understand the biochemical mechanism(s) of supranutritional Se in chemoprevention and to utilize this information for mechanistic clinical studies. A chemopreventive role of selenium (Se) in cancers has been implicated in several clinical and numerous animal studies but whether Se is effective against tobacco smoke (TS)-induced lung cancers is unknown. Nor is it clear in general on the form(s) of Se that are chemopreventive. Lung cancer is a leading cause of cancer death and TS-induced lung cancer may be on the rise worldwide due to growing smoking habit. Thus, the specific aims of this proposal are: 1) To examine whether dietary Se supplement in the form of selenized yeast (Se-yeast) or its major component selenomethionine (Se-Met) is chemopreventive for mice that have """"""""quit"""""""" smoking; 2) To characterize biomarkers of Se action such as apoptotic markers and selenoproteins that have been established in other chemoprevention studies so that Se chemoprevention can be understood better at the molecular level; 3) To investigate whether a synergism exists between Se and other chemopreventive agents such as the glucocorticoid hormone budesonide and retinoid isotretinoin in TS induction of lung cancers. To fulfill these aims, the A/J mice model which is the only animal model for TS-induced lung cancer will be employed. Mice will be pre-exposed to tobacco smoke to induce lung tumors during the recovery phase. The effect of dietary Se-yeast or Se-Met supplement during the recovery phase on tumor incidence and/or multiplicity will be measured to see if Se supplement is effective in reducing tumor formation and if additional Se form(s) in Se-yeast may be active. Major Se metabolites present in Se-yeast in addition to Se-Met will be characterized by a combination of NMR and HPLC coupled to mass spectrometry. The Se action will be characterized both immunocytochemically and in lung extracts by a series of apoptotic markers including cytochrome c release, activation of caspases, production of caspase cleavage products, and DNA fragmentation will be measured, along with the activation of selenoprotein, thioredoxin reductase. These biomarkers are known to be elicited in other Se chemoprevention studies. A similar approach will be used to investigate any interactive effect of Se-yeast supplement and budesonide or isotretinoin administered via inhalation; the latter two agents are also known to cause apoptosis. Biomarker characterization should reveal whether synergism is mediated via apoptosis.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
5R01CA101199-03
Application #
6895899
Study Section
Special Emphasis Panel (ZCA1-SRRB-Y (J2))
Program Officer
Steele, Vernon E
Project Start
2003-06-01
Project End
2007-05-31
Budget Start
2005-06-01
Budget End
2007-05-31
Support Year
3
Fiscal Year
2005
Total Cost
$240,233
Indirect Cost

  Institution

Name
University of California Davis
Department
Type
Organized Research Units
DUNS #
047120084
City
Davis
State
CA
Country
United States
Zip Code
95618

  Publications

Tarrado-Castellarnau, Míriam; Cortés, Roldán; Zanuy, Miriam et al. (2015) Methylseleninic acid promotes antitumour effects via nuclear FOXO3a translocation through Akt inhibition. Pharmacol Res 102:218-34
Sellers, Katherine; Fox, Matthew P; Bousamra 2nd, Michael et al. (2015) Pyruvate carboxylase is critical for non-small-cell lung cancer proliferation. J Clin Invest 125:687-98
Higashi, Richard M; Fan, Teresa W-M; Lorkiewicz, Pawel K et al. (2014) Stable isotope-labeled tracers for metabolic pathway elucidation by GC-MS and FT-MS. Methods Mol Biol 1198:147-67
Fan, Teresa W-M; Lorkiewicz, Pawel K; Sellers, Katherine et al. (2012) Stable isotope-resolved metabolomics and applications for drug development. Pharmacol Ther 133:366-91
Fan, Teresa W-M; Tan, Jinlian; McKinney, Martin M et al. (2012) Stable Isotope Resolved Metabolomics Analysis of Ribonucleotide and RNA Metabolism in Human Lung Cancer Cells. Metabolomics 8:517-527
Fan, Teresa W-M; Lane, Andrew N (2011) NMR-based stable isotope resolved metabolomics in systems biochemistry. J Biomol NMR 49:267-80
Moseley, Hunter N B; Lane, Andrew N; Belshoff, Alex C et al. (2011) A novel deconvolution method for modeling UDP-N-acetyl-D-glucosamine biosynthetic pathways based on (13)C mass isotopologue profiles under non-steady-state conditions. BMC Biol 9:37
Selivanov, Vitaly A; Vizán, Pedro; Mollinedo, Faustino et al. (2010) Edelfosine-induced metabolic changes in cancer cells that precede the overproduction of reactive oxygen species and apoptosis. BMC Syst Biol 4:135
Fan, Teresa W M; Lane, Andrew N; Higashi, Richard M et al. (2009) Altered regulation of metabolic pathways in human lung cancer discerned by (13)C stable isotope-resolved metabolomics (SIRM). Mol Cancer 8:41
Fan, Teresa W M; Kucia, Magda; Jankowski, Kacper et al. (2008) Rhabdomyosarcoma cells show an energy producing anabolic metabolic phenotype compared with primary myocytes. Mol Cancer 7:79

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