Abstract

Our objective is to elucidate the mechanism(s) by which naturally occurring organosulfur compounds (OSCs) inhibit benzo(a)pyrene (BP) induced neoplasia of lung and forestomach in mice. It is well known that BP induced neoplasia depends upon the activation/inactivation pathways of its metabolism. While cytochrome P450 dependent monooxygenases contribute to the generation of reactive metabolites including the ultimate carcinogenic species anti-BPDE, glutathione transferases (GST) and UDP- glucuronyl transferase (UDP-GT) play an important role in detoxification of BP metabolites. Thus, it is reasonable to hypothesize that OSCs may exert anti-neoplastic activity by modulating the activation and/or inactivation pathways of BP metabolism. Although OSC treatment is known to increase GST activity in certain mice tissues, their effect on other pathways of BP metabolism are not fully known. The role of BP activation pathways in chemoprevention by OSCs will be assessed by determining the effect of OSCs on (i) cellular levels as well as catalytic activities of the enzymes involved in bioactivation of BP, (ii) nature and persistence of BP-DNA adduction, and (iii) pattern of BP metabolism in female A/J mice liver, lung and forestomach. Effect of OSCs on inactivation pathways of BP metabolism will also be determined to evaluate their significance in the anti-neoplastic activity of these phytochemicals. To accomplish this, we propose to determine the effect of OSCs on the levels of individual GST isoenzymes and UDP-GT in mice tissues. Substrate specificity and kinetic constants of purified murine GSTs for the conjugation of anti-BPDE with GSH will also be determined. Finally, to establish the significance of GST induction in anti-neoplastic activity of OSCs, we propose to determine the effect of buthionine sulfoximine induced GSH depletion (which will interfere with the GST catalyzed inactivation of anti-BPDE) on BP induced neoplasia of lung and forestomach in control and OSC treated animals. Diallyl sulfide, diallyl disulfide and diallyl trisulfide will be utilized in these studies to uncover the reasons for the differential effectiveness and tissue selectivity of certain OSCs. Saturated analogues of diallyl sulfide and diallyl disulfide (dipropyl sulfide and dipropyl disulfide, respectively), which do not inhibit BP induced neoplasia, will be used as negative controls and may help in identifying the mechanism(s) involved in chemoprevention by OSCs. These studies, in the long term, may prove to be useful in developing strategies for chemoprevention.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
1R01CA055589-01A3
Application #
2096712
Study Section
Metabolic Pathology Study Section (MEP)
Project Start
1995-04-01
Project End
1999-01-31
Budget Start
1995-04-01
Budget End
1996-01-31
Support Year
1
Fiscal Year
1995
Total Cost
Indirect Cost

  Institution

Name
Mercy Hospital of Pittsburgh
Department
Type
DUNS #
City
Pittsburgh
State
PA
Country
United States
Zip Code
15219

  Publications

Herman-Antosiewicz, Anna; Powolny, Anna A; Singh, Shivendra V (2007) Molecular targets of cancer chemoprevention by garlic-derived organosulfides. Acta Pharmacol Sin 28:1355-64
Pal, A; Gu, Y; Pan, S S et al. (2001) C-terminal region amino acid substitutions contribute to catalytic differences between murine class alpha glutathione transferases mGSTA1-1 and mGSTA2-2 toward anti-diol epoxide isomers of benzo[c]phenanthrene. Biochemistry 40:7047-53
Srivastava, S K; Hu, X; Xia, H et al. (1999) Gender related differences in ATP-dependent transport of dinitrophenyl-glutathione conjugate across murine canalicular liver plasma membrane. FEBS Lett 445:291-4
Hu, X; Seidel, A; Frank, H et al. (1998) Differential enantioselectivity of murine glutathione S-transferase isoenzymes in the glutathione conjugation of trans-3,4-dihydroxy-1, 2-oxy-1,2,3,4-tetrahydrobenzo[c]phenanthrene stereoisomers. Arch Biochem Biophys 358:40-8
Hu, X; Singh, S V (1997) Differential catalytic efficiency and enantioselectivity of murine glutathione S-transferase isoenzymes in the glutathione conjugation of carcinogenic anti-diol epoxides of chrysene and benzo(g)chrysene. Arch Biochem Biophys 345:318-24
Hu, X; Singh, S V (1997) Glutathione S-transferases of female A/J mouse lung and their induction by anticarcinogenic organosulfides from garlic. Arch Biochem Biophys 340:279-86
Hu, X; Benson, P J; Srivastava, S K et al. (1997) Induction of glutathione S-transferase pi as a bioassay for the evaluation of potency of inhibitors of benzo(a)pyrene-induced cancer in a murine model. Int J Cancer 73:897-902
Hu, X; O'Donnell, R; Srivastava, S K et al. (1997) Active site architecture of polymorphic forms of human glutathione S-transferase P1-1 accounts for their enantioselectivity and disparate activity in the glutathione conjugation of 7beta,8alpha-dihydroxy-9alpha,10alpha-ox y-7,8,9,10-tetrahydrobenzo(a)pyre Biochem Biophys Res Commun 235:424-8
Hu, X; Benson, P J; Srivastava, S K et al. (1996) Glutathione S-transferases of female A/J mouse liver and forestomach and their differential induction by anti-carcinogenic organosulfides from garlic. Arch Biochem Biophys 336:199-214
Hu, X; Srivastava, S K; Xia, H et al. (1996) An alpha class mouse glutathione S-transferase with exceptional catalytic efficiency in the conjugation of glutathione with 7beta, 8alpha-dihydroxy-9alpha,10alpha-oxy-7,8,9,10-tetrahydrobenzo(a)pyrene. J Biol Chem 271:32684-8