Abstract

Considerable time and effort has been devoted to characterizing pathways of hormonal carcinogenesis with few clear results, although progress can be reported on the general theme of proto-oncogene activation/control/function. This proposal addresses a new approach to identify both molecular events and genes (proto-oncogenes/anti-oncogenes) involved in hormonal carcinogenesis of Syrian hamsters where 100% frequency of leiomyosarcoma induction is observed. Studies will be carried out based upon the hypothesis that hormones induce tumors by upregulating viral long terminal repeats (LTR), which induce retrotransposition, resulting in insertional mutation and neoplasia. There are three interrelated specific aims to accomplish our objectives.
SPECIFIC AIM 1 is to characterize enhancer-promoter activity of the hamster retroviral LTR subcloned into pSVOCAT. This will establish that the LTR is transcriptionally active, therefore, suitable for use in Specific Aim 2.
SPECIFIC AIM 2 has three parts. First, we will establish and validate that the APH(3')II neomycin- resistant gene, interrupted by insertion of an intron, is inactive in bacteria but active in eukaryotic cells. Second, we will construct and test retrotransposons. Third, we will establish and clone cells stably transfected with the above retrotransposons.
SPECIFIC AIM 3 will be to mutagenize stably transfected cells (hormones, growth factors, oncogenes, tumor promoters). The resultant transformed of the integration sites by recovery of the spliced APH(3')II gene and associated genomic DNA. Finally, genes contiguous with integration sites will be characterized for their contribution to the neoplastic process. In the future, based on successful completion of Specific Aim 3, transgenic mice an hamsters containing retrotransposons will be established. Ultimately, tracking of retrotransposition frequency and tissue specificity in the transgenic animals has potential for helping define pathways of hormonal and chemical carcinogenesis, as well as in elucidating the role of retroviral DNA in this process. Extension of this model to human hormonally related neoplastic disease such as prostate, breast, or uterine cancer is feasible in view of the increasing numbers of retroviral elements identified in the human genome.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
5R01CA052085-02
Application #
3196850
Study Section
Chemical Pathology Study Section (CPA)
Project Start
1990-05-01
Project End
1993-04-30
Budget Start
1991-05-01
Budget End
1992-04-30
Support Year
2
Fiscal Year
1991
Total Cost
Indirect Cost

  Institution

Name
Medical University of South Carolina
Department
Type
Schools of Medicine
DUNS #
183710748
City
Charleston
State
SC
Country
United States
Zip Code
29425

  Publications

DeHaven, J E; Schwartz, D A; Dahm, M W et al. (1998) Novel retroviral sequences are expressed in the epididymis and uterus of Syrian hamsters. J Gen Virol 79 ( Pt 11):2687-94
Maggouta, F; Li, S A; Li, J J et al. (1997) Glutathione S-transferase Yc cDNA from Syrian hamster kidney. Biochem J 323 ( Pt 1):147-9
Maggouta, F; Li, S A; Li, J J et al. (1996) Assignment of the mu-class glutathione S-transferase gene (hGSTYBX) to Syrian hamster chromosome 15 by FISH. Mamm Genome 7:469-70
Maxwell, I H; Spitzer, A L; Maxwell, F et al. (1995) The capsid determinant of fibrotropism for the MVMp strain of minute virus of mice functions via VP2 and not VP1. J Virol 69:5829-32
Fan, W; Cooper, T M; Norris, J S (1993) Characterization of selective glucocorticoid-dependent responses in a glucocorticoid-resistant smooth muscle tumor cell line. J Cell Physiol 156:88-95
Schwartz, D A; Dahm, M W; Bai, L et al. (1993) Construction of a retrotransposition indicator sequence using a neomycin resistance-encoding gene containing a functional intron. Gene 127:233-6
Fan, W; Trifiletti, R; Cooper, T et al. (1992) Cloning of a mu-class glutathione S-transferase gene and identification of the glucocorticoid regulatory domains in its 5' flanking sequence. Proc Natl Acad Sci U S A 89:6104-8
Schwartz, D A; Norris, J S (1992) Glucocorticoid, androgen, and retinoic acid regulation of glutathione S-transferase gene expression in hamster smooth muscle tumor cells. Biochem Biophys Res Commun 184:1108-13