Abstract

Our long-term objective has been the study of the molecular/cellular mechanisms for the initiation and promotion phases of carcinogenesis using a variety of in vitro approaches. In this proposal, we plan to focus entirely on the promotion/progression phases of carcinogenesis.
The aim i s to test the specific hypothesis that gap junctional intercellular communication (GJIC) might play a role in tumor promotion and possibly the progression phase of carcinogenesis. The rationale supporting this aim is based on the observations that: (a) most, if not all, malignant cells have altered selective or universal gap junctional communication; (b) most known chemical tumor promoters have been shown to down-regulate gap junction function, in a reversible fashion; (c) several oncogenes (e.g., src, ras, raf, neu, mos, but not myc) are associated with stable down-regulation of GJIC; (d) several anti-tumor promoters or anti-tumor agents (e.g., retinoids and lovastatin) are associated with the MR-regulation of GJIC, and (e) several tumor suppressor genes have been linked to the up-regulation of GJIC. Therefore, we plan to test several hypotheses for the biochemical mechanisms by which two different classes of chemical tumor promoters (phorbol ester; DDT), a few oncogenes (ras and neu), tumor suppressor genes (Stanbridge's human suppressor gene) and anti-tumor promoters or anti-tumor agents (e.g., lovastatin; retinoids) might modulate gap junction function. In addition, in order to directly test the hypothesis that GJIC plays a role in carcinogenesis, an attempt will be made to restore GJIC in GJIC-deficient and tumorigenic rat liver epithelial cell mutants by transfection with several cloned gap junction genes in various expression vectors. We will also transfect GJIC proficient, non-tumorigenic rat liver cells with a gap junction anti-sense gene to test the hypothesis that the specific loss of functional the gap junction message will result in a non-communicating cell which will be tumorigenic when placed back in the rat liver. To accomplish these goals, various biological, biochemical, and molecular techniques available in our laboratory (e.g., fluorescence redistribution after photobleaching, scrape-loading/dye transfer assays, molecular/antibody probing, using cDNAs and antibodies to various gap junction genes and proteins, DNA cloning, amplification, cloning and transfer, etc.) will be employed.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
5R01CA021104-17
Application #
2086904
Study Section
Chemical Pathology Study Section (CPA)
Project Start
1977-06-01
Project End
1996-04-30
Budget Start
1995-05-01
Budget End
1996-04-30
Support Year
17
Fiscal Year
1995
Total Cost
Indirect Cost

  Institution

Name
Michigan State University
Department
Pediatrics
Type
Schools of Medicine
DUNS #
193247145
City
East Lansing
State
MI
Country
United States
Zip Code
48824

  Publications

Upham, Brad L; Suzuki, Junji; Chen, Gang et al. (2003) Reduced gap junctional intercellular communication and altered biological effects in mouse osteoblast and rat liver oval cell lines transfected with dominant-negative connexin 43. Mol Carcinog 37:192-201
Na, Hye-Kyung; Chang, Chia-Cheng; Trosko, James E (2003) Growth suppression of a tumorigenic rat liver cell line by the anticancer agent, ET-18-O-CH(3), is mediated by inhibition of cytokinesis. Cancer Chemother Pharmacol 51:209-15
Holland, Margo S; Tai, Mei-Hui; Trosko, James E et al. (2003) Isolation and differentiation of bovine mammary gland progenitor cell populations. Am J Vet Res 64:396-403
Carruba, Giuseppe; Webber, Mukta M; Quader, Salmaan T A et al. (2002) Regulation of cell-to-cell communication in non-tumorigenic and malignant human prostate epithelial cells. Prostate 50:73-82
Chang, C C; Sun, W; Cruz, A et al. (2001) A human breast epithelial cell type with stem cell characteristics as target cells for carcinogenesis. Radiat Res 155:201-207
Trosko, J E (2001) Commentary: is the concept of ""tumor promotion"" a useful paradigm? Mol Carcinog 30:131-7
Trosko, J E; Chang, C C (2001) Role of stem cells and gap junctional intercellular communication in human carcinogenesis. Radiat Res 155:175-180
Saunders, M M; You, J; Trosko, J E et al. (2001) Gap junctions and fluid flow response in MC3T3-E1 cells. Am J Physiol Cell Physiol 281:C1917-25
Na, H K; Wilson, M R; Kang, K S et al. (2000) Restoration of gap junctional intercellular communication by caffeic acid phenethyl ester (CAPE) in a ras-transformed rat liver epithelial cell line. Cancer Lett 157:31-8
Trosko, J E; Chang, C C (2000) Modulation of cell-cell communication in the cause and chemoprevention/chemotherapy of cancer. Biofactors 12:259-63

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