Abstract

The research proposed in this application is designed to study late stages of tumor progression, especially invasion and metastasis of chemically-induced skin tumors. In this context we intend to study the evolution of markers of malignant conversion that proved useful to predict the early behavior of tumors, (changes in GGT, keratin polypeptide and chromosomal alterations) in invasive and metastasizing tumors produced by different protocols of chemical carcinogenesis. In addition to these parameters we will also investigate changes in cell surface alterations that have been linked to the """"""""advanced carcinoma phenotype"""""""" i.e., binding to laminin, fibronectin collagen IV, and lectins. Furthermore we will probe the biological behavior of tumors by studying their invasive and colonizing abilities. The picture of the invasive- metastasizing phenotype will e completed by correlating these changes with a histopathological and cytogenetical evaluation of the tumors, as well as by a study of eventual oncogene activation. During these planned experiments we propose to prove that the three stage carcinogenesis is more effective in producing invasive and metastasizing tumors than two stage carcinogenesis protocols. In particular we are interested in proving that radicals play an important role in the production of the advanced carcinoma phenotype. A series of experiments using benzoyl peroxide and hydrogen peroxide as third stage agents are proposed to further investigate this topic. Additional experiments using modifiers of free radicals are presented as an approach for a better understanding of the mechanisms by which free radical- generating compounds enhance the aggressive behavior of skin tumors. Our proposal contains experiments to investigate not only eventual differences in the tumor-metastasis yields with different protocols of chemical carcinogenesis; we also propose to study differences in the biological behavior and in some essential characteristics of advanced neoplasia, that have been shown to be important components of the """"""""invasive-metastasizing"""""""" phenotype. This will result in a more complete picture of experimental skin tumor development which has been extremely well studied in its initial stages but whose later stages (evolution of carcinomas, invasion, and metastasis) have not been studied in depth in this model of chemical carcinogenesis.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
2R01CA044980-03
Application #
3187895
Study Section
Chemical Pathology Study Section (CPA)
Project Start
1986-04-01
Project End
1993-01-31
Budget Start
1988-02-01
Budget End
1989-01-31
Support Year
3
Fiscal Year
1988
Total Cost
Indirect Cost

  Institution

Name
Fox Chase Cancer Center
Department
Type
DUNS #
042250712
City
Philadelphia
State
PA
Country
United States
Zip Code
19111

  Publications

Ruggeri, B A; Bauer, B; Zhang, S Y et al. (1994) Murine squamous cell carcinoma cell lines produced by a complete carcinogenesis protocol with benzo[a]pyrene exhibit characteristic p53 mutations and the absence of H-ras and cyl 1/cyclin D1 abnormalities. Carcinogenesis 15:1613-9
Klein-Szanto, A J; Ruggeri, B; Bianchi, A et al. (1993) Cellular and molecular changes during mouse skin tumor progression. Recent Results Cancer Res 128:193-204
Ruggeri, B; Caamano, J; Slaga, T J et al. (1992) Alterations in the expression of uvomorulin and Na+,K(+)-adenosine triphosphatase during mouse skin tumor progression. Am J Pathol 140:1179-85
Ruggeri, B; Caamano, J; Goodrow, T et al. (1991) Alterations of the p53 tumor suppressor gene during mouse skin tumor progression. Cancer Res 51:6615-21
Buchmann, A; Ruggeri, B; Klein-Szanto, A J et al. (1991) Progression of squamous carcinoma cells to spindle carcinomas of mouse skin is associated with an imbalance of H-ras alleles on chromosome 7. Cancer Res 51:4097-101
Chiba, M; Aldaz, C M; Conti, C J et al. (1991) Metastatic potential of mouse skin carcinomas produced by different protocols of chemical carcinogenesis. Invasion Metastasis 11:288-96
Klein-Szanto, A J (1991) The role of chemically induced epithelial hyperplasia in the development of human cancer. Prog Clin Biol Res 369:35-41
Bonfil, R D; Momiki, S; Conti, C J et al. (1989) Benzoyl peroxide enhances the invasive ability of a mouse epidermal carcinoma cell line. Int J Cancer 44:165-9
Klein-Szanto, A J; Larcher, F; Bonfil, R D et al. (1989) Multistage chemical carcinogenesis protocols produce spindle cell carcinomas of the mouse skin. Carcinogenesis 10:2169-72