Abstract

Ultraviolet light (UVL)-induced carcinogenesis in mice represents an excellent model to study tumor immunology. The majority of primary neoplasms induced with this physical agent are immunologically rejected when transplanted to normal syngeneic recipients but capable of progressive growth when transplanted to UVL-exposed animals. This observation has been extensively investigated and appears to be due, at least in part, to effects mediated by UVL directly on the immunological apparatus. To date, UVL-induced tumors have mainly served as a tool to study this biological phenomenon.
The aim of our study is to address a number of questions crucial to the development of this model, using a reversal of the tack taken in past investigations. Employing tumor-specific immunity as a tool, we propose: (1) to question the clonal nature of UVL-induced tumors; (2) to question the possibility that tumor-tumor or tumor-somatic cell hybridization may represent an integral component of normal tumor progression; (3) to further analyze the tumorigenic heterogeneity of cells within primary UVL-induced regressor phenotype tumors; (4) to determine whether the gene(s) which encodes for UVL-mediated transformation and the gene(s) which encodes for a particular TSTA are identical or at least linked; and (5) to investigate further the phenomenon that cloned lines derived from UVL-regressor phenotype tumors can be converted with normal splenocytes (induction, selection, or both) to a virulent progressor which expresses a TSTA identical to the original cell line. The facilities and technical expertise needed to conduct these studies are unique in that a basic understanding of contemporary cellular immunology, tumor immunology, photobiology, somatic cell genetics, and molecular genetics is essential. It is obvious that many aspects of experimental photocarcinogenesis have important human implications. UVL represents a well-recognized and documented human carcinogen, and its ability to modify certain human immune responses is just beginning to be appreciated. (M)

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
5R01CA033065-06
Application #
3170997
Study Section
Experimental Immunology Study Section (EI)
Project Start
1982-08-01
Project End
1988-07-31
Budget Start
1987-08-01
Budget End
1988-07-31
Support Year
6
Fiscal Year
1987
Total Cost
Indirect Cost

  Institution

Name
University of Utah
Department
Type
Schools of Medicine
DUNS #
City
Salt Lake City
State
UT
Country
United States
Zip Code
84112

  Publications

Araneo, B A; Shelby, J; Li, G Z et al. (1993) Administration of dehydroepiandrosterone to burned mice preserves normal immunologic competence. Arch Surg 128:318-25
Daynes, R A; Araneo, B A; Ershler, W B et al. (1993) Altered regulation of IL-6 production with normal aging. Possible linkage to the age-associated decline in dehydroepiandrosterone and its sulfated derivative. J Immunol 150:5219-30
Daynes, R A; Araneo, B A (1992) Programming of lymphocyte responses to activation: extrinsic factors, provided microenvironmentally, confer flexibility and compartmentalization to T-cell function. Chem Immunol 54:1-20
Meikle, A W; Dorchuck, R W; Araneo, B A et al. (1992) The presence of a dehydroepiandrosterone-specific receptor binding complex in murine T cells. J Steroid Biochem Mol Biol 42:293-304
Daynes, R A; Araneo, B A (1992) Natural regulators of T-cell lymphokine production in vivo. J Immunother (1991) 12:174-9
Wiedmeier, S E; Araneo, B A; Huang, K et al. (1991) Thymic modulation of IL-2 and IL-4 synthesis by peripheral T cells. Cell Immunol 135:501-18
Araneo, B A; Dowell, T; Diegel, M et al. (1991) Dihydrotestosterone exerts a depressive influence on the production of interleukin-4 (IL-4), IL-5, and gamma-interferon, but not IL-2 by activated murine T cells. Blood 78:688-99
Daynes, R A; Dowell, T; Araneo, B A (1991) Platelet-derived growth factor is a potent biologic response modifier of T cells. J Exp Med 174:1323-33
Huang, K; Beigi, M; Daynes, R A (1990) Peripheral lymph node-specific and Peyer's patch-specific homing receptors are differentially regulated following lymphocyte activation. Reg Immunol 3:103-11
Daynes, R A; Araneo, B A; Dowell, T A et al. (1990) Regulation of murine lymphokine production in vivo. III. The lymphoid tissue microenvironment exerts regulatory influences over T helper cell function. J Exp Med 171:979-96

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