Abstract

The carcinogen N-methyl-N-nitrosourea (MNU) induces thymic lymphoma development in various inbred mouse strains. The AKR strain is particularly susceptible, experiencing a higher incidence and shorter latency (2-3 months) for MNU-induced lymphoma development than other inbred mouse strains. The molecular basis for the enhanced susceptibility of the AKR strain is not clear. However, in contrast to most inbred strains, untreated AKR mice develop spontaneous thymic lymphoma after 8 months of age due to the generation of recombinant oncogenic murine leukemia viruses (MuLV). Several reports implicate endogenous MuLV as co-factors in chemical carcinogenesis. Therefore, I have proposed that the enhanced susceptibility of AKR mice to MNU-induced lymphomagenesis involves participation of endogenous MuLV in the multistage pathway resulting in neoplastic transformation. Recently, we found aberrant expression of functional interleukin-2 receptors (IL-2Rs) on MNU-induced lymphomas. This is interesting since these tumors correspond to immature T-cells that normally down-regulate IL-2R expression. Furthermore, preliminary data suggest that IL-2Rs on MNU-induced lymphomas are associated with the MuLV envelop glycoprotein, gp70. Similar observations have been made in Friend MuLV induced erythroleukemia in which binding of a defective MuLV envelop protein gp55 to erythropoietin receptors in immature erythroblasts induces prolonged proliferation of the preneoplastic target population. In view of this precedent and preliminary data from our lab, I am proposing that NM activates expression of endogenous MuLV gp70 which can bind to and stimulate lL-2Rs on initiated thymocytes. This event is likely to trigger accelerated expansion and progression of the target population explaining, in part, the predisposition of the AKR strain to develop a high incidence of early appearing MNU-induced lymphomas.
The specific aims for this proposal are: (1). To characterize the IL-2Rs expressed on MNU-induced lymphomas with respect to number, affinity, polypeptide chain structure and functional activity. (2.) To assess IL-2R protein and mRNA expression in specific thymocyte subsets at various intervals after MNU treatment and isolate IL-2R bearing cells for analysis of clonality and oncogene activation. (3.) To determine if there is a specific cell surface and/or intracellular association between IL-2Rs and MuLV gp70 molecules in MNU-induced lymphomas as well as in thymocyte subsets obtained at intervals after MNU treatment. (4.) To identify, using a panel of monoclonal antibodies, the class(es) of endogenous MuLV gp70 molecules expressed on lymphomas and preneoplastic thymocytes as a consequence of MNU activation and to isolate relevant gp70 molecules for analysis of IL-2R binding and stimulation. (5.) To molecularly clone endogenous MuLV sequences that encode the gp70 subclass defined by specific aim #4 and develop constructs for future retroviral mediated gene transfer.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
2R01CA037912-07
Application #
3175859
Study Section
Chemical Pathology Study Section (CPA)
Project Start
1984-08-01
Project End
1997-04-30
Budget Start
1992-07-01
Budget End
1993-04-30
Support Year
7
Fiscal Year
1992
Total Cost
Indirect Cost

  Institution

Name
University of Texas MD Anderson Cancer Center
Department
Type
Organized Research Units
DUNS #
001910777
City
Houston
State
TX
Country
United States
Zip Code
77030

  Publications

Gomez, G; Clarkin, K Z; Kraig, E et al. (2000) TCR v(beta) repertoire restriction and lack of CDR3 conservation implicate TCR-superantigen interactions in promoting the clonal evolution of murine thymic lymphomas. Int Immunol 12:263-70
Richie, E R; Walker, D A (2000) Production and characterization of immature murine T-lymphoma cell lines. Methods Mol Biol 134:177-84
Robles, A I; Larcher, F; Whalin, R B et al. (1996) Expression of cyclin D1 in epithelial tissues of transgenic mice results in epidermal hyperproliferation and severe thymic hyperplasia. Proc Natl Acad Sci U S A 93:7634-8
Richie, E R; Angel, J M; Rinchik, E M (1996) Tlag1, a novel murine tumor susceptibility gene that regulates MNU-induced thymic lymphoma development. Prog Clin Biol Res 395:23-32
Poetschke, H L; Klug, D B; Walker, D et al. (1996) Cross-linking the TCR complex induces apoptosis in CD4+8+ thymocytes in the presence of cyclosporin A. Dev Immunol 5:1-15
Romach, E; Moore, J; Rummel, S et al. (1994) Influence of sex and carcinogen treatment protocol on tumor latency and frequency of K-ras mutations in N-methyl-N-nitrosourea-induced lymphomas. Carcinogenesis 15:2275-80
Richie, E R; McEntire, B B; Coghlan, L et al. (1991) Murine T-lymphomas corresponding to the immature CD4-8+ thymocyte subset. Dev Immunol 1:255-63
Stettner, S L; Rummel, S A; Conti, C J et al. (1991) N-methyl-N-nitrosourea alters thymocyte subset distribution and targets immature CD4-8+ cells for lymphoma development. Cancer Res 51:737-40
Richie, E R; Angel, J M; Cloyd, M W (1991) Influence of murine leukemia proviral integrations on development of N-methyl-N-nitrosourea-induced thymic lymphomas in AKR mice. J Virol 65:5751-6
Nairn, R S; McIntyre, B W; Richie, E R et al. (1989) Characterization of env gene recombination in x-ray--induced thymomas of C57BL/6 mice. Mol Carcinog 2:126-30

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