Abstract

Generation of T call-dependent immune responses involves a series of complex, and generally highly specific cellular interactions. Many of these interactions are controlled by the gene products of the Major Histocompatibility Complex (MHC). In the experiments described in this proposal, we will examine several aspects of MHC Class II restricted antigen presentation. The importance of MHC Class II intracellular trafficking for presentation of protein antigens will be examined through the analysis of sequence variants of these molecules. Wild type MHC molecules will be compared biochemically in order to identify the influence of polymorphism on immunologically relevant intracellular trafficking events. In addition to these studies, the role that conserved features in Class II-molecules have on activation of CD4 T calls will be analyzed, placing special emphasis on the region of the molecules that interact with accessory molecules such as CD4. The intracellular sorting events that control presentation of endogenously synthesized antigen will also be examined. A model antigen synthesized by APC and presented in the context Class II will be modified by recombinant DNA techniques, so that protein expression is redirected to particular subcellular sites. Transfectants bearing the Class II restriction element and the wild type or modified target antigen will be tested for their ability to stimulate a panel of specific T cells, so that the requirements for Class II restricted presentation of internally synthesized antigens can be defined. Finally, in order to study whether Class II positive cells of different lineages possess unique features of antigen processing or Class II trafficking, we propose a strategy to derive autonomously growing calls representing rare cell type in vivo, such as splenic dendritic cells and thymic epithelial calls. Transgenic mice will be constructed that express the SV40 T antigen under the control of the MHC Class II promoter. Class II positive tumors from such mice will be adapted to culture an used for biochemical and functional studies. Together, these studies will clarify the molecular events that control Class II restricted presentation of antigen in vivo. Such knowledge will offer possibilities for the development of rational approaches to modulating T call-dependent immune responses.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Program Projects (P01)
Project #
5P01CA019266-15
Application #
3793629
Study Section
Project Start
Project End
Budget Start
Budget End
Support Year
15
Fiscal Year
1992
Total Cost
Indirect Cost

  Institution

Name
University of Chicago
Department
Type
DUNS #
225410919
City
Chicago
State
IL
Country
United States
Zip Code
60637

  Publications

Hekmatpanah, Javad (2007) Cerebral microvessel perfusion and pathologic alteration of the brain during drowsiness and coma caused by brain tumor: a laboratory study on rats. Surg Neurol 67:564-71;discussion 571
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Bergmann, B M; Rechtschaffen, A; Gilliland, M A et al. (1996) Effect of extended sleep deprivation on tumor growth in rats. Am J Physiol 271:R1460-4
Van Waes, C; Monach, P A; Urban, J L et al. (1996) Immunodominance deters the response to other tumor antigens thereby favoring escape: prevention by vaccination with tumor variants selected with cloned cytolytic T cells in vitro. Tissue Antigens 47:399-407
Cronin 2nd, D C; Stack, R; Fitch, F W (1995) IL-4-producing CD8+ T cell clones can provide B cell help. J Immunol 154:3118-27
Gottschalk, A R; McShan, C L; Kilkus, J et al. (1995) Resistance to anti-IgM-induced apoptosis in a WEHI-231 subline is due to insufficient production of ceramide. Eur J Immunol 25:1032-8
Pekarek, L A; Starr, B A; Toledano, A Y et al. (1995) Inhibition of tumor growth by elimination of granulocytes. J Exp Med 181:435-40
Monach, P A; Meredith, S C; Siegel, C T et al. (1995) A unique tumor antigen produced by a single amino acid substitution. Immunity 2:45-59
Seung, L P; Seung, S K; Schreiber, H (1995) Antigenic cancer cells that escape immune destruction are stimulated by host cells. Cancer Res 55:5094-100
Lancki, D W; Qian, D; Fields, P et al. (1995) Differential requirement for protein tyrosine kinase Fyn in the functional activation of antigen-specific T lymphocyte clones through the TCR or Thy-1. J Immunol 154:4363-70

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