Abstract

This proposal is designed to seek basic information on the properties of unprimed L3T4+ and Lyt-2+ T cell subsets responding to H-2 alloantigens. Particular emphasis is placed on studying Lyt-2+ cells since less is known about these cells than L3T4+ cells. Three broad areas of investigation are proposed: 1) Variation in the responsiveness of Lyt-2+ cells. Although purified Lyt-2+ cells can give very high responses to class I (but not class II) H-2 alloantigens in the absence of added lymphokines, certain class I differences are much less immunogenic than others. Moreover, the general level of responsiveness of Lyt-2+ cells can vary considerably from one strain to another. Various approaches, including the use of thymus-grafted chimeras and recombinant inbred mice, will be used to seek further information on these two levels of variability in the responsiveness of Lyt-2+ cells. 2) Stimulatory requirements for Lyt-2+ cells in vitro. Whereas L3T4+ cells respond solely to Ia+ cells, Lyt-2+ cells can be stimulated by class I differences expressed or certain Ia- cells. Whereas normal allogeneic T cells are nonstimulatory for Lyt-2+ cells unless supplemented with lymphokines, Lyt-2+ cells respond strongly to a subpopulation of Thy 1- Ia- cells present in spleen and marrow. Unprimed Lyt-2+ cells also respond to certain Ia- tumor cells, including T tumors. By scrutinizing the response of Lyt-2+ cells to these tumor cells, we hope to obtain information on what signals are needed for Lyt-2+ cell induction. 3) In vivo functions of T cell subsets. Four approaches will be used to seek further information on the behavior of T cell subsets in vivo. First, the Winn assay will be used to examine the capacity of Lyt-2+ cells to reject various types of allogeneic tumor cells; preliminary work has shown that mixing allogeneic tumor cells with unprimed Lyt-2+ cells and injecting the cells subcutaneously into irradiated mice prevents the appearance of macroscopic tumors. Second, studies with bone marrow chimeras will be used to determine whether Lyt-2+ cells have the capacity to recognize allo class I molecules on non-marrow derived cells. Third, detailed information will be sought on the capacity of L3T4+ and Lyt-2+ cells to cause lethal graft-versus-host disease directed to allo class I vs. class II differences. Fourth, further information will be sought on the capacity of Lyt-2+ cells to mediate rejection of skin allografts.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Method to Extend Research in Time (MERIT) Award (R37)
Project #
4R37CA038355-10
Application #
3482398
Study Section
Special Emphasis Panel (NSS)
Project Start
1984-01-01
Project End
1995-12-31
Budget Start
1993-02-01
Budget End
1993-12-31
Support Year
10
Fiscal Year
1993
Total Cost
Indirect Cost

  Institution

Name
Scripps Research Institute
Department
Type
DUNS #
City
La Jolla
State
CA
Country
United States
Zip Code
92037

  Publications

Boyman, Onur; Ramsey, Chris; Kim, David M et al. (2008) IL-7/anti-IL-7 mAb complexes restore T cell development and induce homeostatic T Cell expansion without lymphopenia. J Immunol 180:7265-75
Rubinstein, Mark P; Kovar, Marek; Purton, Jared F et al. (2006) Converting IL-15 to a superagonist by binding to soluble IL-15R{alpha}. Proc Natl Acad Sci U S A 103:9166-71
Ishimaru, Naozumi; Kishimoto, Hidehiro; Hayashi, Yoshio et al. (2006) Regulation of naive T cell function by the NF-kappaB2 pathway. Nat Immunol 7:763-72
Boyman, Onur; Cho, Jae-Ho; Tan, Joyce T et al. (2006) A major histocompatibility complex class I-dependent subset of memory phenotype CD8+ cells. J Exp Med 203:1817-25
Surh, Charles D; Boyman, Onur; Purton, Jared F et al. (2006) Homeostasis of memory T cells. Immunol Rev 211:154-63
Kovar, Marek; Boyman, Onur; Shen, Xuefei et al. (2006) Direct stimulation of T cells by membrane vesicles from antigen-presenting cells. Proc Natl Acad Sci U S A 103:11671-6
Surh, Charles D; Sprent, Jonathan (2005) Regulation of mature T cell homeostasis. Semin Immunol 17:183-91
Sprent, Jonathan (2005) Direct stimulation of naive T cells by antigen-presenting cell vesicles. Blood Cells Mol Dis 35:17-20
Lenz, Derek C; Kurz, Sabine K; Lemmens, Edward et al. (2004) IL-7 regulates basal homeostatic proliferation of antiviral CD4+T cell memory. Proc Natl Acad Sci U S A 101:9357-62
Hwang, Inkyu; Shen, Xuefei; Sprent, Jonathan (2003) Direct stimulation of naive T cells by membrane vesicles from antigen-presenting cells: distinct roles for CD54 and B7 molecules. Proc Natl Acad Sci U S A 100:6670-5

Showing the most recent 10 out of 142 publications