Abstract

The hallmark of the immune system is its ability to distinguish """"""""self"""""""" from """"""""non-self""""""""; failure to do so may result in autoimmune disease. Education of the immune system as to the concept of self takes place in the thymus wherein autoreactive lymphocytes are deleted, tolerized or actively suppressed. Clonal deletion is a major, albeit not the only, mechanism for self tolerance. The exact process by which clonal deletion takes place is not well understood although there are several autoimmune animal models in which the disease can be ameliorated by the adoptive transfer of normal thymocytes. This suggests that a thymocyte subset(s) may be involved in clonal deletion. The principal investigator has recently identified a novel murine thymocyte subset (NK1.1+, CD3+, CD4-, CD8-, CD5+, CD44+, Thy1+, TCR alpha/beta) which has a spontaneous lytic potential. Upon expansion with interleukin 2 (IL2), this population could kill fresh autologous CD4+, CD8+ thymocytes as well as PHA-activated mature thymocytes. These attributes are the basis of the hypothesis that NK1.1+, CD3+ thymocytes are important in the clonal deletion aspect of thymic selection. This hypothesis will be tested utilizing an in vivo and in vitro strategy. Major emphasis will be placed on examining the effect of neonatal cyclosporine (CSA) administration, which leads to the development of autoimmune disease, on the function and number of these thymocytes. Programmed cell death is another method by which self-tolerization is thought to be accomplished. Anti-CD3, in vivo, induces apoptosis in murine thymocytes. Preliminary data showed that, in addition to apoptosis, anti- CD3 causes near total depletion of CD4+, CD8+ thymocytes with a concomitant expansion of the NK1.1+, CD3+ subset and an insurgence of cytotoxic effector cells; CSA seems to abolish all these changes. The hypothesis to be tested is that the thymic effects of in vivo anti-CD3 are mediated, to a large extent, by cytokine-induced activation and expansion of NK1.1+, CD3+ thymocytes. T cell depletion, in vivo, is already being used clinically in certain autoimmune diseases and in treating organ transplant rejection. There is little known about the effects of such treatment on the immune system as a whole, with its interactive feedback mechanisms, and no attention has been given to the thymus. This proposal is expected to yield fruitful results clinically applicable in the autoimmunity and transplantation areas.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
Research Project (R01)
Project #
5R01AI026460-06
Application #
2063349
Study Section
Experimental Immunology Study Section (EI)
Project Start
1988-07-01
Project End
1995-04-30
Budget Start
1994-05-01
Budget End
1995-04-30
Support Year
6
Fiscal Year
1994
Total Cost
Indirect Cost

  Institution

Name
University of Iowa
Department
Internal Medicine/Medicine
Type
Schools of Medicine
DUNS #
041294109
City
Iowa City
State
IA
Country
United States
Zip Code
52242

  Publications

Li, F; Cook, R T; Alber, C et al. (1997) Ethanol and natural killer cells. II. Stimulation of human natural killer activity by ethanol in vitro. Alcohol Clin Exp Res 21:981-7
Cook, R T; Li, F; Vandersteen, D et al. (1997) Ethanol and natural killer cells. I. Activity and immunophenotype in alcoholic humans. Alcohol Clin Exp Res 21:974-80
Cook, R T; Ballas, Z K; Waldschmidt, T J et al. (1995) Modulation of T-cell adhesion markers, and the CD45R and CD57 antigens in human alcoholics. Alcohol Clin Exp Res 19:555-63
Ballas, Z K; Rasmussen, W (1993) Lymphokine-activated killer cells. VII. IL-4 induces an NK1.1+CD8 alpha+beta- TCR-alpha beta B220+ lymphokine-activated killer subset. J Immunol 150:17-30
Ballas, Z K; Rasmussen, W (1991) Lymphokine-activated killer (LAK) cells. VI. NK1.1+, CD3+ LAK effectors are derived from CD4-, CD8-, NK1.1- precursors. Cell Immunol 134:296-313
Ballas, Z K; Rasmussen, W (1990) NK1.1+ thymocytes. Adult murine CD4-, CD8- thymocytes contain an NK1.1+, CD3+, CD5hi, CD44hi, TCR-V beta 8+ subset. J Immunol 145:1039-45
Ballas, Z K; Rasmussen, W L (1990) Murine natural killer cells express the Ly24 (Pgp-1) marker on their surface. Cell Immunol 125:449-58
Thompson, R A; Ballas, Z K (1990) Lymphokine-activated killer (LAK) cells. V. 8-Mercaptoguanosine as an IL-2-sparing agent in LAK generation. J Immunol 145:3524-31
Ballas, Z K; Rasmussen, W (1990) Lymphokine-activated killer (LAK) cells. IV. Characterization of murine LAK effector subpopulations. J Immunol 144:386-95
Goeken, N E; Staggs, T S; Ballas, Z K (1989) Monocyte suppressor factor is plasminogen activator inhibitor inhibition of membrane bound but not soluble IL-1. J Immunol 143:603-8