This proposal examines the signalling abnormalities in lpr immature T lymphocytes in order to understand the apparent developmental arrest and refractory state of the accumulating CD3+ CD4-CD8- T cells, and its parallels with normal T cell tolerance. It further studies the possible consequences of the signal defect on the regulation of surface CD4, CD8, and T cell antigen receptor (TCR) gamma/delta, as well as aberrant INFgamma, IL4, and TNFalpha lymphokine profiles produced by lpr immature versus mature T cells. These latter studies may be particularly relevant to the autoimmune process in these mice. The first specific aim completes a study of calcium and phosphoinositide flux in lpr CD4-8- T cells that show transmembrane signal events to be intact. It then uses the information of constitutive CD3 zeta tyrosine phosphorylation and delayed proliferative responses in lpr CD4-8- T cells to explore the temporal expression of two T cell tyrosine kinases, lck and fyn. Finally, the expression of IL2 gene nuclear regulatory proteins by lpr CD4-8- cells are used to further assess discrete signal pathway abnormalities.
The second aim examines methylation of the CD8 gene in lpr CD4-8- cells to assess the question of whether these cells underwent thymic selection at a CD4+8+ stage. It will also explore whether the markedly increased levels of TCR gamma and delta mRNA in cultured lpr CD4-8- cells are translated to gamma/delta protein.
The third aim examines aberrantly low lymphokine production by lpr immature T cells, in particular, the absence of INFgamma protein despite the presence of INFgamma mRNA. It also explores the aberrantly high levels of INFgamma and possibly IL4 by lpr mature T cells and normal (Pgp-1+) memory T lymphocytes.

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
First Independent Research Support & Transition (FIRST) Awards (R29)
Project #
5R29AI028892-03
Application #
3455381
Study Section
Immunological Sciences Study Section (IMS)
Project Start
1990-07-01
Project End
1995-04-30
Budget Start
1992-07-01
Budget End
1993-04-30
Support Year
3
Fiscal Year
1992
Total Cost
Indirect Cost
Name
University of Vermont & St Agric College
Department
Type
Schools of Medicine
DUNS #
066811191
City
Burlington
State
VT
Country
United States
Zip Code
05405
Wilson, D J; Fortner, K A; Lynch, D H et al. (1996) JNK, but not MAPK, activation is associated with Fas-mediated apoptosis in human T cells. Eur J Immunol 26:989-94
Mixter, P F; Russell, J Q; Durie, F H et al. (1995) Decreased CD4-CD8- TCR-alpha beta + cells in lpr/lpr mice lacking beta 2-microglobulin. J Immunol 154:2063-74
Budd, R C; Mixter, P F (1995) The origin of CD4-CD8-TCR alpha beta+ thymocytes: a model based on T-cell receptor avidity. Immunol Today 16:428-31
Clements, J L; Wolfe, J; Cooper, S M et al. (1994) Reversal of hyporesponsiveness in lpr CD4-CD8- T cells is achieved by induction of cell cycling and normalization of CD2 and p59fyn expression. Eur J Immunol 24:558-65
Van Houten, N; Mixter, P F; Wolfe, J et al. (1993) CD2 expression on murine intestinal intraepithelial lymphocytes is bimodal and defines proliferative capacity. Int Immunol 5:665-72
Landolfi, M M; Van Houten, N; Russell, J Q et al. (1993) CD2-CD4-CD8- lymph node T lymphocytes in MRL lpr/lpr mice are derived from a CD2+CD4+CD8+ thymic precursor. J Immunol 151:1086-96
Clements, J L; Winslow, G; Donahue, C et al. (1993) Co-stimulation via CD28 induces activation of a refractory subset of MRL-lpr/lpr T lymphocytes. Int Immunol 5:1451-60
Budd, R C; Russell, J Q; van Houten, N et al. (1992) CD2 expression correlates with proliferative capacity of alpha beta + or gamma delta + CD4-CD8- T cells in lpr mice. J Immunol 148:1055-64
Van Houten, N; Budd, R C (1992) Accelerated programmed cell death of MRL-lpr/lpr T lymphocytes. J Immunol 149:2513-7
Budd, R C; Schumacher, J H; Winslow, G et al. (1991) Elevated production of interferon-gamma and interleukin 4 by mature T cells from autoimmune lpr mice correlates with Pgp-1 (CD44) expression. Eur J Immunol 21:1081-4