Abstract

The overall objective of this proposal is to delineate mechanisms of clonal anergy and deletion noted in transplant (Tx) protocols. Using a sensitive, reproducible limiting dilution analysis (LDA) technique, evidence was obtained of a donor-specific regulatory cell that inhibits CTL precursors (CTLp) in long-term renal Tx recipients receiving conventional immunosuppression and in recipients who received pre-Tx donor specific transfusions (DST). In addition, many long-term DST- treated (DST-A) renal allograft recipients demonstrate specific deletion of anti-donor CTLp. to learn whether clonal deletion of donor-reactive CTLp and/or the development of donor-specific suppression contribute to the state of allograft tolerance, we will perform time course studies to follow changes in CTLp with specificity for donor and third party antigens in DST-A and non-DST-A allograft recipients, thereby determining if clonal reduction occurs more rapidly, to a greater extent and with more frequency in DST vs non-DST patients. Moreover, we will evaluate the relationship between donor-specific hyporesponsiveness, deletion of donor-reactive CTLp and the emergence of regulatory cells. Results will be analyzed for correlation with recipient's HLA phenotype, HLA matching with donor, immunosuppressive therapy, renal function, rejection episodes, and long-term graft outcome. If suppression is mediated by a regulatory T cell, we will clone it and test the hypothesis that it is a self-restricted CTL which recognizes donor-specific allopeptides bound to self-HLA. We will determine whether the apparent clonal deletion of anti-donor CTLp represents actual clonal elimination or clonal anergy. If clonal anergy is established as the mechanism, we will determine how it influences CTL responsiveness. Or to prove true deletion of anti- donor CTLp, we will characterize and estimate by semi-quantitative PCR the V gene families present in CD8+ T cells of patient PBL pre-A, post-A, and post-Tx, and look for correlation between elimination of anti-donor alloreactivity and deletion of specific V elements from the repertoire. Anergy/deletion of donor-reactive CTLp may not sufficiently explain tolerance to donor antigens in renal allograft recipients. Therefore, we will evaluate the contribution to acquired immune tolerance of anti- clonotypic antibodies and alterations in the TH cell compartment (e.g., a predominance of TH2 over TH1). Finally, we will determine the immunologic relevance of a CD3/TCR cell population which we observe in DST-A patients. We will probe the origin, phenotype, and functional activities of these cells in order to evaluate if they are recipient's donor-reactive T cells in which down-regulation of CD3/TCR has occurred, or whether they are veto cells of donor origin. These studies on renal allograft recipients provide a unique opportunity to determine which of several immunological mechanisms implicated in animal models operate in human Tx tolerance, and whether they can be associated in a predictable manner with clinical course.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
Research Project (R01)
Project #
5R01AI026934-06
Application #
2063650
Study Section
Surgery, Anesthesiology and Trauma Study Section (SAT)
Project Start
1988-09-30
Project End
1997-03-31
Budget Start
1995-04-01
Budget End
1996-03-31
Support Year
6
Fiscal Year
1995
Total Cost
Indirect Cost

  Institution

Name
Washington University
Department
Surgery
Type
Schools of Medicine
DUNS #
062761671
City
Saint Louis
State
MO
Country
United States
Zip Code
63130

  Publications

Susskind, B; Shornick, M D; Iannotti, M R et al. (1996) Cytolytic effector mechanisms of human CD4+ cytotoxic T lymphocytes. Hum Immunol 45:64-75
Susskind, B; Iannotti, M R; Shornick, M D et al. (1996) Indirect allorecognition of HLA class I peptides by CD4+ cytolytic T lymphocytes. Hum Immunol 46:1-9
Sundaresan, S; Alevy, Y G; Steward, N et al. (1995) Cytokine gene transcripts for tumor necrosis factor-alpha, interleukin-2, and interferon-gamma in human pulmonary allografts. J Heart Lung Transplant 14:512-8
Mathew, J M; Naziruddin, B; Duffy, B et al. (1995) Functional analysis of complement receptor 1 using a new monoclonal antibody, KuN241. Hybridoma 14:29-35
Hadley, G A; Anderson, C B; Mohanakumar, T (1992) Selective loss of functional antidonor cytolytic T cell precursors following donor-specific blood transfusions in long-term renal allograft recipients. Transplantation 54:333-7
Phelan, D L; Hibbett, S; Wetter, L et al. (1991) Recombinant erythropoietin: does it really effect sensitization? Transplant Proc 23:409-10
Phelan, D; Hadley, G; Duffy, B et al. (1991) Antiidiotypic antibodies to HLA class I alloantibodies in normal individuals: a mechanism of tolerance to noninherited maternal HLA antigens. Hum Immunol 31:1-6
Ratner, L E; Hadley, G A; Hanto, D W et al. (1991) Immunology of renal allograft rejection. Arch Pathol Lab Med 115:283-7
Chauhan, B; Mohanakumar, T; Flye, M W (1990) Immunohistological analysis of T lymphocyte subpopulations in needle core biopsies from OKT3-treated renal allograft recipients. Transplantation 50:1058-60
Hadley, G A; Phelan, D; Duffy, B F et al. (1990) Lack of T-cell tolerance of noninherited maternal HLA antigens in normal humans. Hum Immunol 28:373-81

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