Abstract

Monoclonal antibody (mAb) treatment of organ transplant recipients has been a major development in the treatment of allograft rejection. The advantages of mAbs include their known specificity, consistent biological activity, and ease of administration. Of all mAbs clinically and experimentally tested in man, the most efficacious is the OKT3 mAb which recognizes the T cells receptor (TCR) complex on the surface of alloreactive cells. However, several limitations to the use of the OKT3 reagent persists. These include the significant adverse reactions following the initial dose, production by the recipient of antibodies to the OKT3 antibody, and the broad but transient nature of the induced immunosuppression. Our laboratory has recently developed an anti-murine CD3 mAb that reacts with all mouse T cells expressing a TCR complex. Initial studies in the laboratory suggest that treatment with the mAb in vivo has profound long term immunosuppressive effects including prolonged skin graft survival and depressed cellular immunity. Although the initial immunosuppression is a consequence of T cell depletion and receptor blockade, T cells that survive treatment continue to be hyporesponsive. Thus, this hamster mAb provides the first anti-CD3 that can be used in a well-defined small animal model to provide a systematic evaluation of the use of anti-CD3 in vivo to suppress transplantation responses. Since anti-CD3 suppresses the immune response by affecting all T cells, the potential for generalized immunosuppression and susceptibility to opportunistic infections remains a great risk. Therefore, efforts will be designed to focus immunosuppression specifically on T cell subsets critical in allorecognition. Thus, subset-specific, mAbs and other T cell reagents will be used to suppress individual V(beta) expressing T cells which predominate in allorecognition. In addition, anti-CD3 will be coupled to anti-CD4 and anti-CD8 to suppress these subsets of T cells. Thus, the more specific mAb treatment should lead to a more sophisticated immunosuppressive regimen that selectively alters immunity towards the organ transplant.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
Research Program Projects (P01)
Project #
1P01AI029531-01
Application #
3810523
Study Section
Project Start
Project End
Budget Start
Budget End
Support Year
1
Fiscal Year
1990
Total Cost
Indirect Cost

  Institution

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

  Publications

Gajewski, T F; Fallarino, F; Fields, P E et al. (2001) Absence of CTLA-4 lowers the activation threshold of primed CD8+ TCR-transgenic T cells: lack of correlation with Src homology domain 2-containing protein tyrosine phosphatase. J Immunol 166:3900-7
Szot, G L; Zhou, P; Rulifson, I et al. (2001) Different mechanisms of cardiac allograft rejection in wildtype and CD28-deficient mice. Am J Transplant 1:38-46
Alegre, M; Fallarino, F; Zhou, P et al. (2001) Transplantation and the CD28/CTLA4/B7 pathway. Transplant Proc 33:209-11
Zhou, P; Szot, G L; Guo, Z et al. (2000) Role of STAT4 and STAT6 signaling in allograft rejection and CTLA4-Ig-mediated tolerance. J Immunol 165:5580-7
Kulkarni, S; Holman, P O; Kopelan, A et al. (2000) Programmed cell death signaling via cell-surface expression of a single-chain antibody transgene. Transplantation 69:1209-17
Rezai, K A; Semnani, R T; Farrokh-Siar, L et al. (1999) Human fetal retinal pigment epithelial cells induce apoptosis in allogenic T-cells in a Fas ligand and PGE2 independent pathway. Curr Eye Res 18:430-9
van Seventer, G A; Semnani, R T; Palmer, E M et al. (1998) Integrins and T helper cell activation. Transplant Proc 30:4270-4
Smith, J A; Tang, Q; Bluestone, J A (1998) Partial TCR signals delivered by FcR-nonbinding anti-CD3 monoclonal antibodies differentially regulate individual Th subsets. J Immunol 160:4841-9
Fields, P E; Finch, R J; Gray, G S et al. (1998) B7.1 is a quantitatively stronger costimulus than B7.2 in the activation of naive CD8+ TCR-transgenic T cells. J Immunol 161:5268-75
Madrenas, J; Chau, L A; Smith, J et al. (1997) The efficiency of CD4 recruitment to ligand-engaged TCR controls the agonist/partial agonist properties of peptide-MHC molecule ligands. J Exp Med 185:219-29

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