Abstract

Rejection of organ allografts is dependent on T cells. It is now known that T cell stimulation through the T cell receptor (TCR), while required for antigen-specific activation, is not by itself sufficient, as a second (or """"""""costimulatory"""""""") signal is also needed. In fact, TCR stimulation in the absence of a second signal can induce a state of anergy in the T cell, rendering it refractory to subsequent stimulation. The best-characterized costimulatory pathway occurs through interaction of CD28 found on the surface of T cells with either of two ligands, B7-1 or B7-2, found on activated antigen presenting cells. A soluble fusion protein called CTLA4Ig has been developed which is capable of binding to B7-1 and B7-2, blocking the delivery of costimulatory signals to T cells through CD28. Using a cardiac allograft model, we have shown that the combination of donor-specific transfusion (DST) plus CTLA4Ig, blocks rejection and induces long-term graft survival. Interestingly, CTLA4Ig is most effective when its administration is delayed for 2 days post-transplant. When given on the day of transplantation, CTLA4Ig only rarely induces long-term engraftment. Thus delaying T cell costimulatory blockade until after antigenic challenge is essential for tolerance induction. This application will examine the mechanism(s) by which DST plus CTLA4Ig act and the utility of this strategy.
In aim #1, we will determine if DST serves merely as a source of antigen, or if DST-induces chimerism which is required for tolerance. These studies will use extracted soluble histocompatibility antigens as well as synthetic MHC-derived peptides as alternative sources of antigen. The ability of DST to induce chimerism, and the identity of chimeric cells, will be assessed by flow cytometry and PCR. The need for chimerism will be determined by using DST cells containing the herpesvirus thymidine kinase gene, and subsequently deleting these cells in vivo with ganciclovir.
In aim#2 we will investigate the mechanisms of tolerance induction (deletion, anergy, suppression). Deletion will be assessed with in vivo immune responses to antigen where responding T cells can be identified by specific anti- TCRVbeta and V-alpha mAbs. In these models, we will track the fate of antigen-reactive cells in animals treated with CTLA4Ig. If responding T cells are deleted, we will study if CTLA4Ig induces apoptosis by preventing expression of cell survival genes such as bcl-2 and/or bcl-x. To test for anergy we attempt to reverse unresponsiveness with exogenous cytokines or infection. Suppression will be investigated with adoptive transfer studies. Lastly, as there are theoretical reasons why the effects of the CTLA4Ig + DST regimen might be antagonistic with those of cyclosporine, in aim #3 we will determine how CTLA4Ig interacts with standard immunosuppressive agents such as cyclosporine and prednisone in an in vivo transplant model. Through these studies, we hope to learn more about the use of DST in tolerance induction, the mechanism of action of DST and CTLA4Ig, and how best to use CTLA4Ig clinically. These studies also should help lead to the design of new immunosuppressive strategies in the future.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
Research Project (R01)
Project #
5R01AI037691-03
Application #
2376406
Study Section
Special Emphasis Panel (SRC (23))
Project Start
1995-03-15
Project End
2000-02-29
Budget Start
1997-03-01
Budget End
1998-02-28
Support Year
3
Fiscal Year
1997
Total Cost
Indirect Cost

  Institution

Name
University of Pennsylvania
Department
Internal Medicine/Medicine
Type
Schools of Medicine
DUNS #
042250712
City
Philadelphia
State
PA
Country
United States
Zip Code
19104

  Publications

Marangoni, Francesco; Zhang, Ruan; Mani, Vinidhra et al. (2018) Tumor Tolerance-Promoting Function of Regulatory T Cells Is Optimized by CD28, but Strictly Dependent on Calcineurin. J Immunol 200:3647-3661
Zhang, Ruan; Sage, Peter T; Finn, Kelsey et al. (2017) B Cells Drive Autoimmunity in Mice with CD28-Deficient Regulatory T Cells. J Immunol 199:3972-3980
Kean, Leslie S; Turka, Laurence A; Blazar, Bruce R (2017) Advances in targeting co-inhibitory and co-stimulatory pathways in transplantation settings: the Yin to the Yang of cancer immunotherapy. Immunol Rev 276:192-212
Alessandrini, Alessandro; Turka, Laurence A (2017) FOXP3-Positive Regulatory T Cells and Kidney Allograft Tolerance. Am J Kidney Dis 69:667-674
Kamphorst, Alice O; Wieland, Andreas; Nasti, Tahseen et al. (2017) Rescue of exhausted CD8 T cells by PD-1-targeted therapies is CD28-dependent. Science 355:1423-1427
Zhang, Ruan; Borges, Christopher M; Fan, Martin Y et al. (2015) Requirement for CD28 in Effector Regulatory T Cell Differentiation, CCR6 Induction, and Skin Homing. J Immunol 195:4154-61
Vergani, Andrea; Gatti, Francesca; Lee, Kang M et al. (2015) TIM4 Regulates the Anti-Islet Th2 Alloimmune Response. Cell Transplant 24:1599-1614
Kim, James I; Turka, Laurence A (2015) Transplant tolerance: a new role for IL-34. J Clin Invest 125:3751-3
McDonald-Hyman, Cameron; Turka, Laurence A; Blazar, Bruce R (2015) Advances and challenges in immunotherapy for solid organ and hematopoietic stem cell transplantation. Sci Transl Med 7:280rv2
Kawai, Tatsuo; Leventhal, Joseph; Madsen, Joren C et al. (2014) Tolerance: one transplant for life. Transplantation 98:117-21

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