Abstract

Allograft rejection is a CD4+T cell dependent process. These T cells can recognize alloantigen via two distinct, yet not mutually exclusive, pathways. In the """"""""direct"""""""" pathway, T cells recognize intact allo-MHC molecules on the surface of donor antigen-presenting cells (APCs). In the """"""""indirect"""""""" pathway, T cells recognize processed alloantigen (predominantly allo- MHC) presented as peptides by self APCs. Increasing evidence from experimental animals and humans supports a significant role for indirect allorecognition in mediating allograft rejection. It has been hypothesized that this pathway, analogous to the physiologic nominal antigen recognition pathway, may be important in development and progression of chronic rejection, the most important problem in clinical organ transplantation. Therefore, it can be argued that the absence of tolerance to indirect allorecognition is responsible for development of chronic rejection. Definitive experimental evidence supporting these hypotheses is lacking. The purpose of this proposal is to study the role and effector mechanisms of indirect allorecognition in mediating allograft rejection, particularly chronic rejection. The investigators will also study the effects and mechanisms of inhibiting indirect allorecognition on development of the rejection process. In the first specific aim they will determine whether priming animals with donor- derived MHC allopeptides induces/accelerates allograft rejection. They will also study whether inhibiting CD4+T cell activation via the indirect pathway prevents development of acute and chronic rejection.
In specific aim 2 the investigators will use established Th1 and Th2 T cell clones which are self-restricted to recognize and respond to donor class II MHC allopeptides to study whether adoptive transfer of such clones will """"""""promote/enhance"""""""" (Th1) or """"""""regulate"""""""" (Th2) the immune response to vascularized allografts. Finally, in specific aim 3, in collaboration with the laboratory of Dr. Laurence A. Turka, they plan to create a TCR transgenic animal with specificity to donor class II MHC allopeptide presented by self APCs. This animal, when backcrossed onto SCID or RAG2 knockout mice, can only reject an allograft by indirect allorecognition. The above studies are critical to understanding of the contribution and mechanisms of indirect allorecognition in mediating acute and chronic allograft rejection. Results from these studies should yield clinically relevant information facilitating development of novel strategies to induce donor-specific tolerance.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
Research Project (R01)
Project #
5R01AI034965-09
Application #
6532698
Study Section
Surgery, Anesthesiology and Trauma Study Section (SAT)
Program Officer
Kraemer, Kristy A
Project Start
1994-08-01
Project End
2004-06-30
Budget Start
2002-08-01
Budget End
2003-06-30
Support Year
9
Fiscal Year
2002
Total Cost
$324,982
Indirect Cost

  Institution

Name
Brigham and Women's Hospital
Department
Type
DUNS #
071723621
City
Boston
State
MA
Country
United States
Zip Code
02115

  Publications

Kishimoto, Koji; Yuan, Xueli; Auchincloss Jr, Hugh et al. (2004) Mechanism of action of donor-specific transfusion in inducing tolerance: role of donor MHC molecules, donor co-stimulatory molecules, and indirect antigen presentation. J Am Soc Nephrol 15:2423-8
Denton, Mark D; Magee, Colm; Melter, Michael et al. (2004) TNP-470, an angiogenesis inhibitor, attenuates the development of allograft vasculopathy. Transplantation 78:1218-21
Salama, Alan D; Yuan, Xueli; Nayer, Ali et al. (2003) Interaction between ICOS-B7RP1 and B7-CD28 costimulatory pathways in alloimmune responses in vivo. Am J Transplant 3:390-5
Yuan, Xueli; Salama, Alan D; Dong, Victor et al. (2003) The role of the CD134-CD134 ligand costimulatory pathway in alloimmune responses in vivo. J Immunol 170:2949-55
Chung, Doo Ryeon; Kasper, Dennis L; Panzo, Ronald J et al. (2003) CD4+ T cells mediate abscess formation in intra-abdominal sepsis by an IL-17-dependent mechanism. J Immunol 170:1958-63
Kishimoto, Koji; Sandner, Sigrid; Imitola, Jaime et al. (2002) Th1 cytokines, programmed cell death, and alloreactive T cell clone size in transplant tolerance. J Clin Invest 109:1471-9
Dong, Victor M; Yuan, Xueli; Coito, Ana J et al. (2002) Mechanisms of targeting CD28 by a signaling monoclonal antibody in acute and chronic allograft rejection. Transplantation 73:1310-7
Waaga, A M; Gasser, M; Kist-van Holthe, J E et al. (2001) Regulatory functions of self-restricted MHC class II allopeptide-specific Th2 clones in vivo. J Clin Invest 107:909-16
Kishimoto, K; Dong, V M; Issazadeh, S et al. (2000) The role of CD154-CD40 versus CD28-B7 costimulatory pathways in regulating allogeneic Th1 and Th2 responses in vivo. J Clin Invest 106:63-72
Onodera, K; Chandraker, A; Schaub, M et al. (1997) CD28-B7 T cell costimulatory blockade by CTLA4Ig in sensitized rat recipients: induction of transplantation tolerance in association with depressed cell-mediated and humoral immune responses. J Immunol 159:1711-7