Abstract

? Blocking both CD28 and CD154 (CD40L) costimulatory molecules can induce long-term allograft survival and tolerance in some but NOT all transplant models. Under stringent conditions (e.g. the skin transplant model, pre-sensitized hosts, diabetic NOD etc), however, this strategy often completely fails to prevent transplant rejection. Thus, identification of key mechanisms that support the CD28/CD154 blockade resistant rejection is of central importance in transplantation, as the eventual success of costimulatory blockade protocol in the clinic most likely hinges on the identification of these escaping mechanisms. I have constructed a new model in which both CD28 and CD154, two conventional T cell costimulatory molecules, are genetically knocked out (CD28/CD154 double knock out or DKO mice). These mice have a normal T cell repertoire and can readily reject fully MHC-mismatched skin allograft. The overall goal of this proposal is to use this model as a linchpin to critically examine the mechanisms supporting CD28/CD154 blockade resistant rejection and to identify new therapeutic targets in tolerance induction. I hypothesized that costimulation mediated via some of the recently described novel costimulatory pathways (e.g. OX40/OX40 ligand, ICOS/ICOS ligand, 4-1BB/4-1BB ligand, CD27/CD70) and/or the novel T cell growth factors (e.g. IL-7, IL-15, IL-21 ) may support the activation of a subset of T cells that drive the rejection process in CD28/CD154 DKO recipients.
THE SPECIFIC AIMS ARE: 1. To test the hypothesis that a novel T cell subset(s) is responsible for mediating skin allograft rejection in the CD28/CD154 DKO recipients. 2. To test the hypothesis that costimulation mediated via the novel costimulatory molecule ICOS, CD27, CD134 (OX40), and/or CD137 (4-1BB) supports the activation of a subset of T cells in CD28/CD154 DKO mice that mediate the allograft rejection response. 3. To test the hypothesis that, in the absence of both CD28 and CD154 costimulatory molecules, which often render activated T cells to produce high levels of IL-2, activation of a subset of alloreactive T cells involved in CD28/CD154 independent allograft rejection is supported by novel non-T cell-derived T cell growth factors (e.g. IL-7, IL-15, IL-21). ? ? ?

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
Research Project (R01)
Project #
5R01AI057409-03
Application #
7033021
Study Section
Surgery, Anesthesiology and Trauma Study Section (SAT)
Program Officer
Kehn, Patricia J
Project Start
2004-04-01
Project End
2009-03-31
Budget Start
2006-04-01
Budget End
2007-03-31
Support Year
3
Fiscal Year
2006
Total Cost
$249,008
Indirect Cost

  Institution

Name
Beth Israel Deaconess Medical Center
Department
Type
DUNS #
071723621
City
Boston
State
MA
Country
United States
Zip Code
02215

  Publications

Chen, Wenhao; Ghobrial, Rafik M; Li, Xian C (2015) The Evolving Roles of Memory Immune Cells in Transplantation. Transplantation 99:2029-37
Zhao, Picheng; Xiao, Xiang; Ghobrial, Rafik M et al. (2013) IL-9 and Th9 cells: progress and challenges. Int Immunol 25:547-51
Xiao, Xiang; Gong, Weihua; Demirci, Gulcin et al. (2012) New insights on OX40 in the control of T cell immunity and immune tolerance in vivo. J Immunol 188:892-901
Li, Xian Chang (2010) The significance of non-T-cell pathways in graft rejection: implications for transplant tolerance. Transplantation 90:1043-7
Li, Xian C; Raghavan, Malini (2010) Structure and function of major histocompatibility complex class I antigens. Curr Opin Organ Transplant 15:499-504
Habicht, A; Kewalaramani, R; Vu, M D et al. (2007) Striking dichotomy of PD-L1 and PD-L2 pathways in regulating alloreactive CD4(+) and CD8(+) T cells in vivo. Am J Transplant 7:2683-92
Yu, Guang; Xu, Xuemin; Vu, Minh Diem et al. (2006) NK cells promote transplant tolerance by killing donor antigen-presenting cells. J Exp Med 203:1851-8
Vu, Minh Diem; Amanullah, Farhana; Li, Yongsheng et al. (2004) Different costimulatory and growth factor requirements for CD4+ and CD8+ T cell-mediated rejection. J Immunol 173:214-21