Abstract

Donor-specific tolerance would obviate the need for chronic immunosuppressive therapy in organ graft recipients, and might be necessary to overcome the formidable immunologic barriers to xenografts.
We aim to induce T cell and B cell tolerance across a discordant species barrier (pig to mouse). We will first determine the ability of mixed bone marrow chimerism to induce tolerance among pre-existing and newly developing B cells producing NAb against the alpha1,3-galactosyl specificity that is recognized by most human anti-pig Nab. For this purpose, we will transfer alpha1,e-gal+ bone marrow,-alone or with alpha1,3-gal deficient mice receiving lethal and non-lethal conditioning regimens. In addition, alpha1,3-gal deficient, immunodeficient SCID-NOD mice will receive human B cells to determine which subsets produce anti- gal NAb, the effect of these NAb on porcine marrow engraftment and the ability to porcine chimerism to induce tolerance among anti-gal producing human B cells. We will also utilize the swine to SIC-NOD mouse BMT model to determine which cellular components of the human immune system (T cells subsets and NK cells) resist engraftment of swine BMC. Finally, we will induce pig-specific T and B cell tolerance in immunocompetent mice. Discordant pig-specific skin graft tolerance can be induce in normal mice by host thymectomy, mAbs to deplete recipient T cells, and replacement of the host thymus with a pig thymus, in which tolerant, immunocompetent mouse T cells develop. Pig cytokine transgenic mice will receive porcine thymus grafts with various sources of pig hematopoietic cells in an attempt to acheive hematopoietic chimerism. We will evaluate chimeric recipients for pig-specific natural antibody tolerance. We will ultimately attempt to acheive porcine chimerism in euthymic porcine cytokine transgenic recipients. Other studies will involve a species combination in which, like the pig-human combination, cell-cell interactions required for cellular immune responses are largely intact. In the concordant rat>mouse combination, marrow engraftment can be achieved following conditioning with a mild, non-myeloablative regimen. We will evaluate the role of gammadelta T cells and of alphabeta T cells that express NK cell markers in resisting xenogeneic marrow engraftment. By elucidating the components of the immune system that resist xenogeneic marrow engraftment, and in conjunction with results obtained in Project 3, these studies will help to overcome the xenogeneic transplantation barrier. Translation of results in this project to pre- clinical studies will advance the ability to induce donor-specific tolerance to pigs in humans.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Heart, Lung, and Blood Institute (NHLBI)
Type
Research Program Projects (P01)
Project #
3P01HL018646-22S1
Application #
6109464
Study Section
Project Start
1999-04-12
Project End
2000-02-29
Budget Start
1998-10-01
Budget End
1999-09-30
Support Year
22
Fiscal Year
1999
Total Cost
Indirect Cost

  Institution

Name
Massachusetts General Hospital
Department
Type
DUNS #
City
Boston
State
MA
Country
United States
Zip Code
02199

  Publications

Smith, R N; Adam, B A; Rosales, I A et al. (2018) RNA expression profiling of renal allografts in a nonhuman primate identifies variation in NK and endothelial gene expression. Am J Transplant 18:1340-1350
Chatterjee, Debanjana; Moore, Carolina; Gao, Baoshan et al. (2018) Prevalence of polyreactive innate clones among graft--infiltrating B cells in human cardiac allograft vasculopathy. J Heart Lung Transplant 37:385-393
Gonzalez-Nolasco, Bruno; Wang, Mengchuan; Prunevieille, Aurore et al. (2018) Emerging role of exosomes in allorecognition and allograft rejection. Curr Opin Organ Transplant 23:22-27
Smith, R N; Matsunami, M; Adam, B A et al. (2018) RNA expression profiling of nonhuman primate renal allograft rejection identifies tolerance. Am J Transplant 18:1328-1339
Fan, Martin Y; Low, Jun Siong; Tanimine, Naoki et al. (2018) Differential Roles of IL-2 Signaling in Developing versus Mature Tregs. Cell Rep 25:1204-1213.e4
Benichou, Gilles; Prunevieille, Aurore (2018) Graft-derived exosomes. When small vesicles play a big role in transplant rejection. Am J Transplant 18:1585-1586
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
Fan, Martin Y; Turka, Laurence A (2018) Immunometabolism and PI(3)K Signaling As a Link between IL-2, Foxp3 Expression, and Suppressor Function in Regulatory T Cells. Front Immunol 9:69
Wang, Zhaohui; Louras, Nathan J; Lellouch, Alexandre G et al. (2018) Dosing optimization of CCR4 immunotoxin for improved depletion of CCR4+ Treg in nonhuman primates. Mol Oncol 12:1374-1382
Newton, Ryan H; Shrestha, Sharad; Sullivan, Jenna M et al. (2018) Maintenance of CD4 T cell fitness through regulation of Foxo1. Nat Immunol 19:838-848

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