Abstract

Over the past two decades, the development of new immunosuppressive agents has greatly improved early post-transplant survival. Nevertheless, long-term survival has not improved significantly, due to chronic rejection, infections, and malignancies - all attributable to chronic immunosuppression. In lung transplantation, chronic allograft rejection, as manifested by obliterative bronchiolitis, fibrosis, and/or vasculopathy, represents the principal cause of graft loss and patient demise after the first year following transplantation. It is now well established that both antigen-dependent and antigen-independent factors contribute to both acute and chronic rejection in a synergistic manner. We have long held the position that the establishment of transplant tolerance is the paradigm shift that will transform the field of transplantation by obviating the need for long term systemic immunosuppression with its attendant complications (malignancy, toxicity, and infection), while simultaneously preventing both acute and potentially chronic rejection. Tolerance of kidney allografts has been achieved in non-human primates (NHPs) and in humans using a strategy that induces hematopoietic mixed chimerism. We have modified and extended this approach to lung transplantation in NHPs by adding the interleukin (IL)-6 signal blocker tocilizumab (anti-IL6R mAb) to our delayed, non-myeloablative conditioning regimen. This has allowed us to achieve long-term lung allograft tolerance without chronic rejection in NHPs for the first time, albeit only in one-MHC haplotype mismatched donor/recipient pairs. Attempts to cross more stringent histocompatibility barriers have led to acute and/or chronic rejection. From a mechanistic point of view, it appears that the tolerance obtained in NHPs is not simply deletional tolerance, as seen in most murine chimeric models, but is highly dependent on 1) enhancing regulatory responses and 2) dampening pro- inflammatory states. We therefore hypothesize that to successfully induce tolerance of fully MHC-mismatched lung allografts without the development of chronic rejection we must develop protocols which further enhance immune regulation and which prevent antigen-independent inflammation. This hypothesis will be tested in Aim 1. Our overall goal is to generate a tolerance protocol that can be applied to human lung allograft recipients. Thus, once the optimal tolerance induction protocol is identified in Aim 1, attempts will be made to substitute the investigational components of the protocol with FDA-approved agents making it suitable for clinical use in Aim 2. Finally, it is clear that chronic rejection is refractory to current therapies, including in some circumstances, tolerance induction. Therefore, in Aim 3 we will perform integrated mechanistic studies of the pathogenesis of chronic rejection and use the results to design modifications of the optimal protocol achieved in Aim 2 in order to prevent this complication.

Public Health Relevance

Achieving long-term survival of lung allografts without the need for chronic immunosuppression will provide transplant recipients with a healthier and longer life. These studies will explore ways to eliminate the need for chronic immunosuppressive drugs in patients undergoing lung transplantation.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Heart, Lung, and Blood Institute (NHLBI)
Type
Research Program Projects (P01)
Project #
5P01HL018646-38
Application #
9181436
Study Section
Heart, Lung, and Blood Initial Review Group (HLBP)
Program Officer
Schwartz, Lisa
Project Start
Project End
Budget Start
2016-11-01
Budget End
2017-10-31
Support Year
38
Fiscal Year
2017
Total Cost
Indirect Cost

  Institution

Name
Massachusetts General Hospital
Department
Type
DUNS #
073130411
City
Boston
State
MA
Country
United States
Zip Code
02114

  Publications

Robinson, Kortney A; Orent, William; Madsen, Joren C et al. (2018) Maintaining T cell tolerance of alloantigens: Lessons from animal studies. Am J Transplant 18:1843-1856
Sasaki, Hajime; Oura, Tetsu; Spitzer, Thomas R et al. (2018) Preclinical and clinical studies for transplant tolerance via the mixed chimerism approach. Hum Immunol 79:258-265
Tanimine, Naoki; Turka, Laurence A; Priyadharshini, Bhavana (2018) Navigating T-Cell Immunometabolism in Transplantation. Transplantation 102:230-239
Michel, S G; Madariaga, M L L; LaMuraglia 2nd, G M et al. (2018) The effects of brain death and ischemia on tolerance induction are organ-specific. Am J Transplant 18:1262-1269
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

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