Abstract

Induction of allograft tolerance would avoid the need for chronic immunosuppressive therapy with its attendant toxicities. We have recently performed a pilot trial of combined non-myeloabiative bone marrow and kidney transplantation (CKBMT) from related haploidentical donors. Four of 5 patients achieved durable allograft acceptance without maintenance immunosuppression, representing the first successful intentional achievement of tolerance to HLA-mismatched allografts. In vitro studies revealed the development of specific unresponsiveness to the donor in assays that primarily measure direct alloreactivity. Regulatory T cells (Tregs) were enriched in the recovering peripheral blood T cell populations, and suppression of anti-donor reactivity was detected variably within the first year post-transplant. However, early acute humoral rejection episodes occurred in several patients, resulting in the addition of B cell-depleting anti-CD20 mAb to the regimen. Several patients developed autoantibodies and donor-specific alloantibodies in the presence of low T cell counts and/or T cell tolerance in vivo and in vitro. We hypothesize that these antibodies are generated by recovering transitional B cells in the absence of T cell help. However, an alternative hypothesis is that indirectly alloreactive T cells provide help for class-switched Ig responses in these patients, despite the donor unresponsiveness seen in bulk MLR and CML assays. The protocol is now being reopened to include both HLA-haploidentical and more extensively mismatched donors. We propose to address several hypotheses in order to understand the tolerance achieved through CKBMT. We will: 1) Assess tolerance of directly and indirectly donor alloreactive T cells in recipients of HLA-mismatched CKBMT. Indirect responses to both hematopoietic and renal tubular cell-derived antigens will be measured and interpreted in the context of the development of anti-donor antibodies;and 2) Assess the role of regulatory cells, including FoxP3+ Treg and CD127-C025-C04 cells, in the development of donor-specific tolerance in recipients of CKBMT. We will assess the phenotype and function of regulatory cell populations obtained from patient PBMC and expanded from renal biopsy specimens. We hypothesize that donor-specific regulatory cells will be enriched in the renal allograft compared to the PBMC and that donor-specific regulatory capacity will decline over time as deletion of donor-reactive T cells occurs. In combination with studies performed at the ITN core facilities, our studies should promote a comprehensive understanding of the mechanisms involved In tolerance induced by CKBMT.

Public Health Relevance

Induction of allograft tolerance would overcome the current limitations to the success of organ transplantation, namely the toxicities of chronic Immunosuppressive medications and chronic rejection. Combined kidney and non-myeloablative bone marrow transplantation has provided the first and only successful approach to intentional tolerance induction in humans. An understanding of the mechanisms of donor-specific allograft tolerance achieved with combined kidney and non-mye/oablative bone marrow transplantation will allow its refinement and broader application.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
Research Project (R01)
Project #
1R01AI084074-01
Application #
7728635
Study Section
Special Emphasis Panel (ZAI1-PA-I (M3))
Program Officer
Bridges, Nancy D
Project Start
2009-08-11
Project End
2010-03-31
Budget Start
2009-08-11
Budget End
2010-03-31
Support Year
1
Fiscal Year
2009
Total Cost
$234,083
Indirect Cost

  Institution

Name
Massachusetts General Hospital
Department
Type
DUNS #
073130411
City
Boston
State
MA
Country
United States
Zip Code
02199

  Publications

Sykes, Megan (2018) Immune monitoring of transplant patients in transient mixed chimerism tolerance trials. Hum Immunol 79:334-342
Sprangers, B; DeWolf, S; Savage, T M et al. (2017) Origin of Enriched Regulatory T Cells in Patients Receiving Combined Kidney-Bone Marrow Transplantation to Induce Transplantation Tolerance. Am J Transplant 17:2020-2032
Morris, Heather; DeWolf, Susan; Robins, Harlan et al. (2015) Tracking donor-reactive T cells: Evidence for clonal deletion in tolerant kidney transplant patients. Sci Transl Med 7:272ra10
Sykes, M (2015) Immune tolerance in recipients of combined haploidentical bone marrow and kidney transplantation. Bone Marrow Transplant 50 Suppl 2:S82-6
Kawai, T; Sachs, D H; Sprangers, B et al. (2014) Long-term results in recipients of combined HLA-mismatched kidney and bone marrow transplantation without maintenance immunosuppression. Am J Transplant 14:1599-611
Strober, Samuel; Spitzer, Thomas R; Lowsky, Robert et al. (2011) Translational studies in hematopoietic cell transplantation: treatment of hematologic malignancies as a stepping stone to tolerance induction. Semin Immunol 23:273-81
Andreola, G; Chittenden, M; Shaffer, J et al. (2011) Mechanisms of donor-specific tolerance in recipients of haploidentical combined bone marrow/kidney transplantation. Am J Transplant 11:1236-47
Farris, A B; Taheri, D; Kawai, T et al. (2011) Acute renal endothelial injury during marrow recovery in a cohort of combined kidney and bone marrow allografts. Am J Transplant 11:1464-77
LoCascio, Samuel A; Morokata, Tatsuaki; Chittenden, Meredith et al. (2010) Mixed chimerism, lymphocyte recovery, and evidence for early donor-specific unresponsiveness in patients receiving combined kidney and bone marrow transplantation to induce tolerance. Transplantation 90:1607-15