Abstract

If the immune deficiency associated with allogeneic hematopoietic stem cell transplantation (HSCT) could be corrected or even prevented, the therapeutic index of allogeneic HSCT would be significantly improved and its impact greatly enhanced. Our hypothesis is that understanding the pathways that regulate early T cell development, maturation, differentiation, and acquisition of function coupled with the development and clinical translation of specific approaches to enhance each of these steps while controlling alloreactivity will be necessary to achieve this objective. Over the past 2 years, an international team of experts composed of stem cell biologists, basic and clinical immunologists, transplant biologists, transplant clinical investigators, and biostatisticians has been assembled to attack this problem. Each of these individuals brings a strong translational track record and commitment to this challenge. Our goal is to develop translational strategies to foster rapid and, if possible, complete immune reconstitution after HSCT in order to eliminate the multiple complications that accompany acute and chronic immune deficiency. We propose to develop, enable, and standardize these technologies which will in turn impact favorably on GVHD, regimen-related toxicity, and relapse. To this end, seven Projects and five Cores have been developed. Projects 1 and 2 will study the common lymphoid progenitor cell in mice and humans in order to develop strategies to enhance HSCT immune reconstitution. Projects 3 and 4 will attempt to prevent and/or repair HSCT associated thymic damage in murine models and translate these strategies to patients undergoing allogeneic HSCT. Project 5 will attempt to reduce the intensity of conditioning regimens by using veto and regulatory cells to control host anti-donor alloreactivity. This approach has the potential to improve immune reconstitution. Project 6 will attempt to improve ex vivo strategies to anergize donor anti-host alloreactive T cells to control GVHD thereby allowing a broad functional T cell repertoire to be adoptively transferred to HSCT patients. Project 7 will adoptively transfer of alloreactive NK cells following HSCT in order to reduce the intensity of conditioning and tumor relapse. Project 7 also proposes to adoptively transfer T cells of both narrow and broad repertoire to control pathogens. These Projects rely upon the Clinical Trials, Immune Assessment, Biostatistical, Tetramer, and Administrative Cores to provide a platform to foster and facilitate planning, translation, and collaboration. We see this Program as a catalyst to bring others in the field together. The next decade will test the concept whether specific manipulation of the immune system to treat human disease is sound and we are confident that this Program will significantly contribute to this effort.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Program Projects (P01)
Project #
5P01CA100265-02
Application #
6807050
Study Section
Special Emphasis Panel (ZCA1-GRB-2 (O1))
Program Officer
Wu, Roy S
Project Start
2003-09-30
Project End
2008-11-30
Budget Start
2005-06-21
Budget End
2005-11-30
Support Year
2
Fiscal Year
2005
Total Cost
$3,651,182
Indirect Cost

  Institution

Name
Dana-Farber Cancer Institute
Department
Type
DUNS #
076580745
City
Boston
State
MA
Country
United States
Zip Code
02215

  Publications

Perruccio, Katia; Topini, Fabiana; Tosti, Antonella et al. (2015) Differences in Aspergillus-specific immune recovery between T-cell-replete and T-cell-depleted hematopoietic transplants. Eur J Haematol 95:551-7
Hosing, Chitra; Kebriaei, Partow; Wierda, William et al. (2013) CARs in chronic lymphocytic leukemia -- ready to drive. Curr Hematol Malig Rep 8:60-70
Perruccio, K; Topini, F; Tosti, A et al. (2012) Optimizing a photoallodepletion protocol for adoptive immunotherapy after haploidentical SCT. Bone Marrow Transplant 47:1196-200
Kebriaei, Partow; Kelly, Susan S; Manuri, Pallavi et al. (2012) Chimeric antibody receptors (CARs): driving T-cell specificity to enhance anti-tumor immunity. Front Biosci (Schol Ed) 4:520-31
Pos, Wouter; Sethi, Dhruv K; Call, Melissa J et al. (2012) Crystal structure of the HLA-DM-HLA-DR1 complex defines mechanisms for rapid peptide selection. Cell 151:1557-68
Singh, Harjeet; Figliola, Matthew J; Dawson, Margaret J et al. (2011) Reprogramming CD19-specific T cells with IL-21 signaling can improve adoptive immunotherapy of B-lineage malignancies. Cancer Res 71:3516-27
Milstein, Oren; Hagin, David; Lask, Assaf et al. (2011) CTLs respond with activation and granule secretion when serving as targets for T-cell recognition. Blood 117:1042-52
Davies, Jeff K; Singh, Harjeet; Huls, Helen et al. (2010) Combining CD19 redirection and alloanergization to generate tumor-specific human T cells for allogeneic cell therapy of B-cell malignancies. Cancer Res 70:3915-24
Perruccio, Katia; Bonifazi, Pierluigi; Topini, Fabiana et al. (2010) Thymosin alpha1 to harness immunity to pathogens after haploidentical hematopoietic transplantation. Ann N Y Acad Sci 1194:153-61
Romagné, Francois; André, Pascale; Spee, Pieter et al. (2009) Preclinical characterization of 1-7F9, a novel human anti-KIR receptor therapeutic antibody that augments natural killer-mediated killing of tumor cells. Blood 114:2667-77

Showing the most recent 10 out of 27 publications