Nonhematopoietic antigen blocks memory programming of alloreactive CD8+ T cells and drives their eventual exhaustion in mouse models of bone marrow transplantation
Barry Flutter, Noha Edwards, Farnaz Fallah-Arani, Stephen Henderson, Jian-Guo Chai, Shivajanani Sivakumaran, Sara Ghorashian, Clare L. Bennett, Gordon J. Freeman, Megan Sykes, Ronjon Chakraverty
Barry Flutter, Noha Edwards, Farnaz Fallah-Arani, Stephen Henderson, Jian-Guo Chai, Shivajanani Sivakumaran, Sara Ghorashian, Clare L. Bennett, Gordon J. Freeman, Megan Sykes, Ronjon Chakraverty
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Research Article Hematology

Nonhematopoietic antigen blocks memory programming of alloreactive CD8+ T cells and drives their eventual exhaustion in mouse models of bone marrow transplantation

Abstract

Allogeneic blood or BM transplantation (BMT) is the most commonly applied form of adoptive cellular therapy for cancer. In this context, the ability of donor T cells to respond to recipient antigens is coopted to generate graft-versus-tumor (GVT) responses. The major reason for treatment failure is tumor recurrence, which is linked to the eventual loss of functional, host-specific CTLs. In this study, we have explored the role of recipient antigen expression by nonhematopoietic cells in the failure to sustain effective CTL immunity. Using clinically relevant models, we found that nonhematopoietic antigen severely disrupts the formation of donor CD8+ T cell memory at 2 distinct levels that operate in the early and late phases of the response. First, initial and direct encounters between donor CD8+ T cells and nonhematopoietic cells blocked the programming of memory precursors essential for establishing recall immunity. Second, surviving CD8+ T cells became functionally exhausted with heightened expression of the coinhibitory receptor programmed death-1 (PD-1). These 2 factors acted together to induce even more profound failure in long-term immunosurveillance. Crucially, the functions of exhausted CD8+ T cells could be partially restored by late in vivo blockade of the interaction between PD-1 and its ligand, PD-L1, without induction of graft-versus-host disease, suggestive of a potential clinical strategy to prevent or treat relapse following allogeneic BMT.

Authors

Barry Flutter, Noha Edwards, Farnaz Fallah-Arani, Stephen Henderson, Jian-Guo Chai, Shivajanani Sivakumaran, Sara Ghorashian, Clare L. Bennett, Gordon J. Freeman, Megan Sykes, Ronjon Chakraverty

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Nonhematopoietic antigen disrupts memory function and homeostasis.

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Nonhematopoietic antigen disrupts memory function and homeostasis. (A) n...
(A) nhTA+ [B6+BDF1→BDF1] and nhTA [B6+BDF1→B6] allogeneic chimeras were established and 10 weeks later received 3 × 107 CD45.1+ B6 SCs. (B) In vivo cytotoxicity of CFSE-labeled BDF1 target B cells 60 days after SC transfer. (C) IFN-γ production by CD45.1+ CD8+ T cells recovered from the spleens of recipients 60 days after SC transfer, following overnight stimulation with irradiated BDF1 SCs. (D) Absolute number of DLI-derived CD8+ T cells in the spleen, LN, and BM 60 days after SC transfer. (E) Scatter plots show the absolute number of CD44hiCD62Llo and CD44hiCD62Lhi DLI-derived CD8+ cells recovered from spleen. *P < 0.05, **P < 0.01, ***P < 0.001, Mann-Whitney test. (F) SCs (3 × 107) were transferred from CD45.1+ and Thy1.1+ B6 mice to nhTA+ and nhTA chimeras, respectively. At 60 days after transfer, CD8+ T cells were sorted by magnetic selection, mixed at a 1:1 ratio, and incubated in medium alone or with the indicated cytokines. Plots show starting mixture and the relative survival (as a percentage) of CD8+ T cells from nhTA+ or nhTA hosts after 7 days culture.