Overexpression of PD-1 on T cells promotes tolerance in cardiac transplantation via ICOS-dependent mechanisms
Thiago J. Borges, Naoka Murakami, Isadora T. Lape, Rodrigo B. Gassen, Kaifeng Liu, Songjie Cai, Joe Daccache, Kassem Safa, Tetsunosuke Shimizu, Shunsuke Ohori, Alison M. Paterson, Paolo Cravedi, Jamil Azzi, Peter T. Sage, Arlene H. Sharpe, Xian C. Li, Leonardo V. Riella
Thiago J. Borges, Naoka Murakami, Isadora T. Lape, Rodrigo B. Gassen, Kaifeng Liu, Songjie Cai, Joe Daccache, Kassem Safa, Tetsunosuke Shimizu, Shunsuke Ohori, Alison M. Paterson, Paolo Cravedi, Jamil Azzi, Peter T. Sage, Arlene H. Sharpe, Xian C. Li, Leonardo V. Riella
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Research Article Immunology Transplantation

Overexpression of PD-1 on T cells promotes tolerance in cardiac transplantation via ICOS-dependent mechanisms

Abstract

The programmed death 1/programmed death ligand 1 (PD-1/PD-L1) pathway is a potent inhibitory pathway involved in immune regulation and is a potential therapeutic target in transplantation. In this study, we show that overexpression of PD-1 on T cells (PD-1 Tg) promotes allograft tolerance in a fully MHC-mismatched cardiac transplant model when combined with costimulation blockade with CTLA-4–Ig. PD-1 overexpression on T cells also protected against chronic rejection in a single MHC II–mismatched cardiac transplant model, whereas the overexpression still allowed the generation of an effective immune response against an influenza A virus. Notably, Tregs from PD-1 Tg mice were required for tolerance induction and presented greater ICOS expression than those from WT mice. The survival benefit of PD-1 Tg recipients required ICOS signaling and donor PD-L1 expression. These results indicate that modulation of PD-1 expression, in combination with a costimulation blockade, is a promising therapeutic target to promote transplant tolerance.

Authors

Thiago J. Borges, Naoka Murakami, Isadora T. Lape, Rodrigo B. Gassen, Kaifeng Liu, Songjie Cai, Joe Daccache, Kassem Safa, Tetsunosuke Shimizu, Shunsuke Ohori, Alison M. Paterson, Paolo Cravedi, Jamil Azzi, Peter T. Sage, Arlene H. Sharpe, Xian C. Li, Leonardo V. Riella

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Figure 4

Comparison of WT and PD-1 Tg Tregs in allogeneic transplant recipients.

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Comparison of WT and PD-1 Tg Tregs in allogeneic transplant recipients. ...
WT or PD-1 Tg recipients of fully MHC-mismatched cardiac transplantation received a single dose of CTLA-4–Ig (250 μg/mouse, i.p.) on day 2 after transplantation. (A) Seven days after heart transplants, WT and PD-1 Tg splenocyte populations were analyzed by flow cytometry. Tregs (CD4+Foxp3+ cells) were significantly reduced in the PD-1 Tg group (n = 3–5/group) according to 1-way ANOVA with Tukey post hoc test. Data are representative of 4 independent experiments. (B) Representative contour plots of LAP expression and (C) IL-10 production by WT or PD-1 Tg graft-infiltrating Tregs (CD4+Foxp3+ cells). Percentage of LAP+ or IL-10+ (D) infiltrating or (E) splenic Tconv (CD4+Foxp3 cells) and Tregs from WT or PD-1 Tg heart recipients. Data are representative of 2 independent experiments (n = 3 animals/group). Data were analyzed using a 1-way ANOVA with Tukey post hoc test. *P < 0.05, **P < 0.01. For all panels, the bar graphs represent mean ± SD. (F) Allograft survival of BALB/c heart allografts transplanted to PD-1 Tg C57BL/6 mice treated with a single dose of CTLA-4–Ig (250 μg on day 2 after transplant). One group received 100 μg of anti-CD25 Ab on days –7 and –1, which impaired the survival induced by sCTLA-Ig treatment (n = 5 per group; *P = 0.0174). (G) Expression of phosphorylated-STAT5 (pSTAT5) in WT and PD-1 Tg Tregs stimulated with IL-2 (5 ng/mL) for 15 or 30 minutes to induce the expression of pSTAT5 (MFI was obtained by flow cytometry). Experiments were performed in triplicate with a pool of 3 mice and were analyzed using a 2-way ANOVA with Sidak post hoc test. **P < 0.01, ***P < 0.001 versus PD-1 Tg mice.