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CAR Treg synergy with anti-CD154 promotes infectious tolerance and dictates allogeneic heart transplant acceptance
Samarth S. Durgam, Isaac Rosado-Sánchez, Dengping Yin, Madeleine Speck, Majid Mojibian, Ismail Sayin, Grace E. Hynes, Maria-Luisa Alegre, Megan K. Levings, Anita S. Chong
Samarth S. Durgam, Isaac Rosado-Sánchez, Dengping Yin, Madeleine Speck, Majid Mojibian, Ismail Sayin, Grace E. Hynes, Maria-Luisa Alegre, Megan K. Levings, Anita S. Chong
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Research Article Immunology Therapeutics Transplantation

CAR Treg synergy with anti-CD154 promotes infectious tolerance and dictates allogeneic heart transplant acceptance

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Abstract

Successful allograft-specific tolerance induction would eliminate the need for daily immunosuppression and improve posttransplant quality of life. Adoptive cell therapy with regulatory T cells expressing donor-specific chimeric antigen receptors (CAR Tregs) is a promising strategy but, as monotherapy, cannot prolong survival with allografts with multiple MHC mismatches. Using an HLA-A2–transgenic haplo-mismatched heart transplantation model in immunocompetent C57BL/6 recipients, we showed that HLA-A2–specific CAR (A2.CAR) Tregs were able to synergize with a low dose of anti-CD154 to enhance graft survival. Using haplo-mismatched grafts expressing the 2W-OVA transgene and tetramer-based tracking of 2W- and OVA-specific T cells, we showed that in mice with accepted grafts, A2.CAR Tregs inhibited donor-specific T cell, B cell, and antibody responses and promoted a substantial increase in endogenous FOXP3+ Tregs with indirect donor specificity. By contrast, in mice where A2.CAR Tregs failed to prolong graft survival, FOXP3– A2.CAR T cells preferentially accumulated in rejecting allografts, and endogenous donor-specific responses were not controlled. This study therefore provides evidence for synergy between A2.CAR Tregs and CD154 blockade to promote infectious tolerance in immunocompetent recipients of haplo-mismatched heart grafts and defines features of A2.CAR Tregs when they fail to reshape host immunity toward allograft tolerance.

Authors

Samarth S. Durgam, Isaac Rosado-Sánchez, Dengping Yin, Madeleine Speck, Majid Mojibian, Ismail Sayin, Grace E. Hynes, Maria-Luisa Alegre, Megan K. Levings, Anita S. Chong

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Figure 6

A2.CAR Tregs synergize with low anti-CD154 to suppress non-A2 donor-specific B cell responses.

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A2.CAR Tregs synergize with low anti-CD154 to suppress non-A2 donor-spec...
(A) Symbols for B–D and H. (B) Quantification of IgG specific for A2, (C) donor MHC-I IgG, and (D) donor MHC-II at day 45 after HTx. (E–G) Gating strategy to track donor MHC-II I-Ed–specific GC B cells (Fas+GL7+) from (F) +A2.CAR Treg Rej or (G) +A2.CAR Treg Acpt. (H) Total GC B cells (Fas+GL7+ of I-Ed) recovered from draining lymph nodes (normalized to 2 × 106 events). Each symbol represents 1 mouse. Data are presented as mean ± SEM, and statistical significance was determined by 1-way ANOVA (#) and Mann-Whitney test (*). *P or #P < 0.05; ##P < 0.01; ####P < 0.0001. DSA, donor-specific antibody.

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