Selective CD28 blockade attenuates CTLA-4–dependent CD8+ memory T cell effector function and prolongs graft survival
Danya Liu, I. Raul Badell, Mandy L. Ford
Danya Liu, I. Raul Badell, Mandy L. Ford
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Research Article Immunology Transplantation

Selective CD28 blockade attenuates CTLA-4–dependent CD8+ memory T cell effector function and prolongs graft survival

Abstract

Memory T cells pose a significant problem to successful therapeutic control of unwanted immune responses during autoimmunity and transplantation, as they are differentially controlled by cosignaling receptors such as CD28 and CTLA-4. Treatment with abatacept and belatacept impede CD28 signaling by binding to CD80 and CD86, but they also have the unintended consequence of blocking the ligands for CTLA-4, a process that may inadvertently boost effector responses. Here, we show that a potentially novel anti-CD28 domain antibody (dAb) that selectively blocks CD28 but preserves CTLA-4 coinhibition confers improved allograft survival in sensitized recipients as compared with CTLA-4 Ig. However, both CTLA-4 Ig and anti-CD28 dAb similarly and significantly reduced the accumulation of donor-reactive CD8+ memory T cells, demonstrating that regulation of the expansion of CD8+ memory T cell populations is controlled in part by CD28 signals and is not significantly impacted by CTLA-4. In contrast, selective CD28 blockade was superior to CTLA-4 Ig in inhibiting IFN-γ, TNF, and IL-2 production by CD8+ memory T cells, which in turn resulted in reduced recruitment of innate CD11b+ monocytes into allografts. Importantly, this superiority was CTLA-4 dependent, demonstrating that effector function of CD8+ memory T cells is regulated by the balance of CD28 and CTLA-4 signaling.

Authors

Danya Liu, I. Raul Badell, Mandy L. Ford

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Figure 6

Inhibition of IFN-γ– and TNF-mediated signals significantly impairs recruitment of CD11b+ myeloid cells into rejecting allografts and delays graft rejection.

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Inhibition of IFN-γ– and TNF-mediated signals significantly impairs recr...
(A) Experimental design for experiments in which recipients containing memory OT-I T cells generated as above received an OVA-expressing skin graft and were treated with either nothing, CTLA-4 Ig alone, or CTLA-4 Ig and 250 μg of anti–IFN-γ and anti-TNF as described in Methods. (B and C) Summary data of absolute numbers of graft-infiltrating CD11b+ T cells in the 3 groups on day 5 (B) and 10 (C) after transplant. Data shown are n = 5 mice/group, representative of 2 independent experiments with a total of 10 mice per group. *P < 0.05, **P < 0.01 by 1-way ANOVA. (D) Graft survival data of mice treated as above. Kaplan-Meier survival curve of mice treated as above. n=7/group. (E) Survival frequencies of allografts in CTLA-4 Ig– vs. CTLA-4 Ig + anti-TNF + anti–IFN-γ–treated animals on day 21 after transplant. *P = 0.03 by χ2 analysis of frequencies of surviving grafts. dAb, domain antibody.