JCI Insight. 2018 Jan 11;3(1). doi: 10.1172/jci.insight.96378.
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.
记忆 T 细胞在自身免疫和移植过程中对成功治疗控制不必要的免疫反应构成了重大挑战,因为它们受到共刺激受体(如 CD28 和 CTLA-4)的差异调控。阿巴西普和贝利尤单抗的治疗通过与 CD80 和 CD86 结合来阻止 CD28 信号,但它们也产生了阻断 CTLA-4 配体的意外后果,这一过程可能无意中增强了效应器反应。在这里,我们表明一种潜在的新型抗 CD28 结构域抗体(dAb)可选择性阻断 CD28 但保留 CTLA-4 共抑制作用,与 CTLA-4 Ig 相比,可改善致敏受者的移植物存活。然而,CTLA-4 Ig 和抗 CD28 dAb 均显著且显著减少了供体反应性 CD8+记忆 T 细胞的积累,表明 CD8+记忆 T 细胞群体的扩增受到 CD28 信号的部分调控,而不受 CTLA-4 的显著影响。相比之下,选择性 CD28 阻断在抑制 CD8+记忆 T 细胞产生 IFN-γ、TNF 和 IL-2 方面优于 CTLA-4 Ig,这反过来又导致固有 CD11b+单核细胞向移植物的募集减少。重要的是,这种优势依赖于 CTLA-4,表明 CD8+记忆 T 细胞的效应功能受到 CD28 和 CTLA-4 信号的平衡调节。
