The effect of abatacept on T cell activation is not long-lived in vivo

Larissa C da Rosa, H. Scales, R. Benson, James M Brewer, Iain B. McInnes, P. Garside
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Abstract

Abatacept, a co-stimulatory blocker comprising the extracellular portion of human CTLA-4 linked to the Fc region of IgG1, is approved for the treatment of rheumatoid arthritis. By impairing the interaction between CD28 on T cells and CD80/CD86 on APCs, its mechanisms of action include: the suppression of follicular T helper cells (preventing the breach of self-tolerance in B cells), inhibition of cell cycle progression holding T cells in a state described as “induced naïve” and reduction in DC conditioning. However, less is known about how long these inhibitory effects might last, which is a critical question for therapeutic use in patients. Herein, employing a murine model of OVA-induced DTH, we demonstrate that the effect of abatacept is short-lived in vivo and that the inhibitory effects diminish markedly when treatment is ceased.
阿帕他赛对体内 T 细胞活化的影响并不持久
阿巴他赛普是一种共刺激阻断剂,由与 IgG1 的 Fc 区域相连的人类 CTLA-4 细胞外部分组成,已被批准用于治疗类风湿性关节炎。通过损害 T 细胞上的 CD28 与 APC 上的 CD80/CD86 之间的相互作用,它的作用机制包括:抑制滤泡 T 辅助细胞(防止 B 细胞破坏自身耐受性),抑制细胞周期的进展,使 T 细胞处于一种被称为 "诱导幼稚 "的状态,并减少 DC 的调节。然而,人们对这些抑制作用可能会持续多长时间知之甚少,而这正是对患者进行治疗的一个关键问题。在这里,我们利用小鼠 OVA 诱导的 DTH 模型证明,阿巴他赛普在体内的作用是短暂的,而且在停止治疗后抑制作用会明显减弱。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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