Kim Jee-Hae, Jung Seung Hee, Park Chohee, Lee Jong Ran
Department of Life Science, College of Natural Sciences, Ewha Womans University, Seoul, Republic of Korea.
Front Immunol. 2025 Apr 8;16:1556616. doi: 10.3389/fimmu.2025.1556616. eCollection 2025.
We previously reported a novel adaptor protein, ARAP, required for T cell receptor signaling and integrin-mediated adhesion. The present study investigates further the role of ARAP in T cell biology using mice with an gene deficiency. Similar to wild-type mice, ARAP-deficient mice participate in normal breeding and immune cell development. Similar defects were observed in the T cell receptor signaling and adhesion of ARAP-deficient mice, as shown in previous studies investigating ARAP-suppressed Jurkat T cells. ARAP deficiencies analyzed presented a less severe clinical course of experimental autoimmune encephalomyelitis (EAE) following immunization of mice with the myelin oligodendrocyte glycoprotein (MOG). Serum levels of MOG-specific antibodies and IFN-γ were also reduced in ARAP-deficient EAE mice compared to wild-type EAE mice. Moreover, adoptive transfer of ARAP-deficient T cells induced less severe EAE in recombination-activating gene 1-deficient mice than wild-type T cell transfer. These results strongly suggest that ARAP positively regulates T cell function, while ARAP deficiency in T cells reduces the severity and incidence of EAE.
我们之前报道了一种新型衔接蛋白ARAP,它是T细胞受体信号传导和整合素介导的黏附所必需的。本研究使用基因缺陷小鼠进一步探究ARAP在T细胞生物学中的作用。与野生型小鼠相似,ARAP缺陷小鼠参与正常繁殖和免疫细胞发育。如之前对ARAP抑制的Jurkat T细胞的研究所显示,在ARAP缺陷小鼠的T细胞受体信号传导和黏附中观察到了类似缺陷。在用髓鞘少突胶质细胞糖蛋白(MOG)免疫小鼠后,分析的ARAP缺陷表现出实验性自身免疫性脑脊髓炎(EAE)的临床病程较轻。与野生型EAE小鼠相比,ARAP缺陷的EAE小鼠血清中MOG特异性抗体和IFN-γ水平也降低。此外,与野生型T细胞转移相比,ARAP缺陷T细胞的过继转移在重组激活基因1缺陷小鼠中诱导的EAE较轻。这些结果强烈表明,ARAP正向调节T细胞功能,而T细胞中的ARAP缺陷降低了EAE的严重程度和发病率。
