Department of Pathogens and Immunity, John Curtin School of Medical Research, Australian National University, Canberra, ACT 0200, Australia.
Immunity. 2013 Apr 18;38(4):669-80. doi: 10.1016/j.immuni.2013.01.011. Epub 2013 Apr 11.
Accumulation of T follicular helper (Tfh) cells and proinflammatory cytokines drive autoantibody-mediated diseases. The RNA-binding protein Roquin-1 (Rc3h1) represses the inducible costimulator ICOS and interferon-γ (IFN-γ) in T cells to prevent Tfh cell accumulation. Unlike Rc3h1(san) mice with a mutation in the ROQ domain of Roquin-1, mice lacking the protein, paradoxically do not display increased Tfh cells. Here we have analyzed mice with mutations that eliminate the RING domain from Roquin-1 or its paralog, Roquin-2 (Rc3h2). RING or ROQ mutations both disrupted Icos mRNA regulation by Roquin-1, but, unlike the ROQ mutant that still occupied mRNA-regulating stress granules, RING-deficient Roquin-1 failed to localize to stress granules and allowed Roquin-2 to compensate in the repression of ICOS and Tfh cells. These paralogs also targeted tumor necrosis factor (TNF) in nonlymphoid cells, ameliorating autoantibody-induced arthritis. The Roquin family emerges as a posttranscriptional brake in the adaptive and innate phases of antibody responses.
滤泡辅助性 T 细胞(Tfh)的积累和促炎细胞因子驱动自身抗体介导的疾病。RNA 结合蛋白 Roquin-1(Rc3h1)抑制诱导共刺激分子 ICOS 和干扰素-γ(IFN-γ)在 T 细胞中,以防止 Tfh 细胞的积累。与 Roquin-1 的 ROQ 结构域发生突变的 Rc3h1(san) 小鼠不同,缺乏该蛋白的小鼠并没有表现出 Tfh 细胞的增加。在这里,我们分析了 RING 结构域缺失的 Roquin-1 或其同源物 Roquin-2(Rc3h2)发生突变的小鼠。RING 或 ROQ 突变均破坏了 Roquin-1 对 Icos mRNA 的调节,但与仍然占据调节 mRNA 的应激颗粒的 ROQ 突变体不同,RING 缺陷型 Roquin-1 不能定位到应激颗粒,允许 Roquin-2 代偿 ICOS 和 Tfh 细胞的抑制。这些同源物还靶向非淋巴样细胞中的肿瘤坏死因子(TNF),改善了自身抗体诱导的关节炎。Roquin 家族在抗体反应的适应性和固有阶段作为一种转录后制动。