T cell Ig domain and mucin domain protein 1 (TIM-1) is a costimulatory molecule that regulates immune responses by modulating CD4+ T cell effector differentiation. However, the function of TIM-1 on other immune cell populations is unknown. Here, we show that in vivo in mice, TIM-1 is predominantly expressed on B rather than T cells. Importantly, TIM-1 was expressed by a large majority of IL-10-expressing regulatory B cells in all major B cell subpopulations, including transitional, marginal zone, and follicular B cells, as well as the B cell population characterized as CD1d(hi)CD5+. A low-affinity TIM-1-specific antibody that normally promotes tolerance in mice, actually accelerated (T cell-mediated) immune responsiveness in the absence of B cells. TIM-1+ B cells were highly enriched for IL-4 and IL-10 expression, promoted Th2 responses, and could directly transfer allograft tolerance. Both cytokine expression and number of TIM-1+ regulatory B cells (Bregs) were induced by TIM-1-specific antibody, and this was dependent on IL-4 signaling. Thus, TIM-1 is an inclusive marker for IL-10+ Bregs that can be induced by TIM-1 ligation. These findings suggest that TIM-1 may be a novel therapeutic target for modulating the immune response and provide insight into the signals involved in the generation and induction of Bregs.
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机译:T 细胞 Ig 结构域和粘蛋白结构域蛋白 1 (TIM-1) 是一种共刺激分子,通过调节 CD4+ T 细胞效应分化来调节免疫反应。然而,TIM-1 对其他免疫细胞群的功能尚不清楚。在这里,我们表明在小鼠体内,TIM-1主要在B细胞而不是T细胞上表达。重要的是,在所有主要 B 细胞亚群中,绝大多数表达 IL-10 的调节性 B 细胞表达,包括过渡期、边缘区和滤泡 B 细胞,以及以 CD1d(hi)CD5+ 为特征的 B 细胞群。一种低亲和力的 TIM-1 特异性抗体,通常可促进小鼠的耐受性,在没有 B 细胞的情况下实际上加速了(T 细胞介导的)免疫反应。TIM-1+ B 细胞高度富集 IL-4 和 IL-10 表达,促进 Th2 反应,并可直接转移同种异体移植物耐受性。TIM-1 特异性抗体诱导细胞因子表达和 TIM-1+ 调节性 B 细胞 (Bregs) 的数量,这依赖于 IL-4 信号传导。因此,TIM-1 是 IL-10+ Bregs 的包容性标记物,可由 TIM-1 连接诱导。这些发现表明,TIM-1可能是调节免疫反应的新型治疗靶点,并提供了对Bregs产生和诱导所涉及的信号的见解。
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