Department of Immunology, St. Jude Children's Research Hospital, Memphis, TN, 38105;
Adaptive Biotechnologies, Seattle, WA 98102; and.
J Immunol. 2014 Jul 1;193(1):258-67. doi: 10.4049/jimmunol.1400322. Epub 2014 Jun 4.
The TCR:CD3 complex transduces signals that are critical for optimal T cell development and adaptive immunity. In resting T cells, the CD3ε cytoplasmic tail associates with the plasma membrane via a proximal basic-rich stretch (BRS). In this study, we show that mice lacking a functional CD3ε-BRS exhibited substantial reductions in thymic cellularity and limited CD4- CD8- double-negative (DN) 3 to DN4 thymocyte transition, because of enhanced DN4 TCR signaling resulting in increased cell death and TCR downregulation in all subsequent populations. Furthermore, positive, but not negative, T cell selection was affected in mice lacking a functional CD3ε-BRS, which led to limited peripheral T cell function and substantially reduced responsiveness to influenza infection. Collectively, these results indicate that membrane association of the CD3ε signaling domain is required for optimal thymocyte development and peripheral T cell function.
T 细胞受体-CD3 复合物转导信号,这些信号对于最佳 T 细胞发育和适应性免疫至关重要。在静止的 T 细胞中,CD3ε 胞质尾通过近端富含碱性的延伸(BRS)与质膜结合。在这项研究中,我们表明,缺乏功能性 CD3ε-BRS 的小鼠表现出明显的胸腺细胞减少和有限的 CD4-CD8-双阴性(DN)3 到 DN4 胸腺细胞过渡,这是由于 DN4TCR 信号增强导致所有后续群体中的细胞死亡和 TCR 下调增加。此外,缺乏功能性 CD3ε-BRS 的小鼠的阳性而非阴性 T 细胞选择受到影响,这导致外周 T 细胞功能有限,对流感感染的反应大大降低。总之,这些结果表明,CD3ε 信号域的膜结合对于最佳的胸腺细胞发育和外周 T 细胞功能是必需的。
