Department of Immunology, Duke University Medical Center, Durham, NC 27710, USA.
J Immunol. 2013 Mar 15;190(6):2938-47. doi: 10.4049/jimmunol.1203163. Epub 2013 Feb 11.
Linker for activation of T cells (LAT) is a transmembrane adaptor protein that links TCR engagement to downstream signaling events. Although it is clear that LAT is essential in thymocyte development and initiation of T cell activation, its function during T cell expansion, contraction, and memory formation remains unknown. To study the role of TCR-mediated signaling in CD8 T cells during the course of pathogen infection, we used an inducible mouse model to delete LAT in Ag-specific CD8 T cells at different stages of Listeria infection and analyzed the effect of deletion on T cell responses. Our data showed that LAT is important for maintaining CD8 T cell expansion during the priming phase; however, it is not required for CD8 T cell contraction and memory maintenance. Moreover, LAT deficiency accelerates memory differentiation during the effector-to-memory transition, leading to a higher frequency of KLRG1(low)IL-7R(high)CD62L(high) memory T cells. Nonetheless, these LAT-deficient memory T cells were unable to proliferate or produce cytokines upon secondary infection. Our data demonstrated that, although TCR-mediated signaling is dispensable for contraction and memory maintenance, it regulates CD8 T cell memory differentiation and is essential for the memory response against pathogens.
衔接蛋白(Linker for activation of T cells,LAT)是一种跨膜衔接蛋白,可将 TCR 结合与下游信号事件联系起来。虽然 LAT 在胸腺细胞发育和 T 细胞激活起始中是必不可少的,但它在 T 细胞扩增、收缩和记忆形成过程中的功能仍然未知。为了研究 TCR 介导的信号在病原体感染过程中 CD8 T 细胞中的作用,我们使用一种诱导型小鼠模型在李斯特菌感染的不同阶段特异性地删除 CD8 T 细胞中的 LAT,并分析删除对 T 细胞反应的影响。我们的数据表明,LAT 对于维持 CD8 T 细胞在启动阶段的扩增是重要的;然而,它对于 CD8 T 细胞的收缩和记忆维持不是必需的。此外,LAT 缺陷加速了效应向记忆的过渡中的记忆分化,导致更高频率的 KLRG1(low)IL-7R(high)CD62L(high)记忆 T 细胞。尽管如此,这些 LAT 缺陷型记忆 T 细胞在二次感染时无法增殖或产生细胞因子。我们的数据表明,尽管 TCR 介导的信号对于收缩和记忆维持不是必需的,但它调节 CD8 T 细胞记忆分化,对于针对病原体的记忆反应是必不可少的。
