Department of Immunology, University of Washington, Seattle, WA 98195, USA.
J Immunol. 2013 Jun 15;190(12):6180-6. doi: 10.4049/jimmunol.1300181. Epub 2013 May 17.
Recent thymic emigrants (RTEs) are the youngest T cells in the lymphoid periphery and exhibit phenotypic and functional characteristics distinct from those of their more mature counterparts in the naive peripheral T cell pool. We show in this study that the Il2 and Il4 promoter regions of naive CD4(+) RTEs are characterized by site-specific hypermethylation compared with those of both mature naive (MN) T cells and the thymocyte precursors of RTEs. Thus, RTEs do not merely occupy a midpoint between the thymus and the mature T cell pool, but represent a distinct transitional T cell population. Furthermore, RTEs and MN T cells exhibit distinct CpG DNA methylation patterns both before and after activation. Compared with MN T cells, RTEs express higher levels of several enzymes that modify DNA methylation, and inhibiting methylation during culture allows RTEs to reach MN T cell levels of cytokine production. Collectively, these data suggest that the functional differences that distinguish RTEs from MN T cells are influenced by epigenetic mechanisms and provide clues to a mechanistic basis for postthymic maturation.
近期胸腺迁出细胞(RTE)是淋巴器官中最年轻的 T 细胞,与幼稚外周 T 细胞库中的成熟 T 细胞相比,它们具有独特的表型和功能特征。本研究表明,与成熟的幼稚 T 细胞(MN)和 RTE 的胸腺前体细胞相比,幼稚 CD4+RTE 的 Il2 和 Il4 启动子区域具有特异性高甲基化的特点。因此,RTE 不仅占据了胸腺和成熟 T 细胞库之间的中点,而且代表了一个独特的过渡 T 细胞群体。此外,RTE 和 MN T 细胞在激活前后表现出不同的 CpG DNA 甲基化模式。与 MN T 细胞相比,RTE 表达更高水平的几种修饰 DNA 甲基化的酶,并且在培养过程中抑制甲基化可以使 RTE 达到 MN T 细胞产生细胞因子的水平。总的来说,这些数据表明,区分 RTE 和 MN T 细胞的功能差异受表观遗传机制的影响,并为胸腺后成熟的机制基础提供了线索。
