Shakya Arvind, Goren Alon, Shalek Alex, German Cody N, Snook Jeremy, Kuchroo Vijay K, Yosef Nir, Chan Raymond C, Regev Aviv, Williams Matthew A, Tantin Dean
Department of Pathology, University of Utah School of Medicine, Salt Lake City, UT 84112.
Broad Technology Labs, The Broad Institute of MIT and Harvard, Cambridge, MA 02142.
J Exp Med. 2015 Nov 16;212(12):2115-31. doi: 10.1084/jem.20150363. Epub 2015 Oct 19.
Epigenetic changes are crucial for the generation of immunological memory. Failure to generate or maintain these changes will result in poor memory responses. Similarly, augmenting or stabilizing the correct epigenetic states offers a potential method of enhancing memory. Yet the transcription factors that regulate these processes are poorly defined. We find that the transcription factor Oct1 and its cofactor OCA-B are selectively required for the in vivo generation of CD4(+) memory T cells. More importantly, the memory cells that are formed do not respond properly to antigen reencounter. In vitro, both proteins are required to maintain a poised state at the Il2 target locus in resting but previously stimulated CD4(+) T cells. OCA-B is also required for the robust reexpression of multiple other genes including Ifng. ChIPseq identifies ∼50 differentially expressed direct Oct1 and OCA-B targets. We identify an underlying mechanism involving OCA-B recruitment of the histone lysine demethylase Jmjd1a to targets such as Il2, Ifng, and Zbtb32. The findings pinpoint Oct1 and OCA-B as central mediators of CD4(+) T cell memory.
表观遗传变化对于免疫记忆的产生至关重要。无法产生或维持这些变化将导致记忆反应不佳。同样,增强或稳定正确的表观遗传状态提供了一种增强记忆的潜在方法。然而,调节这些过程的转录因子却知之甚少。我们发现转录因子Oct1及其辅因子OCA-B是体内产生CD4(+)记忆T细胞所选择性必需的。更重要的是,形成的记忆细胞对抗原再次接触不能做出适当反应。在体外,这两种蛋白质是维持静息但先前已被刺激的CD4(+) T细胞中Il2靶基因座的准备就绪状态所必需的。OCA-B对于包括Ifng在内的多种其他基因的强劲重新表达也是必需的。ChIPseq鉴定出约50个差异表达的直接Oct1和OCA-B靶标。我们确定了一种潜在机制,涉及OCA-B将组蛋白赖氨酸去甲基化酶Jmjd1a招募至Il2、Ifng和Zbtb32等靶标。这些发现明确指出Oct1和OCA-B是CD4(+) T细胞记忆的核心介质。
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