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重新编程组蛋白甲基化控制单核细胞分化为巨噬细胞。

Reprogramming of histone methylation controls the differentiation of monocytes into macrophages.

机构信息

Department of Basic Medical Sciences, Medical College, Xiamen University, China.

State Key Laboratory of Cellular Stress Biology, Xiamen University, China.

出版信息

FEBS J. 2017 May;284(9):1309-1323. doi: 10.1111/febs.14060. Epub 2017 Apr 4.

DOI:10.1111/febs.14060
PMID:28304152
Abstract

Subset heterogeneity of the mononuclear phagocyte system (MPS) is controlled by defined transcriptional networks and programs; however, the dynamic establishment of programs that control broad, orchestrated expression of transcription factors (TFs) during the progression of monocyte-into-phagocyte (MP) differentiation remains largely unexplored. By using chromatin immunoprecipitation assays, we show the extensive trimethylation of histone H3 lysine 4 (H3K4me3) as well as histone H3 lysine 27 (H3K27me3) occupancy with broad footprints at the promoters of MP differentiation-related TFs, such as HOXA and FOXO genes, KLF4, IRF8 and others. The rapid repression of HOXA genes was closely associated with the MP differentiation program. H3K4me3 participates in regulating HOXA genes at mild and terminal differentiation periods, while H3K27me3 maintains low-level expression of HOXA genes at phagocytic maintenance periods. Furthermore, the reprogramming of H3K27me3 plays a major role in the up-regulation of KLF4 and FOXO genes during MP differentiation. Importantly, the pharmacological inhibition of H3K4me3 and/or H3K27me3 strikingly promotes the differentiation programs of THP-1 and K562 cells. Together, these findings elucidate mechanisms crucial to the dynamic establishment of epigenetic memory, which is central to the maintenance of the MP differentiation blockade.

摘要

单核吞噬细胞系统 (MPS) 的子集异质性受特定的转录网络和程序控制;然而,在单核细胞向吞噬细胞 (MP) 分化过程中,控制广泛协调的转录因子 (TFs) 表达的程序的动态建立在很大程度上仍未得到探索。通过使用染色质免疫沉淀测定法,我们显示了 H3K4me3 和 H3K27me3 的广泛三甲基化以及在与 MP 分化相关的 TF 如 HOXA 和 FOXO 基因、KLF4、IRF8 等的启动子上具有广泛足迹的 H3K27me3 占据。HOXA 基因的快速抑制与 MP 分化程序密切相关。H3K4me3 参与调节轻度和终末分化期的 HOXA 基因,而 H3K27me3 在吞噬维持期维持 HOXA 基因的低水平表达。此外,H3K27me3 的重编程在 MP 分化过程中对 KLF4 和 FOXO 基因的上调起着主要作用。重要的是,H3K4me3 和/或 H3K27me3 的药理学抑制显著促进了 THP-1 和 K562 细胞的分化程序。总之,这些发现阐明了对动态建立表观遗传记忆至关重要的机制,这是维持 MP 分化阻断的核心。

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