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多能细胞系的染色质特征

Chromatin signatures of pluripotent cell lines.

作者信息

Azuara Véronique, Perry Pascale, Sauer Stephan, Spivakov Mikhail, Jørgensen Helle F, John Rosalind M, Gouti Mina, Casanova Miguel, Warnes Gary, Merkenschlager Matthias, Fisher Amanda G

机构信息

Lymphocyte Development Group, MRC Clinical Sciences Centre, Imperial College School of Medicine, Hammersmith Hospital, Du Cane Road, London W12 ONN, UK.

出版信息

Nat Cell Biol. 2006 May;8(5):532-8. doi: 10.1038/ncb1403. Epub 2006 Mar 29.

Abstract

Epigenetic genome modifications are thought to be important for specifying the lineage and developmental stage of cells within a multicellular organism. Here, we show that the epigenetic profile of pluripotent embryonic stem cells (ES) is distinct from that of embryonic carcinoma cells, haematopoietic stem cells (HSC) and their differentiated progeny. Silent, lineage-specific genes replicated earlier in pluripotent cells than in tissue-specific stem cells or differentiated cells and had unexpectedly high levels of acetylated H3K9 and methylated H3K4. Unusually, in ES cells these markers of open chromatin were also combined with H3K27 trimethylation at some non-expressed genes. Thus, pluripotency of ES cells is characterized by a specific epigenetic profile where lineage-specific genes may be accessible but, if so, carry repressive H3K27 trimethylation modifications. H3K27 methylation is functionally important for preventing expression of these genes in ES cells as premature expression occurs in embryonic ectoderm development (Eed)-deficient ES cells. Our data suggest that lineage-specific genes are primed for expression in ES cells but are held in check by opposing chromatin modifications.

摘要

表观遗传基因组修饰被认为对于确定多细胞生物体内细胞的谱系和发育阶段很重要。在此,我们表明多能胚胎干细胞(ES)的表观遗传特征与胚胎癌细胞、造血干细胞(HSC)及其分化后代的表观遗传特征不同。沉默的、谱系特异性基因在多能细胞中比在组织特异性干细胞或分化细胞中更早复制,并且具有出乎意料的高水平乙酰化H3K9和甲基化H3K4。不同寻常的是,在ES细胞中,这些开放染色质的标记物在一些未表达基因处也与H3K27三甲基化相结合。因此,ES细胞的多能性以特定的表观遗传特征为特征,其中谱系特异性基因可能是可及的,但如果是这样,则携带抑制性H3K27三甲基化修饰。H3K27甲基化在防止这些基因在ES细胞中表达方面具有重要功能,因为在胚胎外胚层发育(Eed)缺陷的ES细胞中会出现过早表达。我们的数据表明,谱系特异性基因在ES细胞中已准备好表达,但受到相反染色质修饰的抑制。

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