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胚胎干细胞衍生的血岛细胞保持表观遗传可塑性,并需要 PRC1 来防止神经基因表达。

Embryonic stem cell-derived hemangioblasts remain epigenetically plastic and require PRC1 to prevent neural gene expression.

机构信息

Lymphocyte Development Group, Medical Research Council Clinical Sciences Centre, Faculty of Medicine, Imperial College London, London, United Kingdom.

出版信息

Blood. 2011 Jan 6;117(1):83-7. doi: 10.1182/blood-2010-03-273128. Epub 2010 Sep 28.

Abstract

Many lineage-specific developmental regulator genes are transcriptionally primed in embryonic stem (ES) cells; RNA Pol(II) is bound at their promoters but is prevented from productive elongation by the activity of polycomb repressive complexes (PRC) 1 and 2. This epigenetically poised state is thought to enable ES cells to rapidly execute multiple differentiation programs and is recognized by a simultaneous enrichment for trimethylation of lysine 4 and trimethylation of lysine 27 of histone H3 (bivalent chromatin) across promoter regions. Here we show that the chromatin profile of this important cohort of genes is progressively modified as ES cells differentiate toward blood-forming precursors. Surprisingly however, neural specifying genes, such as Nkx2-2, Nkx2-9, and Sox1, remain bivalent and primed even in committed hemangioblasts, as conditional deletion of PRC1 results in overt and inappropriate expression of neural genes in hemangioblasts. These data reinforce the importance of PRC1 for normal hematopoietic differentiation and reveal an unexpected epigenetic plasticity of mesoderm-committed hemangioblasts.

摘要

许多谱系特异性发育调控基因在胚胎干细胞(ES 细胞)中被转录激活;RNA 聚合酶 II 结合在它们的启动子上,但被多梳抑制复合物 1 和 2 的活性阻止了有效的延伸。这种表观遗传上的平衡状态被认为使 ES 细胞能够快速执行多个分化程序,并通过组蛋白 H3 赖氨酸 4 的三甲基化和赖氨酸 27 的三甲基化在启动子区域的同时富集来识别(双重染色质)。在这里,我们表明,随着 ES 细胞向造血前体细胞分化,这一重要基因群的染色质特征逐渐发生改变。然而,令人惊讶的是,神经特化基因,如 Nkx2-2、Nkx2-9 和 Sox1,即使在定向的造血母细胞中仍然保持双重状态和转录激活,因为多梳抑制复合物 1 的条件性缺失导致神经基因在造血母细胞中明显和不适当的表达。这些数据强调了多梳抑制复合物 1 对于正常造血分化的重要性,并揭示了中胚层定向造血母细胞出人意料的表观遗传可塑性。

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