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H3K4me3 Breadth Is Linked to Cell Identity and Transcriptional Consistency

机译:H3K4me3宽度链接到细胞身份和转录一致性

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摘要

Trimethylation of histone H3 at lysine 4 (H3K4me3) is a chromatin modification known to mark the transcription start sites of active genes. Here, we show that H3K4me3 domains that spread more broadly over genes in a given cell type preferentially mark genes that are essential for the identity and function of that cell type. Using the broadest H3K4me3 domains as a discovery tool in neural progenitor cells, we identify novel regulators of these cells. Machine learning models reveal that the broadest H3K4me3 domains represent a distinct entity, characterized by increased marks of elongation. The broadest H3K4me3 domains also have more paused polymerase at their promoters, suggesting a unique transcriptional output. Indeed, genes marked by the broadest H3K4me3 domains exhibit enhanced transcriptional consistency rather than increased transcriptional levels, and perturbation of H3K4me3 breadth leads to changes in transcriptional consistency. Thus, H3K4me3 breadth contains information that could ensure transcriptional precision at key cell identity/function genes.
机译:组蛋白H3在赖氨酸4(H3K4me3)处的三甲基化是一种染色质修饰,已知可以标记活性基因的转录起始位点。在这里,我们显示了在给定细胞类型中的基因上更广泛分布的H3K4me3域优先标记对于该细胞类型的身份和功能必不可少的基因。使用最广泛的H3K4me3域作为神经祖细胞中的发现工具,我们确定了这些细胞的新型调节剂。机器学习模型表明,最广泛的H3K4me3域代表一个独特的实体,其特征是延伸标记的增加。最广泛的H3K4me3结构域在其启动子处还具有更多暂停的聚合酶,表明具有独特的转录输出。确实,以最广泛的H3K4me3结构域标记的基因显示出增强的转录一致性,而不是增加的转录水平,并且H3K4me3宽度的扰动导致转录一致性的变化。因此,H3K4me3的宽度包含可以确保关键细胞身份/功能基因的转录精度的信息。

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