Department of Cellular and Molecular Pharmacology, University of California, San Francisco, California, USA.
Nat Struct Mol Biol. 2010 Dec;17(12):1495-9. doi: 10.1038/nsmb.1924. Epub 2010 Nov 7.
While much attention has been focused on chromatin at promoters and exons, human genes are mostly composed of intronic sequences. Analyzing published surveys of nucleosomes and 41 chromatin marks in humans, we identified histone modifications specifically associated with 5' intronic sequences, distinguishable from promoter marks and bulk nucleosomes. These intronic marks were spatially reciprocal to trimethylated histone H3 Lys36 (H3K36me3), typically transitioning near internal exons. Several marks transitioned near bona fide exons, but not near nucleosomes at exon-like sequences. Therefore, we examined whether splicing affects histone marking. Even with considerable changes in regulated alternative splicing, histone marks were stable. Notably, these findings are consistent with exon definition influencing histone marks. In summary, we show that the location of many intragenic marks in humans can be distilled into a simple organizing principle: association with 5' intronic or 3' exonic regions.
尽管人们对启动子和外显子的染色质给予了极大的关注,但人类基因主要由内含子序列组成。通过分析已发表的人类核小体和 41 种染色质标记物的调查,我们鉴定出了与 5'内含子序列特异性相关的组蛋白修饰,这些修饰与启动子标记物和核小体有明显区别。这些内含子标记在空间上与三甲基化组蛋白 H3 赖氨酸 36(H3K36me3)相互转化,通常在内部外显子附近发生。有几个标记物在真正的外显子附近发生转化,但不在类似外显子的序列处的核小体附近发生转化。因此,我们研究了剪接是否会影响组蛋白标记。即使在受调控的可变剪接发生了相当大的变化,组蛋白标记仍然是稳定的。值得注意的是,这些发现与外显子定义影响组蛋白标记的观点一致。总之,我们表明,人类许多基因内标记的位置可以归结为一个简单的组织原则:与 5'内含子或 3'外显子区域相关联。
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