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Promoter-like epigenetic signatures in exons displaying cell type-specific splicing

机译:显示细胞类型特异性剪接的外显子中的启动子样表观遗传学签名

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Background: Pre-m RNA splicing occurs mainly co-transcriptionally, and both nucleosome density and histone modifications have been proposed to play a role in splice site recognition and regulation. However, the extent and mechanisms behind this interplay remain poorly understood. Results: We use transcriptomic and epigenomic data generated by the ENCODE project to investigate the association between chromatin structure and alternative splicing. We find a strong and significant positive association between H3K9ac, H3K27ac, H3K4me3, epigenetic marks characteristic of active promoters, and exon inclusion in a small but well-defined class of exons, representing approximately 4 % of all regulated exons. These exons are systematically maintained at comparatively low levels of inclusion across cell types, but their inclusion is significantly enhanced in particular cell types when in physical proximity to active promoters. Conclusion: Histone modifications and other chromatin features that activate transcription can be co-opted to participate in the regulation of the splicing of exons that are in physical proximity to promoter regions.
机译:背景:pre-m RNA剪接主要通过转录共发生,并且已经提出核小体密度和组蛋白修饰均在剪接位点识别和调控中发挥作用。但是,这种相互作用背后的程度和机制仍然知之甚少。结果:我们使用由ENCODE项目生成的转录组和表观基因组数据来研究染色质结构与选择性剪接之间的关联。我们发现H3K9ac,H3K27ac,H3K4me3,活性启动子的表观遗传标记特征以及小但定义明确的外显子类别中的外显子之间存在强而显着的正相关,约占所有受调控外显子的4%。这些外显子被系统地维持在跨细胞类型的相对较低的包涵水平,但是当它们与活性启动子物理接近时,它们的包涵在特定细胞类型中显着增强。结论:组蛋白修饰和激活转录的其他染色质特征可以共同参与调节与启动子区域物理接近的外显子的剪接。

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