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Transcription of intragenic CpG islands influences spatiotemporal host gene pre-mRNA processing

机译:腺体CpG岛的转录影响时尚血宿主基因前mRNA加工

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摘要

Alternative splicing (AS) and alternative polyadenylation (APA) generate diverse transcripts in mammalian genomes during development and differentiation. Epigenetic marks such as trimethylation of histone H3 lysine 36 (H3K36me3) and DNA methylation play a role in generating transcriptome diversity. Intragenic CpG islands (iCGIs) and their corresponding host genes exhibit dynamic epigenetic and gene expression patterns during development and between different tissues. We hypothesise that iCGI-associated H3K36me3, DNA methylation and transcription can influence host gene AS and/or APA. We investigate H3K36me3 and find that this histone mark is not a major regulator of AS or APA in our model system. Genomewide, we identify over 4000 host genes that harbour an iCGI in the mammalian genome, including both previously annotated and novel iCGI/host gene pairs. The transcriptional activity of these iCGIs is tissue- and developmental stage-specific and, for the first time, we demonstrate that the premature termination of host gene transcripts upstream of iCGIs is closely correlated with the level of iCGI transcription in a DNA-methylation independent manner. These studies suggest that iCGI transcription, rather than H3K36me3 or DNA methylation, interfere with host gene transcription and pre-mRNA processing genomewide and contributes to the spatiotemporal diversification of both the transcriptome and proteome.
机译:替代剪接(AS)和替代的聚腺苷酸(APA)在发育和分化期间在哺乳动物基因组中产生不同的转录物。表观遗传标记如组蛋白H3赖氨酸36(H3K36ME3)和DNA甲基化的三甲基化起发挥转录组多样性的作用。腺癌CpG岛(ICGIS)及其相应的宿主基因在发育期间和不同组织之间表现出动态表观遗传和基因表达模式。我们假设ICGI相关的H3K36ME3,DNA甲基化和转录可以影响宿主基因和/或APA。我们调查H3K36ME3,发现该组型标记不是我们模型系统中AS或APA的主要调节器。基因面,我们鉴定了哺乳动物基因组中含有ICGI的4000多种宿主基因,包括先前注释和新的ICGI /宿主基因对。这些ICGIS的转录活性是组织和发育阶段特异性,并且我们首次证明ICGIS上游的宿主基因转录物的过早终止与DNA-甲基化独立方式的ICGI转录的水平密切相关。这些研究表明,ICGI转录而不是H3K36ME3或DNA甲基化,干扰宿主基因转录和前mRNA加工基因面,并有助于转录组和蛋白质组的时空多样化。

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