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发育中和发育成熟的斑马鱼中CpG甲基化的基因组学

Genomics of CpG methylation in developing and developed zebrafish.

作者信息

McGaughey David M, Abaan Hatice Ozel, Miller Ryan M, Kropp Peter A, Brody Lawrence C

机构信息

Molecular Pathogenesis Section, Genome Technology Branch, National Human Genome Research Institute, National Institutes of Health, Bethesda, Maryland.

Molecular Pathogenesis Section, Genome Technology Branch, National Human Genome Research Institute, National Institutes of Health, Bethesda, Maryland

出版信息

G3 (Bethesda). 2014 Mar 21;4(5):861-9. doi: 10.1534/g3.113.009514.

Abstract

DNA methylation is a dynamic process through which specific chromatin modifications can be stably transmitted from parent to daughter cells. A large body of work has suggested that DNA methylation influences gene expression by silencing gene promoters. However, these conclusions were drawn from data focused mostly on promoter regions. Regarding the entire genome, it is unclear how methylation and gene transcription patterns are related during vertebrate development. To identify the genome-wide distribution of CpG methylation, we created series of high-resolution methylome maps of Danio rerio embryos during development and in mature, differentiated tissues. We found that embryonic and terminal tissues have unique methylation signatures in CpG islands and repetitive sequences. Fully differentiated tissues have increased CpG and LTR methylation and decreased SINE methylation relative to embryonic tissues. Unsupervised clustering analyses reveal that the embryonic and terminal tissues can be classified solely by their methylation patterning. Novel analyses also identify a previously undescribed genome-wide exon methylation signature. We also compared whole genome methylation with genome-wide mRNA expression levels using publicly available RNA-seq datasets. These comparisons revealed previously unrecognized relationships between gene expression, alternative splicing, and exon methylation. Surprisingly, we found that exonic methylation is a better predictor of mRNA expression level than promoter methylation. We also found that transcriptionally skipped exons have significantly less methylation than retained exons. Our integrative analyses reveal highly complex interplay between gene expression, alternative splicing, development, and methylation patterning in zebrafish.

摘要

DNA甲基化是一个动态过程,通过该过程特定的染色质修饰能够从亲代细胞稳定地传递给子代细胞。大量研究表明,DNA甲基化通过使基因启动子沉默来影响基因表达。然而,这些结论大多是基于聚焦于启动子区域的数据得出的。对于整个基因组而言,在脊椎动物发育过程中甲基化与基因转录模式之间的关系尚不清楚。为了确定全基因组范围内CpG甲基化的分布情况,我们绘制了斑马鱼胚胎发育过程中以及成熟分化组织的一系列高分辨率甲基化组图谱。我们发现,胚胎组织和终末组织在CpG岛和重复序列中具有独特的甲基化特征。相对于胚胎组织,完全分化的组织中CpG和LTR甲基化增加,而SINE甲基化减少。无监督聚类分析表明,胚胎组织和终末组织可以仅根据其甲基化模式进行分类。新的分析还鉴定出一种以前未描述的全基因组外显子甲基化特征。我们还使用公开可用的RNA测序数据集,将全基因组甲基化与全基因组mRNA表达水平进行了比较。这些比较揭示了基因表达、可变剪接和外显子甲基化之间以前未被认识到的关系。令人惊讶的是,我们发现外显子甲基化比启动子甲基化更能预测mRNA表达水平。我们还发现,转录跳过的外显子的甲基化明显少于保留的外显子。我们的综合分析揭示了斑马鱼中基因表达、可变剪接、发育和甲基化模式之间高度复杂的相互作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/45a6/4025485/3899b577f2a9/861f1.jpg

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