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Genome-wide DNA methylation map of human neutrophils reveals widespread inter-individual epigenetic variation

机译:人类嗜中性粒细胞的全基因组DNA甲基化图谱揭示了广泛的个体间表观遗传变异

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摘要

The extent of variation in DNA methylation patterns in healthy individuals is not yet well documented. Identification of inter-individual epigenetic variation is important for understanding phenotypic variation and disease susceptibility. Using neutrophils from a cohort of healthy individuals, we generated base-resolution DNA methylation maps to document inter-individual epigenetic variation. We identified 12851 autosomal inter-individual variably methylated fragments (iVMFs). Gene promoters were the least variable, whereas gene body and upstream regions showed higher variation in DNA methylation. The iVMFs were relatively enriched in repetitive elements compared to non-iVMFs, and were associated with genome regulation and chromatin function elements. Further, variably methylated genes were disproportionately associated with regulation of transcription, responsive function and signal transduction pathways. Transcriptome analysis indicates that iVMF methylation at differentially expressed exons has a positive correlation and local effect on the inclusion of that exon in the mRNA transcript.
机译:健康个体中DNA甲基化模式的变化程度尚未得到充分证明。个体间表观遗传变异的鉴定对于理解表型变异和疾病易感性很重要。使用来自健康个体的中性粒细胞,我们生成了基本分辨率的DNA甲基化图谱,以记录个体间表观遗传变异。我们鉴定了12851个常染色体个体间可变甲基化片段(iVMFs)。基因启动子的可变性最小,而基因体和上游区域在DNA甲基化方面表现出更高的变化。与非iVMF相比,iVMF的重复元件相对丰富,并且与基因组调控和染色质功能元件相关。此外,可变甲基化的基因与转录,响应功能和信号转导途径的调节不成比例地相关。转录组分析表明,差异表达的外显子上的iVMF甲基化与该外显子在mRNA转录物中的包容具有正相关和局部影响。

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