Center for Epigenetics, Van Andel Research Institute, Grand Rapids, MI, USA.
Center for Bioinformatics and Functional Genomics, Cedars-Sinai Medical Center, Los Angeles, CA, USA.
Nat Genet. 2018 Apr;50(4):591-602. doi: 10.1038/s41588-018-0073-4. Epub 2018 Apr 2.
DNA methylation loss occurs frequently in cancer genomes, primarily within lamina-associated, late-replicating regions termed partially methylated domains (PMDs). We profiled 39 diverse primary tumors and 8 matched adjacent tissues using whole-genome bisulfite sequencing (WGBS) and analyzed them alongside 343 additional human and 206 mouse WGBS datasets. We identified a local CpG sequence context associated with preferential hypomethylation in PMDs. Analysis of CpGs in this context ('solo-WCGWs') identified previously undetected PMD hypomethylation in almost all healthy tissue types. PMD hypomethylation increased with age, beginning during fetal development, and appeared to track the accumulation of cell divisions. In cancer, PMD hypomethylation depth correlated with somatic mutation density and cell cycle gene expression, consistent with its reflection of mitotic history and suggesting its application as a mitotic clock. We propose that late replication leads to lifelong progressive methylation loss, which acts as a biomarker for cellular aging and which may contribute to oncogenesis.
DNA 甲基化丢失在癌症基因组中经常发生,主要发生在称为部分甲基化域(PMD)的核纤层相关、晚期复制区域内。我们使用全基因组亚硫酸氢盐测序(WGBS)对 39 种不同的原发性肿瘤和 8 种匹配的相邻组织进行了分析,并与 343 个人类和 206 种小鼠 WGBS 数据集进行了分析。我们鉴定了与 PMD 中优先低甲基化相关的局部 CpG 序列上下文。在这种情况下对 CpG 进行分析('solo-WCGWs'),几乎在所有健康组织类型中都发现了以前未检测到的 PMD 低甲基化。PMD 低甲基化随年龄增长而增加,始于胎儿发育时期,并似乎与细胞分裂的积累有关。在癌症中,PMD 低甲基化深度与体细胞突变密度和细胞周期基因表达相关,这与其反映有丝分裂历史一致,并表明其可作为有丝分裂时钟的应用。我们提出,晚期复制导致终身进行性甲基化丢失,这可作为细胞衰老的生物标志物,并且可能有助于肿瘤发生。
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