比较有和无砷暴露的膀胱癌患者全基因组 DNA 甲基化。
Comparison of genome-wide DNA methylation in urothelial carcinomas of patients with and without arsenic exposure.
机构信息
Graduate Institute of Life Science, National Defense Medical Center, Taipei, Taiwan; Genomics Research Center, Academia Sinica, Taipei, Taiwan; Molecular and Genomic Epidemiology Center, China Medical University Hospital, Taichung, Taiwan; China Medical University, Taichung, Taiwan.
Genomics Research Center, Academia Sinica, Taipei, Taiwan.
出版信息
Environ Res. 2014 Jan;128:57-63. doi: 10.1016/j.envres.2013.10.006. Epub 2013 Nov 22.
BACKGROUND
Arsenic is a well-documented carcinogen of human urothelial carcinoma (UC) with incompletely understood mechanisms.
OBJECTIVES
This study aimed to compare the genome-wide DNA methylation profiles of arsenic-induced UC (AsUC) and non-arsenic-induced UC (Non-AsUC), and to assess associations between site-specific methylation levels and cumulative arsenic exposure.
METHODS
Genome-wide DNA methylation profiles in 14 AsUC and 14 non-AsUC were analyzed by Illumina Infinium methylation27 BeadChip and validated by bisulfite pyrosequencing. Mean methylation levels (β¯) in AsUC and non-AsUC were compared by their ratio (β¯ ratio) and difference (Δβ¯). Associations between site-specific methylation levels in UC and cumulative arsenic exposure were examined.
RESULTS
Among 27,578 methylation sites analyzed, 231 sites had β¯ ratio >2 or <0.5 and 45 sites had Δβ¯ >0.2 or <-0.2. There were 13 sites showing statistically significant (q<0.05) differences in β¯ between AsUC and non-AsUC including 12 hypermethylation sites in AsUC and only one hypermethylation site in non-AsUC. Significant associations between cumulative arsenic exposure and DNA methylation levels of 28 patients were observed in nine CpG sites of nine gens including PDGFD (Spearman rank correlation, 0.54), CTNNA2 (0.48), KCNK17 (0.52), PCDHB2 (0.57), ZNF132 (0.48), DCDC2 (0.48), KLK7 (0.48), FBXO39 (0.49), and NPY2R (0.45). These associations remained statistically significant for CpG sites in CTNNA2, KLK7, NPY2R, ZNF132 and KCNK17 in 20 non-smoking women after adjustment for tumor stage and age.
CONCLUSIONS
Significant associations between cumulative arsenic exposure and methylation level of CTNNA2, KLK7, NPY2R, ZNF132 and KCNK17 were found in smoking-unrelated urothelial carcinoma. Arsenic exposure may cause urothelial carcinomas through the hypermethylation of genes involved in cell adhesion, proteolysis, transcriptional regulation, neuronal pathway, and ion transport. The findings of this study, which are limited by its small sample size and moderate dose-response relation, remain to be validated by further studies with large sample sizes.
背景
砷是一种已被充分证实的人类尿路上皮癌(UC)致癌物质,其作用机制尚未完全阐明。
目的
本研究旨在比较砷诱导的 UC(AsUC)和非砷诱导的 UC(Non-AsUC)的全基因组 DNA 甲基化谱,并评估特定部位甲基化水平与累积砷暴露之间的关联。
方法
采用 Illumina Infinium methylation27 BeadChip 分析 14 例 AsUC 和 14 例 Non-AsUC 的全基因组 DNA 甲基化谱,并通过亚硫酸氢盐焦磷酸测序进行验证。通过其比值(β¯ ratio)和差异(Δβ¯)比较 AsUC 和 Non-AsUC 中的平均甲基化水平(β¯)。检测 UC 中特定部位的甲基化水平与累积砷暴露之间的关联。
结果
在分析的 27578 个甲基化位点中,有 231 个位点的β¯ ratio>2 或<0.5,有 45 个位点的Δβ¯>0.2 或<-0.2。在 AsUC 和 Non-AsUC 之间,有 13 个位点的β¯存在统计学显著差异(q<0.05),其中 12 个在 AsUC 中呈高甲基化,而在 Non-AsUC 中仅 1 个呈高甲基化。在 28 例患者中,观察到累积砷暴露与 9 个基因的 28 个 CpG 位点的 DNA 甲基化水平之间存在显著关联,包括 PDGFD(Spearman 秩相关系数,0.54)、CTNNA2(0.48)、KCNK17(0.52)、PCDHB2(0.57)、ZNF132(0.48)、DCDC2(0.48)、KLK7(0.48)、FBXO39(0.49)和 NPY2R(0.45)。在调整肿瘤分期和年龄后,在 20 名不吸烟的女性中,CTNNA2、KLK7、NPY2R、ZNF132 和 KCNK17 中的 CpG 位点的关联仍然具有统计学意义。
结论
在与吸烟无关的尿路上皮癌中,发现累积砷暴露与 CTNNA2、KLK7、NPY2R、ZNF132 和 KCNK17 的甲基化水平之间存在显著关联。砷暴露可能通过参与细胞黏附、蛋白水解、转录调控、神经元通路和离子转运的基因的高甲基化导致尿路上皮癌。本研究的发现受到其小样本量和中等剂量-反应关系的限制,需要进一步的大样本量研究来验证。
Zotero 插件