Department of Epidemiology, School of Public Health, University of Washington, Seattle, Washington.
Program in Biostatistics, Division of Public Health Sciences, Fred Hutchinson Cancer Research Center, Seattle, Washington.
Cancer Epidemiol Biomarkers Prev. 2018 Jun;27(6):689-695. doi: 10.1158/1055-9965.EPI-17-0951. Epub 2018 Mar 14.
Differential DNA methylation as measured in blood is a promising marker of bladder cancer susceptibility. However, previous studies have exclusively used postdiagnostic blood samples, meaning that observed associations may be markers of disease rather than susceptibility. Genome-wide methylation was measured in prediagnostic blood samples, using the Illumina Infinium HumanMethylation450 Bead Array, among 440 bladder cancer cases with the transitional cell carcinoma (TCC) subtype and 440 matched cancer-free controls from the Women's Health Initiative cohort. After normalization and probe filtering, we used conditional logistic regression models to test for associations between methylation measurements at 361,184 CpG sites and bladder cancer risk. Increased methylation at cg22748573, located in a CpG island within the 5'-UTR/first exon of the gene, was associated with an 82% decreased risk of bladder cancer after adjusting for race/ethnicity, smoking status, pack-years of smoking, and leukocyte cell profile and accounting for multiple testing (OR = 0.18, q-value = 0.05). The result was robust to sensitivity analyses accounting for time between enrollment and diagnosis, race, tumor subtype, and secondhand smoke exposure. Although results need to be confirmed in additional prospective studies, differential methylation in , as measured in blood, is a promising marker of bladder cancer susceptibility. Identification of biomarkers of bladder cancer susceptibility in easily accessible tissues may allow targeting of screening efforts so as to improve bladder cancer prognosis. This is particularly important among women, who tend to have poorer bladder cancer outcomes than men. .
血液中差异的 DNA 甲基化作为膀胱癌易感性的标志物是很有前景的。然而,之前的研究仅使用了诊断后的血液样本,这意味着观察到的关联可能是疾病的标志物,而不是易感性的标志物。在 Women's Health Initiative 队列中,440 例膀胱癌病例(其中包括移行细胞癌(TCC)亚型)和 440 例匹配的无癌症对照者的诊断前血液样本中,使用 Illumina Infinium HumanMethylation450 Bead Array 进行了全基因组甲基化测量。在标准化和探针过滤后,我们使用条件逻辑回归模型来检验 361184 个 CpG 位点的甲基化测量值与膀胱癌风险之间的关联。位于基因 5'UTR/第一外显子内的 CpG 岛中的 cg22748573 位点的甲基化增加与膀胱癌风险降低 82%相关,在调整了种族/民族、吸烟状况、吸烟包年数和白细胞细胞图谱,并考虑到多重检验后(OR = 0.18,q 值 = 0.05)。该结果在考虑到登记和诊断之间的时间、种族、肿瘤亚型和二手烟暴露的敏感性分析中是稳健的。虽然需要在更多的前瞻性研究中进行确认,但血液中 基因的差异甲基化是膀胱癌易感性的一个有前途的标志物。在易于获取的组织中识别膀胱癌易感性的生物标志物,可能会使筛查工作更有针对性,从而改善膀胱癌的预后。这在女性中尤为重要,因为她们的膀胱癌预后往往比男性差。
