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Mechanisms of Breast Cancer in Shift Workers: DNA Methylation in Five Core Circadian Genes in Nurses Working Night Shifts

机译:轮班工人的乳腺癌机制:夜班护士的五个核心生物钟基因中的DNA甲基化

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摘要

Shift work has been suggested to be associated with breast cancer risk, and circadian disruption in shift workers is hypothesized as one of the mechanisms of increased cancer risk. There is, however, insufficient molecular evidence supporting this hypothesis. Using the quantitative methodology of pyrosequencing, epigenetic changes in 5-methyl cytosine (5mC) in five circadian genes CLOCK, BMAL1, CRY1, PER1 and PER2 in female nurses working night shift work (278 breast cancer cases, 280 controls) were analyzed. In breast cancer cases, a medium exposure to night work was associated with increased methylation levels of the CLOCK (p=0.050), BMAL1 (p=0.001) and CRY1 (p=0.040) genes, compared with controls. Within the cases, analysis of the effects of shift work on the methylation patterns showed that methylation of CRY1 was lower in those who had worked night shift and had a high exposure (p=0.006) compared with cases that had worked only days. For cases with a medium exposure to night work, an increase in BMAL1 (p=0.003) and PER1 (p=0.035) methylation was observed compared with day working (unexposed) cases. The methylation levels of the five core circadian genes were also analyzed in relation to the estrogen and progesterone receptors status of the tumors in the cases, and no correlations were observed. Furthermore, nineteen polymorphisms in the five circadian genes were assessed for their effects on the methylation levels of the respective genes, but no associations were found. In summary, our data suggest that epigenetic regulation of CLOCK, BMAL1, CRY1 and PER1 may contribute to breast cancer in shift workers.
机译:轮班工作已被证明与患乳腺癌的风险有关,而轮班工作人员的昼夜节律紊乱被认为是增加患癌风险的机制之一。但是,没有足够的分子证据支持这一假设。使用焦磷酸测序的定量方法,分析了夜班工作的女护士(278名乳腺癌病例,280名对照)中五个昼夜节律基因CLOCK,BMAL1,CRY1,PER1和PER2中5-甲基胞嘧啶(5mC)的表观遗传变化。与对照相比,在乳腺癌病例中,夜间工作的中等程度暴露与CLOCK(p = 0.050),BMAL1(p = 0.001)和CRY1(p = 0.040)基因的甲基化水平升高有关。在这些病例中,对轮班工作对甲基化模式的影响的分析表明,与仅工作数天的病例相比,夜班工作且暴露量较高的患者中CRY1的甲基化程度较低(p = 0.006)。对于夜班中度暴露的病例,与白天(未暴露)的病例相比,观察到BMAL1(p = 0.003)和PER1(p = 0.035)的甲基化增加。还分析了与病例中肿瘤的雌激素和孕激素受体状态相关的五个核心昼夜节律基因的甲基化水平,未发现相关性。此外,评估了五个昼夜节律基因中的十九个多态性对各自基因甲基化水平的影响,但未发现关联。总之,我们的数据表明,CLOCK,BMAL1,CRY1和PER1的表观遗传调控可能会导致轮班工作人员患乳腺癌。

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