联合癌症研究联盟中昼夜节律基因的遗传变异与前列腺癌及其他三个癌症部位的风险
Inherited variation in circadian rhythm genes and risks of prostate cancer and three other cancer sites in combined cancer consortia.
作者信息
Gu Fangyi, Zhang Han, Hyland Paula L, Berndt Sonja, Gapstur Susan M, Wheeler William, Ellipse Consortium The, Amos Christopher I, Bezieau Stephane, Bickeböller Heike, Brenner Hermann, Brennan Paul, Chang-Claude Jenny, Conti David V, Doherty Jennifer Anne, Gruber Stephen B, Harrison Tabitha A, Hayes Richard B, Hoffmeister Michael, Houlston Richard S, Hung Rayjean J, Jenkins Mark A, Kraft Peter, Lawrenson Kate, McKay James, Markt Sarah, Mucci Lorelei, Phelan Catherine M, Qu Conghui, Risch Angela, Rossing Mary Anne, Wichmann H-Erich, Shi Jianxin, Schernhammer Eva, Yu Kai, Landi Maria Teresa, Caporaso Neil E
机构信息
Division of Cancer Epidemiology and Genetics, National Cancer Institute, Rockville, MD.
Department of Cancer Prevention and Control, Roswell Park Cancer Institute, Buffalo, NY.
出版信息
Int J Cancer. 2017 Nov 1;141(9):1794-1802. doi: 10.1002/ijc.30883. Epub 2017 Jul 29.
Circadian disruption has been linked to carcinogenesis in animal models, but the evidence in humans is inconclusive. Genetic variation in circadian rhythm genes provides a tool to investigate such associations. We examined associations of genetic variation in nine core circadian rhythm genes and six melatonin pathway genes with risk of colorectal, lung, ovarian and prostate cancers using data from the Genetic Associations and Mechanisms in Oncology (GAME-ON) network. The major results for prostate cancer were replicated in the Prostate, Lung, Colorectal and Ovarian (PLCO) cancer screening trial, and for colorectal cancer in the Genetics and Epidemiology of Colorectal Cancer Consortium (GECCO). The total number of cancer cases and controls was 15,838/18,159 for colorectal, 14,818/14,227 for prostate, 12,537/17,285 for lung and 4,369/9,123 for ovary. For each cancer site, we conducted gene-based and pathway-based analyses by applying the summary-based Adaptive Rank Truncated Product method (sARTP) on the summary association statistics for each SNP within the candidate gene regions. Aggregate genetic variation in circadian rhythm and melatonin pathways were significantly associated with the risk of prostate cancer in data combining GAME-ON and PLCO, after Bonferroni correction (p < 0.00625). The two most significant genes were NPAS2 (p = 0.0062) and AANAT (p = 0.00078); the latter being significant after Bonferroni correction. For colorectal cancer, we observed a suggestive association with the circadian rhythm pathway in GAME-ON (p = 0.021); this association was not confirmed in GECCO (p = 0.76) or the combined data (p = 0.17). No significant association was observed for ovarian and lung cancer. These findings support a potential role for circadian rhythm and melatonin pathways in prostate carcinogenesis. Further functional studies are needed to better understand the underlying biologic mechanisms.
昼夜节律紊乱在动物模型中已被证明与致癌作用有关,但在人类中的证据尚无定论。昼夜节律基因的遗传变异为研究此类关联提供了一种工具。我们使用肿瘤学中的遗传关联和机制(GAME-ON)网络的数据,研究了9个核心昼夜节律基因和6个褪黑素途径基因的遗传变异与结直肠癌、肺癌、卵巢癌和前列腺癌风险之间的关联。前列腺癌的主要研究结果在前列腺、肺、结肠直肠和卵巢(PLCO)癌症筛查试验中得到重复,结直肠癌的研究结果在结直肠癌联盟(GECCO)的遗传学和流行病学研究中得到重复。结直肠癌的癌症病例和对照总数分别为15838/18159,前列腺癌为14818/14227,肺癌为12537/17285,卵巢癌为4369/9123。对于每个癌症部位,我们通过对候选基因区域内每个SNP的汇总关联统计应用基于汇总的自适应秩截尾乘积法(sARTP),进行了基于基因和基于途径的分析。在结合GAME-ON和PLCO的数据中,经过Bonferroni校正后(p < 0.00625),昼夜节律和褪黑素途径中的总体遗传变异与前列腺癌风险显著相关。两个最显著的基因是NPAS2(p = 0.0062)和AANAT(p = 0.00078);后者在Bonferroni校正后具有显著性。对于结直肠癌,我们在GAME-ON中观察到与昼夜节律途径存在提示性关联(p = 0.021);在GECCO(p = 0.76)或合并数据(p = 0.17)中未证实这种关联。卵巢癌和肺癌未观察到显著关联。这些发现支持了昼夜节律和褪黑素途径在前列腺癌发生中的潜在作用。需要进一步的功能研究以更好地理解潜在的生物学机制。
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