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Polymorphisms in inflammatory genes, plasma antioxidants, and prostate cancer risk.

机译:炎症基因,血浆抗氧化剂和前列腺癌的风险多态性。

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BACKGROUND: Presence of xenotropic murine leukemia virus-related virus and chronic inflammation in prostate tumor suggests that inflammation plays a role in prostate cancer etiology. This study investigated whether variants in inflammatory genes act alone or interact with plasma antioxidants to influence prostate cancer risk in a population-based case-control study in Central Arkansas. METHODS: Cases (n = 193) were men, aged 40-80, diagnosed with prostate cancer in three major hospitals in 1998-2003, and controls (n = 197) were matched to cases by age, race, and county of residence. RESULTS: After adjustment for confounders, polymorphisms in COX-2 (rs689466) and IL-8 (rs4073) were not significantly associated with prostate cancer risk. However, apparent interactions were observed between these genetic variants and plasma antioxidants on the risk of this malignancy. The protective effect of the mutant allele of the COX-2 polymorphism was more pronounced among subjects with high plasma levels of beta-cryptoxanthin, lycopene, beta-carotene, or selenium (>or=median) [e.g., OR (95% CI): 0.37 (0.15, 0.86) (AG/GG vs. AA) for beta-cryptoxanthin]. Conversely, the promoting effect of the variant allele of the IL-8 polymorphism was more remarkable in subjects with low plasma levels of Lutein/zeaxanthin, beta-cryptoxanthin, and beta-carotene (
机译:背景:异种鼠白血病病毒相关病毒的存在和前列腺肿瘤的慢性炎症提示炎症在前列腺癌的病因中起作用。这项研究在阿肯色州中部一项基于人群的病例对照研究中,调查了炎症基因的变异是单独起作用还是与血浆抗氧化剂相互作用,从而影响前列腺癌的风险。方法:病例(n = 193)是男性,年龄在40-80岁,在1998-2003年间在三家主要医院中被诊断出患有前列腺癌,对照组(n = 197)按年龄,种族和居住县匹配。结果:调整混杂因素后,COX-2(rs689466)和IL-8(rs4073)的多态性与前列腺癌风险没有显着相关。但是,观察到这些遗传变异与血浆抗氧化剂之间存在明显的相互作用,从而具有这种恶性肿瘤的风险。在血浆中高浓度的β-隐黄质,番茄红素,β-胡萝卜素或硒(>或=中位数)[例如,OR(中位数为95%) :β-隐黄质:0.37(0.15,0.86)(AG / GG vs.AA)。相反,在血浆叶黄素/玉米黄质,β-隐黄质和β-胡萝卜素(<中值)[例如,OR(95%CI) :β-胡萝卜素为2.44(1.08,5.75)(AT / TT对AA)。结论:我们发现炎症基因的序列变异体与血浆抗氧化剂相互作用,调节前列腺癌的风险。

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