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Oxidative response gene polymorphisms and risk of adult brain tumors

机译:氧化反应基因多态性与成人脑瘤的风险

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Oxidative stress is believed to play a key role in tumor formation. Although this mechanism could be especially pertinent for brain tumors given the high oxygen consumption of the brain, very little has been published regarding brain tumor risk with respect to genes mediating oxidative stress. Using data from non-Hispanic whites in a hospital-based case-control study conducted by the National Cancer Institute between 1994 and 1998, we evaluated risk of glioma (n = 362), meningioma (n = 134), and acoustic neuroma (n = 69) compared to noncancer controls (n = 494) with respect to nine single nucleotide polymorphisms from seven genes involved in oxidative stress response (CAT, GPX1, NOS3, PON1, SOD1, SOD2, and SOD3). We observed increased risk of glioma (odds ratio [OR]_(CT/CC) = 1.3; 95% confidence interval [95% CI], 1.0-1.7) and meningioma (OR_(CT/CC) = 1.7; 95% CI, 1.1-2.7) with the C variant of SOD3 rs699473. There was also indication of increased acoustic neuroma risk with the SOD2 rs4880 Ala variant (OR_(CT/CC) = 2.0; 95% CI, 1.0-4.2) and decreased acoustic neuroma risk with the CAT rsl001179 T allele variant (OR_(CT/TT) = 0.6; 95% CI, 0.3-1.0). These relationships persisted when major groups of disease controls were excluded from the analysis. Our results suggest that common variants in the SOD2, SOD3, and CAT genes may influence brain tumor risk.
机译:据信氧化应激在肿瘤形成中起关键作用。尽管鉴于大脑的高氧消耗,这种机制可能与脑肿瘤特别相关,但是关于介导氧化应激的基因对脑肿瘤风险的报道很少。在1994年至1998年间由美国国家癌症研究所进行的一项基于医院的病例对照研究中,使用非西班牙裔白人的数据,我们评估了神经胶质瘤(n = 362),脑膜瘤(n = 134)和听神经瘤(n (69)与非癌症对照(n = 494)相比,涉及来自氧化应激反应的七个基因(CAT,GPX1,NOS3,PON1,SOD1,SOD2和SOD3)的九个单核苷酸多态性。我们观察到脑胶质瘤(比值[OR] _(CT / CC)= 1.3; 95%置信区间[95%CI],1.0-1.7)和脑膜瘤(OR_(CT / CC)= 1.7; 95%CI)的风险增加(1.1-2.7),以及SOD3 rs699473的C变体。也有迹象表明SOD2 rs4880 Ala变体会增加听觉神经瘤的风险(OR_(CT / CC)= 2.0; 95%CI,1.0-4.2),而CAT rsl001179 T等位基因变体会降低听觉神经瘤的风险(OR_(CT / TT)= 0.6; 95%CI,0.3-1.0)。当从分析中排除主要疾病控制组时,这些关系仍然存在。我们的结果表明,SOD2,SOD3和CAT基因中的常见变异可能会影响脑瘤风险。

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