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Association of IL-10 polymorphisms with prostate cancer risk and grade of disease.

机译:IL-10多态性与前列腺癌风险和疾病等级的关联。

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Animal and in vitro models of prostate cancer demonstrate high IL-10 levels result in smaller tumors, fewer metastases, and reduced angiogenesis compared to controls. We sought to examine the hypothesis that genotypes correlated with low IL-10 production may be associated with increased prostate cancer risk among Finnish male participants from the Alpha-tocopherol Beta-carotene Cancer Prevention Study. DNA from 584 prostate cancer cases and 584 controls was genotyped for four IL-10 alleles, -1082, -819, -592, and 210. DNA from more of the controls than cases failed to amplify, resulting in 509 cases and 382 controls with genotype data for -1082; 507 and 384 for -819; 511 and 386 for -592; and 491 and 362 for 210. Odds ratios for the association between the IL-10 genotypes and risk of prostate cancer or, among cases only, high-grade disease were calculated using logistic regression. In this population, the -819 TT and -592 AA low expression genotypes were highly correlated. These two genotypes also wereassociated with increased prostate cancer susceptibility (OR = 1.92, 95% CI 1.07-3.43 for -819) and, among cases, with high-grade tumors (OR = 2.56, 95% CI 1.26-5.20 for -819). These data demonstrate genotypes correlated with low IL-10 production are associated with increased risk of prostate cancer and with high-grade disease in this population.
机译:前列腺癌的动物模型和体外模型显示,与对照组相比,高IL-10水平可导致较小的肿瘤,较少的转移并减少血管生成。我们试图检验一种假设,即与低IL-10产生量相关的基因型可能与阿尔法-生育酚-β-胡萝卜素癌症预防研究中的芬兰男性参与者中增加的前列腺癌风险相关。对来自584个前列腺癌病例和584个对照的DNA进行了四个IL-10等位基因-1082,-819,-592和210的基因分型。来自更多对照的DNA未能扩增,导致509例和382个对照被扩增。 -1082的基因型数据; 507和384表示-819; 511和386表示-592;对于210,则分别为491和362。IL-10基因型与前列腺癌或仅在某些情况下为高病的风险之间的关联的几率使用对数回归进行了计算。在该人群中,-819 TT和-592 AA低表达基因型高度相关。这两种基因型还与增加的前列腺癌易感性相关(OR = 1.92,-819的OR为1.92,95%CI 1.07-3.43),在某些情况下还与高级别肿瘤相关(OR = 2.56,-819的OR为2.56,95%CI 1.26-5.20)。 。这些数据表明,与低IL-10产生量相关的基因型与该人群中前列腺癌的风险增加和高度疾病相关。

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