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首页> 外文期刊>Cancer epidemiology, biomarkers and prevention: A publication of the American Association for Cancer Research >Variants in the prostate-specific antigen (PSA) gene and prostate cancer risk, survival, and circulating PSA.
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Variants in the prostate-specific antigen (PSA) gene and prostate cancer risk, survival, and circulating PSA.

机译:前列腺特异性抗原(PSA)基因的变异以及前列腺癌的风险,存活率和循环PSA。

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An A to G substitution, rs925013, in the promoter of the prostate-specific antigen gene (PSA) was recently found to be associated with promoter activity and circulating PSA levels. The objective of this study was to test the associations between rs925013 and another A to G substitution, rs266882, in the PSA gene with prostate cancer risk using a population-based case-control study of 821 prostate cancer cases and 734 controls carried out in Perth and Melbourne, Australia. The study focused on young (i.e., < 70 years) and aggressive cases (i.e., well-differentiated tumors were excluded). Cases in the Melbourne arm of the study (N = 638) were followed up prospectively for an average period of 8.2 years and deaths from prostate cancer ascertained through record linkage to study the possible association between genetic variants and disease-specific survival. PSA-circulating levels were measured in controls to test the association with the genetic variants using a cross-sectional design. Linear regression of log PSA levels, unconditional logistic regression, Cox regression, and haplotype analyses were undertaken. For rs925013, the G allele was associated with an increased risk of prostate cancer [odds ratio, 1.4; 95% confidence interval (95% CI), 1.1-1.7; P = 0.001], and the hazard ratio for survival for cases homozygous for the G allele compared with cases homozygous for the A allele was increased but not statistically significant (hazard ratio, 2.3; 95% CI, 1-5.6; P = 0.06). For rs266882, there was no association with overall prostate cancer risk and survival (all P > 0.1). Men homozygous or heterozygous for the G/G (rs925013/rs266882) haplotype were at higher risk of prostate cancer than men homozygous for the A/A haplotype (odds ratio, 1.3; 95% CI, 1.1-1.7; P = 0.009). Adjusted geometric means of circulating PSA levels in controls were similar in men with zero, one, and two copies of the G allele in rs266882 (1.2, 1.1, and 1.3 ng/mL, respectively; all P > or = 0.2) and rs925013 (1.1, 1.2, and 1.5 ng/mL, respectively; all P > 0.1). For rs925013, our study provides good evidence of association with prostate cancer risk, marginal evidence of association with survival, and little evidence of detectable association with circulating PSA levels in controls. We found no evidence of an independent association between rs266882 and any of the outcomes. The genotypes and haplotypes studied might be associated with the PSA gene function or be in linkage disequilibrium with other unmeasured and functional variants in the PSA or other genes.
机译:最近发现,前列腺特异性抗原基因(PSA)启动子中的A至G取代rs925013与启动子活性和循环PSA水平相关。这项研究的目的是使用一项基于人群的821例前列腺癌病例和734例对照的病例对照研究,检验PSA基因中具有前列腺癌风险的rs925013与另一种A到G替代rs266882之间的关联。和澳大利亚墨尔本。该研究集中在年轻(即70岁以下)和侵袭性病例(即高分化肿瘤除外)上。对墨尔本研究部门的病例(N = 638)进行了平均8.2年的前瞻性随访,并通过记录联系确定了前列腺癌的死亡病例,以研究遗传变异与疾病特异性生存之间的可能联系。在对照中测量PSA循环水平,以使用横断面设计测试与遗传变异的关联。进行log PSA水平的线性回归,无条件logistic回归,Cox回归和单倍型分析。对于rs925013,G等位基因与前列腺癌的风险增加相关[比值比为1.4; 95%置信区间(95%CI),1.1-1.7; P = 0.001],与G等位基因纯合的病例相比,G等位基因纯合的病例生存风险比增加,但无统计学意义(危险比,2.3; 95%CI,1-5.6; P = 0.06) 。对于rs266882,与总体前列腺癌风险和生存率无关(所有P> 0.1)。 G / G(rs925013 / rs266882)单倍型纯合子或杂合子的男性患前列腺癌的风险高于A / A单倍型纯合子的男性(奇数比,1.3; 95%CI,1.1-1.7; P = 0.009)。 rs266882(分别为1.2、1.1和1.3 ng / mL;所有P>或= 0.2)和rs925013(分别为1.2、1.1和1.3 ng / mL; G等位基因分别为零,一和两个副本)的男性中,调整后的循环PSA水平的几何平均值相似。分别为1.1、1.2和1.5 ng / mL;所有P> 0.1)。对于rs925013,我们的研究提供了与前列腺癌风险相关的良好证据,与生存相关的边缘证据,以及与对照中循环PSA水平可检测到的相关证据很少。我们没有发现rs266882与任何结果之间存在独立关联的证据。研究的基因型和单倍型可能与PSA基因的功能有关,或者与PSA或其他基因中其他未测及功能性变体连锁不平衡。

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