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首页> 外文期刊>Urologic oncology >Despite the lack of association between different genotypes and the presence of prostate cancer, endothelial nitric oxide synthase a/b (eNOS4a/b) polymorphism may be associated with advanced clinical stage and bone metastasis.
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Despite the lack of association between different genotypes and the presence of prostate cancer, endothelial nitric oxide synthase a/b (eNOS4a/b) polymorphism may be associated with advanced clinical stage and bone metastasis.

机译:尽管缺乏不同基因型之间的关联以及存在前列腺癌,但内皮一氧化氮合酶a / b(eNOS4a / b)多态性可能与晚期临床阶段和骨转移有关。

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摘要

OBJECTIVES: To investigate the relationship between the distribution of endothelial NO synthase (eNOS4a/b) gene polymorphism and clinical features of prostate cancer (PCa). METHODS AND MATERIALS: One hundred thirty-two patients with PCa (mean age 64.10 +/- 7.23 years) and 158 healthy controls (mean age 62.50 +/- 7.53 years) with normal serum total prostate specific antigen (PSA) levels (<4 ng/ml) and digital rectal examinations (DRE) were enrolled in this prospectively designed study. PCa patients were classified as clinical T1 and T2 stages (Group 1), clinical T3 and T4 stages without bone metastasis (Group 2), and patients with bone metastasis (Group 3). Genotypes (aa, bb, ab) for eNOS4a/b gene polymorphisms were identified by polymerase chain reaction analysis. Meanwhile, plasma nitrate and nitrite levels (NO(x)) were used to estimate the amounts of endogenous NO formation for both groups of patients. RESULTS: Despite lack of statistically significant differences between PCa patients and the control group in terms of distribution of genotypes and frequency of alleles, plasma NO(x) levels were found to be significantly increased in PCa patients compared with controls. Meanwhile, there was no significant difference between the group of PCa patients with high and low grade tumors (Gleason score >/= 7 vs. < 7) in terms of genotype (aa + ab genotypes or a-allele vs. bb genotype) distribution. However, bb genotype was observed to be present at a higher frequency (85.1% vs. 60%) in Group 1; whereas a-allele was more frequent in Group 2 (13.3% vs. 5.7%) and Group 3 (26.7 vs. 9.2). In addition, patients with a-allele had a 3.79-fold risk of having advanced disease and bone metastasis in comparison with bb genotype. Moreover, multivariable logistic regression analysis revealed that eNOS4a/b polymorphism and plasma NOx levels were predictive factors for developing bone metastasis and high stage disease after adjustment for age and BMI. CONCLUSIONS: Our data did not reveal any relationship between any of these genotypes and the presence of PCa. However, the finding that PCa patients with bb genotype generally manifest localized disease and develop bone metastasis less frequently in comparison patients with a-allele may indicate an important role for this polymorphism in the molecular pathophysiology of PCa.
机译:目的:探讨内皮NO合酶(eNOS4a / b)基因多态性的分布与前列腺癌(PCa)临床特征的关系。方法和材料:132例PCa(平均年龄64.10 +/- 7.23岁)和158名健康对照(平均年龄62.50 +/- 7.53岁)的血清前列腺总特异性抗原(PSA)正常(<4) ng / ml)和直肠指检(DRE)参与了这项前瞻性设计研究。 PCa患者分为临床T1和T2期(第1组),无骨转移的临床T3和T4期(第2组)和有骨转移的患者(第3组)。通过聚合酶链反应分析确定了eNOS4a / b基因多态性的基因型(aa,bb,ab)。同时,血浆硝酸盐和亚硝酸盐水平(NO(x))用于估计两组患者的内源性NO形成量。结果:尽管在基因型分布和等位基因频率方面,PCa患者和对照组之间在统计学上没有显着差异,但发现PCa患者的血浆NO(x)水平与对照组相比显着增加。同时,就基因型(aa + ab基因型或a-等位基因vs. bb基因型)分布而言,患有高低度肿瘤的PCa患者组(格里森评分> / = 7 vs. <7)之间没有显着差异。 。但是,在第1组中,发现bb基因型的出现频率更高(85.1%比60%)。第2组(13.3%vs. 5.7%)和第3组(26.7 vs. 9.2)中a等位基因更为常见。此外,与bb基因型相比,a等位基因患者罹患晚期疾病和骨转移的风险高3.79倍。此外,多因素logistic回归分析显示,eNOS4a / b基因多态性和血浆NOx水平是在调整年龄和BMI后发展骨转移和晚期疾病的预测因素。结论:我们的数据没有揭示这些基因型与PCa的存在之间的任何关系。然而,与a等位基因相比,具有bb基因型的PCa患者通常表现出局部疾病并且较少发生骨转移的发现可能表明这种多态性在PCa的分子病理生理中具有重要作用。

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