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首页> 外文期刊>International Journal of Cancer =: Journal International du Cancer >Angiogenesis genes, dietary oxidative balance and breast cancer risk and progressions The Breast Cancer Health Disparities Study
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Angiogenesis genes, dietary oxidative balance and breast cancer risk and progressions The Breast Cancer Health Disparities Study

机译:血管生成基因,饮食中的氧化平衡以及乳腺癌的风险和进展乳腺癌健康差异研究

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Angiogenesis is essential for tumor development and progression. Genetic variation in angiogenesis-related genes may influence breast carcinogenesis. We evaluated dietary factors associated with oxidative balance, DDIT4 (one SNP), FLT1 (35 SNPs), HIF1A (four SNPs), KDR (19 SNPs), MPO (one SNP), NOS2A (15 SNPs), TEK (40 SNPs) and VEGFA (eight SNPs) and breast cancer risk among Hispanic (2,111 cases and 2,597 controls) and non-Hispanic white (1,481 cases and 1,586 controls) women in the Breast Cancer Health Disparities Study, Adaptive rank truncated product (ARTP) analysis was used to determine gene and pathway significance with breast cancer. TEK was associated with breast cancer overall (pARTP = 0.03) and with breast cancer survival (partp = 0.01). KDR was of borderline significance overall (pARTP = 0,07), although significantly associated with breast cancer in both low and intermediate Native American (NA) ancestry groups (pARTP = 0.02) and estrogen receptor (ER)+/proges-terone receptor (PR)- tumor phenotype (pARTP = 0.008). Both VEGFA and NOS2A were associated with ER-/PR- tumor pheno-type (pARTP = 0.01 and (pARTP = 0.04, respectively). FLTl was associated with breast cancer survival among those with low NA ancestry (pARTP =0.009). With respect to diet, having a higher dietary oxidative balance score (DOBS) was significantly associated with lower breast cancer risk [odds ratio (OR) 0.74, 95% confidence interval (CI) 0.64-0.84], with the strongest associations observed for women with the highest NA ancestry (OR 0.44, 95% CI 0.30-0.65). We observed few interactions between DOBS and angiogenesis-reiated genes. Our data suggest that dietary factors and genetic variation in angiogenesis-related genes contribute to breast cancer carcinogenesis.
机译:血管生成对于肿瘤的发展和进展至关重要。血管生成相关基因的遗传变异可能影响乳腺癌的发生。我们评估了与氧化平衡,DDIT4(一个SNP),FLT1(35个SNP),HIF1A(四个SNP),KDR(19个SNP),MPO(一个SNP),NOS2A(15个SNP),TEK(40个SNP)相关的饮食因素。乳腺癌健康差异研究中使用西班牙裔(2,111例和2,597例对照)和非西班牙裔白人(1,481例和1,586例对照)的女性和VEGFA(八种SNP)和乳腺癌风险,采用了适应性截短乘积(ARTP)分析确定乳腺癌的基因和途径意义。 TEK与乳腺癌总体(pARTP = 0.03)和乳腺癌生存率(partp = 0.01)有关。 KDR总体上具有临界意义(pARTP = 0,07),尽管在中低美洲原住民(NA)血统(pARTP = 0.02)和雌激素受体(ER)+ / proges-terone受体( PR)-肿瘤表型(pARTP = 0.008)。 VEGFA和NOS2A均与ER- / PR-肿瘤表型有关(分别为pARTP = 0.01和(pARTP = 0.04)。FLT1与低NA血统的患者(pARTP = 0.009)相关。饮食中,较高的饮食氧化平衡评分(DOBS)与较低的乳腺癌风险显着相关[比值比(OR)0.74,95%置信区间(CI)0.64-0.84],并且观察到的女性与女性之间的关联性最强NA祖先最高(OR 0.44,95%CI 0.30-0.65)我们观察到DOBS与血管生成相关基因之间的相互作用极少,我们的数据表明饮食因素和血管生成相关基因的遗传变异有助于乳腺癌的癌变。

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