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首页> 外文期刊>American Journal of Epidemiology >Comprehensive evaluation of the impact of 14 genetic variants on colorectal cancer phenotype and risk
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Comprehensive evaluation of the impact of 14 genetic variants on colorectal cancer phenotype and risk

机译:综合评估14种遗传变异对大肠癌表型和风险的影响

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摘要

To comprehensively evaluate the impact of recently identified colorectal cancer (CRC) variants at 1q41, 3q26.2, 8q23.3, 8q24.21, 10p14, 11q23.1, 12q13.13, 14q22.2, 15q13.3, 16q22.1, 18q21.1, 19q13.11, 20p12.3, and 20q13.33 on risk and CRC phenotype, the authors analyzed 8,878 cases and 6,051 controls from the United Kingdom ascertained in 1999-2007. The impact of variants on the familial CRC risk was enumerated from age-, sex-, and calendar-specific CRC rates in the 50,924 first-degree relatives of cases. Each of the 14 susceptibility loci independently influences CRC with the risk increasing with increasing number of risk alleles carried (per allele odds ratio = 1.13; P = 2.99 × 10 -58) and, for those within the upper quintile, there is a 2.3-fold increased risk. In first-degree relatives of cases with ≤17, 18-21, and ≥22 risk alleles, standardized incidence ratios were 1.76, 2.08, and 2.25, respectively. Although the discriminatory attributes of the 14 CRC susceptibility loci for individual risk prediction are poor (area under the curve = 0.58), they may allow subgroups of the population at different CRC risks to be distinguished.
机译:要全面评估最近发现的大肠癌(CRC)变异在1q41、3q26.2、8q23.3、8q24.21、10p14、11q23.1、12q13.13、14q22.2、15q13.3、16q22.1的影响,18q21.1、19q13.11、20p12.3和20q13.33的风险和CRC表型,作者分析了1999-2007年来自英国的8,878例病例和6,051例对照。从50,924例一级亲属的年龄,性别和日历特定的CRC率中可以列举出变体对家族性CRC风险的影响。 14个易感基因座中的每个基因座均独立影响CRC,风险随携带的风险等位基因数目的增加而增加(每个等位基因比值比= 1.13; P = 2.99×10 -58),而在上五分位数中,则为2.3-倍增加风险。在风险等位基因≤17、18-21和≥22的一级亲属中,标准发生率分别为1.76、2.08和2.25。尽管14个CRC易感性基因座的个体风险预测的区分性较差(曲线下面积= 0.58),但它们可以区分处于不同CRC风险的人群的亚组。

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