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The Relationship Between Environmental Exposure and Genetic Architecture of the 2q33 Locus With Esophageal Cancer in South Africa

机译:南非食管癌2q33基因座环境暴露与遗传结构的关系

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摘要

Esophageal squamous cell carcinoma (ESCC) has a high prevalence in several countries in Africa and Asia. Previous genome-wide association studies (GWAS) in Chinese populations have identified several ESCC susceptibility loci, including variants on chromosome 2q33 and 6p21, but the contribution of these loci to risk in African populations is unknown. In this study we tested the association of 10 genetic variants at these two risk loci on susceptibility to ESCC in two South African ethnic groups. Variants at 2q33 (rs3769823, rs10931936, rs13016963, rs7578456, rs2244438) and 6p21 (rs911178, rs3763338, rs2844695, rs17533090, rs1536501) were genotyped in a set of Black Xhosa (463 cases and 480 controls) and Mixed Ancestry (269 cases and 288 controls) individuals. Genotyping was performed using TaqMan allelic discrimination assays. The Pearson’s chi-squared test was used to compare the allele frequency between cases and controls. Gene-environment interactions with tobacco smoking and alcohol consumption were investigated in a case-control analysis. A logistic regression analysis was further performed to elucidate the independent effect of each association signal on the risk of ESCC. The 2q33 variants rs10931936, rs7578456, and rs2244438 were marginally associated with higher risk of ESCC in the Mixed Ancestry population (ORs = 1.39–1.58, p ≤ 0.035), of which rs7578456 and rs2244438 remained significant after multiple correction (p < 0.005). The associations with rs7578456 and rs2244438 were also observed across strata of tobacco smoking (ORs = 1.47–2.75, p ≤ 0.035) and alcohol consumption (ORs = 1.45–2.06, p ≤ 0.085) status. However, only the association with rs2244438, which lies within an exon of TRAK2, remained significant after adjustment for the other variants in the region. Interestingly, none of the variants tested were significantly associated with ESCC in the Black South African population. These finding implicate TRAK2 as a casual gene for ESCC risk in the Mixed Ancestry population of South Africa and confirm prior evidence of population-specific differences in the genetic contribution to ESCC, which may reflect differences in genetic architecture and environmental exposure across ethnic groups.
机译:食道鳞状细胞癌(ESCC)在非洲和亚洲的几个国家中普遍流行。先前在中国人群中进行的全基因组关联研究(GWAS)已经确定了几个ESCC易感基因座,包括2q33和6p21染色体上的变异体,但是这些基因座对非洲人群的风险的贡献尚不清楚。在这项研究中,我们测试了两个南非族裔人群中这两个风险基因座上10个遗传变异对ESCC易感性的关联。在一组黑色Xhosa(463例和480例(480例)和288例(603例和288例)混合先祖中对2q33(rs3769823,rs10931936,rs13016963,rs7578456,rs2244438)和6p21(rs911178,rs3763338,rs2844695,rs17533090,rs1536501)的变体进行基因分型。控制)个人。使用TaqMan等位基因鉴别测定法进行基因分型。皮尔逊(Pearson)卡方检验用于比较病例与对照组之间的等位基因频率。在病例对照分析中,研究了基因环境与吸烟和饮酒的相互作用。进一步进行逻辑回归分析,以阐明每种关联信号对ESCC风险的独立影响。 2q33的rs10931936,rs7578456和rs2244438变异与混合祖先人群的ESCC风险较高相关(OR = 1.39–1.58,p≤0.035),其中rs7578456和rs2244438在多次校正后仍显着(p <0.005)。在吸烟(OR = 1.47–2.75,p≤0.035)和饮酒(OR = 1.45–2.06,p≤0.085)状态的各个阶层中也观察到与rs7578456和rs2244438的关联。但是,在调整了该区域的其他变体之后,只有与位于TRAK2外显子内的rs2244438的关联才保持显着。有趣的是,在南非黑人中,测试的变异均未与ESCC显着相关。这些发现暗示了TRAK2作为南非混合祖先人群ESCC风险的偶然基因,并证实了对ESCC的遗传贡献存在特定于人群的差异的先前证据,这可能反映了种族之间遗传结构和环境暴露的差异。

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