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Editors choice: Replication of Breast Cancer Susceptibility Loci in Whites and African Americans Using a Bayesian Approach

机译:编辑选择:使用贝叶斯方法在白人和非裔美国人中复制乳腺癌易感性基因座

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摘要

Genome-wide association studies (GWAS) and candidate gene analyses have led to the discovery of several dozen genetic polymorphisms associated with breast cancer susceptibility, many of which are considered well-established risk factors for the disease. Despite attempts to replicate these same variant-disease associations in African Americans, the evaluable populations are often too small to produce precise or consistent results. We estimated the associations between 83 previously identified single nucleotide polymorphisms (SNPs) and breast cancer among Carolina Breast Cancer Study (1993–2001) participants using maximum likelihood, Bayesian, and hierarchical methods. The selected SNPs were previous GWAS hits (n = 22), near-hits (n = 19), otherwise well-established risk loci (n = 5), or located in the same genes as selected variants (n = 37). We successfully replicated 18 GWAS-identified SNPs in whites (n = 2,352) and 10 in African Americans (n = 1,447). SNPs in the fibroblast growth factor receptor 2 gene (FGFR2) and the TOC high mobility group box family member 3 gene (TOX3) were strongly associated with breast cancer in both races. SNPs in the mitochondrial ribosomal protein S30 gene (MRPS30), mitogen-activated protein kinase kinase kinase 1 gene (MAP3K1), zinc finger, MIZ-type containing 1 gene (ZMIZ1), and H19, imprinted maternally expressed transcript gene (H19) were associated with breast cancer in whites, and SNPs in the estrogen receptor 1 gene (ESR1) and H19 gene were associated with breast cancer in African Americans. We provide precise and well-informed race-stratified odds ratios for key breast cancer–related SNPs. Our results demonstrate the utility of Bayesian methods in genetic epidemiology and provide support for their application in small, etiologically driven investigations.
机译:全基因组关联研究(GWAS)和候选基因分析已导致发现数​​十种与乳腺癌易感性相关的遗传多态性,其中许多被认为是该疾病的公认危险因素。尽管试图在非裔美国人中复制这些相同的变异疾病关联,但可评估的人群通常太小而无法产生精确或一致的结果。我们使用最大似然,贝叶斯和分层方法,估计了卡罗来纳州乳腺癌研究(1993-2001年)参与者中83个先前确定的单核苷酸多态性(SNP)与乳腺癌之间的关联。选定的SNP为先前的GWAS命中(n = 22),近乎命中(n = 19),否则建立良好的风险基因座(n = 5)或位于与选定变体相同的基因中(n = 37)。我们成功地在白人中复制了18个GWAS鉴定的SNP(n = 2,352),在非洲裔美国人中复制了10个(n = 1,447)。在这两个种族中,成纤维细胞生长因子受体2基因(FGFR2)和TOC高迁移率族框家族成员3基因(TOX3)中的SNP与乳腺癌密切相关。线粒体核糖体蛋白S30基因(MRPS30),有丝分裂原激活的蛋白激酶激酶激酶1基因(MAP3K1),锌指,含有1个基因的MIZ型(ZMIZ1)和H19(印有母亲表达的转录本基因(H19))中的SNP分别为与白人乳腺癌有关,而雌激素受体1基因(ESR1)和H19基因中的SNP与非裔美国人的乳腺癌有关。我们为与乳腺癌相关的主要SNP提供准确且信息灵通的种族分层比值比。我们的结果证明了贝叶斯方法在遗传流行病学中的实用性,并为它们在小型病因驱动的研究中的应用提供了支持。

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