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Admixture Mapping Identifies a Quantitative Trait Locus Associated with FEV1/FVC in the COPDGene Study

机译:混合映射确定了COPD基因研究中与FEV1 / FVC相关的定量性状基因座

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摘要

African Americans are admixed with genetic contributions from European and African ancestral populations. Admixture mapping leverages this information to map genes influencing differential disease risk across populations. We performed admixture and association mapping in 3,300 African American current or former smokers from the COPDGene Study. We analyzed estimated local ancestry and SNP genotype information to identify regions associated with FEV1/FVC, the ratio of forced expiratory volume in one second to forced vital capacity, measured by spirometry performed after bronchodilator administration. Global African ancestry inversely associated with FEV1/FVC (P = 0.035). Genome-wide admixture analysis, controlling for age, gender, body mass index, current smoking status, pack-years smoked, and four principal components summarizing the genetic background of African Americans in the COPDGene Study, identified a region on chromosome 12q14.1 associated with FEV1/FVC (P = 2.1 x 10(-6)) when regressed on local ancestry. Allelic association in this region of chromosome 12 identified an intronic variant in FAM19A2 (rs348644) as associated with FEV1/FVC (P = 1.76 x 10(-6)). By combining admixture and association mapping, a marker on chromosome 12q14.1 was identified as being associated with reduced FEV1/FVC ratio among African Americans in the COPDGene Study.
机译:非裔美国人与欧洲和非洲祖先群体的遗传贡献混在一起。混合作图利用此信息来对影响人群间不同疾病风险的基因作图。我们对3,300名来自COPDGene研究的非裔美国人现时或以前的吸烟者进行了混合和关联作图。我们分析了估计的本地血统和SNP基因型信息,以识别与FEV1 / FVC相关的区域,即一秒钟用力呼气量与用力肺活量的比值,这是通过在支气管扩张剂给药后进行的肺活量测定来测量的。全球非洲血统与FEV1 / FVC呈负相关(P = 0.035)。全基因组混合分析,控制年龄,性别,体重指数,当前吸烟状况,吸烟年数以及在COPDGene研究中概述非裔美国人遗传背景的四个主要成分,确定了与染色体12q14.1相关的区域在本地血统上回归时使用FEV1 / FVC(P = 2.1 x 10(-6))。在12号染色体此区域的等位基因关联确定FAM19A2(rs348644)中的一个内含子变异体与FEV1 / FVC相关(P = 1.76 x 10(-6))。通过混合和关联映射,在COPDGene研究中,染色体12q14.1上的标记被鉴定为与非洲裔美国人FEV1 / FVC比率降低相关。

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