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GWAS of five gynecologic diseases and cross-trait analysis in Japanese

机译:五种妇科疾病的GWA和日语交叉特征分析

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摘要

We performed genome-wide association studies of five gynecologic diseases using data of 46,837 subjects (5236 uterine fibroid, 645 endometriosis, 647 ovarian cancer (OC), 909 uterine endometrial cancer (UEC), and 538 uterine cervical cancer (UCC) cases allowing overlaps, and 39,556 shared female controls) from Biobank Japan Project. We used the population-specific imputation reference panel (n = 3541), yielding 7,645,193 imputed variants. Analyses performed under logistic model, linear mixed model, and model incorporating correlations identified nine significant associations with three gynecologic diseases including four novel findings (rs79219469:C > T, LINC02183, P = 3.3 x 10(-8) and rs567534295: C > T, BRCA1, P = 3.1 x 10(-8) with OC, rs150806792:C > T, INS-IGF2, P = 4.9 x 10(-8) and rs140991990:A > G, SOX9, P = 3.3 x 10(-8) with UCC). Random-effect meta-analysis of the five GWASs correcting for the overlapping subjects suggested one novel shared risk locus (rs937380553:A > G, LOC730100, P = 2.0 x 10(-8)). Reverse regression analysis identified three additional novel associations (rs73494486:C > T, GABBR2, P = 4.8 x 10(-8), rs145152209:A > G, SH3GL3/BNC1, P = 3.3 x 10(-8), and rs147427629:G > A, LOC107985484, P = 3.8 x 10(-8)). Estimated heritability ranged from 0.026 for OC to 0.220 for endometriosis. Genetic correlations were relatively strong between OC and UEC, endometriosis and OC, and uterine fibroid and OC (r(g) > 0.79) compared with relatively weak correlations between UCC and the other four (rg = -0.08 similar to 0.25). We successfully identified genetic associations with gynecologic diseases in the Japanese population. Shared genetic effects among multiple related diseases may help understanding the pathophysiology.
机译:我们使用46,837个受试者的数据进行了全基因组关联研究(5236子宫肌瘤,645个子宫内膜异位症,647个卵巢癌(OC),909例子宫内膜癌(UEC)和538例宫颈癌(UCC)病例,允许重叠来自Biobank Japan项目的39,556个共同的女性控制。我们使用了人口特定的撤销参考面板(n = 3541),产生了7,645,193级障碍。在逻辑模型,线性混合模型和模型中进行的分析和结合相关性鉴定了九个重要关联,其中九种妇科疾病包括四种新发现(RS79219469:C> T,LINC02183,P = 3.3×10(-8)和RS567534295:C> T ,BRCA1,P = 3.1 x 10(-8)带OC,RS150806792:C> T,INS-IGF2,P = 4.9 x 10(-8)和RS140991990:A> G,SOX9,P = 3.3 x 10( - 8)与UCC)。随机效应元分析重叠主题的五个Gwass校正建议了一部新颖的共享风险基因座(RS937380553:A> G,LOC730100,P = 2.0 x 10(-8))。反向回归分析确定了三个额外的新型关联(RS73494486:C> T,GABBR2,P = 4.8×10(-8),RS145152209:A> G,SH3GL3 / BNC1,P = 3.3×10(-8),以及RS147427629: G> A,LOM107985484,P = 3.8 x 10(-8))。估计遗传性为子宫内膜异位症的OC至0.220的0.026。与UEC,子宫内膜异位症和OC之间的遗传相关性相对较强,与UCC和其他四个(RG = -0.08类似的相似的相关性,子宫肌瘤和OC(R(g)> 0.79)。我们成功地将遗传学协会与日本人口中的妇科疾病进行了鉴定。多种相关疾病之间的共同遗传效应可能有助于理解病理生理学。

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  • 作者单位

    Osaka Univ Dept Stat Genet Grad Sch Med Suita Osaka 5650871 Japan;

    RIKEN Lab Stat Anal Ctr Integrat Med Sci Yokohama Kanagawa 2300045 Japan;

    RIKEN Lab Stat Anal Ctr Integrat Med Sci Yokohama Kanagawa 2300045 Japan;

    Univ Tokyo Inst Med Sci Lab Genome Technol Tokyo 1088639 Japan;

    Osaka Univ Dept Obstet &

    Gynecol Grad Sch Med Suita Osaka 5650871 Japan;

    Univ Tokyo Grad Sch Frontier Sci Dept Computat Biol &

    Med Sci Tokyo 1088639 Japan;

    Osaka Univ Dept Obstet &

    Gynecol Grad Sch Med Suita Osaka 5650871 Japan;

    Univ Tokyo Inst Med Sci Div Mol Pathol Tokyo 1088639 Japan;

    RIKEN Ctr Integrat Med Sci Yokohama Kanagawa 2300045 Japan;

    RIKEN Lab Stat Anal Ctr Integrat Med Sci Yokohama Kanagawa 2300045 Japan;

    Osaka Univ Dept Stat Genet Grad Sch Med Suita Osaka 5650871 Japan;

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  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 医学遗传学;
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