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首页> 外文期刊>Genetics: A Periodical Record of Investigations Bearing on Heredity and Variation >A Large Multiethnic Genome-Wide Association Study of Adult Body Mass Index Identifies Novel Loci
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A Large Multiethnic Genome-Wide Association Study of Adult Body Mass Index Identifies Novel Loci

机译:成人体重指数的大型多民族基因组 - 宽协会研究标识了新的基因座

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Body mass index (BMI), a proxy measure for obesity, is determined by both environmental (including ethnicity, age, and sex) and genetic factors, with > 400 BMI-associated loci identified to date. However, the impact, interplay, and underlying biological mechanisms among BMI, environment, genetics, and ancestry are not completely understood. To further examine these relationships, we utilized 427,509 calendar year-averaged BMI measurements from 100,418 adults from the single large multiethnic Genetic Epidemiology Research on Adult Health and Aging (GERA) cohort. We observed substantial independent ancestry and nationality differences, including ancestry principal component interactions and nonlinear effects. To increase the list of BMI-associated variants before assessing other differences, we conducted a genome-wide association study (GWAS) in GERA, with replication in the Genetic Investigation of Anthropomorphic Traits (GIANT) consortium combined with the UK Biobank (UKB), followed by GWAS in GERA combined with GIANT, with replication in the UKB. We discovered 30 novel independent BMI loci (P < 5.0 x 10(-8)) that replicated. We then assessed the proportion of BMI variance explained by sex in the UKB using previously identified loci compared to previously and newly identified loci and found slight increases: from 3.0 to 3.3% for males and from 2.7 to 3.0% for females. Further, the variance explained by previously and newly identified variants decreased with increasing age in the GERA and UKB cohorts, echoed in the variance explained by the entire genome, which also showed gene-age interaction effects. Finally, we conducted a tissue expression QTL enrichment analysis, which revealed that GWAS BMI-associated variants were enriched in the cerebellum, consistent with prior work in humans and mice.
机译:体重指数(BMI)是肥胖的代理衡量标准,由环境(包括种族,年龄和性别)和遗传因素决定,迄今确定的> 400 BMI相关的基因座。然而,BMI,环境,遗传和祖先的影响,相互作用和潜在的生物机制并不完全理解。为了进一步检查这些关系,我们利用来自198,418名成年人的成人健康和老化(GERA)队列的来自单一大型多民族遗传流行病学研究的100,418名成年人的427,509个日历年平均的BMI测量。我们观察了大量独立的祖先和国籍差异,包括祖先主要成分相互作用和非线性效应。为了增加BMI相关变体的列表,在评估其他差异之前,我们在GERA中进行了一种基因组 - 宽协会研究(GWAS),其复制在拟人(巨头)联合联合英国BIOBANK(UKB)的基因调查中,其次是Gera的Gwas与巨人结合在一起,在UKB中复制。我们发现了30个新颖的独立BMI基因座(P <5.0×10(-8))复制。然后,我们评估了与先前和新鉴定的基因座相比使用先前鉴定的基因座对UKB中性别解释的BMI方差的比例,并发现略有增加:雄性的3.0至3.3%,女性的2.7%至3.0%。此外,通过GERA和UKB群组中的增加的年龄增加,先前和新鉴定的变体解释的方差随着整个基因组解释的差异而回声,这也显示出基因时期相互作用效应。最后,我们进行了组织表达QTL富集分析,揭示了GWAS BMI相关的变体富集在小脑中,与人类和小鼠的事先工作一致。

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