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首页> 外文期刊>Human Molecular Genetics >Gene-centric meta-analyses of 108 912 individuals confirm known body mass index loci and reveal three novel signals
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Gene-centric meta-analyses of 108 912 individuals confirm known body mass index loci and reveal three novel signals

机译:以基因为中心的荟萃分析对108 912个个体进行了验证,证实了已知的体重指数基因座并揭示了三个新信号

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Recent genetic association studies have made progress in uncovering components of the genetic architecture of the body mass index (BMI). We used the ITMAT-Broad-Candidate Gene Association Resource (CARe) (IBC) array comprising up to 49 320 single nucleotide polymorphisms (SNPs) across ~2100 metabolic and cardiovascular-related loci to genotype up to 108 912 individuals of European ancestry (EA), African-Americans, Hispanics and East Asians, from 46 studies, to provide additional insight into SNPs underpinning BMI. We used a five-phase study design: Phase I focused on meta-analysis of EA studies providing individual level genotype data; Phase II performed a replication of cohorts providing summary level EA data; Phase III meta-analyzed results from the first two phases; associated SNPs from Phase III were used for replication in Phase IV; finally in Phase V, a multi-ethnic meta-analysis of all samples from four ethnicities was performed. At an array-wide significance (P< 2.40E-06), we identify novel BMI associations in loci translocase of outer mitochondrial membrane 40 homolog (yeast) - apolipoprotein E - apolipoprotein C-l (TOMM40-APOE-APOC1) (rs2075650, P= 2.95E-10), sterol regulatory element binding transcription factor 2 (SREBF2, rs5996074, P= 9.43E-07) and neurotrophic tyroslne kinase, receptor, type 2 [NTRK2, a brain-derived neuro-trophic factor (BDNF) receptor gene, rs1211166, P= 1.04E-06] in the Phase IV meta-analysis. Of 10 loci with previous evidence for BMI association represented on the IBC array, eight were replicated, with the remaining two showing nominal significance. Conditional analyses revealed two independent BMI-asso-ciated signals in BDNF and melanocortin 4 receptor (MC4R) regions. Of the 11 array-wide significant SNPs, three are associated with gene expression levels in both primary B-cells and monocytes; with rs4788099 in SH2B adaptor protein 1 (SH2B1) notably being associated with the expression of multiple genes in cis. These multi-ethnic meta-analyses expand our knowledge of BMI genetics.
机译:最近的遗传关联研究在揭示体重指数(BMI)的遗传结构组成部分方面取得了进展。我们使用了ITMAT广泛候选基因协会资源(CARe)(IBC)阵列,该阵列包含跨越约2100个代谢和心血管相关基因座的多达49320个单核苷酸多态性(SNP),以对多达108912例欧洲血统(EA)个体进行基因分型),非裔美国人,西班牙裔和东亚人(来自46项研究),以进一步了解支撑BMI的SNP。我们使用了一个分为五个阶段的研究设计:第一阶段专注于提供个体水平基因型数据的EA研究的荟萃分析;第二阶段进行了队列的复制,提供了汇总级别的EA数据;第三阶段的前两阶段荟萃分析结果;来自阶段III的相关SNP在阶段IV中进行复制;最终,在第五阶段,对来自四个种族的所有样本进行了多种族的荟萃分析。在整个阵列意义上(P <2.40E-06),我们在线粒体外膜40同源物(酵母)-载脂蛋白E-载脂蛋白C1(TOMM40-APOE-APOC1)(rs2075650,P = 2.95E-10),固醇调节元件结合转录因子2(SREBF2,rs5996074,P = 9.43E-07)和2型神经营养性酪氨酸激酶受体[NTRK2,一种脑源性神经营养因子(BDNF)受体基因,rs1211166,P = 1.04E-06]。在IBC阵列上代表BMI关联的先前证据的10个基因座中,有8个被复制,其余两个显示出名义意义。条件分析显示,BDNF和黑皮质素4受体(MC4R)区域中存在两个独立的BMI相关信号。在11种阵列范围内的重要SNP中,有3种与原代B细胞和单核细胞中的基因表达水平相关; SH2B衔接蛋白1(SH2B1)中带有rs4788099的蛋白与顺式中多个基因的表达相关。这些多民族的荟萃分析扩展了我们对BMI遗传学的认识。

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