Meta-analysis of genome-wide association data identifies a risk locus for major mood disorders on 3p21.1.

McMahon FJ; Akula N; Schulze TG; Muglia P; Tozzi F; Detera Wadleigh SD; Steele CJ; Breuer R; Strohmaier J; Wendland JR; Mattheisen M; Muhleisen TW; Maier W; Nothen MM; Cichon S; Farmer A; Vincent JB; Holsboer F; Preisig M; Rietschel M

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Meta-analysis of genome-wide association data identifies a risk locus for major mood disorders on 3p21.1.

机译：对全基因组关联数据的荟萃分析确定了3p21.1上主要情绪障碍的风险源。

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The major mood disorders, which include bipolar disorder and major depressive disorder (MDD), are considered heritable traits, although previous genetic association studies have had limited success in robustly identifying risk loci. We performed a meta-analysis of five case-control cohorts for major mood disorder, including over 13,600 individuals genotyped on high-density SNP arrays. We identified SNPs at 3p21.1 associated with major mood disorders (rs2251219, P = 3.63 x 10(-8); odds ratio = 0.87; 95% confidence interval, 0.83-0.92), with supportive evidence for association observed in two out of three independent replication cohorts. These results provide an example of a shared genetic susceptibility locus for bipolar disorder and MDD.

机译：主要的情绪障碍，包括躁郁症和主要的抑郁症（MDD），被认为是可遗传的特征，尽管以前的遗传学关联研究在有效地识别风险基因座方面取得的成功有限。我们对五个主要情绪障碍病例对照队列进行了荟萃分析，包括在高密度SNP阵列上进行基因分型的13,600多个个体。我们在3p21.1处发现了与主要情绪障碍相关的SNP（rs2251219，P = 3.63 x 10（-8）;优势比= 0.87; 95％置信区间为0.83-0.92），并且有两个证据表明存在关联三个独立的复制群组。这些结果提供了双相情感障碍和MDD共有遗传易感性基因座的例子。

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《Nature Genetics》 |2010年第2期|共4页
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McMahon FJ; Akula N; Schulze TG; Muglia P; Tozzi F; Detera Wadleigh SD; Steele CJ; Breuer R; Strohmaier J; Wendland JR; Mattheisen M; Muhleisen TW; Maier W; Nothen MM; Cichon S; Farmer A; Vincent JB; Holsboer F; Preisig M; Rietschel M;
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正文语种 eng
中图分类医学遗传学;自然研究、自然历史;
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1. Meta-analysis of genome-wide association data identifies a risk locus for major mood disorders on 3p21.1. [J] . McMahon FJ, Akula N, Schulze TG, Nature Genetics . 2010,第2期

机译：对全基因组关联数据的荟萃分析确定了3p21.1上主要情绪障碍的风险源。
2. Meta-analysis of genome-wide association data of bipolar disorder and major depressive disorder [J] . Y Liu, D H Blackwood, S Caesar, Molecular Psychiatry . 2011,第1期

机译：双相情感障碍和重性抑郁症全基因组关联数据的荟萃分析
3. Genome-wide association study identifies a single major locus contributing to survival into old age; the APOE locus revisited [J] . Aging cell. . 2011,第4期

机译：全基因组关联研究确定了一个有助于老年生存的主要基因座;再谈APOE的所在地
4. Data Mining Approaches for Genome-Wide Association of Mood Disorders [C] . Mehdi Pirooznia, Fayaz Seifuddin, Jennifer Judy, International Conference on Bioinformatics and Computational Biology . 2010

机译：关于全基因组心情障碍协会的数据挖掘方法
5. Meta-analysis strategies for heterogeneous studies in genome-wide association studies. [D] . Hong, Jaeyoung. 2016

机译：在全基因组关联研究中进行异构研究的荟萃分析策略。
6. Meta-analysis of genome-wide association data detects a risk locus for major mood disorders on chromosome 3p21.1 [O] . Francis J. McMahon, Nirmala Akula, Thomas G. Schulze, -1

机译：基因组关联数据的Meta分析检测到染色体上的主要情绪障碍风险基因座3p21.1
7. Meta-analysis of genome-wide association data identifies a risk locus for major mood disorders on 3p21.1 [O] . McMahon, Francis J., Akula, Nirmala, Schulze, Thomas G., 2010

机译：对全基因组关联数据的荟萃分析确定了3p21.1上主要情绪障碍的风险源

Meta-analysis of genome-wide association data identifies a risk locus for major mood disorders on 3p21.1.

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