A Genome-Wide Search for Bipolar Disorder Risk Loci Modified by Mitochondrial Genome Variation.

Molecular Neuropsychiatry Pub Date : 2018-02-01 Epub Date: 2017-10-28 DOI:10.1159/000464444
Euijung Ryu, Malik Nassan, Gregory D Jenkins, Sebastian M Armasu, Ana Andreazza, Susan L McElroy, Marquis P Vawter, Mark A Frye, Joanna M Biernacka
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引用次数: 17

Abstract

Mitochondrial DNA mutations have been reported to be associated with bipolar disorder (BD). In this study, we performed genome-wide analyses to assess mitochondrial single-nucleotide polymorphism (mtSNP) effects on BD risk and early-onset BD (EOBD) among BD patients, focusing on interaction effects between nuclear SNPs (nSNPs) and mtSNPs. Common nSNP and mtSNP data from European American BD cases (n = 1,001) and controls (n = 1,034) from the Genetic Association Information Network BD study were analyzed to assess the joint effect of nSNP and nSNP-mtSNP interaction on the risk of BD and EOBD. The effect of nSNP-mtSNP interactions was also assessed. For BD risk, the strongest evidence of an association was obtained for nSNP rs1880924 in MGAM and mtSNP rs3088309 in CytB (pjoint = 8.2 × 10-8, pint = 1.4 × 10-4). Our results also suggest that the minor allele of the nSNP rs583990 in CTNNA2 increases the risk of EOBD among carriers of the mtSNP rs3088309 minor allele, while the nSNP has no effect among those carrying the mtSNP major allele (OR = 4.53 vs. 1.05, pjoint = 2.1 × 10-7, pint = 1.16 × 10-6). While our results are not statistically significant after multiple testing correction and a large-sample replication is required, our exploratory study demonstrates the potential importance of considering the mitochondrial genome for identifying genetic factors associated with BD.

Abstract Image

Abstract Image

线粒体基因组变异修饰双相情感障碍风险位点的全基因组搜索。
据报道,线粒体DNA突变与双相情感障碍(BD)有关。在这项研究中,我们进行了全基因组分析,以评估线粒体单核苷酸多态性(mtSNP)对BD患者BD风险和早发性BD (EOBD)的影响,重点关注核snp (nsnp)和mtSNP之间的相互作用。分析来自遗传关联信息网络BD研究的欧美BD病例(n = 1,001)和对照组(n = 1,034)的常见nSNP和mtSNP数据,以评估nSNP和nSNP-mtSNP相互作用对BD和EOBD风险的共同影响。我们还评估了nSNP-mtSNP相互作用的影响。对于BD风险,最有力的证据表明,nSNP rs1880924与MGAM相关,mtSNP rs3088309与CytB相关(pjoint = 8.2 × 10-8, pint = 1.4 × 10-4)。我们的研究结果还表明,CTNNA2中nSNP rss583990的次要等位基因增加了mtSNP rs3088309次要等位基因携带者患EOBD的风险,而nSNP在mtSNP主要等位基因携带者中没有影响(OR = 4.53 vs. 1.05, pjoint = 2.1 × 10-7, pint = 1.16 × 10-6)。虽然我们的结果在多次测试校正后没有统计学意义,并且需要大样本复制,但我们的探索性研究表明,考虑线粒体基因组对于识别与双相障碍相关的遗传因素具有潜在的重要性。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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