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首页> 外文期刊>International journal of geriatric psychiatry >Mitochondrial DNA m.13514GA DNA m.13514G>A heteroplasmy is associated with depressive symptoms in the elderly
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Mitochondrial DNA m.13514GA DNA m.13514G>A heteroplasmy is associated with depressive symptoms in the elderly

机译:线粒体DNA m.13514g& DNA m.13514g>异质瘤与老年人的抑郁症状有关

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Objectives Mitochondrial DNA (mtDNA) heteroplasmy is a mixture of normal and mutated mtDNA molecules in a cell. High levels of heteroplasmy at several mtDNA sites in complex I lead to inherited neurological neurologic diseases and brain magnetic resonance imaging (MRI) abnormalities. Here, we test the hypothesis that mtDNA heteroplasmy at these complex I sites is associated with depressive symptoms in the elderly. Methods We examined platelet mtDNA heteroplasmy for associations with depressive symptoms among 137 participants over age 70 from the community‐based Health, Aging and Body Composition Study. Depressive symptoms were assessed using the 10‐point version of the Center for Epidemiologic Studies Depression Scale (CES‐D 10). Complete mtDNA sequencing was performed and heteroplasmy derived for 5 mtDNA sites associated with neurologic mitochondrial diseases and tested for associations with depressive symptoms. Results Of 5 candidate complex I mtDNA mutations examined for effects on depressive symptoms, increased heteroplasmy at m.13514AG, ND5 , was significantly associated with higher CES‐D score ( P ?=?.01). A statistically significant interaction between m.13514A??G heteroplasmy and sex was detected ( P ?=?.04); in sex‐stratified analyses, the impact of m.13514AG heteroplasmy was stronger in male ( P ?=?.003) than in female ( P ?=?.98) participants. Men in highest tertile of mtDNA heteroplasmy exhibited significantly higher ( P ?=?.0001) mean?±?SE CES‐D 10 scores, 5.37?±?0.58, when compared with those in the middle, 2.13?±?0.52, and lowest tertiles, 2.47?±?0.58. No associations between the 4 other candidate sites and depressive symptoms were observed. Conclusions Increased mtDNA heteroplasmy at m.13514AG is associated with depressive symptoms in older men. Heteroplasmy may represent a novel biological risk factor for depression.
机译:目的线粒体DNA(MTDNA)异质性是细胞中正常和突变的MTDNA分子的混合物。在络合物中的几个MTDNA位点高水平的异质性导致遗传性神经系统疾病和脑磁共振成像(MRI)异常。在这里,我们测试这些复合物I位点上的MTDNA异质性的假设与老年人的抑郁症状有关。方法采用基于社区的健康,老龄化和身体成分研究的70岁以上70岁以上的137名参与者抑郁症状的抑郁症状相关的血小板mtdna异质。利用流行病学研究中心的10点版本评估抑郁症状抑郁尺:CES-D 10)。进行完整的MTDNA测序,并衍生出与神经系统线粒体疾病相关的5个MTDNA位点的异质性,并测试与抑郁症状的关联。结果5候选复合物I MTDNA突变检查对抑郁症状的影响,M.13514A&GT的异质增加,ND5的异质性显着与CES-D得分显着相关(P?= 01)。在m.13514a之间的统计学上显着的相互作用?&Δg异质和性别(p?=Δ.04);在性分析分析中,Ma13514a& g heferoplasmy的影响比女性(p?= = 003)更强(p?=〜98)参与者。 MTDNA异质的最高型截头的男性显着更高(P?=×0001)平均值?±α?SE CES-D 10分数,5.37?±0.58,与中间的那些相比,2.13?±0.52,和最低的截头,2.47?±0.58。没有观察到其他4个候选地点和抑郁症状之间的关联。结论M.13514A&GT的MTDNA异质增加。G与老年人的抑郁症状有关。异质可能代表抑郁症的新生物危险因素。

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