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首页> 外文期刊>European neuropsychopharmacology: the journal of the European College of Neuropsychopharmacology >Schizophrenia risk variants affecting nnicroRNA function and site-specific regulation of NT5C2 by miR-206
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Schizophrenia risk variants affecting nnicroRNA function and site-specific regulation of NT5C2 by miR-206

机译:精神分裂症的风险变异体会影响miR-206的nnicroRNA功能和NT5C2的位点特异性调控

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摘要

Despite the identification of numerous schizophrenia-associated genetic variants, few have been examined functionally to identify and characterize the causal variants. To mitigate this, we aimed at identifying functional variants affecting miRNA function. Using data from a large-scale genome-wide association study of schizophrenia, we looked for schizophrenia risk variants altering either miRNA binding sites, miRNA genes, promoters for miRNA genes, or variants that were expression quantitative trait loci (eQTLs) for miRNA genes. We hereby identified several potentially functional variants relating to miRNA function with our top finding being a schizophrenia protective allele that disrupts miR-206's binding to NT5C2 thus leading to increased expression of this gene. A subsequent experimental follow-up of the variant using a luciferase-based reporter assay confirmed that the allele disrupts the binding. Our study therefore suggests that miR-206 may contribute to schizophrenia risk through allele-dependent regulation of the genome-wide significant gene NT5C2. (C) 2016 Elsevier B.V. and ECNP. All rights reserved.
机译:尽管鉴定了许多精神分裂症相关的遗传变异,但在功能上很少检查以鉴定和表征因果变异。为了减轻这种情况,我们旨在鉴定影响miRNA功能的功能变体。使用来自大规模精神分裂症全基因组关联研究的数据,我们寻找了可以改变miRNA结合位点,miRNA基因,miRNA基因的启动子或miRNA基因表达定量特征位点(eQTL)的变异的精神分裂症风险变异。我们在此鉴定了几个与miRNA功能有关的潜在功能性变异,我们的首要发现是精神分裂症保护性等位基因,它破坏了miR-206与NT5C2的结合,从而导致该基因的表达增加。随后使用基于荧光素酶的报告基因检测法对该变体进行实验跟踪,证实了等位基因破坏了结合。因此,我们的研究表明,miR-206可能通过全基因组范围内重要基因NT5C2的等位基因依赖性调节而导致精神分裂症风险。 (C)2016 Elsevier B.V.和ECNP。版权所有。

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