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首页> 外文期刊>Neuropsychopharmacology >Further Evidence for the Impact of a Genome-Wide-Supported Psychosis Risk Variant in ZNF804A on the Theory of Mind Network
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Further Evidence for the Impact of a Genome-Wide-Supported Psychosis Risk Variant in ZNF804A on the Theory of Mind Network

机译:ZNF804A中基因组广泛支持的精神病风险变异对心理网络理论影响的进一步证据

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摘要

The single-nucleotide polymorphism (SNP) rs1344706 in ZNF804A is one of the best-supported risk variants for psychosis. We hypothesized that this SNP contributes to the development of schizophrenia by affecting the ability to understand other people’s mental states. This skill, commonly referred to as Theory of Mind (ToM), has consistently been found to be impaired in schizophrenia. Using functional magnetic resonance imaging, we previously showed that in healthy individuals rs1344706 impacted on activity and connectivity of key areas of the ToM network, including the dorsomedial prefrontal cortex, temporo-parietal junction, and the posterior cingulate cortex, which show aberrant activity in schizophrenia patients, too. We aimed to replicate these results in an independent sample of 188 healthy German volunteers. In order to assess the reliability of brain activity elicited by the ToM task, 25 participants performed the task twice with an interval of 14 days showing excellent accordance in recruitment of key ToM areas. Confirming our previous results, we observed decreasing activity of the left temporo-parietal junction, dorsomedial prefrontal cortex, and the posterior cingulate cortex with increasing number of risk alleles during ToM. Complementing our replication sample with the discovery sample, analyzed in a previous report (total N=297), further revealed negative genotype effects in the left dorsomedial prefrontal cortex as well as in the temporal and parietal regions. In addition, as shown previously, rs1344706 risk allele dose positively predicted increased frontal–temporo-parietal connectivity. These findings confirm the effects of the psychosis risk variant in ZNF804A on the dysfunction of the ToM network.
机译:ZNF804A中的单核苷酸多态性(SNP)rs1344706是精神病获得最佳支持的风险变异之一。我们假设该SNP通过影响了解他人心理状态的能力来促进精神分裂症的发展。一直被认为是精神分裂症的一种技能,通常被称为心理理论(ToM)。使用功能性磁共振成像,我们先前显示,在健康个体中,rs1344706影响ToM网络关键区域的活动和连通性,包括背侧前额叶皮层,颞顶叶连接和扣带后皮层,这些细胞在精神分裂症中表现出异常活动病人也一样。我们旨在将这些结果复制到188名健康的德国志愿者的独立样本中。为了评估由ToM任务引起的脑部活动的可靠性,有25名参与者以14天的间隔执行了两次任务,显示出与关键ToM区域的招聘情况非常一致。确认我们之前的结果,我们观察到在ToM期间,随着风险等位基因数量的增加,左颞顶叶连接,背侧前额叶皮层和后扣带皮层的活动减少。在以前的报告中对我们的复制样本与发现样本进行了补充(总N = 297),进一步揭示了在左背核前额叶皮层以及颞叶和顶叶区域的基因型负面影响。此外,如先前所示,rs1344706风险等位基因剂量可肯定地预测额-颞-顶壁连接性的增加。这些发现证实了ZNF804A中精神病风险变异对ToM网络功能障碍的影响。

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