首页> 美国卫生研究院文献>Translational Psychiatry >Hippocampal–prefrontal coherence mediates working memory and selective attention at distinct frequency bands and provides a causal link between schizophrenia and its risk gene GRIA1
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Hippocampal–prefrontal coherence mediates working memory and selective attention at distinct frequency bands and provides a causal link between schizophrenia and its risk gene GRIA1

机译:海马-前额叶相干性在不同的频段介导工作记忆和选择性注意并在精神分裂症及其危险基因GRIA1之间提供因果关系

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摘要

Increased fronto-temporal theta coherence and failure of its stimulus-specific modulation have been reported in schizophrenia, but the psychological correlates and underlying neural mechanisms remain elusive. Mice lacking the putative schizophrenia risk gene GRIA1 (Gria1–/–), which encodes GLUA1, show strongly impaired spatial working memory and elevated selective attention owing to a deficit in stimulus-specific short-term habituation. A failure of short-term habituation has been suggested to cause an aberrant assignment of salience and thereby psychosis in schizophrenia. We recorded hippocampal–prefrontal coherence while assessing spatial working memory and short-term habituation in these animals, wildtype (WT) controls, and Gria1–/– mice in which GLUA1 expression was restored in hippocampal subfields CA2 and CA3. We found that beta (20–30 Hz) and low-gamma (30–48 Hz) frequency coherence could predict working memory performance, whereas—surprisingly—theta (6–12 Hz) coherence was unrelated to performance and largely unaffected by genotype in this task. In contrast, in novel environments, theta coherence specifically tracked exploration-related attention in WT mice, but was strongly elevated and unmodulated in Gria1-knockouts, thereby correlating with impaired short-term habituation. Strikingly, reintroduction of GLUA1 selectively into CA2/CA3 restored abnormal short-term habituation, theta coherence, and hippocampal and prefrontal theta oscillations. Although local oscillations and coherence in other frequency bands (beta, gamma), and theta-gamma cross-frequency coupling also showed dependence on GLUA1, none of them correlated with short-term habituation. Therefore, sustained elevation of hippocampal–prefrontal theta coherence may underlie a failure in regulating novelty-related selective attention leading to aberrant salience, and thereby represents a mechanistic link between GRIA1 and schizophrenia.
机译:精神分裂症中已报道额颞叶theta相干性增加和其刺激特异性调节的失败,但是心理关联和潜在的神经机制仍然难以捉摸。缺乏假定的精神分裂症危险基因GRIA1(Gria1 – / – )编码GLUA1的小鼠,由于特定于刺激的短期习性不足,显示出严重削弱的空间工作记忆和选择性注意力。短期的习惯化失败被认为会导致显着性异常分配,从而导致精神分裂症的精神病。我们记录了海马-前额叶相干性,同时评估了这些动物,野生型(WT)对照和Gria1 – / – 小鼠的空间工作记忆和短期习性,其中GLUA1表达在海马亚域CA2和CA3。我们发现,β(20–30 Hz)和低伽玛(30–48 Hz)频率一致性可以预测工作记忆性能,而–令人惊讶的是,θ(6–12 Hz)一致性与性能无关,并且在很大程度上不受基因型的影响。这个任务。相比之下,在新颖的环境中,theta相干性专门跟踪了WT小鼠中与探索相关的注意力,但在Gria1基因敲除中却强烈升高且不受调节,从而与短期习惯受损相关。令人惊讶的是,将GLUA1选择性地重新引入CA2 / CA3可恢复异常的短期习性,θ相干性以及海马和前额叶θ振荡。尽管其他频带(β,γ)的局部振荡和相干性以及θ-γ跨频耦合也显示出对GLUA1的依赖性,但它们均与短期适应性无关。因此,持续升高的海马-前额叶theta连贯性可能是调节与新颖性相关的选择性注意力而导致异常显着性失败的原因,从而代表了GRIA1与精神分裂症之间的机制联系。

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