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首页> 外文期刊>Neuropsychologia >Spatial working memory deficits in GluA1 AMPA receptor subunit knockout mice reflect impaired short-term habituation: evidence for Wagner's dual-process memory model.
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Spatial working memory deficits in GluA1 AMPA receptor subunit knockout mice reflect impaired short-term habituation: evidence for Wagner's dual-process memory model.

机译:GluA1 AMPA受体亚基敲除小鼠的空间工作记忆缺陷反映出短期习性受损:Wagner的双过程记忆模型的证据。

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摘要

Genetically modified mice, lacking the GluA1 AMPA receptor subunit, are impaired on spatial working memory tasks, but display normal acquisition of spatial reference memory tasks. One explanation for this dissociation is that working memory, win-shift performance engages a GluA1-dependent, non-associative, short-term memory process through which animals choose relatively novel arms in preference to relatively familiar options. In contrast, spatial reference memory, as exemplified by the Morris water maze task, reflects a GluA1-independent, associative, long-term memory mechanism. These results can be accommodated by Wagner's dual-process model of memory in which short and long-term memory mechanisms exist in parallel and, under certain circumstances, compete with each other. According to our analysis, GluA1(-/-) mice lack short-term memory for recently experienced spatial stimuli. One consequence of this impairment is that these stimuli should remain surprising and thus be better able to form long-term associative representations. Consistent with this hypothesis, we have recently shown that long-term spatial memory for recently visited locations is enhanced in GluA1(-/-) mice, despite impairments in hippocampal synaptic plasticity. Taken together, these results support a role for GluA1-containing AMPA receptors in short-term habituation, and in modulating the intensity or perceived salience of stimuli.
机译:缺少GluA1 AMPA受体亚基的转基因小鼠在空间工作记忆任务中受损,但显示出正常的空间参考记忆任务。这种分离的一种解释是,工作记忆,胜胜表现参与了GluA1依赖性,非关联性的短期记忆过程,通过这种过程,动物优先选择相对新颖的手臂,而不愿选择相对熟悉的选项。相反,以莫里斯水迷宫任务为例的空间参考内存反映了独立于GluA1的联想长期记忆机制。 Wagner的记忆双过程模型可以容纳这些结果,在该模型中,短期和长期记忆机制并行存在,并且在某些情况下会相互竞争。根据我们的分析,GluA1(-/-)小鼠缺乏近期记忆的空间刺激的短期记忆。这种损伤的一个后果是这些刺激应该仍然令人惊讶,因此能够更好地形成长期的联想表现。与此假设相符,我们最近表明,尽管海马突触可塑性受损,但GluA1(-/-)小鼠的近期访问位置的长期空间记忆得到了增强。综上所述,这些结果支持了含GluA1的AMPA受体在短期适应以及调节刺激强度或显着性方面的作用。

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