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GRM2/3(mGlu2/mGlu3)双敲除小鼠中海马空间记忆的分馏揭示了 II 组代谢型谷氨酸受体在觉醒和认知之间的作用。

Fractionation of spatial memory in GRM2/3 (mGlu2/mGlu3) double knockout mice reveals a role for group II metabotropic glutamate receptors at the interface between arousal and cognition.

机构信息

Department of Psychiatry, University of Oxford, Warneford Hospital, Oxford, UK.

出版信息

Neuropsychopharmacology. 2011 Dec;36(13):2616-28. doi: 10.1038/npp.2011.145. Epub 2011 Aug 10.

Abstract

Group II metabotropic glutamate receptors (mGluR2 and mGluR3, encoded by GRM2 and GRM3) are implicated in hippocampal function and cognition, and in the pathophysiology and treatment of schizophrenia and other psychiatric disorders. However, pharmacological and behavioral studies with group II mGluR agonists and antagonists have produced complex results. Here, we studied hippocampus-dependent memory in GRM2/3 double knockout (GRM2/3(-/-)) mice in an iterative sequence of experiments. We found that they were impaired on appetitively motivated spatial reference and working memory tasks, and on a spatial novelty preference task that relies on animals' exploratory drive, but were unimpaired on aversively motivated spatial memory paradigms. GRM2/3(-/-) mice also performed normally on an appetitively motivated, non-spatial, visual discrimination task. These results likely reflect an interaction between GRM2/3 genotype and the arousal-inducing properties of the experimental paradigm. The deficit seen on appetitive and exploratory spatial memory tasks may be absent in aversive tasks because the latter induce higher levels of arousal, which rescue spatial learning. Consistent with an altered arousal-cognition relationship in GRM2/3(-/-) mice, injection stress worsened appetitively motivated, spatial working memory in wild-types, but enhanced performance in GRM2/3(-/-) mice. GRM2/3(-/-) mice were also hypoactive in response to amphetamine. This fractionation of hippocampus-dependent memory depending on the appetitive-aversive context is to our knowledge unique, and suggests a role for group II mGluRs at the interface of arousal and cognition. These arousal-dependent effects may explain apparently conflicting data from previous studies, and have translational relevance for the involvement of these receptors in schizophrenia and other disorders.

摘要

II 组代谢型谷氨酸受体(mGluR2 和 mGluR3,由 GRM2 和 GRM3 编码)参与海马功能和认知,以及精神分裂症和其他精神障碍的病理生理学和治疗。然而,用 II 组 mGluR 激动剂和拮抗剂进行的药理学和行为学研究产生了复杂的结果。在这里,我们在迭代实验中研究了 GRM2/3 双敲除(GRM2/3(-/-))小鼠中海马依赖性记忆。我们发现它们在有吸引力的空间参考和工作记忆任务以及依赖动物探索驱动的空间新颖性偏好任务中受损,但在厌恶驱动的空间记忆范式中不受影响。GRM2/3(-/-) 小鼠在有吸引力的、非空间的、视觉辨别任务中也表现正常。这些结果可能反映了 GRM2/3 基因型与实验范式的唤醒诱导特性之间的相互作用。在有吸引力和探索性空间记忆任务中看到的缺陷可能在厌恶任务中不存在,因为后者诱导更高水平的唤醒,从而挽救空间学习。与 GRM2/3(-/-) 小鼠中唤醒认知关系改变一致,注射应激恶化了野生型动物有吸引力的空间工作记忆,但增强了 GRM2/3(-/-) 小鼠的表现。GRM2/3(-/-) 小鼠对安非他命的反应也较低。这种根据有吸引力和厌恶的上下文对海马依赖性记忆的细分在我们的知识中是独特的,并且表明 II 组 mGluRs 在唤醒和认知的接口处发挥作用。这些唤醒依赖性效应可能解释了先前研究中明显矛盾的数据,并对这些受体在精神分裂症和其他疾病中的参与具有转化意义。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/e808/3230485/be636f3b55d3/npp2011145f1.jpg

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