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安帕金CX717对非人类灵长类动物认知增强及认知缺陷逆转的潜在机制。

Mechanisms underlying cognitive enhancement and reversal of cognitive deficits in nonhuman primates by the ampakine CX717.

作者信息

Hampson R E, España R A, Rogers G A, Porrino L J, Deadwyler S A

机构信息

Department of Physiology and Pharmacology, Wake Forest University Health Sciences, Medical Center Boulevard, Winston-Salem, NC 27157-1083, USA.

出版信息

Psychopharmacology (Berl). 2009 Jan;202(1-3):355-69. doi: 10.1007/s00213-008-1360-z. Epub 2008 Nov 5.

Abstract

RATIONALE

Performance of cognitive tasks in nonhuman primates (NHPs) requires specific brain regions to make decisions under different degrees of difficulty or "cognitive load."

OBJECTIVE

Local cerebral metabolic activity ([18F]FDG PET imaging) in dorsolateral prefrontal cortex (DLPFC), medial temporal lobe (MTL), and dorsal striatum (DStr) is examined in NHPs performing a delayed-match-to-sample (DMS) task with variable degrees of cognitive load.

MATERIALS AND METHODS

Correlations between cognitive load and degree of brain metabolic activity were obtained with respect to the influence of the ampakine CX717 (Cortex Pharmaceuticals), using brain imaging and recordings of neuronal activity in NHPs and measures of intracellular calcium release in rat hippocampal slices.

RESULTS

Activation of DLPFC, MTL, and DStr reflected changes in performance related to cognitive load within the DMS task and were engaged primarily on high load trials. Similar increased activation patterns and improved performance were also observed following administration of CX717. Sleep deprivation in NHPs produced impaired performance and reductions in brain activation which was reversed by CX717. One potential basis for this facilitation of cognition by CX717 was increased firing of task-specific hippocampal cells. Synaptic mechanisms affected by CX717 were examined in rat hippocampal slices which showed that N-methyl-D-aspartic acid-mediated release of intracellular calcium was reduced in slices from sleep-deprived rats and reversed by application of CX717 to the bathing medium.

CONCLUSIONS

The findings provide insight into how cognition is enhanced by CX717 in terms of brain, and underlying neural, processes that are activated on high vs. low cognitive load trials.

摘要

原理

非人类灵长类动物(NHPs)执行认知任务需要特定脑区在不同难度或“认知负荷”下做出决策。

目的

在执行具有不同认知负荷程度的延迟匹配样本(DMS)任务的NHPs中,检测背外侧前额叶皮层(DLPFC)、内侧颞叶(MTL)和背侧纹状体(DStr)的局部脑代谢活动([18F]FDG PET成像)。

材料与方法

使用脑成像和NHPs神经元活动记录以及大鼠海马切片细胞内钙释放测量,研究氨吡啶酮CX717(Cortex制药公司)的影响,从而获得认知负荷与脑代谢活动程度之间的相关性。

结果

DLPFC、MTL和DStr的激活反映了DMS任务中与认知负荷相关的表现变化,并且主要在高负荷试验中起作用。给予CX717后也观察到类似的激活模式增加和表现改善。NHPs睡眠剥夺导致表现受损和脑激活减少,而CX717可逆转这种情况。CX717促进认知的一个潜在基础是特定任务海马细胞的放电增加。在大鼠海马切片中研究了受CX717影响的突触机制,结果表明,睡眠剥夺大鼠切片中N-甲基-D-天冬氨酸介导的细胞内钙释放减少,而将CX717应用于浴液可逆转这种情况。

结论

这些发现揭示了CX717在高认知负荷试验与低认知负荷试验中激活大脑及潜在神经过程方面如何增强认知。

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