转基因
神经科学
前脑
长时程增强
记忆巩固
海马体
海马结构
纹状体
扁桃形结构
转基因小鼠
生物
即刻早期基因
基因表达
受体
基因
遗传学
多巴胺
中枢神经系统
作者
Mark Mayford,Mary Elizabeth Bach,Yan-You Huang,Lei Wang,Robert D. Hawkins,Eric R. Kandel
出处
期刊:Science
[American Association for the Advancement of Science]
日期:1996-12-06
卷期号:274 (5293): 1678-1683
被引量:1535
标识
DOI:10.1126/science.274.5293.1678
摘要
One of the major limitations in the use of genetically modified mice for studying cognitive functions is the lack of regional and temporal control of gene function. To overcome these limitations, a forebrain-specific promoter was combined with the tetracycline transactivator system to achieve both regional and temporal control of transgene expression. Expression of an activated calcium-independent form of calcium-calmodulin-dependent kinase II (CaMKII) resulted in a loss of hippocampal long-term potentiation in response to 10-hertz stimulation and a deficit in spatial memory, a form of explicit memory. Suppression of transgene expression reversed both the physiological and the memory deficit. When the transgene was expressed at high levels in the lateral amygdala and the striatum but not other forebrain structures, there was a deficit in fear conditioning, an implicit memory task, that also was reversible. Thus, the CaMKII signaling pathway is critical for both explicit and implicit memory storage, in a manner that is independent of its potential role in development.
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