首页> 美国卫生研究院文献>Frontiers in Behavioral Neuroscience >Mice Lacking Ras-GRF1 Show Contextual Fear Conditioning but not Spatial Memory Impairments: Convergent Evidence from Two Independently Generated Mouse Mutant Lines
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Mice Lacking Ras-GRF1 Show Contextual Fear Conditioning but not Spatial Memory Impairments: Convergent Evidence from Two Independently Generated Mouse Mutant Lines

机译:缺少Ras-GRF1的小鼠显示情境恐惧条件但未显示空间记忆障碍:来自两个独立生成的小鼠突变株的证据。

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摘要

Ras-GRF1 is a neuronal specific guanine exchange factor that, once activated by both ionotropic and metabotropic neurotransmitter receptors, can stimulate Ras proteins, leading to long-term phosphorylation of downstream signaling. The two available reports on the behavior of two independently generated Ras-GRF1 deficient mouse lines provide contrasting evidence on the role of Ras-GRF1 in spatial memory and contextual fear conditioning. These discrepancies may be due to the distinct alterations introduced in the mouse genome by gene targeting in the two lines that could differentially affect expression of nearby genes located in the imprinted region containing the Ras-grf1 locus. In order to determine the real contribution of Ras-GRF1 to spatial memory we compared in Morris Water Maze learning Brambilla’s mice with a third mouse line (GENA53) in which a non-sense mutation was introduced in the Ras-GRF1 coding region without additional changes in the genome and we found that memory in this task is normal. Also, we measured both contextual and cued fear conditioning, which were previously reported to be affected in Brambilla’s mice, and we confirmed that contextual learning but not cued conditioning is impaired in both mouse lines. In addition, we also tested both lines for the first time in conditioned place aversion in the Intellicage, an ecological and remotely controlled behavioral test, and we observed normal learning. Finally, based on previous reports of other mutant lines suggesting that Ras-GRF1 may control body weight, we also measured this non-cognitive phenotype and we confirmed that both Ras-GRF1 deficient mutants are smaller than their control littermates. In conclusion, we demonstrate that Ras-GRF1 has no unique role in spatial memory while its function in contextual fear conditioning is likely to be due not only to its involvement in amygdala functions but possibly to some distinct hippocampal connections specific to contextual learning.
机译:Ras-GRF1是一种神经元特异性鸟嘌呤交换因子,一旦被离子型和代谢型神经递质受体激活,就可以刺激Ras蛋白,导致下游信号的长期磷酸化。关于两个独立生成的Ras-GRF1缺陷小鼠系的行为的两个可用报告提供了有关Ras-GRF1在空间记忆和情境恐惧调节中作用的对比证据。这些差异可能是由于在两个品系中通过基因靶向在小鼠基因组中引入的明显变化,这些变化可能差异地影响位于包含Ras-grf1基因座的印迹区域的附近基因的表达。为了确定Ras-GRF1对空间记忆的真正贡献,我们在Morris Water Maze学习Brambilla小鼠与第三只小鼠系(GENA53)中进行了比较,在该小鼠系中,无义突变被引入Ras-GRF1编码区,没有其他变化在基因组中,我们发现此任务中的记忆是正常的。另外,我们同时测量了情境和暗示恐惧条件,这两种报道以前曾在Brambilla的小鼠中受到影响,并且我们确认,在这两种小鼠品系中,情境学习而非暗示条件都受到了损害。此外,我们还首次在Intellicage的条件位置厌恶测试中对这两条线进行了测试,这是一种生态和远程控制的行为测试,并且观察到正常学习。最后,根据其他突变株系的先前报道表明,Ras-GRF1可能控制体重,我们也测量了这种非认知表型,并且我们确认了两个缺少Ras-GRF1的突变体都比其对照同窝仔小。总之,我们证明Ras-GRF1在空间记忆中没有独特的作用,而其在情境恐惧调节中的功能可能不仅是由于其参与了杏仁核的功能,而且可能是由于情境学习所特有的一些不同的海马连接。

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