首页> 美国卫生研究院文献>Frontiers in Cellular Neuroscience >Shank3-mutant mice lacking exon 9 show altered excitation/inhibition balance, enhanced rearing, and spatial memory deficit
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Shank3-mutant mice lacking exon 9 show altered excitation/inhibition balance, enhanced rearing, and spatial memory deficit

机译:缺乏外显子9的Shank3突变小鼠表现出改变的兴奋/抑制平衡,增强的饲养和空间记忆缺陷

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摘要

Shank3 is a postsynaptic scaffolding protein implicated in synapse development and autism spectrum disorders. The Shank3 gene is known to produce diverse splice variants whose functions have not been fully explored. In the present study, we generated mice lacking Shank3 exon 9 (Shank3Δ9 mice), and thus missing five out of 10 known Shank3 splice variants containing the N-terminal ankyrin repeat region, including the longest splice variant, Shank3a. Our X-gal staining results revealed that Shank3 proteins encoded by exon 9-containing splice variants are abundant in upper cortical layers, striatum, hippocampus, and thalamus, but not in the olfactory bulb or cerebellum, despite the significant Shank3 mRNA levels in these regions. The hippocampal CA1 region of Shank3Δ9 mice exhibited reduced excitatory transmission at Schaffer collateral synapses and increased frequency of spontaneous inhibitory synaptic events in pyramidal neurons. In contrast, prelimbic layer 2/3 pyramidal neurons in the medial prefrontal cortex displayed decreased frequency of spontaneous inhibitory synaptic events, indicating alterations in the ratio of excitation/inhibition (E/I ratio) in the Shank3Δ9 brain. These mice displayed a mild increase in rearing in a novel environment and mildly impaired spatial memory, but showed normal social interaction and repetitive behavior. These results suggest that ankyrin repeat-containing Shank3 splice variants are important for E/I balance, rearing behavior, and spatial memory.
机译:Shank3是一种突触后支架蛋白,与突触发展和自闭症谱系障碍有关。已知Shank3基因会产生各种剪接变体,其功能尚未得到充分探索。在本研究中,我们产生了缺少Shank3外显子9的小鼠(Shank3 Δ9小鼠),因此缺少了10个已知的包含N末端锚蛋白重复区的Shank3剪接变体中的5个,包括最长的剪接变体,Shank3a。我们的X-gal染色结果表明,由含外显子9的剪接变体编码的Shank3蛋白在上皮层,纹状体,海马和丘脑中丰富,但在嗅球或小脑中却不丰富,尽管在这些区域中Shank3 mRNA的水平很高。 Shank3 Δ9小鼠的海马CA1区在Schaffer侧突触处的兴奋性传递减少,并且锥体神经元的自发抑制突触事件的频率增加。相比之下,内侧前额叶皮层的前边缘2/3锥体神经元显示出自发抑制性突触事件的频率降低,表明Shank3 Δ9的兴奋/抑制比(E / I比)发生了变化。脑。这些小鼠在新颖的环境中显示出轻微的饲养增加,并且空间记忆轻微受损,但表现出正常的社交互动和重复行为。这些结果表明,含锚蛋白重复序列​​的Shank3剪接变体对E / I平衡,饲养行为和空间记忆很重要。

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