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首页> 外文期刊>Scientific reports. >Soluble amyloid beta oligomers block the learning-induced increase in hippocampal sharp wave-ripple rate and impair spatial memory formation
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Soluble amyloid beta oligomers block the learning-induced increase in hippocampal sharp wave-ripple rate and impair spatial memory formation

机译:可溶性淀粉样蛋白β低聚物阻断了学习诱导的海马尖锐波纹率的增加和损害空间记忆形成

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Post-learning hippocampal sharp wave-ripples (SWRs) generated during slow wave sleep are thought to play a crucial role in memory formation. While in Alzheimer's disease, abnormal hippocampal oscillations have been reported, the functional contribution of SWRs to the typically observed spatial memory impairments remains unclear. These impairments have been related to degenerative synaptic changes produced by soluble amyloid beta oligomers (Aβos) which, surprisingly, seem to spare the SWR dynamics during routine behavior. To unravel a potential effect of Aβos on SWRs in cognitively-challenged animals, we submitted vehicle- and Aβo-injected mice to spatial recognition memory testing. While capable of forming short-term recognition memory, Aβ mice exhibited faster forgetting, suggesting successful encoding but an inability to adequately stabilize and/or retrieve previously acquired information. Without prior cognitive requirements, similar properties of SWRs were observed in both groups. In contrast, when cognitively challenged, the post-encoding and -recognition peaks in SWR occurrence observed in controls were abolished in Aβ mice, indicating impaired hippocampal processing of spatial information. These results point to a crucial involvement of SWRs in spatial memory formation and identify the Aβ-induced impairment in SWRs dynamics as a disruptive mechanism responsible for the spatial memory deficits associated with Alzheimer's disease.
机译:在慢波睡眠期间产生的后学习海马尖锐波纹(SWRS)被认为在记忆形成中发挥至关重要的作用。虽然在阿尔茨海默病的疾病中,报告了异常的海马振荡,但SWR对通常观察到的空间记忆障碍的功能贡献仍不清楚。这些损伤与可溶性淀粉样蛋白β低聚物(AβOS)产生的退行性突触变化有关,令人惊讶的是,似乎在常规行为期间播放SWR动态。为了解开Aβ在认知挑战动物中的SWR上的潜在影响,我们将载体和Aβ注射的小鼠提交到空间识别记忆测试。虽然能够形成短期识别记忆,但Aβ小鼠表现出更快的遗忘,表明成功编码,而是无法充分稳定和/或检索先前获取的信息。如果没有先前的认知要求,两组中观察到类似SWR的性质。相反,当认知地攻击时,在Aβ小鼠中消除了在对照中观察到的SWR发生后的编码后和预防峰,表明空间信息的海马处理受损。这些结果指出了SWR在空间记忆形成中的关键累及,并确定SWRS动态的Aβ诱导的损伤作为负责与阿尔茨海默病相关的空间记忆缺陷的破坏性机制。

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