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首页> 外文期刊>Behavioural Brain Research: An International Journal >Spatial learning and memory impairment and increased locomotion in a transgenic amyloid precursor protein mouse model of Alzheimer's disease.
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Spatial learning and memory impairment and increased locomotion in a transgenic amyloid precursor protein mouse model of Alzheimer's disease.

机译:在阿尔茨海默氏病的转基因淀粉样蛋白前体蛋白小鼠模型中,空间学习和记忆障碍以及运动增加。

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This study provides an examination of spatial learning and a behavioral assessment of irritability and locomotion in TgCRND8 mice, an amyloid precursor protein transgenic model of Alzheimer's disease. Performance was assessed using the Barnes maze, the touch escape test, and an open-field test. While past research focused primarily on 2-5-month-old TgCRND8 mice, the present study used an older age cohort (9-month-old female mice), in addition to a 4-month-old cohort of both transgenic (Tg) and wildtype female mice. Both younger and older Tg mice displayed poor spatial learning in the Barnes maze task compared to their wildtype littermates, as demonstrated by significantly longer latencies and more errors both during acquisition and at a 2-week retest. No differences in irritability were found between Tg and control mice in the younger cohort; however, older Tg mice displayed significantly higher irritability compared with wildtype littermates, as measured by the touch escape test. Additionally, Tg mice of both age cohorts showed increased locomotion and slowed habituation during a 60-min open-field test over 3 days of testing. These results demonstrate that TgCRND8 mice show significant deficits in spatial and nonspatial behavioral tasks at advanced stages of amyloid pathology.
机译:这项研究为TgCRND8小鼠(阿尔茨海默氏病的淀粉样蛋白前体蛋白转基因模型)提供了空间学习检查,并对易怒性和运动能力进行了行为评估。使用Barnes迷宫,接触逃逸测试和开放测试来评估性能。尽管过去的研究主要针对2-5个月大的TgCRND8小鼠,但本研究使用了两个转基因(Tg)的4个月大的队列(9个月大的雌性小鼠)。和野生雌性小鼠。与野生型同窝幼仔相比,年轻和老年Tg小鼠在Barnes迷宫任务中均显示出较差的空间学习能力,这在采集和2周重新测试期间均表现出更长的潜伏期和更多的错误,从而证明了这一点。在较年轻的队列中,Tg和对照小鼠之间没有发现烦躁性差异;然而,通过触摸逃避测试,与野生型同窝仔相比,年长的Tg小鼠表现出明显更高的易怒性。此外,两个年龄段的Tg小鼠在3天的测试中进行60分钟的野外测试期间均显示出增加的运动能力和减慢了的习性。这些结果表明,TgCRND8小鼠在淀粉样蛋白病理学的晚期显示出空间和非空间行为任务的显着缺陷。

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