首页> 外文期刊>Neurobiology of learning and memory >Exploratory, anxiety and spatial memory impairments are dissociated in mice lacking the LPA1 receptor.
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Exploratory, anxiety and spatial memory impairments are dissociated in mice lacking the LPA1 receptor.

机译:在缺乏LPA1受体的小鼠中,探索性,焦虑性和空间记忆障碍得以消除。

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摘要

Lysophosphatidic acid (LPA) is a new, intercellular signalling molecule in the brain that has an important role in adult hippocampal plasticity. Mice lacking the LPA(1) receptor exhibit motor, emotional and cognitive alterations. However, the potential relationship among these concomitant impairments was unclear. Wild-type and maLPA(1)-null mice were tested on the hole-board for habituation and spatial learning. MaLPA(1)-null mice exhibited reduced exploration in a novel context and a defective intersession habituation that also revealed increased anxiety-like behaviour throughout the hole-board testing. In regard to spatial memory, maLPA(1) nulls failed to reach the controls' performance at the end of the reference memory task. Moreover, their defective working memory on the first training day suggested a delayed acquisition of the task's working memory rule, which is also a long term memory component. The temporal interval between trials and the task's difficulty may explain some of the deficits found in these mice. Principal components analysis revealed that alterations found in each behavioural dimension were independent. Therefore, exploratory and emotional impairments did not account for the cognitive deficits that may be attributed to maLPA(1) nulls' hippocampal malfunction.
机译:溶血磷脂酸(LPA)是大脑中一种新型的细胞间信号分子,在成人海马可塑性中具有重要作用。缺乏LPA(1)受体的小鼠表现出运动,情绪和认知改变。但是,这些伴随损害之间的潜在关系尚不清楚。在孔板上测试了野生型和maLPA(1)-null小鼠的习惯性和空间学习能力。 MaLPA(1)空小鼠表现出减少的探索在一个新的上下文和有缺陷的休会习惯,这也表明整个孔板测试中增加了类似焦虑的行为。关于空间内存,在参考内存任务结束时,maLPA(1)空值无法达到控件的性能。此外,他们在第一个训练日的工作记忆缺陷表明建议延迟获取任务的工作记忆规则,这也是长期记忆的组成部分。试验与任务难度之间的时间间隔可以解释这些小鼠中发现的某些缺陷。主成分分析表明,在每个行为维度上发现的变化都是独立的。因此,探索性和情感性障碍并不能解决可能归因于maLPA(1)nulls海马功能障碍的认知缺陷。

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