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Memory formation and retention are affected in adult miR-132/212 knockout mice

机译:内存形成和保留在成人miR-132/212敲除小鼠中受到影响

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The miR-132/212 family is thought to play an important role in neural function and plasticity, while its misregulation has been observed in various neurodegenerative disorders. In this study, we analyzed 6-month-old miR-132/212 knockout mice in a battery of cognitive and non-cognitive behavioral tests. No significant changes were observed in reflexes and basic sensorimotor functions as determined by the SHIRPA primary screen. Accordingly, miR-132/212 knockout mice did not differ from wild-type controls in general locomotor activity in an open-field test. Furthermore, no significant changes of anxiety were measured in an elevated plus maze task. However, the mutant mice showed retention phase defects in a novel object recognition test and in the T-water maze. Moreover, the learning and probe phases in the Barnes maze were clearly altered in knockout mice when compared to controls. Finally, changes in BDNF, CREB, and MeCP2 were identified in the miR-132/212-deficient mice, providing a potential mechanism for promoting memory loss. Taken together, these results further strengthen the role of miR-132/212 in memory formation and retention, and shed light on the potential consequences of its deregulation in neurodegenerative diseases. (C) 2015 Elsevier B.V. All rights reserved.
机译:MiR-132/212家族被认为在神经功能和可塑性中发挥重要作用,而在各种神经退行性障碍中已经观察到其误解。在这项研究中,我们在认知和非认知行为测试的电池中分析了6个月大的miR-132/212敲除小鼠。在Shirpa主屏幕确定的反射和基本感觉运动功能中没有观察到显着变化。因此,MiR-132/212敲除小鼠与开放场测试中的通用运动活动中的野生型对照没有不同。此外,在升高的加迷宫任务中没有测量焦虑的显着变化。然而,突变小鼠在新型物体识别试验和T水迷宫中显示出保持阶段缺陷。此外,与对照相比,在敲除小鼠中明显改变了Barnes迷宫中的学习和探针阶段。最后,在MiR-132/212缺陷小鼠中鉴定了BDNF,CREB和MECP2的变化,提供了促进内存损耗的潜在机制。总之,这些结果进一步加强了miR-132/212在记忆形成和保留中的作用,并阐明了其放松生命疾病的潜在后果。 (c)2015 Elsevier B.v.保留所有权利。

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