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Social deficits in the AY-9944 mouse model of atypical absence epilepsy

机译:AY-9944鼠标模型的社会赤字,非典型缺席癫痫

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Atypical absence epilepsy (AAE) showing slow spike-and-wave discharges (SWD) is characterized by severely abnormal cognition and neurodevelopmental or neurological outcomes in humans. However, despite the severe behavioral outcomes in AAE, the relationship between AAE and social-behavioral dysfunctions has not defined well, either experimentally or in patients with AAE. Experimentally, AAE can be produced by administering AY-9944 (AY), a cholesterol biosynthesis inhibitor. In this study, we characterized social behavior in the AY mouse model of AAE. AAE in the mouse was induced by repeated postnatal administration of AY every 6 days from postnatal day (P) 2 to P20. AY-treated mice exhibited spontaneous, recurrent, and synchronous SWD (4-5 Hz) in electroencephalographic recordings. AY-treated mice performed tasks involving sociability/social novelty preference, social interaction with a juvenile conspecific, observational fear, and resident-intruder aggression. They showed behavioral dysfunction in social interactions with a juvenile conspecific and sociability/social novelty preference tasks. They also exhibited reduced social fear learning in observational fear conditioning. Interestingly, they showed increased levels of offensive behaviors in a resident-intruder task. However, AY-treated mice displayed normal levels of anxiety in light/dark transition and the elevated plus maze tasks, and showed slightly increased locomotor activity in an open-field task. These results demonstrate social dysfunction in the AY-induced AAE model. Our study of social behavior can also provide valuable information about Lennox-Gastaut syndrome, in which AAE is a component. Thus, our findings may help to understand behavioral pathogenesis or characteristics of patients with AAE. (c) 2012 Elsevier B.V. All rights reserved.
机译:非典型缺乏癫痫(AAE)显示缓慢尖峰和波浪排放(SWD)的特征在于人类的严重认知和神经发育或神经病学结果严重。然而,尽管AAE中的严重行为结果,但是,AAE和社会行为功能障碍之间的关系尚未确定,实验或患者患者。通过实验,可以通过施用AY-9944(AY),胆固醇生物合成抑制剂来生产AAE。在这项研究中,我们在AY的AAE鼠标模型中表征了社会行为。通过从后期(P)2至P20的每6天反复出生地施用鼠标诱导小鼠的AAE。 AY治疗的小鼠在脑电图记录中表现出自发性,复发性和同步的SWD(4-5Hz)。 AY对待的小组执行了涉及社会性/社会新颖性偏好的任务,与少年同一,观察恐惧和居民入侵者侵略的社会互动。他们表现出与少年同一和社会性/社会新颖性偏好任务的社会互动中的行为功能障碍。他们在观察恐惧调理中也表现出减少社会恐惧学习。有趣的是,他们在居民入侵者任务中表现出令人反感行为的增加。然而,AY治疗的小鼠在光/暗过渡和升高的加上迷宫任务中显示出正常的焦虑水平,并且在开放场任务中显示出略微增加的运动活动。这些结果表明了AY诱导的AAE模型中的社会功能障碍。我们对社会行为的研究还可以提供有关Lennox-Gastaut综合征的宝贵信息,其中AAE是一个组成部分。因此,我们的研究结果可能有助于了解AAE患者的行为发病机制或特征。 (c)2012 Elsevier B.V.保留所有权利。

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