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缺乏突触结合蛋白 III 的小鼠表现出明显记忆和条件性恐惧异常。

Mice lacking synapsin III show abnormalities in explicit memory and conditioned fear.

机构信息

Department of Psychiatry and Human Behavior, Brown University, BioMedical Center, Providence, RI 02912, USA.

出版信息

Genes Brain Behav. 2010 Apr;9(3):257-68. doi: 10.1111/j.1601-183X.2009.00555.x. Epub 2009 Nov 24.

Abstract

Synapsin III is a neuron-specific phosphoprotein that plays an important role in synaptic transmission and neural development. While synapsin III is abundant in embryonic brain, expression of the protein in adults is reduced and limited primarily to the hippocampus, olfactory bulb and cerebral cortex. Given the specificity of synapsin III to these brain areas and because it plays a role in neurogenesis in the dentate gyrus, we investigated whether it may affect learning and memory processes in mice. To address this point, synapsin III knockout mice were examined in a general behavioral screen, several tests to assess learning and memory function, and conditioned fear. Mutant animals displayed no anomalies in sensory and motor function or in anxiety- and depressive-like behaviors. Although mutants showed minor alterations in the Morris water maze, they were deficient in object recognition 24 h and 10 days after training and in social transmission of food preference at 20 min and 24 h. In addition, mutants displayed abnormal responses in contextual and cued fear conditioning when tested 1 or 24 h after conditioning. The synapsin III knockout mice also showed aberrant responses in fear-potentiated startle. As synapsin III protein is decreased in schizophrenic brain and because the mutant mice do not harbor obvious anatomical deficits or neurological disorders, these mutants may represent a unique neurodevelopmental model for dissecting the molecular pathways that are related to certain aspects of schizophrenia and related disorders.

摘要

突触结合蛋白 III 是一种神经元特异性磷酸蛋白,在突触传递和神经发育中发挥重要作用。虽然突触结合蛋白 III 在胚胎脑中含量丰富,但在成人中的表达减少,主要局限于海马体、嗅球和大脑皮层。鉴于突触结合蛋白 III 对这些脑区的特异性,以及它在齿状回神经发生中的作用,我们研究了它是否可能影响小鼠的学习和记忆过程。为了解决这一问题,我们在一般行为筛查、几项评估学习和记忆功能的测试以及条件性恐惧测试中检查了突触结合蛋白 III 敲除小鼠。突变动物在感觉和运动功能、焦虑和抑郁样行为方面没有异常。尽管突变体在 Morris 水迷宫中表现出轻微改变,但在训练后 24 小时和 10 天的物体识别以及在 20 分钟和 24 小时的食物偏好社会传递中表现出缺陷。此外,在条件性恐惧测试中,当在条件作用后 1 小时或 24 小时测试时,突变体在情境和线索恐惧条件下的反应异常。突触结合蛋白 III 敲除小鼠在恐惧增强性惊跳反应中也表现出异常反应。由于突触结合蛋白 III 蛋白在精神分裂症大脑中减少,并且突变体小鼠没有明显的解剖缺陷或神经障碍,因此这些突变体可能代表一种独特的神经发育模型,用于剖析与精神分裂症和相关障碍的某些方面相关的分子途径。

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