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首页> 外文期刊>Neuroscience: An International Journal under the Editorial Direction of IBRO >Learning deficits in forebrain-restricted brain-derived neurotrophic factor mutant mice.
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Learning deficits in forebrain-restricted brain-derived neurotrophic factor mutant mice.

机译:前脑受限的脑源性神经营养因子突变小鼠的学习缺陷。

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Brain-derived neurotrophic factor (BDNF) participates in synaptic plasticity and the adaptive changes in the strength of communication between neurons thought to underlie aspects of behavioral adaptation. By selectively deleting BDNF from the forebrain of mice using the Cre site-specific DNA recombinase, we were able to study the requirements for BDNF in behaviors such as learning and anxiety. Early-onset forebrain-restricted BDNF mutant mice (Emx-BDNF(KO)) that develop in the absence of BDNF in the dorsal cortex, hippocampus, and parts of the ventral cortex and amygdala failed to learn the Morris Water Maze task, a hippocampal-dependent visuo-spatial learning task. Freezing during all phases of cued-contextual fear conditioning, a behavioral task designed to study hippocampal-dependent associative learning, was enhanced. These mice learned a brightness discrimination task well but were impaired in a more difficult pattern discrimination task. Emx-BDNF(KO) mice did not exhibit altered sensory processing and gating, as measured by the acoustic startle response or prepulse inhibition of the startle response. Although they were less active in an open-field arena, they did not show alterations in anxiety, as measured in the elevated-plus maze, black-white chamber or mirrored chamber tasks. Combined, these data indicate that although an absence of forebrain BDNF does not disrupt acoustic sensory processing or alter baseline anxiety, specific forms of learning are severely impaired.
机译:脑源性神经营养因子(BDNF)参与突触可塑性和神经元之间交流强度的适应性变化,这些行为被认为是行为适应方面的基础。通过使用Cre位点特异性DNA重组酶选择性地从小鼠前脑中删除BDNF,我们能够研究BDNF在学习和焦虑等行为中的需求。前背受限的BDNF突变小鼠(Emx-BDNF(KO))在背皮质,海马以及腹皮质和杏仁核的部分区域缺少BDNF的情况下发育,因此未能学习Morris Water Maze任务(海马)依赖的视觉空间学习任务。在提示语境恐惧调节的所有阶段都冻结,这项旨在研究海马依赖性学习的行为任务得到了加强。这些小鼠很好地学习了亮度识别任务,但在较困难的模式识别任务中受到了损害。 Emx-BDNF(KO)小鼠没有表现出改变的感觉过程和门控,通过听觉惊吓反应或惊吓反应的前脉冲抑制来测量。尽管它们在露天场地上的活动性较差,但在高架迷宫,黑白密室或镜像密室任务中,它们并未显示出焦虑的变化。综合来看,这些数据表明,尽管缺乏前脑BDNF并不会破坏声音感觉过程或改变基线焦虑,但严重损害了特定形式的学习。

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