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自闭症催产素受体缺陷模型小鼠对新奇事物的探索能力受损及纹状体改变。

Impaired approach to novelty and striatal alterations in the oxytocin receptor deficient mouse model of autism.

机构信息

CNR, Institute of Neuroscience, Milan, Italy; Department of Medical Biotechnology and Translational Medicine, Università degli Studi di Milano, Milan, Italy.

Department of Medical Biotechnology and Translational Medicine, Università degli Studi di Milano, Milan, Italy.

出版信息

Horm Behav. 2019 Aug;114:104543. doi: 10.1016/j.yhbeh.2019.06.007. Epub 2019 Jul 19.

Abstract

Long-standing studies established a role for the oxytocin system in social behavior, social reward, pair bonding and affiliation. Oxytocin receptors, implicated in pathological conditions affecting the social sphere such as autism spectrum disorders, can also modulate cognitive processes, an aspect generally overlooked. Here we examined the effect of acute (pharmacological) or genetic (Oxtr) inactivation of oxytocin receptor-mediated signaling, in male mice, in several cognitive tests. In the novel object recognition test, both oxytocin receptor antagonist treated wild type animals and Oxtr mice lacked the typical preference for novelty. Oxtr mice even preferred the familiar object; moreover, their performance in the Morris water maze did not differ from wild types, suggesting that oxytocin receptor inactivation did not disrupt learning. Because the preference for novel objects could be rescued in Oxtr mice with longer habituation periods, we propose that the loss of novelty preferences following Oxtr inactivation is due to altered processing of novel contextual information. Finally, we observed an increased expression of excitatory synaptic markers in the striatum of Oxtr mice and a greater arborization and higher number of spines/neuron in the dorsolateral area of this structure, which drives habit formation. Our data also indicate a specific reshaping of dorsolateral striatal spines in Oxtr mice after exposure to a novel environment, which might subtend their altered approach to novelty, and support previous work pointing at this structure as an important substrate for autistic behaviors.

摘要

长期以来的研究确立了催产素系统在社会行为、社会奖励、伴侣关系和依恋中的作用。催产素受体参与了影响社交领域的病理状况,如自闭症谱系障碍,也可以调节认知过程,这一方面通常被忽视。在这里,我们在雄性小鼠中检查了急性(药理学)或遗传(Oxtr)失活催产素受体介导的信号转导对几种认知测试的影响。在新物体识别测试中,催产素受体拮抗剂处理的野生型动物和 Oxtr 小鼠都缺乏对新奇性的典型偏好。Oxtr 小鼠甚至更喜欢熟悉的物体;此外,它们在 Morris 水迷宫中的表现与野生型没有区别,这表明催产素受体失活不会干扰学习。由于较长的习惯化期可以挽救 Oxtr 小鼠对新物体的偏好,我们提出 Oxtr 失活后对新物体的偏好丧失是由于对新的上下文信息处理的改变。最后,我们观察到 Oxtr 小鼠纹状体中兴奋性突触标记物的表达增加,并且该结构的背外侧区域的分支和更多的棘突/神经元数量增加,这驱动了习惯的形成。我们的数据还表明,在暴露于新环境后,Oxtr 小鼠的背外侧纹状体棘突发生了特定的重塑,这可能会改变它们对新奇的接近方式,并支持以前的工作,即该结构是自闭症行为的重要基础。

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