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CA3在社会识别记忆中的作用。

A role for CA3 in social recognition memory.

作者信息

Chiang Ming-Ching, Huang Arthur J Y, Wintzer Marie E, Ohshima Toshio, McHugh Thomas J

机构信息

Laboratory for Circuit and Behavioral Physiology, RIKEN Brain Science Institute, Wako-shi, Saitama, Japan; Laboratory for Molecular Brain Science, Department of Life Sciences and Biomedical Science, Graduate School of Advanced Science and Engineering, Waseda University, Shinjuku-ku, Tokyo, Japan.

Laboratory for Circuit and Behavioral Physiology, RIKEN Brain Science Institute, Wako-shi, Saitama, Japan.

出版信息

Behav Brain Res. 2018 Nov 15;354:22-30. doi: 10.1016/j.bbr.2018.01.019. Epub 2018 Feb 3.

Abstract

Social recognition memory is crucial for survival across species, underlying the need to correctly identify conspecifics, mates and potential enemies. In humans the hippocampus is engaged in social and episodic memory, however the circuit mechanisms of social memory in rodent models has only recently come under scrutiny. Work in mice has established that the dorsal CA2 and ventral CA1 regions play critical roles, however a more comprehensive comparative analyses of the circuits and mechanisms required has not been reported. Here we employ conditional genetics to examine the differential contributions of the hippocampal subfields to social memory. We find that the deletion of NMDA receptor subunit 1 gene (NR1), which abolishes NMDA receptor synaptic plasticity, in CA3 pyramidal cells led to deficits in social memory; however, mice lacking the same gene in DG granule cells performed indistinguishable from controls. Further, we use conditional pharmacogenetic inhibition to demonstrate that activity in ventral, but not dorsal, CA3 is necessary for the encoding of a social memory. These findings demonstrated CA3 pyramidal cell plasticity and transmission contribute to the encoding of social stimuli and help further identify the distinct circuits underlying the role of the hippocampus in social memory.

摘要

社会识别记忆对于物种生存至关重要,它是正确识别同种个体、配偶和潜在敌人的基础。在人类中,海马体参与社会记忆和情景记忆,然而,啮齿动物模型中社会记忆的神经回路机制直到最近才受到审视。对小鼠的研究已经证实,背侧CA2区和腹侧CA1区起着关键作用,然而,尚未有关于所需神经回路和机制的更全面比较分析的报道。在这里,我们采用条件遗传学方法来研究海马亚区对社会记忆的不同贡献。我们发现,CA3锥体细胞中NMDA受体亚基1基因(NR1)的缺失消除了NMDA受体突触可塑性,导致社会记忆缺陷;然而DG颗粒细胞中缺乏相同基因的小鼠表现与对照组无异。此外,我们使用条件性药物遗传学抑制来证明,腹侧而非背侧CA3的活动对于社会记忆的编码是必要的。这些发现表明CA3锥体细胞的可塑性和传递有助于社会刺激的编码,并有助于进一步识别海马体在社会记忆中所起作用的不同神经回路。

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