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2
Role of densin-180 in mouse ventral hippocampal neurons in 24-hr retention of contextual fear conditioning.densin-180 在小鼠腹侧海马神经元中 24 小时保持情景性恐惧条件反射中的作用。
Brain Behav. 2020 Dec;10(12):e01891. doi: 10.1002/brb3.1891. Epub 2020 Oct 16.
3
False Opposing Fear Memories Are Produced as a Function of the Hippocampal Sector Where Glucocorticoid Receptors Are Activated.错误的对立恐惧记忆是作为糖皮质激素受体被激活的海马区的一个功能而产生的。
Front Behav Neurosci. 2020 Aug 26;14:144. doi: 10.3389/fnbeh.2020.00144. eCollection 2020.
4
Role of dorsal and ventral hippocampal muscarinic receptor activity in acquisition and retention of contextual fear conditioning.背侧和腹侧海马脑区毒蕈碱型乙酰胆碱受体活性在情景性恐惧条件反射获得和保持中的作用。
Behav Neurosci. 2020 Oct;134(5):460-470. doi: 10.1037/bne0000411.
5
Contextual fear memory retrieval by correlated ensembles of ventral CA1 neurons.腹侧 CA1 神经元相关神经元簇的情境性恐惧记忆检索。
Nat Commun. 2020 Jul 13;11(1):3492. doi: 10.1038/s41467-020-17270-w.
6
A Novel Sulfonamide, 4-FS, Reduces Ethanol Drinking and Physical Withdrawal Associated With Ethanol Dependence.一种新型磺胺类药物 4-FS 可减少与乙醇依赖相关的乙醇摄入和躯体戒断。
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Differential Phosphorylation of the Glucocorticoid Receptor in Hippocampal Subregions Induced by Contextual Fear Conditioning Training.情境恐惧条件训练诱导海马亚区糖皮质激素受体的差异磷酸化
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8
Effect of Alcohol on Hippocampal-Dependent Plasticity and Behavior: Role of Glutamatergic Synaptic Transmission.酒精对海马体依赖性可塑性及行为的影响:谷氨酸能突触传递的作用
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Sex Differences in Remote Contextual Fear Generalization in Mice.小鼠远程情境恐惧泛化中的性别差异
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异恶唑-9 可降低乙醇依赖雄性大鼠的增强恐惧反应和提取。

Isoxazole-9 reduces enhanced fear responses and retrieval in ethanol-dependent male rats.

机构信息

VA San Diego Healthcare System, San Diego, CA, USA.

Department of Pharmacology, Bowles Center for Alcohol Studies, University of North Carolina School of Medicine, Chapel Hill, NC, USA.

出版信息

J Neurosci Res. 2021 Nov;99(11):3047-3065. doi: 10.1002/jnr.24932. Epub 2021 Sep 8.

DOI:10.1002/jnr.24932
PMID:34496069
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC10112848/
Abstract

Plasticity in the dentate gyrus (DG) is strongly influenced by ethanol, and ethanol experience alters long-term memory consolidation dependent on the DG. However, it is unclear if DG plasticity plays a role in dysregulation of long-term memory consolidation during abstinence from chronic ethanol experience. Outbred male Wistar rats experienced 7 weeks of chronic intermittent ethanol vapor exposure (CIE). Seventy-two hours after CIE cessation, CIE and age-matched ethanol-naïve Air controls experienced auditory trace fear conditioning (TFC). Rats were tested for cue-mediated retrieval in the fear context either twenty-four hours (24 hr), ten days (10 days), or twenty-one days (21 days) later. CIE rats showed enhanced freezing behavior during TFC acquisition compared to Air rats. Air rats showed significant fear retrieval, and this behavior did not differ at the three time points. In CIE rats, fear retrieval increased over time during abstinence, indicating an incubation in fear responses. Enhanced retrieval at 21 days was associated with reduced structural and functional plasticity of ventral granule cell neurons (GCNs) and reduced expression of synaptic proteins important for neuronal plasticity. Systemic treatment with the drug Isoxazole-9 (Isx-9; small molecule that stimulates DG plasticity) during the last week and a half of CIE blocked altered acquisition and retrieval of fear memories in CIE rats during abstinence. Concurrently, Isx-9 modulated the structural and functional plasticity of ventral GCNs and the expression of synaptic proteins in the ventral DG. These findings identify that abstinence-induced disruption of fear memory consolidation occurs via altered plasticity within the ventral DG, and that Isx-9 prevented these effects.

摘要

齿状回(DG)的可塑性受乙醇的强烈影响,乙醇的体验改变了依赖 DG 的长期记忆巩固。然而,尚不清楚 DG 可塑性是否在慢性乙醇体验戒断期间长期记忆巩固失调中发挥作用。近交系雄性 Wistar 大鼠经历了 7 周的慢性间歇性乙醇蒸气暴露(CIE)。CIE 停止后 72 小时,CIE 和年龄匹配的乙醇-naive Air 对照经历了听觉痕迹恐惧条件反射(TFC)。大鼠在 24 小时(24 小时)、10 天(10 天)或 21 天(21 天)后在恐惧环境中进行线索介导的检索测试。与 Air 大鼠相比,CIE 大鼠在 TFC 获得期间表现出增强的冻结行为。Air 大鼠表现出明显的恐惧检索,并且这种行为在三个时间点没有差异。在 CIE 大鼠中,随着戒断时间的延长,恐惧检索增加,表明恐惧反应的潜伏期。21 天时的增强检索与腹侧颗粒细胞神经元(GCNs)的结构和功能可塑性降低以及对神经元可塑性很重要的突触蛋白表达降低有关。在 CIE 的最后一周半期间,全身给予伊唑唑-9(Isx-9;刺激 DG 可塑性的小分子)可阻止 CIE 大鼠在戒断期间改变恐惧记忆的获得和检索。同时,Isx-9 调节了腹侧 GCNs 的结构和功能可塑性以及腹侧 DG 中的突触蛋白表达。这些发现表明,戒断引起的恐惧记忆巩固中断是通过腹侧 DG 内的可塑性改变发生的,而 Isx-9 可预防这些影响。