幼年时期的慢性社会压力会使小鼠容易产生反社会的虐待行为。

Encephalitis (Seoul, Korea) Pub Date : 2024-04-01 Epub Date: 2024-03-06 DOI:10.47936/encephalitis.2023.00199
Daejong Jeon, Sangwoo Kim, Sang Kun Lee, Kon Chu
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引用次数: 0

摘要

目的:在之前的研究中,我们开发了一套检测系统,利用施暴者-受害者范式来评估同种小鼠的反社会虐待行为。我们还通过模拟虐待或凌辱儿童的行为建立了虐待行为小鼠模型。在此,我们将使用抗攻击性药物和抗精神病药物进一步研究小鼠的反社会行为:方法:将依次接受母体分离(MS)、社会挫败(SD)和社会隔离(SI)的模型小鼠(MS/SD/SI 模型)置于虐待行为任务中。MS/SD/SI小鼠分别接受催产素(OXY)、氯氮平(CLZ)、氟哌啶醇(HAL)和8-羟基-2-(二正丙基氨基)四氢呋喃(8-OH-DPAT)治疗。蛋白质分析采用了 Western 印迹法和酶联免疫吸附法:相当一部分 MS/SD/SI 模型小鼠(46% 的雄性小鼠和 40% 的雌性小鼠)的戳鼻次数高于对照组。OXY或8-OH-DPAT处理可减少MS/SD/SI小鼠捅鼻子的次数,而HAL则会增加捅鼻子的次数。CLZ不会影响MS/SD/SI小鼠戳鼻子的次数。有趣的是,虽然MS/SD/SI小鼠体内的OXY水平与对照组相似,但MS/SD/SI小鼠体内的OXY受体量却较低。MS/SD/SI小鼠的5-HT1A受体数量也有所减少:结论:童年时期的慢性社会压力可能会导致小鼠出现反社会行为。我们的虐待行为检测系统,包括 MS/SD/SI 模型,是研究和筛选与反社会或精神病行为相关的脑部疾病药物的良好动物系统。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Chronic social stress in early life can predispose mice to antisocial maltreating behavior.

Chronic social stress in early life can predispose mice to antisocial maltreating behavior.

Chronic social stress in early life can predispose mice to antisocial maltreating behavior.

Chronic social stress in early life can predispose mice to antisocial maltreating behavior.

Purpose: In our previous study, we developed an assay system to evaluate antisocial maltreating behavior of conspecific mice using a perpetrator-victim paradigm. We also generated a mouse model for the maltreating behavior by mimicking child maltreatment or abuse. Here, we further investigate the antisocial behavior using anti-aggressive and antipsychotic drugs.

Methods: Model mice sequentially subjected to maternal separation (MS), social defeat (SD), and social isolation (SI) in that order (MS/SD/SI model) were subjected to a maltreating behavioral task. The MS/SD/SI mice were treated with oxytocin (OXY), clozapine (CLZ), haloperidol (HAL), and 8-hydroxy-2-(di-n-propylamino)tetralin (8-OH-DPAT). Western blotting and enzyme-linked immunosorbent assay were used for protein analysis.

Results: A substantial portion of the MS/SD/SI model mice (46% of males and 40% of females) showed a higher number of nose pokes than the control. OXY or 8-OH-DPAT treatment reduced the high number of nose pokes by the MS/SD/SI mice, whereas HAL increased it. CLZ did not affect the number of nose pokes by the MS/SD/SI mice. Interestingly, although the OXY level in the MS/SD/SI mice was similar to that in the control, the amount of OXY receptor was lower in the MS/SD/SI mice. The amount of 5-HT1A receptor was also decreased in the MS/SD/SI mice.

Conclusion: Chronic social stress in childhood might predispose a mouse to antisocial behavior. Our maltreating behavior assay system, including the MS/SD/SI model, is a good animal system for research on and drug screening for brain disorders associated with antisocial or psychotic behavior.

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