小鼠早期发育过程中的慢性社会压力与反社会虐待行为有关。

Encephalitis (Seoul, Korea) Pub Date : 2022-10-01 Epub Date: 2022-09-21 DOI:10.47936/encephalitis.2022.00038
Daejong Jeon, Sangwoo Kim, Jiye Choi, Ah Reum Yang, Sang Kun Lee, Kon Chu
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引用次数: 0

摘要

目的:早年的生活压力会导致大脑发炎,并影响成年后的社会行为。在人类中,受虐待(受凌辱或被忽视)的儿童在成年后往往会表现出反社会行为,包括暴力和虐待狂行为。然而,虐待行为是否会发生在啮齿类动物身上还不得而知。在此,我们开发了一种检测系统来评估小鼠的同种虐待行为:为了评估虐待行为,我们设计了一个由透明隔板隔开的两室装置,其中一室设有戳鼻孔,戳鼻孔会触发脚部冲击另一室。利多卡因用于抑制体内神经活动。大脑振荡通过脑电图进行研究。酶联免疫吸附试验用于蛋白质检测。小鼠模型依次接受母体分离(MS)、社会挫败(SD)和社会隔离(SI)(MS/SD/SI 模型):结果:前扣带回皮层和内侧前额叶皮层失活会增加戳鼻子的程度。虐待行为引起催产素、皮质酮和脑源性神经营养因子水平的变化。在实验过程中,MS/SD/SI小鼠表现出更持久的杵鼻行为,从而导致对室小鼠的足部冲击增加。MS/SD/SI小鼠的大脑振荡异常:结论:MS/SD/SI模型和虐待行为测定不仅可用于研究儿童期社会压力与成年期反社会行为之间的关系,还可用于研究精神变态等脑部疾病的病因、病理或治疗。
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 during early development is involved in antisocial maltreatment behavior in mice.

Chronic social stress during early development is involved in antisocial maltreatment behavior in mice.

Chronic social stress during early development is involved in antisocial maltreatment behavior in mice.

Chronic social stress during early development is involved in antisocial maltreatment behavior in mice.

Purpose: Early-life stress can cause brain inflammation and affect social behavior in adulthood. In humans, maltreated (abused or neglected) children often exhibit antisocial behavior, including violent and sadistic behavior, in adulthood. However, it is unknown whether maltreatment behavior occurs in rodents. Here, we developed an assay system to evaluate conspecific maltreatment behavior in the mouse.

Methods: To assess maltreatment behavior, we devised a two-chamber apparatus separated by a transparent partition, in which one chamber was provided with a nose-poking hole that would trigger foot shocks onto the other. Lidocaine was used to inhibit neural activity in vivo. Brain oscillations were investigated by electroencephalograph. Enzyme-linked immunosorbent assay was used for protein assay. The mouse model was sequentially subjected to maternal separation (MS), social defeat (SD), and social isolation (SI) in that order (MS/SD/SI model).

Results: Inactivation of the anterior cingulate cortex and medial prefrontal cortex increased the level of nose-poking. Maltreatment behavior provoked changes in oxytocin, corticosterone, and brain-derived neurotrophic factor levels. MS/SD/SI mice exhibited more sustained nose-poking behavior during the experiment, resulting in increased foot shocks to the mouse in the opposite chamber. Abnormal brain oscillations were observed in the MS/SD/SI mice.

Conclusion: The MS/SD/SI model and maltreatment-behavior assay may be useful not only to study the relationship between social stress in childhood and antisocial behavior in adulthood, but also for study of etiology, pathology, or treatment for brain disorders, such as psychopathy.

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