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躁狂症潜在新小鼠模型的行为和药理学评估。

Behavioral and pharmacological assessment of a potential new mouse model for mania.

机构信息

Department of Psychiatry, University of Illinois at Chicago, Chicago, IL, United States.

出版信息

Physiol Behav. 2011 Jun 1;103(3-4):376-83. doi: 10.1016/j.physbeh.2011.03.005. Epub 2011 Mar 22.

Abstract

Bipolar disorder (BPD) is a devastating long-term disease for which a significant symptom is mania. Rodent models for mania include psychostimulant-induced hyperactivity and single gene alterations, such as in the Clock or DAT genes, but there is still a pressing need for additional models. Recently, our lab isolated a line of mice, termed Madison (MSN), that exhibit behavioral characteristics that may be analogous to symptoms of mania. In this study we quantified possible traits for mania and tested the response to common anti-BPD drugs in altering the behavioral profiles observed in this strain. Relative to other mouse lines, MSN mice showed significant elevations of in-cage hyperactivity levels, significant decreases in daytime sleep, and significant increases in time swimming in the forced swim test. In terms of sexual behavior, the MSN mice showed significantly higher number of mounts and a trend toward higher time mounting. In separate studies, olanzapine and lithium (or respective controls) were administered to MSN mice for at least 2weeks and response to treatments was evaluated. Olanzapine (1mg/kg/day) significantly decreased in-cage hyperactivity and significantly increased time sleeping. Lithium (0.2-0.4% in food) significantly decreased in-cage hyperactivity. Given the behavioral phenotypes and the response to anti-BPD treatments, we propose that MSN mice may provide a possible new model for understanding the neural and genetic basis of phenotypes related to mania and for developing pharmaceutical treatments.

摘要

双相情感障碍(BPD)是一种严重的长期疾病,其主要症状之一是躁狂。躁狂的啮齿动物模型包括精神兴奋剂引起的多动和单个基因改变,如 Clock 或 DAT 基因,但仍迫切需要其他模型。最近,我们实验室分离出一种名为 Madison(MSN)的小鼠品系,其表现出的行为特征可能与躁狂症状类似。在这项研究中,我们量化了可能与躁狂有关的特征,并测试了常见抗 BPD 药物对改变该品系观察到的行为特征的反应。与其他小鼠品系相比,MSN 小鼠的笼内多动水平显著升高,白天睡眠时间显著减少,强迫游泳试验中游泳时间显著增加。在性行为方面,MSN 小鼠的交配次数明显增加,交配时间也有增加的趋势。在单独的研究中,奥氮平(olanzapine)和锂(或各自的对照)至少给 MSN 小鼠施用 2 周,并评估了对治疗的反应。奥氮平(1mg/kg/天)显著降低了笼内多动,显著增加了睡眠时间。锂(食物中 0.2-0.4%)显著降低了笼内多动。鉴于行为表型和对抗 BPD 治疗的反应,我们提出 MSN 小鼠可能为理解与躁狂相关的表型的神经和遗传基础以及开发药物治疗方法提供一个可能的新模型。

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