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Lsamp基因的缺失会导致在新环境中行为激活过度。

Genetic deletion of Lsamp causes exaggerated behavioral activation in novel environments.

作者信息

Catania Elizabeth Haldeman, Pimenta Aurea, Levitt Pat

机构信息

Neuroscience Graduate Program, Vanderbilt University, Nashville, TN 37232, USA.

出版信息

Behav Brain Res. 2008 Apr 9;188(2):380-90. doi: 10.1016/j.bbr.2007.11.022. Epub 2007 Dec 7.

Abstract

The limbic system-associated membrane protein (LAMP) is a GPI-anchored cell adhesion molecule expressed heavily in limbic and limbic-associated regions of the developing and adult brain. Experimental studies show that LAMP promotes the growth of limbic neurons and guides the projections of limbic fibers. In order to examine the functional consequences of disrupting limbic circuit assembly, we generated a mouse line in which the Lsamp gene encoding LAMP was deleted. Basic neuroanatomical organization and sensory and motor development are normal in Lsamp(-/-) mice. The most profound change in behavior in both male and female Lsamp(-/-) mice is a heightened reactivity to novelty exhibited in several behavioral tests. Lsamp(-/-) mice display hyperactivity in a novel arena and both sexes habituate to the same activity levels as their wild type littermates, but at different rates. In the elevated plus maze, Lsamp(-/-) mice exhibit increased total arm entries, with a bias towards the open arms; they spend more time in the open arms and have a substantial increase in the amount of risk assessment in unprotected areas of the maze. In the y-maze, Lsamp(-/-) mice exhibit characteristic hyperactivity and a decreased level of spontaneous alternation during the period when their novelty-induced hyperactivity is at its peak. We hypothesize that Lsamp(-/-) mice may not simply exhibit a decrease in anxiety, but may have a heightened, and possibly maladaptive, response to novel environmental stressors. Genetic deletion of Lsamp may thus cause circumscribed changes in the fine connectivity of specific circuits that underlie these behaviors.

摘要

边缘系统相关膜蛋白(LAMP)是一种糖基磷脂酰肌醇锚定的细胞粘附分子,在发育中和成年大脑的边缘及边缘相关区域大量表达。实验研究表明,LAMP促进边缘神经元的生长并引导边缘纤维的投射。为了研究破坏边缘回路组装的功能后果,我们构建了一个小鼠品系,其中编码LAMP的Lsamp基因被删除。Lsamp基因敲除(-/-)小鼠的基本神经解剖组织结构以及感觉和运动发育均正常。雄性和雌性Lsamp基因敲除(-/-)小鼠行为上最显著的变化是在多项行为测试中对新事物表现出更高的反应性。Lsamp基因敲除(-/-)小鼠在新环境中表现出多动,两性都会适应与野生型同窝小鼠相同的活动水平,但速度不同。在高架十字迷宫实验中,Lsamp基因敲除(-/-)小鼠进入总臂数增加,且偏向于开放臂;它们在开放臂中停留的时间更长,并且在迷宫无保护区域的风险评估量大幅增加。在Y迷宫实验中,当Lsamp基因敲除(-/-)小鼠由新事物诱导的多动达到峰值时,它们表现出典型的多动,并且自发交替水平降低。我们推测,Lsamp基因敲除(-/-)小鼠可能不仅仅表现出焦虑降低,而是对新的环境应激源有增强的、可能是适应不良的反应。因此,Lsamp基因的缺失可能会导致这些行为背后特定回路精细连接性的局限性变化。

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