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CREB 基因缺陷型小鼠在新环境中表现出抑制和低活性,且应激反应无变化。

CREB deficient mice show inhibition and low activity in novel environments without changes in stress reactivity.

作者信息

Hebda-Bauer Elaine K, Watson Stanley J, Akil Huda

机构信息

Mental Health Research Institute, University of Michigan, 205 Zina Pitcher Place, Ann Arbor, Michigan 48109, USA.

出版信息

Eur J Neurosci. 2004 Jul;20(2):503-13. doi: 10.1111/j.1460-9568.2004.03487.x.

Abstract

The ability to respond to unexpected or novel stimuli is critical for survival. Determining that a stimulus is indeed novel requires memory to ascertain its lack of familiarity. As the long-term synaptic changes involved in memory formation require the cAMP response element binding protein (CREB), we examined the extent to which CREB is involved in responses to novel environments. These environments typically trigger an endocrine stress response. Thus, we measured behavioural and stress hormone responses to three novel and one familiar environment in mice with a targeted disruption of the alpha and delta isoforms of the CREB gene (CREB(alphadelta-) deficient mice). We found CREB(alphadelta-) deficient mice to be less active and more inhibited in the elevated plus maze, open field, and light/dark box, without showing differences in anxiety-like behaviour. This inhibition is unique to novel environments because these mice display a normal phenotype in the home cage, a familiar environment. Although CREB(alphadelta-) deficient mice exhibit altered behaviour in novel environments, they show normal reactivity to mild and moderate stress as both basal and stress levels of corticosterone are similar to those of wild-type controls. This is the first report of CREB(alphadelta-) deficient mice to: (i) show altered behaviour, not related to learning and memory-associated behaviours, upon initial exposure to environments and (ii) serve as an animal model that can dissociate locomotor activity from anxiety-like behaviour in novel environments.

摘要

对意外或新异刺激做出反应的能力对生存至关重要。确定一种刺激确实是新异的需要记忆来确定其缺乏熟悉度。由于记忆形成过程中涉及的长期突触变化需要环磷酸腺苷反应元件结合蛋白(CREB),我们研究了CREB在对新环境反应中的参与程度。这些环境通常会引发内分泌应激反应。因此,我们在有针对性地破坏了CREB基因的α和δ亚型的小鼠(CREB(αδ-)缺陷小鼠)中,测量了对三种新环境和一种熟悉环境的行为和应激激素反应。我们发现CREB(αδ-)缺陷小鼠在高架十字迷宫、旷场和明暗箱中活动较少且受到更多抑制,但在焦虑样行为方面没有差异。这种抑制在新环境中是独特的,因为这些小鼠在熟悉的环境即家笼中表现出正常的表型。尽管CREB(αδ-)缺陷小鼠在新环境中表现出行为改变,但它们对轻度和中度应激的反应正常,因为皮质酮的基础水平和应激水平与野生型对照相似。这是关于CREB(αδ-)缺陷小鼠的第一份报告,该报告表明:(i)在初次接触环境时表现出与学习和记忆相关行为无关的行为改变,以及(ii)作为一种动物模型,可以在新环境中将运动活动与焦虑样行为区分开来。

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