首页> 外文期刊>Behavioural Brain Research: An International Journal >Lack of cyclin D2 impairing adult brain neurogenesis alters hippocampal-dependent behavioral tasks without reducing learning ability
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Lack of cyclin D2 impairing adult brain neurogenesis alters hippocampal-dependent behavioral tasks without reducing learning ability

机译:缺乏细胞周期蛋白D2损害成人脑神经发生改变了海马依赖的行为任务而不降低学习能力

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The exact function of the adult brain neurogenesis remains elusive, although it has been suggested to play a role in learning and memory processes. In our studies, we employed cyclin D2 gene knockout (cD2 KO) mice showing impaired neurogenesis as well as decreased hippocampal size. However, irrespectively of the genetic background of cD2 KO mice, this phenotype resulted in neither deficits in the hippocampal-dependent learning ability nor the memory formation. In the present study, cD2 KO mice and control littermates were subjected to hippocampal-dependent behavioral tests with little or no learning component. The knockout mice showed significant impairment in such species-typical behaviors as nest construction, digging, and marble burying. They were building none or poorer nests, digging less robustly, and burying fewer marbles than control mice. Such impairments were previously described, e.g., in animals with hippocampal lesions. Moreover, cD2 KO animals were also more active in the open field and automated motility chamber as well as showed increased explorative behavior in IntelliCage. Both increased motility and explorative behaviors were previously observed in hippocampally lesioned animals. Finally, cD2 KO mice showed normal sucrose preference, however starting from the second exposure to the sweetened solution, while control animals displayed a strong preference immediately. Presented results suggest that either morphological abnormalities of the hippocampal formation or adult brain neurogenesis impairment (or both) alter hippocampal-dependent behaviors of mutant mice without influencing learning abilities. These results may also suggest that adult brain neurogenesis is involved in species-typical behaviors.
机译:尽管已经建议成人脑神经发生的确切功能在学习和记忆过程中起作用。在我们的研究中,我们采用了细胞周期蛋白D2基因敲除(cD2 KO)小鼠,这些小鼠显示出神经发生受损以及海马体大小减少。但是,无论cD2 KO小鼠的遗传背景如何,该表型都不会导致海马依赖性学习能力不足或记忆形成。在本研究中,对cD2 KO小鼠和对照同窝仔进行了海马依赖性行为测试,几乎没有学习成分。敲除小鼠在筑巢,挖掘和埋藏大理石等物种典型行为中表现出明显的损伤。他们没有筑巢或更差的巢,挖得更少,埋藏的大理石比对照组小鼠少。先前例如在具有海马损伤的动物中描述了这种损伤。此外,cD2 KO动物在开阔地带和自动运动室中也更加活跃,并且在IntelliCage中显示出更多的探索行为。先前在海马病变动物中观察到运动性和探索行为的增加。最后,cD2 KO小鼠表现出正常的蔗糖偏好,但是从第二次暴露于甜味溶液开始,而对照动物立即表现出强烈的偏好。提出的结果表明,海马形成的形态异常或成年脑神经发生障碍(或两者)可改变突变小鼠的海马依赖性行为,而不会影响学习能力。这些结果也可能表明成人脑神经发生参与了物种典型行为。

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